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Summary of National Guidance for Lipid Management for
Primary and Secondary Prevention of CVD

Summary of National Guidance for Lipid Management for...Text is not SVG - cannot display
PRIMARY PREVENTION
PRIMARY PREVENTION
SEVERE HYPERLIPIDAEMIA
SEVERE HYPERLIPIDAEMIA
SECONDARY PREVENTION
SECONDARY PREVENTION
PRIMARY PREVENTION
Offer lifestyle changes and consider statin therapy for adults who do not have established CVD but fall into the categories below. Use QRISK risk assessment tool where appropriate           
PRIMARY PREVENTION...
Age ≤ 84 
& 
QRISK ≥ 10% over next 10 years
Age ≤ 84...
Type 2 
diabetes 
&
QRISK ≥ 10% over next
10 years
Type 2...
Age ≥ 85 years if appropriate 
consider 
co-morbidities, 
frailty & life expectancy
Age ≥ 85 years...
CKD 
eGFR < 60 
mL/min/1.73m2
and/or
albuminuria
CKD...
Type 1 diabetes, if they have one or more of the following:
• Over 40 years
• Had diabetes for >10 years
• Have established nephropathy
• Have other CVD risk factors
Type 1 diabetes, if they have...
Discuss the benefits of lifestyle changes and identify and address all modifiable risk
factors - smoking, diet, obesity, alcohol intake, physical activity, blood pressure and HbA1c.
Offer people the opportunity to have their risk of CVD assessed again after they
have tried to change their lifestyle (where applicable)
Discuss the benefits of lifestyle changes and identify and address all modifiable risk...
Consider additional risk factors, if present, together with QRISK score (treated for HIV,
severe mental illness, taking medicines that cause dyslipidaemia, systemic inflammatory
disorder (e.g. SLE), impaired fasting glycaemia, recent change in risk factors)
Consider additional risk factors, if present, together with QRISK score (treated for HI...
PRIMARY PREVENTION
If lifestyle modification is ineffective or inappropriate, discuss the risks and benefits
of statins, and offer treatment based on an informed shared-decision.
Atorvastatin 20mg daily
PRIMARY PREVENTION...
• Measure full lipid profile again after 2-3 months (non-fasting).
• High intensity statin treatment should achieve reduction of non-HDL-C > 40% from baseline.
• If not achieved after 2-3 months;
• Measure full lipid profile again after 2-3 months (non-fasting)....
see ‘Primary Prevention Risk Assessment’
see ‘Primary Prevention Risk Assessment’
- Discuss treatment adherence, timing of dose, diet and lifestyle
- If at higher risk (based on comorbidities, risk score or clinical judgement) 


- For how to increase in people with CKD 
- Discuss treatment adherence, timing of dose, diet and lifestyle...
consider increasing the dose every 2-3 months
up to a maximum dose of atorvastatin 80mg daily.
consider increasing the dose every 2-3 months...
• If patients on a high‑intensity statin have side effects, offer a lower dose or an alternative statin
• 
• If maximum tolerated dose of statin does not achieve non-HDL-C reduction > 40% of baseline
• value after 2-3 months consider adding Ezetimibe 10mg daily (NICE TA385)
• If statin treatment is contraindicated or not tolerated;
• - See AAC Statin Intolerance Algorithm for advice regarding adverse effects (click here)
• - Ezetimibe 10mg monotherapy may be considered. Assess response after 2-3 months.
• - Ezetimibe 10mg/bempedoic acid 180 mg combination may be considered when ezetimibe
• - alone does not control non-HDL-C/LDL-C well enough (NICE TA694).
• If patients on a high‑intensity statin have side effects, offer a lower dose or an alte...
If non-HDL-C reduction remains < 40% of baseline despite maximal tolerated lipid lowering
therapy (including people with intolerances and contraindications) consider referral to
specialist lipid management clinic according to local arrangements
If non-HDL-C reduction remains < 40% of baseline despite maximal tolerated lipid loweri...Text is not SVG - cannot display
ABBREVIATIONS
Statin intolerance is defined as the presence of clinically significant adverse effects from statin therapy that are considered to represent an unacceptable risk to the patient or that may result in adherence to therapy being compromised.
For people who are intolerant of the recommended statin treatment see the NHSE AAC statin intolerance algorithm, available on the NHSE AAC page (Click here)
Statin intolerance is defined as the presence of clinically significant adv...
“This summary accurately reflects NICE guidance and JBS3 recommendations”, NICE March 2024
“This summary accurately reflects NICE guidan... STATIN INTOLERANCE
ALT: alanine aminotransferase
AST: aspartate aminotransferase
CHD: coronary heart disease
CKD: chronic kidney disease
CVD: cardiovascular disease
FH: familial hypercholesterolaemia
JBS: Joint British Societies
LDL-C: low density lipoprotein cholesterol
ALT: alanine aminotransferase...
non-HDL-C: non-high density lipoprotein cholesterol
PCSK9i: proprotein convertase subtilisin kexin 9
PCSK9i: monoclonal antibody inhibitor
QOF: Quality and Outcomes Framework
SLE: systemic lupus erythematosus
SPC: summary of product characteristics
TC: total cholesterol
non-HDL-C: non-high density lipoprotein cholest...
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Subgroup.
Updated by NHSE Cholesterol Expert Advisory Group.
March 2024. Review date: March 2026.
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Sub...
References
References
JBS3. 2014. www.jbs3risk.com/pages/6.htm
Kirsten et al. 2005. Hospital Pharmacy 40(8):687-692
Navarese et al. 2015. Annals of internal medicine 163(1):40-51
Soon Jun Hong et al. 2018. Clinical therapeutics 40(2): 226-241.e4
NICE 2016. TA385 www.nice.org.uk/guidance/ta385
NICE 2016. TA393 www.nice.org.uk/guidance/TA393
NICE 2016. TA394 www.nice.org.uk/guidance/TA394
JBS3. 2014. www.jbs3risk.com/pages/6.htm...
NICE 2008. CG71 www.nice.org.uk/guidance/cg71
NICE 2021. TA694 www.nice.org.uk/guidance/TA694
NICE 2021. TA733 www.nice.org.uk/guidance/TA733
NICE 2022. TA805 www.nice.org.uk/guidance/ta805
NICE 2023. NG238 www.nice.org.uk/guidance/ng238
NICE 2023. CG189 www.nice.org.uk/guidance/cg189
NICE 2008. CG71 www.nice.org.uk/guidance/cg71...
Original PDF version of the guideline:  A summary of national guidance for lipid management for primary and secondary prevention of  cardiovascular disease (CVD).
Original PDF version of the guideline:  A summary of national guidance for lipid managem...
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.Text is not SVG - cannot display

Type 1 Diabetes
While NICE recommends offering statins to patients with Type 1 diabetes as detailed in the algorithm, it also states to consider statins in those aged 18 to 40 with type 1 diabetes, including those who have had diabetes for ≤ 10 years

Discuss the benefits of lifestyle changes, address all modifiable risk factors, and offer reassessment of CVD risk (where applicable)
Consider additional risk factors, if present, together with QRISK score
Atorvastatin 20mg daily
Measure full lipid profile again after 2-3 months (non-fasting).

TARGET a reduction of non-HDL-C > 40% from baseline

If not achieved click for more information
If patients on a high‑intensity statin have side effects, offer a lower dose or an alternative statin

If maximum tolerated dose of statin does not achieve non-HDL-C reduction > 40% of baseline value after 2-3 months consider adding Ezetimibe 10mg daily

If statin treatment is contraindicated or not tolerated click for more information
N
N
CKS
CKSText is not SVG - cannot display How should I interpret and communicate the estimated CVD risk score?
N
N
CKS
CKSText is not SVG - cannot display When should I offer lipid modification therapy for primary prevention of cardiovascular disease?
N
N
CKS
CKSText is not SVG - cannot display Which lipid-lowering treatment should I offer for the primary prevention of cardiovascular disease?
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N
CKS
CKSText is not SVG - cannot display How should I assess response to lipid-lowering treatment for the primary prevention of cardiovascular disease?
PRIMARY PREVENTION
PRIMARY PREVENTION
SEVERE HYPERLIPIDAEMIA
SEVERE HYPERLIPIDAEMIA
SECONDARY PREVENTION
SECONDARY PREVENTION
SEVERE HYPERLIPIDAEMIA
If TC >7.5mmol/L and/or LDL-C >4.9mmol/L and/or non-HDL-C >5.9mmol/L,
a personal and/or family history of confirmed CHD (<60 years) and with no secondary causes:
suspect familial hypercholesterolaemia (possible heterozygous FH)
Do not use QRISK risk assessment tool
SEVERE HYPERLIPIDAEMIA...
DIAGNOSIS AND REFERRAL
Take fasting blood for repeat lipid profile to measure LDL-C.
Use the Simon Broome or Dutch Lipid Clinic Network (DLCN) criteria
to make a clinical diagnosis of FH.
Use clinical findings, a full lipid profile and family history to judge the likelihood of a familial
lipid disorder, rather than using strict lipid cut-off values alone.
Refer to Lipid Clinic for further assessment if clinical diagnosis of FH or
if TC>9.0mmol/L and/or LDL-C >6.5mmol/L and/or non-HDL-C >7.5mmol/L or
Fasting triglycerides > 10mmol/L (regardless of family history) (see 'Specialist Services')
DIAGNOSIS AND REFERRAL...
TREATMENT TARGETS IN FH
If clinical diagnosis of FH and/or other risk factors present follow the recommended treatment management pathway for primary or secondary prevention as for non-FH, BUT
Aim to achieve at least a 50% reduction of LDL-C (or non-fasting non-HDL-C) from baseline.
Consider specialist referral for further treatment and/or consideration of PCSK9i therapy IF
- they are assessed to be at very high risk of a coronary event**
- OR therapy is not tolerated
- OR LDL-C remains >5mmol/L (primary prevention)
- OR LDL-C remains >3.5mmol/L (secondary prevention)
- despite maximal tolerated statin and ezetimibe therapy.
TREATMENT TARGETS IN FH...
**defined as any of the following:
• Established coronary heart disease
• Two or more other CVD risk factors
**defined as any of the following:...Text is not SVG - cannot display
ABBREVIATIONS
Statin intolerance is defined as the presence of clinically significant adverse effects from statin therapy that are considered to represent an unacceptable risk to the patient or that may result in adherence to therapy being compromised.
For people who are intolerant of the recommended statin treatment see the NHSE AAC statin intolerance algorithm, available on the NHSE AAC page (Click here)
Statin intolerance is defined as the presence of clinically significant adv...
“This summary accurately reflects NICE guidance and JBS3 recommendations”, NICE March 2024
“This summary accurately reflects NICE guidan... STATIN INTOLERANCE
ALT: alanine aminotransferase
AST: aspartate aminotransferase
CHD: coronary heart disease
CKD: chronic kidney disease
CVD: cardiovascular disease
FH: familial hypercholesterolaemia
JBS: Joint British Societies
LDL-C: low density lipoprotein cholesterol
ALT: alanine aminotransferase...
non-HDL-C: non-high density lipoprotein cholesterol
PCSK9i: proprotein convertase subtilisin kexin 9
PCSK9i: monoclonal antibody inhibitor
QOF: Quality and Outcomes Framework
SLE: systemic lupus erythematosus
SPC: summary of product characteristics
TC: total cholesterol
non-HDL-C: non-high density lipoprotein cholest...
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Subgroup.
Updated by NHSE Cholesterol Expert Advisory Group.
March 2024. Review date: March 2026.
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Sub...
References
References
JBS3. 2014. www.jbs3risk.com/pages/6.htm
Kirsten et al. 2005. Hospital Pharmacy 40(8):687-692
Navarese et al. 2015. Annals of internal medicine 163(1):40-51
Soon Jun Hong et al. 2018. Clinical therapeutics 40(2): 226-241.e4
NICE 2016. TA385 www.nice.org.uk/guidance/ta385
NICE 2016. TA393 www.nice.org.uk/guidance/TA393
NICE 2016. TA394 www.nice.org.uk/guidance/TA394
JBS3. 2014. www.jbs3risk.com/pages/6.htm...
NICE 2008. CG71 www.nice.org.uk/guidance/cg71
NICE 2021. TA694 www.nice.org.uk/guidance/TA694
NICE 2021. TA733 www.nice.org.uk/guidance/TA733
NICE 2022. TA805 www.nice.org.uk/guidance/ta805
NICE 2023. NG238 www.nice.org.uk/guidance/ng238
NICE 2023. CG189 www.nice.org.uk/guidance/cg189
NICE 2008. CG71 www.nice.org.uk/guidance/cg71...
Original PDF version of the guideline:  A summary of national guidance for lipid management for primary and secondary prevention of  cardiovascular disease (CVD).
Original PDF version of the guideline:  A summary of national guidance for lipid managem...
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.Text is not SVG - cannot display
Suspect familial hypercholesterolaemia IF
Suspect familial hypercholesterolaemia IF
non-HDL-C > 5.9 mmol/L
non-HDL-C > 5.9 mmol/L
TC > 7.5 mmol/L
TC > 7.5 mmol/L
 or 
 or 
 or 
 or 
LDL-C > 4.9 mmol/L
LDL-C > 4.9 mmol/L
with no secondary causes AND a personal and/or family history of confirmed CHD (< 60 years)
with no secondary causes AND a personal and/or family history of confirmed CHD (< 60 ye...Text is not SVG - cannot display
DIAGNOSIS AND REFERRAL
Take fasting blood for repeat lipid profile to measure LDL-C.
Use the Simon Broome or Dutch Lipid Clinic Network criteria to make a clinical diagnosis of FH.
Refer to Lipid Clinic for further assessment if 

