Raised blood lipid levels are important risk factors for coronary artery disease (CAD). 

The relationship between CAD and total cholesterol levels is continuous and curvilinear. LDL cholesterol (LDL-C) is a well-established risk for CAD1​.​password content

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  • Please refer to the Cardiovascular Risk Assess​ment Protocol and 10 Year Cardiovascular Disease Risk Calculator​ where needed.

  • Screening for lipids should be performed as part of a global cardiovascular/cardiometabolic risk assessment. Clinicians should also consider screening for other risk factors such as blood pressure and blood glucose.

  • In the prevention of CAD, the intensity of risk reduction therapy should be adjusted to a person’s risk of developing future coronary events. As such, the first step should be to assess the individual’s risk status and assignment to one of four risk categories.

    R
    isk Stratification and Treatment Goals (adapted from MOH CPG on Lipids Dec 2016) .​

    • Cardiovascular Disease Risk Calculator​

    • Estimation of 10-Year Coronary Artery Disease Risk for Men .​

    • Estimation of 10-Year Coronary Artery Disease Risk for Women .​

    • Secondary dyslipidaemia should be excluded in selected patients diagnosed with lipid disorders .​

  • Hypertriglyceridaemia

    • Elevated blood TG levels are associated with CAD. However, this association is significantly attenuated after adjustment for other blood lipid levels.

    • Individuals with very high levels of fasting TG, i.e. >4.5mmol/L (400mg/dL) or especially >10mmol/L >900mg/dL), have an increased risk of acute pancreatitis. For such patients, the priority is to reduce the TG level to prevent acute pancreatitis through the initiation of fibrates.

    • For patients with very high or high CAD risk who have TG levels between 2.3mmol/L (200/dL) to 4.5mmol/L (400mg/dL), statins (with or without ezetimibe) should be used primarily to lower non-HDL C.

Special Considerations1

  • Elderly

    • In the elderly (age >75 years), the decision to start treatment should consider the potential risk-reduction associated with treatment, risk of adverse effects, drug-drug interactions, and patient preferences.

    • In very high-risk elderly patients, more intensive therapy (achieving LDL-C in the range of 2.1mmol/L or 80mg/dL) has not shown additional benefit over less intensive therapy. Treatment for such patients should be individualised.

    • When used, lipid-lowering medications in the elderly should be started at the lowest dose and then titrated to achieve optimal LDL-C levels, in order to reduce possible statin-associated side effects. For patients on treatment with a statin and LDL-C <2.1mmol/L or 80mg/dL when they turn >75 years of age, there is no need to reduce therapy if the treatment is well-tolerated without any adverse effects.

  • Women

    • Statins are contraindicated in women who are pregnant, likely to be pregnant, or breastfeeding.

  • Renal Disease

    • The starting dose of statins in chronic kidney disease should be low (e.g. 10mg simvastatin or equivalent ). During therapy, serum creatine kinase (CK) and renal function should both be carefully monitored.

    • Fibrates can be used in patients with chronic kidney disease in stages 1 to 3, but the dosages should be reduced, with appropriate monitoring for side effects, especially myopathy.

    • When creatinine clearance is less than 30 ml/min (stage 4 or 5), fibrates are contraindicated.

    • In patients with end stage chronic kidney disease on dialysis, statins did not significantly improve cardiovascular outcomes.

  • Liver Disease

    • In patients with dyslipidemia and chronic liver disease, if the level of the two transaminases (ALT and/or AST) are elevated but < 3 times the upper limit of the normal range, statins can be given but the starting dose should be low. Careful monitoring of the serum transaminases and CK after commencement are  recommended.

    • Fibrates can be given in patients whose transaminase levels are elevated < 3 times the upper limit of the normal range, but at a lower starting dosage. Careful monitoring of the serum transaminases and CK after commencement is recommended.

  • Familial Hypercholesterolaemia (FH)

    • Screening of all first degree relatives of diagnosed FH patients is recommended.

    • Clinical diagnosis may be made by the Simon Broome Trust diagnostic criteria .​

    • Offer patients with possible or definite FH a referral to a specialist to make a recommendation on the need for therapy.