DIAGNOSIS AND REFERRAL...
or
or
or
or
or
or
TC > 9.0 mmol/L
TC > 9.0 mmol/L
LDL-C > 6.5 mmol/L
LDL-C > 6.5 mmol/L
non-HDL-C > 7.5 mmol/L
non-HDL-C > 7.5 mmol/L
Fasting triglycerides > 10 mmol/L
Fasting triglycerides > 10 mmol...
clinical diagnosis of FH or if:
clinical diagnosis of FH or i...
(regardless of family history)
(regardless of family histo...Text is not SVG - cannot display
TREATMENT TARGETS IN FH
Follow the recommended treatment management pathway for primary or secondary prevention as for non-FH, BUT
TREATMENT TARGETS IN FH...
Aim to achieve at least a 50% reduction of LDL-C (or non-fasting non-HDL-C) from baseline.
Aim to achieve at least a 50% reduction of LDL-C (or non-fasting non-HDL-C) from basel...
patient assessed to be at very high risk of a coronary event defined as any of the following:
patient assessed to be at very high risk of a coronary event defined as any of the following:
Consider specialist referral for further treatment and/or consideration of PCSK9i therapy IF
Consider specialist referral for further treatment and/or consideration of PCSK9i therap...
therapy is not tolerated
therapy is not tolera...
or
or
or
or
LDL-C remains > 5mmol/L
LDL-C remains > 5mmol/L
or
or
LDL-C remains > 3.5mmol/L
LDL-C remains > 3.5mmol/L
(secondary prevention)
(secondary prevention)
(primary prevention)
(primary prevention)
despite maximal tolerated statin and ezetimibe therapy.
despite maximal tolerated statin and ezetimibe therapy.
• Established coronary heart disease
• Two or more other CVD risk factors
• Established coronary heart diseas...Text is not SVG - cannot display
N
N
CKS
CKSText is not SVG - cannot display How can I identify people with possible familial hypercholesterolaemia?
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N
CKS
CKSText is not SVG - cannot display How should I assess a person with possible familial hypercholesterolaemia?


PRIMARY PREVENTION
PRIMARY PREVENTION
SEVERE HYPERLIPIDAEMIA
SEVERE HYPERLIPIDAEMIA
SECONDARY PREVENTION
SECONDARY PREVENTION
SECONDARY PREVENTION
Offer statin therapy to adults with CVD, this includes CHD, angina, Acute Coronary Syndrome (MI or unstable angina), revascularisation, stroke or TIA, or symptomatic peripheral arterial disease.
Do not delay statin treatment if a person has acute coronary syndrome. Take a lipid sample on admission (within 24 hours).
SECONDARY PREVENTION...
Identify and address all modifiable risk factors - smoking, diet, obesity, alcohol intake, physical activity, blood pressure and HbA1c.
Identify and address all modifiable risk factors - smoking, diet, obesity, alcohol intake, phy...
SECONDARY PREVENTION
Do not delay statin treatment in secondary prevention while managing modifiable risk factors. Prescribe a high intensity statin:
Atorvastatin 80mg daily
Use a lower dose of atorvastatin if there is a potential drug interaction, high risk of or experiencing adverse effects, or patient preference.
Offer atorvastatin 20mg if CKD (people with GFR< 60 mL/min/1.73m2)
SECONDARY PREVENTION...
• Measure full lipid profile again after 2-3 months (non-fasting).
• Aim for an LDL-C of ≤ 2.0 mmol/L, or non-HDL-C of ≤ 2.6 mmol/L.
• LDL-C and non-HDL-C  levels should be reduced as much as possible. Personalise targets based on
• clinical judgement and an informed discussion with patient. See Titration Thresholds / Targets
• If high intensity statin treatment does not achieve expected reduction after 2 to 3 months
• 
• - Discuss treatment adherence, timing of dose, diet and lifestyle measures
• - If started on less than atorvastatin 80mg and the person is judged to be at higher risk (based on
• - co-morbidities or clinical judgment), consider increasing to 80mg atorvastatin or maximally tolerated
• - dose.
• - For how to increase in people with CKD see ‘Special Patient Populations’
• If patients on a high-intensity statin have side effects, offer a lower dose or an alternative statin 
• Measure full lipid profile again after 2-3 months (non-fasting)....
Escalating lipid therapy
Escalating lipid therapyText is not SVG - cannot display
SECONDARY PREVENTION
Offer statin therapy to adults with CVD
Do not delay statin treatment if a person has acute coronary syndrome. Take a full lipid profile on admission (within 24 hours).
Identify and address all modifiable risk factors
Atorvastatin 80mg daily
Use a lower dose of atorvastatin if there is a potential drug interaction, high risk of or experiencing adverse effects, or patient preference.

Offer atorvastatin 20mg if CKD (people with GFR< 60 mL/min/1.73m2)
Measure full lipid profile again after 2-3 months (non-fasting)

Aim for an LDL-C of ≤ 2.0 mmol/L, or non-HDL-C of ≤ 2.6 mmol/L
LDL-C and non-HDL-C levels should be reduced as much as possible. Personalise targets based on clinical judgement and an informed discussion with patient.

If high intensity statin treatment does not achieve expected reduction click for more information
N
N
CKS
CKSText is not SVG - cannot display Which lipid-lowering treatment should I offer for the secondary prevention of cardiovascular disease?
N
N
CKS
CKSText is not SVG - cannot display How should I assess response to lipid-lowering treatment for the secondary prevention of cardiovascular disease?

Consider ezetimibe in addition to the maximum tolerated intensity and dose of statin to reduce CVD risk further,
even if the lipid target for secondary prevention of CVD is met. (NG238)
Consider ezetimibe in addition to the maximum tolerated intensity and dose of statin to reduce CVD...
Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosapent ethyl.

Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosa...
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
• Ensure an informed discussion between the clinician and the person about the risks and benefits of
• additional lipid lowering treatments.
• Take into account the person’s preferences, the presence of any comorbidities, whether they are on
• multiple medications,  whether they have frailty and their life expectancy.
• Do not routinely de-escalate lipid lowering therapies when levels are lower than NICE target, except if
• clinically indicated or based on the person’s needs or preferences
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapies ABBREVIATIONS
Statin intolerance is defined as the presence of clinically significant adverse effects from statin therapy that are considered to represent an unacceptable risk to the patient or that may result in adherence to therapy being compromised.
For people who are intolerant of the recommended statin treatment see the NHSE AAC statin intolerance algorithm, available on the NHSE AAC page (Click here)
Statin intolerance is defined as the presence of clinically significant adv...
“This summary accurately reflects NICE guidance and JBS3 recommendations”, NICE March 2024
“This summary accurately reflects NICE guidan... STATIN INTOLERANCE
ALT: alanine aminotransferase
AST: aspartate aminotransferase
CHD: coronary heart disease
CKD: chronic kidney disease
CVD: cardiovascular disease
FH: familial hypercholesterolaemia
JBS: Joint British Societies
LDL-C: low density lipoprotein cholesterol
ALT: alanine aminotransferase...
non-HDL-C: non-high density lipoprotein cholesterol
PCSK9i: proprotein convertase subtilisin kexin 9
PCSK9i: monoclonal antibody inhibitor
QOF: Quality and Outcomes Framework
SLE: systemic lupus erythematosus
SPC: summary of product characteristics
TC: total cholesterol
non-HDL-C: non-high density lipoprotein cholest...
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Subgroup.
Updated by NHSE Cholesterol Expert Advisory Group.
March 2024. Review date: March 2026.
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Sub...
References
References
JBS3. 2014. www.jbs3risk.com/pages/6.htm
Kirsten et al. 2005. Hospital Pharmacy 40(8):687-692
Navarese et al. 2015. Annals of internal medicine 163(1):40-51
Soon Jun Hong et al. 2018. Clinical therapeutics 40(2): 226-241.e4
NICE 2016. TA385 www.nice.org.uk/guidance/ta385
NICE 2016. TA393 www.nice.org.uk/guidance/TA393
NICE 2016. TA394 www.nice.org.uk/guidance/TA394
JBS3. 2014. www.jbs3risk.com/pages/6.htm...
NICE 2008. CG71 www.nice.org.uk/guidance/cg71
NICE 2021. TA694 www.nice.org.uk/guidance/TA694
NICE 2021. TA733 www.nice.org.uk/guidance/TA733
NICE 2022. TA805 www.nice.org.uk/guidance/ta805
NICE 2023. NG238 www.nice.org.uk/guidance/ng238
NICE 2023. CG189 www.nice.org.uk/guidance/cg189
NICE 2008. CG71 www.nice.org.uk/guidance/cg71...
Original PDF version of the guideline:  A summary of national guidance for lipid management for primary and secondary prevention of  cardiovascular disease (CVD).
Original PDF version of the guideline:  A summary of national guidance for lipid managem...
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.Text is not SVG - cannot display

SELECT
SELECT
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well e...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapiesText is not SVG - cannot display

Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosapent ethyl.

Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosa...
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
• Ensure an informed discussion between the clinician and the person about the risks and benefits of
• additional lipid lowering treatments.
• Take into account the person’s preferences, the presence of any comorbidities, whether they are on
• multiple medications,  whether they have frailty and their life expectancy.
• Do not routinely de-escalate lipid lowering therapies when levels are lower than NICE target, except if
• clinically indicated or based on the person’s needs or preferences
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapies
If recommended statin treatment is contraindicated or not tolerated - follow AAC Statin Intolerance Algorithm for advice regarding adverse effects (click here).
If recommended statin treatment is contraindicated or not tolerated - follow AAC Statin Into...
If statin intolerance is confirmed, consider:
- Ezetimibe 10mg monotherapy. Assess response after 3 months (TA385)
- Ezetimibe 10mg/bempedoic acid 180 mg combination when ezetimibe alone does not control non-HDL-C sufficiently. (NICE TA694)
If statin intolerance is confirmed, consider:...
If non HDL-C remains > 2.6mmol/L despite other lipid lowering therapies consider Injectable therapies - arrange a fasting blood test and assess eligibility criteria (TA393/TA394, TA733)
If non HDL-C remains > 2.6mmol/L despite other lipid lowering therapies consider Injectable...
Injectable therapies**
Injectable therapies**
- Inclisiran - if fasting LDL-C ≥ 2.6mmol/L despite maximum tolerated lipid lowering therapy (TA733)
- Inclisiran - if fasting LDL-C ≥ 2.6mmol/L despite maximum tolerated lipid lowering thera...
- PCSK9i - see 'Specialist Services' for LDL-C thresholds. (TA393/TA394)
- PCSK9i - see 'Specialist Services' for LDL-C thresholds. (TA393/TA394)
OR
OR
** Inclisiran and PCSK9i should not be prescribed concurrently
** Inclisiran and PCSK9i should not be prescribed concurrently ABBREVIATIONS
Statin intolerance is defined as the presence of clinically significant adverse effects from statin therapy that are considered to represent an unacceptable risk to the patient or that may result in adherence to therapy being compromised.
For people who are intolerant of the recommended statin treatment see the NHSE AAC statin intolerance algorithm, available on the NHSE AAC page (Click here)
Statin intolerance is defined as the presence of clinically significant adv...
“This summary accurately reflects NICE guidance and JBS3 recommendations”, NICE March 2024
“This summary accurately reflects NICE guidan... STATIN INTOLERANCE
ALT: alanine aminotransferase
AST: aspartate aminotransferase
CHD: coronary heart disease
CKD: chronic kidney disease
CVD: cardiovascular disease
FH: familial hypercholesterolaemia
JBS: Joint British Societies
LDL-C: low density lipoprotein cholesterol
ALT: alanine aminotransferase...
non-HDL-C: non-high density lipoprotein cholesterol
PCSK9i: proprotein convertase subtilisin kexin 9
PCSK9i: monoclonal antibody inhibitor
QOF: Quality and Outcomes Framework
SLE: systemic lupus erythematosus
SPC: summary of product characteristics
TC: total cholesterol
non-HDL-C: non-high density lipoprotein cholest...
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Subgroup.
Updated by NHSE Cholesterol Expert Advisory Group.
March 2024. Review date: March 2026.
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Sub...
References
References
JBS3. 2014. www.jbs3risk.com/pages/6.htm
Kirsten et al. 2005. Hospital Pharmacy 40(8):687-692
Navarese et al. 2015. Annals of internal medicine 163(1):40-51
Soon Jun Hong et al. 2018. Clinical therapeutics 40(2): 226-241.e4
NICE 2016. TA385 www.nice.org.uk/guidance/ta385
NICE 2016. TA393 www.nice.org.uk/guidance/TA393
NICE 2016. TA394 www.nice.org.uk/guidance/TA394
JBS3. 2014. www.jbs3risk.com/pages/6.htm...
NICE 2008. CG71 www.nice.org.uk/guidance/cg71
NICE 2021. TA694 www.nice.org.uk/guidance/TA694
NICE 2021. TA733 www.nice.org.uk/guidance/TA733
NICE 2022. TA805 www.nice.org.uk/guidance/ta805
NICE 2023. NG238 www.nice.org.uk/guidance/ng238
NICE 2023. CG189 www.nice.org.uk/guidance/cg189
NICE 2008. CG71 www.nice.org.uk/guidance/cg71...
Original PDF version of the guideline:  A summary of national guidance for lipid management for primary and secondary prevention of  cardiovascular disease (CVD).
Original PDF version of the guideline:  A summary of national guidance for lipid managem...
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.Text is not SVG - cannot display

SELECT
SELECT
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well e...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapiesText is not SVG - cannot display
LDL-C results
LDL-C results
Statin treatment contraindicated or not tolerated
Statin treatment contraindicated or not tolerated
Follow AAC Statin Intolerance Algorithm. If statin intolerance is confirmed, offer:
  1. Ezetimibe 10mg daily. Assess response after 3 months (TA385)
  2. Ezetimibe 10mg/bempedoic acid 180 mg combination when ezetimibe alone does not control non-HDL-C sufficiently. (NICE TA694)
Follow AAC Statin Intolerance Algorithm. If statin into...
If non HDL-C remains > 2.6 mmol/L
If non HDL-C remains > 2.6 mmol/L
Arrange a fasting blood test to measure LDL-C and triglycerides to assess eligibility criteria and consider 
Injectable therapies
Arrange a fasting blood test to meas...
 Inclisiran and PCSK9i should not be prescribed concurrently
 Inclisiran and PCSK9i should not be prescribed concurrently
≥ 2.6 mmol/L
≥ 2.6 mmol/L
1.04 - 2.6 mmol/L
1.04 - 2.6 mmol/L
> 3.5 mmol/L
> 3.5 mmol/L
> 4.0 mmol/L
> 4.0 mmol/L
PCSK9 inhibitors
PCSK9 inhibitors
High risk of CVD
High risk of CVD
+
+
Inclisiran
Inclisiran
Icosapent ethyl
Icosapent ethyl
YES
YES
NO
NO
Very high risk of CVD
Very high risk of C...
+
+
consider
consider
Triglycerides > 1.7 mmol/L
+
Statin therapy
Triglycerides > 1.7 mmol/...

+
+
Alirocumab
Alirocumab
Evolocumab
EvolocumabText is not SVG - cannot display

Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosapent ethyl.

Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosa...
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
• Ensure an informed discussion between the clinician and the person about the risks and benefits of
• additional lipid lowering treatments.
• Take into account the person’s preferences, the presence of any comorbidities, whether they are on
• multiple medications,  whether they have frailty and their life expectancy.
• Do not routinely de-escalate lipid lowering therapies when levels are lower than NICE target, except if
• clinically indicated or based on the person’s needs or preferences
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapies
Injectable therapies**
Injectable therapies**
** Inclisiran and PCSK9i should not be prescribed concurrently
** Inclisiran and PCSK9i should not be prescribed concurrently
Inclisiran - if fasting LDL-C ≥ 2.6mmol/L despite maximum tolerated lipid lowering therapy (TA733)
OR
PCSK9i - see 'Specialist Services' for LDL-C thresholds. (TA393/TA394)
Inclisiran - if fasting LDL-C ≥ 2.6mmol/L despite maximum tolerated lipid lowering therapy (T...
Ezetimibe 10mg daily (NICE TA385). 
Reassess after three months.

If non-HDL-C remains >2.6mmol/L; consider injectable therapies arrange a fasting blood test and assess eligibility
Ezetimibe 10mg daily (NICE TA385).... ABBREVIATIONS
Statin intolerance is defined as the presence of clinically significant adverse effects from statin therapy that are considered to represent an unacceptable risk to the patient or that may result in adherence to therapy being compromised.
For people who are intolerant of the recommended statin treatment see the NHSE AAC statin intolerance algorithm, available on the NHSE AAC page (Click here)
Statin intolerance is defined as the presence of clinically significant adv...
“This summary accurately reflects NICE guidance and JBS3 recommendations”, NICE March 2024
“This summary accurately reflects NICE guidan... STATIN INTOLERANCE
ALT: alanine aminotransferase
AST: aspartate aminotransferase
CHD: coronary heart disease
CKD: chronic kidney disease
CVD: cardiovascular disease
FH: familial hypercholesterolaemia
JBS: Joint British Societies
LDL-C: low density lipoprotein cholesterol
ALT: alanine aminotransferase...
non-HDL-C: non-high density lipoprotein cholesterol
PCSK9i: proprotein convertase subtilisin kexin 9
PCSK9i: monoclonal antibody inhibitor
QOF: Quality and Outcomes Framework
SLE: systemic lupus erythematosus
SPC: summary of product characteristics
TC: total cholesterol
non-HDL-C: non-high density lipoprotein cholest...
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Subgroup.
Updated by NHSE Cholesterol Expert Advisory Group.
March 2024. Review date: March 2026.
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Sub...
References
References
JBS3. 2014. www.jbs3risk.com/pages/6.htm
Kirsten et al. 2005. Hospital Pharmacy 40(8):687-692
Navarese et al. 2015. Annals of internal medicine 163(1):40-51
Soon Jun Hong et al. 2018. Clinical therapeutics 40(2): 226-241.e4
NICE 2016. TA385 www.nice.org.uk/guidance/ta385
NICE 2016. TA393 www.nice.org.uk/guidance/TA393
NICE 2016. TA394 www.nice.org.uk/guidance/TA394
JBS3. 2014. www.jbs3risk.com/pages/6.htm...
NICE 2008. CG71 www.nice.org.uk/guidance/cg71
NICE 2021. TA694 www.nice.org.uk/guidance/TA694
NICE 2021. TA733 www.nice.org.uk/guidance/TA733
NICE 2022. TA805 www.nice.org.uk/guidance/ta805
NICE 2023. NG238 www.nice.org.uk/guidance/ng238
NICE 2023. CG189 www.nice.org.uk/guidance/cg189
NICE 2008. CG71 www.nice.org.uk/guidance/cg71...
Original PDF version of the guideline:  A summary of national guidance for lipid management for primary and secondary prevention of  cardiovascular disease (CVD).
Original PDF version of the guideline:  A summary of national guidance for lipid managem...
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.Text is not SVG - cannot display