    • Coronary artery disease risk estimation tools should not be used because patients with FH are already at a high risk of premature coronary artery disease. 

    • Early screening provides the opportunity to teach good eating habits from a young age, if a child is identified to have FH. Children who have a first degree relative diagnosed with FH can be screened within specialist centres starting from the age of 2 years.​


Treatment Goals

  • Please refer to the Risk Stratification and Treatment Goals template under Clinical Approach (3) .

  • Recommended Care Components

​Recommended Care Components

​Minimum Freq​uency*

​Remarks

​Lipid Profile

​Annually

​All patients should be risk stratified (as recommended in the Lipids CPG)

Targets of treatment should be personalised by levels of risk 

​Smoking Assessment

​Annually for smokers;

Once-off for non-smokers, unless there is a change in smoking habit

​Assessment on smoking habits (estimated sticks/day; zero for non- or ex-smoker) and provide smoking cessation counselling

For more details, please refer to the Smoking Cessation care protocol.

​Serum transaminases (ALT/AST)

​Before starting statins and as clinically indicated (e.g. symptoms suggestive of heptatotoxicity, increase in statin dose)

​Especially when the statin dose is increased or when combination therapy is initiated​

Stop the statin / fibrate if patient is symptomatic or if transaminases exceed 3 times the upper limit of normal range.

​Serum creatine kinase

​Before starting statins and as indicated (e.g. muscle symptoms)

​Look out for rapid increase in creatine kinase post-initiation or increase of statin or fibrate dose. Stop the medication if the CK is three times upper limit of normal (ULN)) or at about 800 IU/L (whichever is lower)


  • ​Lifestyle Changes1

    • Smoking cessation and abstinence

    • Weight reduction

    • Exercise

    • Diet

    • Alcohol consumption reduction and abstinence

    • Plant sterols and stanols consumption

  • Pharmacological1

    • Drug classes.

    • Initiating therapy.

    • ​Monitoring side effects of therapy.


Consideration for Specialist Referral
2​

​Specialist Referral Recommended​

Referral to Gastroenterologist

  • Pre-treatment sustained transaminases 3 times above normal range

  • Clinical presentation of acute hepatitis 

  • If the ALT/A​ST is persistently elevated ≥ 3X Upper Limit Normal despite stopping statins.

Patients who are clinically unwell, jaundiced or who will benefit from urgent evaluation should be referred to the A&E.

​Consider Specialist Input

Consider Referral to an Endocrinologist

  • Triglyceride level more than 4.5mmol/L (400mg/dL) despite dietary changes and maximum tolerated drug therapy

  • Target parameters not achieved despite maximal drug therapy

  • Definite or possible familial hypercholesterolemia on Simon Broome Trust diagnostic criteria (or other validated criteria)



The following data fields should be documented in your case notes as part of good clinical practice for all patients enrolled to your practice.

Submission of data fields marked with asterisks* is required for subsidy claims and Healthier SG payments. 

Lipid Profile

  • LDL-C (mmol/L or mg/dL) *

  • HDL-C (mmol/L or mg/dL)

  • Triglycerides (mmol/L or mg/dL)

  • Total Cholesterol (mmol/L or mg/dL)

  • Date*

Blood Pressure 

  • Systolic BP (mmHg)

  • Diastolic BP (mmHg)

  • Date

Blood Glucose

  • HbA1c (%) OR Fasting Plasma Glucose (FPG) (mmol/L or mg/ dL)

  • Date

Weight

  • BMI (kg/m2), calculated from height*, weight*

  • Waist Circumference (in cm; optional field to fill)

  • Date*

Smoking History

  • Smoking Status (Never smoker, Ex-smoker, Current Smoker) *

  • Year started smoking (if smoker)

  • No. of sticks smoked/day (if smoker) *

  • State of change: (i) Pre-contemplation, (ii) Contemplation, (iii) Preparation (iv) Action, OR (v) Maintenance. 

CHAS/PG/MG cardholders who are Healthier SG enrollees would be eligible for the Healthier SG Chronic Tier, which provides percentage-based subsidies for a whitelist of drug products (see XX for the full list) at capped selling prices. For subsidy claim, GPs should document the quantities and selling prices for each whitelisted drug product prescribed.

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