SELECT
SELECT
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well e...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapiesText is not SVG - cannot display
LDL-C results
LDL-C results
If non HDL-C remains > 2.6 mmol/L
If non HDL-C remains > 2.6 mmol/L
Arrange a fasting blood test to measure LDL-C and triglycerides to assess eligibility criteria and consider 
Injectable therapies
Arrange a fasting blood test to meas...
Ezetimibe 10mg daily.
Assess response after 3 months (TA385) 
Ezetimibe 10mg daily....
 Inclisiran and PCSK9i should not be prescribed concurrently
 Inclisiran and PCSK9i should not be prescribed concurrently
≥ 2.6 mmol/L
≥ 2.6 mmol/L
1.04 - 2.6 mmol/L
1.04 - 2.6 mmol/L
> 3.5 mmol/L
> 3.5 mmol/L
> 4.0 mmol/L
> 4.0 mmol/L
PCSK9 inhibitors
PCSK9 inhibitors
High risk of CVD
High risk of CVD
+
+
Inclisiran
Inclisiran
Icosapent ethyl
Icosapent ethyl
YES
YES
NO
NO
Very high risk of CVD
Very high risk of C...
+
+
consider
consider
Triglycerides > 1.7 mmol/L
+
Statin therapy
Triglycerides > 1.7 mmol/...

+
+
Alirocumab
Alirocumab
Evolocumab
EvolocumabText is not SVG - cannot display

If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
• Ensure an informed discussion between the clinician and the person about the risks and benefits of
• additional lipid lowering treatments.
• Take into account the person’s preferences, the presence of any comorbidities, whether they are on
• multiple medications,  whether they have frailty and their life expectancy.
• Do not routinely de-escalate lipid lowering therapies when levels are lower than NICE target, except if
• clinically indicated or based on the person’s needs or preferences
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapies
Injectable therapies**
Injectable therapies**
If non-HDL-C > 2.6mmol/L; Arrange fasting blood test to measure LDL-C to assess eligibility:
If non-HDL-C > 2.6mmol/L; Arrange fasting blood test to measure LDL-C to assess eligibility:
- Inclisiran - if fasting LDL-C ≥ 2.6mmol/L despite maximum tolerated lipid lowering therapy (TA733)
- Inclisiran - if fasting LDL-C ≥ 2.6mmol/L despite maximum tolerated lipid lowering thera...
- PCSK9i - see 'Specialist Services' for LDL-C thresholds. (TA393/TA394)
- PCSK9i - see 'Specialist Services' for LDL-C thresholds. (TA393/TA394)
OR
OR
** Inclisiran and PCSK9i should not be prescribed concurrently
** Inclisiran and PCSK9i should not be prescribed concurrently

If eligibility criteria not met, consider: 
If eligibility criteria not met, consider: 
Ezetimibe 10mg daily (if not previously considered) NICE TA385 
Reassess after three months.
Ezetimibe 10mg daily (if not previously considered) NICE...
If non-HDL-C remains >2.6mmol/L; consider injectable therapies arrange a fasting blood test and assess eligibility
If non-HDL-C remains >2.6mmol/L; consider injectable therapi...
Consider ezetimibe in addition to the maximum tolerated intensity and dose of statin to reduce CVD risk further,
even if the lipid target for secondary prevention of CVD is met. (NG238)
Consider ezetimibe in addition to the maximum tolerated intensity and dose of statin to reduce CVD...
Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosapent ethyl.

Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosa... ABBREVIATIONS
Statin intolerance is defined as the presence of clinically significant adverse effects from statin therapy that are considered to represent an unacceptable risk to the patient or that may result in adherence to therapy being compromised.
For people who are intolerant of the recommended statin treatment see the NHSE AAC statin intolerance algorithm, available on the NHSE AAC page (Click here)
Statin intolerance is defined as the presence of clinically significant adv...
“This summary accurately reflects NICE guidance and JBS3 recommendations”, NICE March 2024
“This summary accurately reflects NICE guidan... STATIN INTOLERANCE
ALT: alanine aminotransferase
AST: aspartate aminotransferase
CHD: coronary heart disease
CKD: chronic kidney disease
CVD: cardiovascular disease
FH: familial hypercholesterolaemia
JBS: Joint British Societies
LDL-C: low density lipoprotein cholesterol
ALT: alanine aminotransferase...
non-HDL-C: non-high density lipoprotein cholesterol
PCSK9i: proprotein convertase subtilisin kexin 9
PCSK9i: monoclonal antibody inhibitor
QOF: Quality and Outcomes Framework
SLE: systemic lupus erythematosus
SPC: summary of product characteristics
TC: total cholesterol
non-HDL-C: non-high density lipoprotein cholest...
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Subgroup.
Updated by NHSE Cholesterol Expert Advisory Group.
March 2024. Review date: March 2026.
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Sub...
References
References
JBS3. 2014. www.jbs3risk.com/pages/6.htm
Kirsten et al. 2005. Hospital Pharmacy 40(8):687-692
Navarese et al. 2015. Annals of internal medicine 163(1):40-51
Soon Jun Hong et al. 2018. Clinical therapeutics 40(2): 226-241.e4
NICE 2016. TA385 www.nice.org.uk/guidance/ta385
NICE 2016. TA393 www.nice.org.uk/guidance/TA393
NICE 2016. TA394 www.nice.org.uk/guidance/TA394
JBS3. 2014. www.jbs3risk.com/pages/6.htm...
NICE 2008. CG71 www.nice.org.uk/guidance/cg71
NICE 2021. TA694 www.nice.org.uk/guidance/TA694
NICE 2021. TA733 www.nice.org.uk/guidance/TA733
NICE 2022. TA805 www.nice.org.uk/guidance/ta805
NICE 2023. NG238 www.nice.org.uk/guidance/ng238
NICE 2023. CG189 www.nice.org.uk/guidance/cg189
NICE 2008. CG71 www.nice.org.uk/guidance/cg71...
Original PDF version of the guideline:  A summary of national guidance for lipid management for primary and secondary prevention of  cardiovascular disease (CVD).
Original PDF version of the guideline:  A summary of national guidance for lipid managem...
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.Text is not SVG - cannot display

SELECT
SELECT
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well enough after 2-3 months confirm statin adherence,  then consider the following escalation of treatment options based on shared decision making with the patient.
If maximum tolerated dose of statin does not control non-HDL-C/LDL-C well e...
Statin Intolerance
Statin Intolerance
Ezetimibe
Ezetimibe
Injectable therapies
Injectable therapiesText is not SVG - cannot display
LDL-C results
LDL-C results
If non HDL-C remains > 2.6 mmol/L
If non HDL-C remains > 2.6 mmol/L
Arrange a fasting blood test to measure LDL-C and triglycerides to assess eligibility criteria and consider 
Injectable therapies
Arrange a fasting blood test to meas...
If eligibility criteria not met, consider Ezetimibe 10mg daily
(if not previously considered)
If eligibility criteria not met,...
 Injectable therapies
 Injectable therapies
 Inclisiran and PCSK9i should not be prescribed concurrently
 Inclisiran and PCSK9i should not be prescribed concurrently
≥ 2.6 mmol/L
≥ 2.6 mmol/L
1.04 - 2.6 mmol/L
1.04 - 2.6 mmol/L
> 3.5 mmol/L
> 3.5 mmol/L
> 4.0 mmol/L
> 4.0 mmol/L
PCSK9 inhibitors
PCSK9 inhibitors
High risk of CVD
High risk of CVD
+
+
Inclisiran
Inclisiran
Icosapent ethyl
Icosapent ethyl
YES
YES
NO
NO
Very high risk of CVD
Very high risk of C...
+
+
consider
consider
Triglycerides > 1.7 mmol/L
+
Statin therapy
Triglycerides > 1.7 mmol/...

+
+
Alirocumab
Alirocumab
Evolocumab
EvolocumabText is not SVG - cannot display
INITIAL CONSIDERATIONS:
  • Measure non-fasting full lipid profile (total cholesterol, HDL-C, non-HDL-C, LDL-C, triglycerides) as part of an initial baseline assessment.
  • Consider secondary causes of hyperlipidaemia and manage as needed.
  • Ensure appropriate baseline and follow up tests.
    Measure BMI.
  • Identify and exclude people with contraindications/drug interactions.
  • If non-fasting triglyceride above 4.5mmol/L
Scenario
4 Baseline tests
5 Triglycerides
1a6 Primary prevention risk assessment
1a24 Management
1a7 Additional Risk Factors
1a8 Special populations
1a16 Extent of lipid lowering with available therapies
1b20 Refer
1c22 Titration Thresholds / Targets
1c26 Management
1c28 Special populations
1c30 Extent of lipid lowering with available therapies
Escalating lipid lowering treatment
Escalating therapy
MONITORING
MONITORING
Provide annual medication reviews for people taking statins to discuss effectiveness of therapy,
medicines adherence, lifestyle modification and address CVD risk factors.
*Offer in secondary prevention, and consider in primary prevention an annual non-fasting full lipid
profile to inform the discussion around effectiveness of lipid lowering therapy and any medicines non-adherence.
Provide annual medication reviews for people taking statins to discuss effectiven...
Baseline Measurements
In addition to full lipid profile, measure renal, thyroid and liver profiles (including albumin) and HbA1c to exclude secondary causes and co-morbidities.
Measure baseline liver transaminase (ALT or AST) before starting a statin.
Measure CK if unexplained muscle pain before starting a statin.
CK should not be measured routinely especially if a patient is asymptomatic.
Baseline Measurements...Primary PreventionSecondary preventionLipid ProfileALT or ASTLipid ProfileALT or ASTBaseline
✔
✔
✔
✔
✔
✔
✔
✔2-3 months
✔
✔
✔
✔
✔
✔
✔
✔6-9 months
If targets are not met, and up-titration is agreed, repeat full lipid
profile and ALT or AST within 2-3 months of each up-titration
of statin dose or addition of ezetimibe as required
If targets are not met, and up-titration is agreed, repeat full l...12 months
✔
✔
✔
✔
✔
✔
✔
✔Yearly
✔*
✔*
✔*
✔*
Monitoring
Repeat full lipid profile is non-fasting.
Do not stop statins because of an increase in blood glucose level or HbA1c
Advise that the risk of muscle pain, tenderness or weakness associated with statins is small and the rate of severe muscle adverse effects (rhabdomyolysis) is extremely low.
Monitoring...
Liver Transaminases
Measure liver transaminase within 3 months of starting treatment and then within 2-3
months of every additional up titration and then again at 12 months, but not again
unless clinically indicated.
Liver Transaminases...
If ALT or AST are greater than 3 times the upper limit of normal then do not initiate a statin
or discontinue statin therapy already prescribed and repeat the LFTs in a month.
If ALT or AST are greater than 3 times the upper limit of normal then do not init...
If ALT or AST are elevated but are less than 3 times the upper limit of normal then:
• Do not routinely exclude from statin treatment
• Continue the statin and repeat in a month.
• If they remain elevated but are less than 3 times the upper limit of normal then continue statin and repeat again in 6 months.
If ALT or AST are elevated but are less than 3 times the upper limit of normal th...Text is not SVG - cannot display
Triglyceride
concentration
Triglyceride...
Action
Action
Greater than
20mmol/L
Greater than...
Refer to lipid clinic for urgent specialist review if not a result of
excess alcohol or poor glycaemic control. At risk of acute pancreatitis.
Refer to lipid clinic for urgent specialist review if not a resu...
10 - 20mmol/L
10 - 20mmol/L
Repeat the TG measurement with a fasting test (after an interval of 5
days, but within 2 weeks) and review for potential secondary causes
of hyperlipidaemia. Seek specialist advice if the TG concentration
remains > 10mmol/litre. At risk of acute pancreatitis
Repeat the TG measurement with a fasting test (after an interval...
4.5 - 9.9mmol/L
4.5 - 9.9mmol/L
If non-fasting triglycerides are greater than 4.5mmol/L, repeat with
a fasting TG measurement Be aware that the CVD risk may be
underestimated by risk assessment tools, optimise the management
of other CVD risk factors present and seek specialist advice if non-
HDL-C concentration is > 7.5 mmol/litre.
If non-fasting triglycerides are greater than 4.5mmol/L, repeat...TRIGLYCERIDES
Icosapent ethyl (TA805)
• Check fasting triglycerides levels.
• Manage secondary causes of hypertriglyceridaemia.
• Consider icosapent ethyl (TA805) if patient has established cardiovascular disease
  (secondary prevention) and
    - on statins and fasting TG ≥ 1.7mmol/L and LDL-C* between 1.04‡ and ≤2.6mmol/L
• See table above and refer as appropriate.
Icosapent ethyl (TA805)...
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with your lab. Consider using an alternative equation (eg Sampson, doi: 10.1001/jamacardio.2020.0013) or beta-quantification.
‡ labs don’t report calculated LDL-C beyond one decimal point
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with y...Text is not SVG - cannot display
PRIMARY PREVENTION RISK ASSESSMENT
Use QRISK3 version of the calculator (or QRISK2 if not available).
- Do not use this risk assessment tool for people with established CVD or those who are already at high risk of developing CVD because of FH or other inherited disorders of lipid metabolism.
- Do not use a risk assessment tool to assess CVD risk in people with type 1 diabetes, or eGFR < 60 mL/min/1.73 m2 and/or albuminuria (as already at high risk of developing CVD).
- Consider people aged ≥ 85 at increased risk of CVD because of age alone particularly people who smoke or have raised BP.
- If QRISK <10% over next 10 years, do not rule out treatment if there is an informed preference for taking a statin or a concern that risk may be underestimated.
- Consider a lifetime risk tool (e.g.QRISK3-lifetime) to inform discussions on CVD risk and to motivate lifestyle changes, particularly for people with a 10‑year score < 10%, and people < 40 who have CVD risk factors.
Use QRISK3 version of the calculator (or QRISK2 if not available)....
Additional Risk Factors
Note, standard CVD risk scores including QRISK may underestimate risk in people who have additional risk because of underlying medical conditions or treatments. These include, but not limited to the following group of people;
• obesity increases CVD risk (NICE CG189)
• treated for HIV
• severe mental illness
• taking medicines that can cause dyslipidaemia such as antipsychotic medication, • corticosteroids or immunosuppressant drugs
• already taking medicines to treat CVD risk factors
• autoimmune disorders such as SLE, and other systemic inflammatory disorders
• non-diabetic hyperglycaemia
• significant hypertriglyceridaemia (fasting triglycerides 4.5-9.9mmol/L)
• recent risk factor changes e.g. quit smoking, BP or lipid treatment
Consider socio-economic status as an additional factor contributing to CVD risk (if not already in the risk calculator).
Additional Risk Factors...Text is not SVG - cannot display
MANAGEMENT
This guidance applies to new patients and may also be taken into consideration for those already on statins at their annual review. If 40% reduction of non-HDL-C, or target levels are not achieved, offer high intensity statins. Discuss with people who are stable on a low- or medium-intensity statin the likely benefits and potential risk of side effects if changed to a high-intensity statin when they have a medication review and agree with the person whether a change is needed.
Ezetimibe, alirocumab, evolocumab or inclisiran can be added when patients’ LDL-C levels are not lowered enough with the maximally tolerated dose of statins. If statins are contraindicated or not tolerated and ezetimibe alone does not control LDL-C well enough, bempedoic acid with ezetimibe is an option. Do not offer a fibrate, nicotinic acid, bile acid binder or omega-3 fatty acids alone or in combination with statin, for the prevention of CVD (check NICE NG238 and TA805 for exceptions).
This guidance applies to new patients and may also be taken into considerat...Text is not SVG - cannot display
ADDITIONAL RISK FACTORS
Additional Risk Factors
Note, standard CVD risk scores including QRISK may underestimate risk in people who have additional risk because of underlying medical conditions or treatments. These include, but not limited to the following group of people;
• obesity increases CVD risk (NICE CG189)
• treated for HIV
• severe mental illness
• taking medicines that can cause dyslipidaemia such as antipsychotic medication, corticosteroids or immunosuppressant drugs
• already taking medicines to treat CVD risk factors
• autoimmune disorders such as SLE, and other systemic inflammatory disorders
• non-diabetic hyperglycaemia
• significant hypertriglyceridaemia (fasting triglycerides 4.5-9.9mmol/L)
• recent risk factor changes e.g. quit smoking, BP or lipid treatment
Consider socio-economic status as an additional factor contributing to CVD risk (if not already in the risk calculator).
Additional Risk Factors...Text is not SVG - cannot display
SPECIAL PATIENT POPULATIONS
Type 1 Diabetes
While NICE recommends offering statins to patients with Type 1 diabetes as detailed in
the algorithm, it also states to consider statins in those aged 18 to 40 with type 1 diabetes,
including those who have had diabetes for ≤ 10 years.
Type 1 Diabetes...
Chronic Kidney Disease
Offer atorvastatin 20mg for the primary or secondary prevention of CVD to people with CKD (eGFR less than 60 mL/min/1.73m2 and/or albuminuria).
Increase the dose if target is not achieved and eGFR is 30 mL/min/1.73m2 or more.
Agree the use of higher doses with a renal specialist if eGFR is less than 30 mL/min/1.73m2
Chronic Kidney Disease...
Statins in Pregnancy and Lactation
Statins should be stopped 3 months before attempting to conceive and not be restarted
until breastfeeding is finished. Stop statins if pregnancy is a possibility.
Statins in Pregnancy and Lactation...Text is not SVG - cannot display
EXTENT OF LIPID LOWERING WITH AVAILABLE THERAPIES
• Rosuvastatin may be used as an alternative to atorvastatin if compatible with other
• drug therapy. Some people may need a lower starting dose (see BNF).
• Low/medium intensity statins should only be used if intolerance or drug interactions.
• Ezetimibe when combined with any statin is likely to give greater reduction in non-HDL-C
• or LDL-C than doubling the dose of the statin.
• PCSK9i (NICE TA393, TA394) alone or in combination with statins or ezetimibe produce
• an additional LDL-C reduction of approximately 50% (range 25-70%).
• Bempedoic acid when combined with ezetimibe (TA694) produces an additional LDL-C
• reduction of approximately 28% (range 22-33%).
• Inclisiran (TA733) alone or in combination with statins or ezetimibe produces an
• additional LDL-C reduction of approximately 50% (range 48-52%) but no clinical outcome
• evidence is currently available.
• Rosuvastatin may be used as an alternative to atorvastatin if compatible with ot...Approximate reduction in LDL-CStatin dose mg/day510204080Fluvastatin21%27%33%Pravastatin20%24%29%Simvastatin27%32%37%42%Atorvastatin37%43%49%55%Rosuvastatin38%43%48%53%Atorvastatin + Ezetimibe 10mg52%54%57%61%
Low intensity statins will produce an LDL-C reduction of 20-30%
Low intensity statins will produce an LDL-C reduction of 20-30%
Medium intensity statins will produce an LDL-C reduction of 31-40%
Medium intensity statins will produce an LDL-C reduction of 31-40%
High intensity statins will produce an LDL-C reduction above 40%
High intensity statins will produce an LDL-C reduction above 40%
Simvastatin 80mg is not recommended due to risk of muscle toxicity
Simvastatin 80mg is not recommended due to risk of muscle toxicityText is not SVG - cannot display
SPECIALIST SERVICES
Scope of specialist service available locally may include; lipid clinic, PCSK9i clinic
(offering initiation and subsequent follow up), FH genetic diagnosis and cascade
testing, lipoprotein apheresis service. NICE eligibility criteria for PCSK9i and fasting
LDL-C thresholds are summarised below.
Scope of specialist service available locally may include; lipid clinic, PC...
NICE TA393 Alirocumab
NICE TA394 Evolocumab
NICE TA393 Alirocumab...
Without CVD
Without CVD
With CVD
With CVD
High risk 1
High risk 1
Very high risk 2
Very high risk 2
Primary non-FH or mixed
dyslipidaemia
Primary non-FH or mixed...
Not recommended
Not recommended
LDL C > 4.0
mmoL/L
LDL C > 4.0...
LDL C > 3.5
mmoL/L
LDL C > 3.5...
Primary heterozygous-FH
Primary heterozygous-FH
LDL C > 5.0 mmoL/L
LDL C > 5.0 mmoL/L
LDL C > 3.5 mmoL/L
LDL C > 3.5 mmoL/L
1 History of any of the following: ACS; coronary or other arterial revascularisation procedures; CHD, ischaemic stroke; PAD. 2 Recurrent CV events or CV events in more than 1 vascular bed (that is, polyvascular disease).
1 History of any of the following: ACS; coronary or other arterial revascularisation pro...
Bempedoic acid/ezetimibe and inclisiran are available in primary care and do not
require initiation by specialist services.’ PCSK9i may be available for prescribing in
primary care: see local initiation pathways.
Bempedoic acid/ezetimibe and inclisiran are available in primary care and d...Text is not SVG - cannot display
MANAGEMENT
This guidance applies to new patients and may also be taken into consideration for those already on statins at their annual review. If 40% reduction of non-HDL-C, or target levels are not achieved, offer high intensity statins. Discuss with people who are stable on a low- or medium-intensity statin the likely benefits and potential risk of side effects if changed to a high-intensity statin when they have a medication review and agree with the person whether a change is needed.
Ezetimibe, alirocumab, evolocumab or inclisiran can be added when patients’ LDL-C levels are not lowered enough with the maximally tolerated dose of statins. If statins are contraindicated or not tolerated and ezetimibe alone does not control LDL-C well enough, bempedoic acid with ezetimibe is an option. Do not offer a fibrate, nicotinic acid, bile acid binder or omega-3 fatty acids alone or in combination with statin, for the prevention of CVD (check NICE NG238 and TA805 for exceptions).
This guidance applies to new patients and may also be taken into considerat...Text is not SVG - cannot display
TITRATION THRESHOLD / TARGETSNICE titration threshold / QOFJBS3**PrimarypreventionEscalate lipid lowering therapy ifnon-HDL-C reduction from baseline ≤ 40%
non-HDL-C < 2.5mmol/L 
(LDL-C < 1.8mmol/L)
non-HDL-C < 2.5mmol/L...SecondarypreventionAim for an LDL-C of ≤ 2.0 mmol/L, ornon-HDL-C of ≤ 2.6 mmol/L at least*FHOptimise lipid lowering therapy to achieve atleast 50% reduction in LDL-C (or non-HDL-C.)
*Consider ezetimibe to reduce CVD risk further, even if the NICE lipid target for
*secondary prevention of CVD is met.
**LDL-C and non-HDL-C levels should be reduced as much as possible in people
**with CVD. Consider a personalised target, as clinically indicated, e.g. JBS3
**consensus recommendation
*Consider ezetimibe to reduce CVD risk further, even if the NICE lipid targ...
Non-HDL-C = TC minus HDL-C
Non-HDL-C = TC minus HDL-C
LDL-C = non-HDL-C minus (Fasting triglyceridesa/2.2)
LDL-C = non-HDL-C minus (Fasting triglyceridesa/2....
a valid only when fasting triglycerides are less than 4.5 mmol/L
a valid only when fasting triglycerides are less than 4.5 m...Text is not SVG - cannot display
EXTENT OF LIPID LOWERING WITH AVAILABLE THERAPIES
• Rosuvastatin may be used as an alternative to atorvastatin if compatible with other
• drug therapy. Some people may need a lower starting dose (see BNF).
• Low/medium intensity statins should only be used if intolerance or drug interactions.
• Ezetimibe when combined with any statin is likely to give greater reduction in non-HDL-C
• or LDL-C than doubling the dose of the statin.
• PCSK9i (NICE TA393, TA394) alone or in combination with statins or ezetimibe produce
• an additional LDL-C reduction of approximately 50% (range 25-70%).
• Bempedoic acid when combined with ezetimibe (TA694) produces an additional LDL-C
• reduction of approximately 28% (range 22-33%).
• Inclisiran (TA733) alone or in combination with statins or ezetimibe produces an
• additional LDL-C reduction of approximately 50% (range 48-52%) but no clinical outcome
• evidence is currently available.
• Rosuvastatin may be used as an alternative to atorvastatin if compatible with ot...Approximate reduction in LDL-CStatin dose mg/day510204080Fluvastatin21%27%33%Pravastatin20%24%29%Simvastatin27%32%37%42%Atorvastatin37%43%49%55%Rosuvastatin38%43%48%53%Atorvastatin + Ezetimibe 10mg52%54%57%61%
Low intensity statins will produce an LDL-C reduction of 20-30%
Low intensity statins will produce an LDL-C reduction of 20-30%
Medium intensity statins will produce an LDL-C reduction of 31-40%
Medium intensity statins will produce an LDL-C reduction of 31-40%
High intensity statins will produce an LDL-C reduction above 40%
High intensity statins will produce an LDL-C reduction above 40%
Simvastatin 80mg is not recommended due to risk of muscle toxicity
Simvastatin 80mg is not recommended due to risk of muscle toxicityText is not SVG - cannot display
SPECIAL PATIENT POPULATIONS
Type 1 Diabetes
While NICE recommends offering statins to patients with Type 1 diabetes as detailed in
the algorithm, it also states to consider statins in those aged 18 to 40 with type 1 diabetes,
including those who have had diabetes for ≤ 10 years.
Type 1 Diabetes...
Chronic Kidney Disease
Offer atorvastatin 20mg for the primary or secondary prevention of CVD to people with CKD (eGFR less than 60 mL/min/1.73m2 and/or albuminuria).
Increase the dose if target is not achieved and eGFR is 30 mL/min/1.73m2 or more.
Agree the use of higher doses with a renal specialist if eGFR is less than 30 mL/min/1.73m2
Chronic Kidney Disease...
Statins in Pregnancy and Lactation
Statins should be stopped 3 months before attempting to conceive and not be restarted
until breastfeeding is finished. Stop statins if pregnancy is a possibility.
Statins in Pregnancy and Lactation...Text is not SVG - cannot display
48 Instructions on
54 Instructions off
MANAGEMENT
This guidance applies to new patients and may also be taken into consideration for those already on statins at their annual review. If 40% reduction of non-HDL-C, or target levels are not achieved, offer high intensity statins. Discuss with people who are stable on a low- or medium-intensity statin the likely benefits and potential risk of side effects if changed to a high-intensity statin when they have a medication review and agree with the person whether a change is needed.
Ezetimibe, alirocumab, evolocumab or inclisiran can be added when patients’ LDL-C levels are not lowered enough with the maximally tolerated dose of statins. If statins are contraindicated or not tolerated and ezetimibe alone does not control LDL-C well enough, bempedoic acid with ezetimibe is an option. Do not offer a fibrate, nicotinic acid, bile acid binder or omega-3 fatty acids alone or in combination with statin, for the prevention of CVD (check NICE NG238 and TA805 for exceptions).
This guidance applies to new patients and may also be taken into considerat...Text is not SVG - cannot display
PRIMARY PREVENTION RISK ASSESSMENT
Use QRISK3 version of the calculator (or QRISK2 if not available).
- Do not use this risk assessment tool for people with established CVD or those who are already at high risk of developing CVD because of FH or other inherited disorders of lipid metabolism.
- Do not use a risk assessment tool to assess CVD risk in people with type 1 diabetes, or eGFR < 60 mL/min/1.73 m2 and/or albuminuria (as already at high risk of developing CVD).
- Consider people aged ≥ 85 at increased risk of CVD because of age alone particularly people who smoke or have raised BP.
- If QRISK <10% over next 10 years, do not rule out treatment if there is an informed preference for taking a statin or a concern that risk may be underestimated.
- Consider a lifetime risk tool (e.g.QRISK3-lifetime) to inform discussions on CVD risk and to motivate lifestyle changes, particularly for people with a 10‑year score < 10%, and people < 40 who have CVD risk factors.
Use QRISK3 version of the calculator (or QRISK2 if not available)....
Additional Risk Factors
Note, standard CVD risk scores including QRISK may underestimate risk in people who have additional risk because of underlying medical conditions or treatments. These include, but not limited to the following group of people;
• obesity increases CVD risk (NICE CG189)
• treated for HIV
• severe mental illness
• taking medicines that can cause dyslipidaemia such as antipsychotic medication, • corticosteroids or immunosuppressant drugs
• already taking medicines to treat CVD risk factors
• autoimmune disorders such as SLE, and other systemic inflammatory disorders
• non-diabetic hyperglycaemia
• significant hypertriglyceridaemia (fasting triglycerides 4.5-9.9mmol/L)
• recent risk factor changes e.g. quit smoking, BP or lipid treatment
Consider socio-economic status as an additional factor contributing to CVD risk (if not already in the risk calculator).
Additional Risk Factors...Text is not SVG - cannot display
SPECIAL PATIENT POPULATIONS
Type 1 Diabetes
While NICE recommends offering statins to patients with Type 1 diabetes as detailed in
the algorithm, it also states to consider statins in those aged 18 to 40 with type 1 diabetes,
including those who have had diabetes for ≤ 10 years.
Type 1 Diabetes...
Chronic Kidney Disease
Offer atorvastatin 20mg for the primary or secondary prevention of CVD to people with CKD (eGFR less than 60 mL/min/1.73m2 and/or albuminuria).
Increase the dose if target is not achieved and eGFR is 30 mL/min/1.73m2 or more.
Agree the use of higher doses with a renal specialist if eGFR is less than 30 mL/min/1.73m2
Chronic Kidney Disease...
Statins in Pregnancy and Lactation
Statins should be stopped 3 months before attempting to conceive and not be restarted
until breastfeeding is finished. Stop statins if pregnancy is a possibility.
Statins in Pregnancy and Lactation...Text is not SVG - cannot display
EXTENT OF LIPID LOWERING WITH AVAILABLE THERAPIES
• Rosuvastatin may be used as an alternative to atorvastatin if compatible with other
• drug therapy. Some people may need a lower starting dose (see BNF).
• Low/medium intensity statins should only be used if intolerance or drug interactions.
• Ezetimibe when combined with any statin is likely to give greater reduction in non-HDL-C
• or LDL-C than doubling the dose of the statin.
• PCSK9i (NICE TA393, TA394) alone or in combination with statins or ezetimibe produce
• an additional LDL-C reduction of approximately 50% (range 25-70%).
• Bempedoic acid when combined with ezetimibe (TA694) produces an additional LDL-C
• reduction of approximately 28% (range 22-33%).
• Inclisiran (TA733) alone or in combination with statins or ezetimibe produces an
• additional LDL-C reduction of approximately 50% (range 48-52%) but no clinical outcome
• evidence is currently available.
• Rosuvastatin may be used as an alternative to atorvastatin if compatible with ot...Approximate reduction in LDL-CStatin dose mg/day510204080Fluvastatin21%27%33%Pravastatin20%24%29%Simvastatin27%32%37%42%Atorvastatin37%43%49%55%Rosuvastatin38%43%48%53%Atorvastatin + Ezetimibe 10mg52%54%57%61%
Low intensity statins will produce an LDL-C reduction of 20-30%
Low intensity statins will produce an LDL-C reduction of 20-30%
Medium intensity statins will produce an LDL-C reduction of 31-40%
Medium intensity statins will produce an LDL-C reduction of 31-40%
High intensity statins will produce an LDL-C reduction above 40%
High intensity statins will produce an LDL-C reduction above 40%
Simvastatin 80mg is not recommended due to risk of muscle toxicity
Simvastatin 80mg is not recommended due to risk of muscle toxicityText is not SVG - cannot display
MONITORING
MONITORING
Provide annual medication reviews for people taking statins to discuss effectiveness of therapy,
medicines adherence, lifestyle modification and address CVD risk factors.
*Offer in secondary prevention, and consider in primary prevention an annual non-fasting full lipid
profile to inform the discussion around effectiveness of lipid lowering therapy and any medicines non-adherence.
Provide annual medication reviews for people taking statins to discuss effectiven...
Baseline Measurements
In addition to full lipid profile, measure renal, thyroid and liver profiles (including albumin) and HbA1c to exclude secondary causes and co-morbidities.
Measure baseline liver transaminase (ALT or AST) before starting a statin.
Measure CK if unexplained muscle pain before starting a statin.
CK should not be measured routinely especially if a patient is asymptomatic.
Baseline Measurements...Primary PreventionSecondary preventionLipid ProfileALT or ASTLipid ProfileALT or ASTBaseline
✔
✔
✔
✔
✔
✔
✔
✔2-3 months
✔
✔
✔
✔
✔
✔
✔
✔6-9 months
If targets are not met, and up-titration is agreed, repeat full lipid
profile and ALT or AST within 2-3 months of each up-titration
of statin dose or addition of ezetimibe as required
If targets are not met, and up-titration is agreed, repeat full l...12 months
✔
✔
✔
✔
✔
✔
✔
✔Yearly
✔*
✔*
✔*
✔*
Monitoring
Repeat full lipid profile is non-fasting.
Do not stop statins because of an increase in blood glucose level or HbA1c
Advise that the risk of muscle pain, tenderness or weakness associated with statins is small and the rate of severe muscle adverse effects (rhabdomyolysis) is extremely low.
Monitoring...
Liver Transaminases
Measure liver transaminase within 3 months of starting treatment and then within 2-3
months of every additional up titration and then again at 12 months, but not again
unless clinically indicated.
Liver Transaminases...
If ALT or AST are greater than 3 times the upper limit of normal then do not initiate a statin
or discontinue statin therapy already prescribed and repeat the LFTs in a month.
If ALT or AST are greater than 3 times the upper limit of normal then do not init...
If ALT or AST are elevated but are less than 3 times the upper limit of normal then:
• Do not routinely exclude from statin treatment
• Continue the statin and repeat in a month.
• If they remain elevated but are less than 3 times the upper limit of normal then continue statin and repeat again in 6 months.
If ALT or AST are elevated but are less than 3 times the upper limit of normal th...Text is not SVG - cannot display
TITRATION THRESHOLD / TARGETSNICE titration threshold / QOFJBS3**PrimarypreventionEscalate lipid lowering therapy ifnon-HDL-C reduction from baseline ≤ 40%
non-HDL-C < 2.5mmol/L 
(LDL-C < 1.8mmol/L)
non-HDL-C < 2.5mmol/L...SecondarypreventionAim for an LDL-C of ≤ 2.0 mmol/L, ornon-HDL-C of ≤ 2.6 mmol/L at least*FHOptimise lipid lowering therapy to achieve atleast 50% reduction in LDL-C (or non-HDL-C.)
*Consider ezetimibe to reduce CVD risk further, even if the NICE lipid target for
*secondary prevention of CVD is met.
**LDL-C and non-HDL-C levels should be reduced as much as possible in people
**with CVD. Consider a personalised target, as clinically indicated, e.g. JBS3
**consensus recommendation
*Consider ezetimibe to reduce CVD risk further, even if the NICE lipid targ...
Non-HDL-C = TC minus HDL-C
Non-HDL-C = TC minus HDL-C
LDL-C = non-HDL-C minus (Fasting triglyceridesa/2.2)
LDL-C = non-HDL-C minus (Fasting triglyceridesa/2....
a valid only when fasting triglycerides are less than 4.5 mmol/L
a valid only when fasting triglycerides are less than 4.5 m...Text is not SVG - cannot display
SPECIALIST SERVICES
Scope of specialist service available locally may include; lipid clinic, PCSK9i clinic
(offering initiation and subsequent follow up), FH genetic diagnosis and cascade
testing, lipoprotein apheresis service. NICE eligibility criteria for PCSK9i and fasting
LDL-C thresholds are summarised below.
Scope of specialist service available locally may include; lipid clinic, PC...
NICE TA393 Alirocumab
NICE TA394 Evolocumab
NICE TA393 Alirocumab...
Without CVD
Without CVD
With CVD
With CVD
High risk 1
High risk 1
Very high risk 2
Very high risk 2
Primary non-FH or mixed
dyslipidaemia
Primary non-FH or mixed...
Not recommended
Not recommended
LDL C > 4.0
mmoL/L
LDL C > 4.0...
LDL C > 3.5
mmoL/L
LDL C > 3.5...
Primary heterozygous-FH
Primary heterozygous-FH
LDL C > 5.0 mmoL/L
LDL C > 5.0 mmoL/L
LDL C > 3.5 mmoL/L
LDL C > 3.5 mmoL/L
1 History of any of the following: ACS; coronary or other arterial revascularisation procedures; CHD, ischaemic stroke; PAD. 2 Recurrent CV events or CV events in more than 1 vascular bed (that is, polyvascular disease).
1 History of any of the following: ACS; coronary or other arterial revascularisation pro...
Bempedoic acid/ezetimibe and inclisiran are available in primary care and do not
require initiation by specialist services.’ PCSK9i may be available for prescribing in
primary care: see local initiation pathways.
Bempedoic acid/ezetimibe and inclisiran are available in primary care and d...Text is not SVG - cannot display
Triglyceride
concentration
Triglyceride...
Action
Action
Greater than
20mmol/L
Greater than...
Refer to lipid clinic for urgent specialist review if not a result of
excess alcohol or poor glycaemic control. At risk of acute pancreatitis.
Refer to lipid clinic for urgent specialist review if not a resu...
10 - 20mmol/L
10 - 20mmol/L
Repeat the TG measurement with a fasting test (after an interval of 5
days, but within 2 weeks) and review for potential secondary causes
of hyperlipidaemia. Seek specialist advice if the TG concentration
remains > 10mmol/litre. At risk of acute pancreatitis
Repeat the TG measurement with a fasting test (after an interval...
4.5 - 9.9mmol/L
4.5 - 9.9mmol/L
If non-fasting triglycerides are greater than 4.5mmol/L, repeat with
a fasting TG measurement Be aware that the CVD risk may be
underestimated by risk assessment tools, optimise the management
of other CVD risk factors present and seek specialist advice if non-
HDL-C concentration is > 7.5 mmol/litre.
If non-fasting triglycerides are greater than 4.5mmol/L, repeat...TRIGLYCERIDES
Icosapent ethyl (TA805)
• Check fasting triglycerides levels.
• Manage secondary causes of hypertriglyceridaemia.
• Consider icosapent ethyl (TA805) if patient has established cardiovascular disease
  (secondary prevention) and
    - on statins and fasting TG ≥ 1.7mmol/L and LDL-C* between 1.04‡ and ≤2.6mmol/L
• See table above and refer as appropriate.
Icosapent ethyl (TA805)...
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with your lab. Consider using an alternative equation (eg Sampson, doi: 10.1001/jamacardio.2020.0013) or beta-quantification.
‡ labs don’t report calculated LDL-C beyond one decimal point
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with y...Text is not SVG - cannot display
HOW TO USE THIS INTERACTIVE PATHWAY
This is an interactive digital version of the Summary of national guidance for lipid management for primary and secondary prevention of cardiovascular disease PDF document
This is an interactive digital version of the Summary of national guidance...
Follow pathway and advice
Follow pathway and advice
1
1
Select clinical scenario 
Select clinical scenario 
2
2
These buttons will adapt the pathway 
These buttons will adapt the pathway 
Click buttons for guideline notes
Click buttons for guideline notes
3
3

  • Selecting from the drop down above


When multiple information boxes are displayed, they may be layered; clicking on a box will elevate it to the top of the stack.
Selecting from the drop down above...
Notes from the guideline are revealed by:
  • Toggling the smaller buttons on the pathway



Notes from the guideline are revealed by:...
Click icons for more information
Click icons for more information
4
4
Rotation icons reveal further information from the original pathway
Rotation icons reveal further information fr...
NICE link icons navigate to related resources provided by NICE in the UK 
NICE link icons navigate to related resource...
N
NText is not SVG - cannot display
HOW TO USE THIS INTERACTIVE PATHWAY
This is an interactive digital version of the Summary of national guidance for lipid management for primary and secondary prevention of cardiovascular disease PDF document
This is an interactive digital version of the Summary of national guidance...
Follow pathway and advice
Follow pathway and advice
1
1
Select clinical scenario 
Select clinical scenario 
2
2
These buttons will adapt the pathway 
These buttons will adapt the pathway 
Click buttons for guideline notes
Click buttons for guideline notes
3
3

  • Selecting from the drop down above


When multiple information boxes are displayed, they may be layered; clicking on a box will elevate it to the top of the stack.
Selecting from the drop down above...
Notes from the guideline are revealed by:
  • Toggling the smaller buttons on the pathway



Notes from the guideline are revealed by:...
Click icons for more information
Click icons for more information
4
4
Rotation icons reveal further information from the original pathway
Rotation icons reveal further information fr...
NICE link icons navigate to related resources provided by NICE in the UK 
NICE link icons navigate to related resource...
N
NText is not SVG - cannot display
HOW TO USE THIS INTERACTIVE PATHWAY
This is an interactive digital version of the Summary of national guidance for lipid management for primary and secondary prevention of cardiovascular disease PDF document
This is an interactive digital version of the Summary of national guidance...
Follow pathway and advice
Follow pathway and advice
1
1
Select clinical scenario 
Select clinical scenario 
2
2
These buttons will adapt the pathway 
These buttons will adapt the pathway 
Click buttons for guideline notes
Click buttons for guideline notes
3
3

  • Selecting from the drop down above


When multiple information boxes are displayed, they may be layered; clicking on a box will elevate it to the top of the stack.
Selecting from the drop down above...
Notes from the guideline are revealed by:
  • Toggling the smaller buttons on the pathway



Notes from the guideline are revealed by:...
Click icons for more information
Click icons for more information
4
4
Rotation icons reveal further information from the original pathway
Rotation icons reveal further information fr...
NICE link icons navigate to related resources provided by NICE in the UK 
NICE link icons navigate to related resource...
N
NText is not SVG - cannot display
1c49 Specialist services
SPECIALIST SERVICES
Scope of specialist service available locally may include; lipid clinic, PCSK9i clinic
(offering initiation and subsequent follow up), FH genetic diagnosis and cascade
testing, lipoprotein apheresis service. NICE eligibility criteria for PCSK9i and fasting
LDL-C thresholds are summarised below.
Scope of specialist service available locally may include; lipid clinic, PC...
NICE TA393 Alirocumab
NICE TA394 Evolocumab
NICE TA393 Alirocumab...
Without CVD
Without CVD
With CVD
With CVD
High risk 1
High risk 1
Very high risk 2
Very high risk 2
Primary non-FH or mixed
dyslipidaemia
Primary non-FH or mixed...
Not recommended
Not recommended
LDL C > 4.0
mmoL/L
LDL C > 4.0...
LDL C > 3.5
mmoL/L
LDL C > 3.5...
Primary heterozygous-FH
Primary heterozygous-FH
LDL C > 5.0 mmoL/L
LDL C > 5.0 mmoL/L
LDL C > 3.5 mmoL/L
LDL C > 3.5 mmoL/L
1 History of any of the following: ACS; coronary or other arterial revascularisation procedures; CHD, ischaemic stroke; PAD. 2 Recurrent CV events or CV events in more than 1 vascular bed (that is, polyvascular disease).
1 History of any of the following: ACS; coronary or other arterial revascularisation pro...
Bempedoic acid/ezetimibe and inclisiran are available in primary care and do not
require initiation by specialist services.’ PCSK9i may be available for prescribing in
primary care: see local initiation pathways.
Bempedoic acid/ezetimibe and inclisiran are available in primary care and d...Text is not SVG - cannot display
1c32 47 Triglycerides Escalating therapy - statin intolerance
Triglyceride
concentration
Triglyceride...
Action
Action
Greater than
20mmol/L
Greater than...
Refer to lipid clinic for urgent specialist review if not a result of
excess alcohol or poor glycaemic control. At risk of acute pancreatitis.
Refer to lipid clinic for urgent specialist review if not a resu...
10 - 20mmol/L
10 - 20mmol/L
Repeat the TG measurement with a fasting test (after an interval of 5
days, but within 2 weeks) and review for potential secondary causes
of hyperlipidaemia. Seek specialist advice if the TG concentration
remains > 10mmol/litre. At risk of acute pancreatitis
Repeat the TG measurement with a fasting test (after an interval...
4.5 - 9.9mmol/L
4.5 - 9.9mmol/L
If non-fasting triglycerides are greater than 4.5mmol/L, repeat with
a fasting TG measurement Be aware that the CVD risk may be
underestimated by risk assessment tools, optimise the management
of other CVD risk factors present and seek specialist advice if non-
HDL-C concentration is > 7.5 mmol/litre.
If non-fasting triglycerides are greater than 4.5mmol/L, repeat...TRIGLYCERIDES
Icosapent ethyl (TA805)
• Check fasting triglycerides levels.
• Manage secondary causes of hypertriglyceridaemia.
• Consider icosapent ethyl (TA805) if patient has established cardiovascular disease
  (secondary prevention) and
    - on statins and fasting TG ≥ 1.7mmol/L and LDL-C* between 1.04‡ and ≤2.6mmol/L
• See table above and refer as appropriate.
Icosapent ethyl (TA805)...
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with your lab. Consider using an alternative equation (eg Sampson, doi: 10.1001/jamacardio.2020.0013) or beta-quantification.
‡ labs don’t report calculated LDL-C beyond one decimal point
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with y...Text is not SVG - cannot display
1c32 58 Triglycerides Escalating therapy
Triglyceride
concentration
Triglyceride...
Action
Action
Greater than
20mmol/L
Greater than...
Refer to lipid clinic for urgent specialist review if not a result of
excess alcohol or poor glycaemic control. At risk of acute pancreatitis.
Refer to lipid clinic for urgent specialist review if not a resu...
10 - 20mmol/L
10 - 20mmol/L
Repeat the TG measurement with a fasting test (after an interval of 5
days, but within 2 weeks) and review for potential secondary causes
of hyperlipidaemia. Seek specialist advice if the TG concentration
remains > 10mmol/litre. At risk of acute pancreatitis
Repeat the TG measurement with a fasting test (after an interval...
4.5 - 9.9mmol/L
4.5 - 9.9mmol/L
If non-fasting triglycerides are greater than 4.5mmol/L, repeat with
a fasting TG measurement Be aware that the CVD risk may be
underestimated by risk assessment tools, optimise the management
of other CVD risk factors present and seek specialist advice if non-
HDL-C concentration is > 7.5 mmol/litre.
If non-fasting triglycerides are greater than 4.5mmol/L, repeat...TRIGLYCERIDES
Icosapent ethyl (TA805)
• Check fasting triglycerides levels.
• Manage secondary causes of hypertriglyceridaemia.
• Consider icosapent ethyl (TA805) if patient has established cardiovascular disease
  (secondary prevention) and
    - on statins and fasting TG ≥ 1.7mmol/L and LDL-C* between 1.04‡ and ≤2.6mmol/L
• See table above and refer as appropriate.
Icosapent ethyl (TA805)...
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with your lab. Consider using an alternative equation (eg Sampson, doi: 10.1001/jamacardio.2020.0013) or beta-quantification.
‡ labs don’t report calculated LDL-C beyond one decimal point
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with y...Text is not SVG - cannot display
1c32 59 Triglycerides Escalating therapy
Triglyceride
concentration
Triglyceride...
Action
Action
Greater than
20mmol/L
Greater than...
Refer to lipid clinic for urgent specialist review if not a result of
excess alcohol or poor glycaemic control. At risk of acute pancreatitis.
Refer to lipid clinic for urgent specialist review if not a resu...
10 - 20mmol/L
10 - 20mmol/L
Repeat the TG measurement with a fasting test (after an interval of 5
days, but within 2 weeks) and review for potential secondary causes
of hyperlipidaemia. Seek specialist advice if the TG concentration
remains > 10mmol/litre. At risk of acute pancreatitis
Repeat the TG measurement with a fasting test (after an interval...
4.5 - 9.9mmol/L
4.5 - 9.9mmol/L
If non-fasting triglycerides are greater than 4.5mmol/L, repeat with
a fasting TG measurement Be aware that the CVD risk may be
underestimated by risk assessment tools, optimise the management
of other CVD risk factors present and seek specialist advice if non-
HDL-C concentration is > 7.5 mmol/litre.
If non-fasting triglycerides are greater than 4.5mmol/L, repeat...TRIGLYCERIDES
Icosapent ethyl (TA805)
• Check fasting triglycerides levels.
• Manage secondary causes of hypertriglyceridaemia.
• Consider icosapent ethyl (TA805) if patient has established cardiovascular disease
  (secondary prevention) and
    - on statins and fasting TG ≥ 1.7mmol/L and LDL-C* between 1.04‡ and ≤2.6mmol/L
• See table above and refer as appropriate.
Icosapent ethyl (TA805)...
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with your lab. Consider using an alternative equation (eg Sampson, doi: 10.1001/jamacardio.2020.0013) or beta-quantification.
‡ labs don’t report calculated LDL-C beyond one decimal point
* LDL-C cannot be calculated using Friedewald’s formula if TG >4.5. Discuss with y...Text is not SVG - cannot display
Consider ezetimibe in addition to the maximum tolerated intensity and dose of statin to reduce CVD risk further,
even if the lipid target for secondary prevention of CVD is met. (NG238)
Consider ezetimibe in addition to the maximum tolerated intensity and dose of statin to reduce CVD...
Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosapent ethyl.

Additional CV risk reduction considerations - check fasting triglycerides levels and consider icosa... ABBREVIATIONS
Statin intolerance is defined as the presence of clinically significant adverse effects from statin therapy that are considered to represent an unacceptable risk to the patient or that may result in adherence to therapy being compromised.
For people who are intolerant of the recommended statin treatment see the NHSE AAC statin intolerance algorithm, available on the NHSE AAC page (Click here)
Statin intolerance is defined as the presence of clinically significant adv...
“This summary accurately reflects NICE guidance and JBS3 recommendations”, NICE March 2024
“This summary accurately reflects NICE guidan... STATIN INTOLERANCE
ALT: alanine aminotransferase
AST: aspartate aminotransferase
CHD: coronary heart disease
CKD: chronic kidney disease
CVD: cardiovascular disease
FH: familial hypercholesterolaemia
JBS: Joint British Societies
LDL-C: low density lipoprotein cholesterol
ALT: alanine aminotransferase...
non-HDL-C: non-high density lipoprotein cholesterol
PCSK9i: proprotein convertase subtilisin kexin 9
PCSK9i: monoclonal antibody inhibitor
QOF: Quality and Outcomes Framework
SLE: systemic lupus erythematosus
SPC: summary of product characteristics
TC: total cholesterol
non-HDL-C: non-high density lipoprotein cholest...
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Subgroup.
Updated by NHSE Cholesterol Expert Advisory Group.
March 2024. Review date: March 2026.
Authors: Dr Rani Khatib & Dr Dermot Neely on behalf of the AAC Clinical Sub...
References
References
JBS3. 2014. www.jbs3risk.com/pages/6.htm
Kirsten et al. 2005. Hospital Pharmacy 40(8):687-692
Navarese et al. 2015. Annals of internal medicine 163(1):40-51
Soon Jun Hong et al. 2018. Clinical therapeutics 40(2): 226-241.e4
NICE 2016. TA385 www.nice.org.uk/guidance/ta385
NICE 2016. TA393 www.nice.org.uk/guidance/TA393
NICE 2016. TA394 www.nice.org.uk/guidance/TA394
JBS3. 2014. www.jbs3risk.com/pages/6.htm...
NICE 2008. CG71 www.nice.org.uk/guidance/cg71
NICE 2021. TA694 www.nice.org.uk/guidance/TA694
NICE 2021. TA733 www.nice.org.uk/guidance/TA733
NICE 2022. TA805 www.nice.org.uk/guidance/ta805
NICE 2023. NG238 www.nice.org.uk/guidance/ng238
NICE 2023. CG189 www.nice.org.uk/guidance/cg189
NICE 2008. CG71 www.nice.org.uk/guidance/cg71...
Original PDF version of the guideline:  A summary of national guidance for lipid management for primary and secondary prevention of  cardiovascular disease (CVD).
Original PDF version of the guideline:  A summary of national guidance for lipid managem...
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.
If you have any enquiries about the tool, please contact us. If you have any issues with using the tool please get in touch with Clinical Pathways.Text is not SVG - cannot display