Management of Hyperlipidemia

Question 1

Chylomicrons transport fats from where to where?

In the liver, chylomicrons release what? 2
What do they become then?

LDL then carries fat and cholesterol to where?

High-density lipoproteins (HDL) carry fat and cholesterol back where?

When oxidized what increases?
And what forms and what does this cause?

HDL cholesterol is able to go and remove cholesterol from where?

Answer 1

the intestinal mucosa to the liver

1. triglycerides, some
2. cholesterol and they become low-density liproproteins (LDL)

The body’s cell

back to the liver for excretion

LDL cholesterol increases, and
atheroma formation occurs in the walls of the arteries, which causes atherosclerosis

from the atheroma

Question 2

Primary (Hereditary)
Causes of Dsylipidemia
3

Answer 2

1. Familial Hypercholesterolemia
2. Familial Combined Hyperlipidemia
3. Dysbetalipoproteinemia

Question 3

What is Familial Hypercholesterolemia?

What are they at high risk for?
4

Answer 3

Mutation in LDL receptor, they are absent or defective, resulting in unregulated synthesis of LDL

High risk for

1. atherosclerosis,
2. tendon xanthomas (75% of patients),
3. tuberous xanthomas and
4. xanthelasmas of eyes.

Question 4

What is Familial Combined Hyperlipidemia?

Answer 4

Autosomal dominant

Increased secretions of VLDLs

Question 5

What is Dysbetalipoproteinemia?

What does the defective substance usually play a role in?

Increased risk for what?
4

Answer 5

Results in apo E2, a binding-defective form of apoE

Usually plays important role in catabolism of chylomicron and VLDL

Increased risk for

1. atherosclerosis,
2. peripheral vascular disease
3. Tuberous xanthomas,
4. striae palmaris

Question 6

What are Xanthomas?

Especially likely to be found on skin of patients with what?

Answer 6

Soft, yellow skin plaques or nodules that contain deposits of lipoproteins inside histiocytes

Hyperlipidemia

Question 7

Secondary Causes
of hyperlipidemia?
10

Answer 7

1. Most common cause in developed countries: sedentary lifestyle with excessive dietary intake of saturated fat, cholesterol, and trans fats
2. Uncontrolled Type 2 DM /
3. Metabolic Syndrome
4. Hypothyroidism
5. Liver Disease
6. Renal Disease
7. Corticosteroid Use
8. Progestin Use
9. Anabolic Steroid Use
10. ETOH use / abuse

Question 8

Metabolic Syndrome
Must meet 3 of the following criteria: 4

Two things that has to be under control to start streating cholesterol?

Answer 8

1. Abdominal obesity (> 40 in men, > 35 in women)
2. High triglyceride level (> 150)
3. Low HDL (130/85 mmHg)
4. Impaired Fasting Glucose level > 100

smoking and diabetes under control

Question 9

Monounsaturated Effect on Cholesterol levels?

Polyunsaturated Effect on Cholesterol levels?

Saturated effect on cholesterol levels?

Trans fat effect on cholesterol levels?

Answer 9

Lowers LDL, Raises HDL

Lowers LDL, Raises HDL

Raises both

Raises LDL

Question 10

Five major steps which serve as basis for treatment recommendations for hyperlipidemia:

Answer 10

1) Obtain fasting lipid profile
2) Identify if there are any CHD risk equivalents
3) Identify if there are major CHD risk factors other than LDL
4) If patient has a CHD risk equivalent, or has 2 or more risk factors (other than LDL), calculate 10 year risk of CHD
5) Determine the risk category, in order to establish the LDL goal, when to initiate therapeutic lifestyle changes, and when to consider drug therapy

1. fasting lipid profile
2. CHD risk equivalents
3. major CHD risk factors other than LDL
4. Calculate 10 year risk for CHD
5. risk category

Question 11

What is the primary and secondary prevention of CVD?

What are our risk equivalent disease? 2

Answer 11

Optimum treatment of lipids

Diabetes and any vascular disease

Question 12

ATP III is based on epidemiologic observations that showed graded relationship between what two things?

Answer 12

the total cholesterol concentration and coronary risk

Question 13

Step 1: Check Lipid Panel
ATP III Guidelines
Healthy adults with no risk factors?

Answer 13

Healthy adults, no risk factors – every 5 yrs starting at age 20

Obtain a fasting (9 to 12 hour) serum lipid profile consisting of total cholesterol, LDL, HDL and triglycerides

Question 14

How do we calculate LDL?

Answer 14

LDL = TC – (HDL + TGs / 5)

Question 15

If on a statin medication, recheck FLP how often and how would we adjust the statin?

Answer 15

every 6 wks and uptitrate statin to achieve LDL goal, then q 6 months once at goal

Question 16

Lipid Panel Goals
Total Cholesterol?
LDL (low density lipoprotein)?
HDL (high density lipoprotein)?
		in men
		in women
		is considered cardio protective
Triglycerides?

Answer 16

TC- less than 200
LDL- less than 100
HDL
men- less than 40
women- less than 50
cardio protective is less than 60

TG- less than 150 is normal

Question 17

Identify CHD Risk Equivalents:

5

Answer 17

1. Diabetes
Other forms of clinical atherosclerotic disease
2. Clinical CHD
3. Abdominal Aortic Aneurysm
4. Peripheral arterial disease
5. Symptomatic carotid artery disease

Question 18

Diabetes is a Risk Equivalent
Men with DM and risk factors?
Without?

Women with DM and risk factors?
Without?

Men or women of any age who have had DM (type I or II) for over how many years with risk factor?
Without?

Answer 18

Men over age 40 with type II DM and any other risk factor, or over age 50 with or without other CHD risk factors

Women over age 45 with type II DM and any other CHD risk factor, or over age 55 with or without other CHD risk factors

Men or women of any age who have had DM (type I or II) for over 20 years if they have another risk factor or more than 25 years without another risk factor

Question 19

Determine Major Risk Factors (other than LDL)?

3

Answer 19

1. Cigarette smoking
2. HTN (BP > 140/90 mmHg or on antiHTN meds)
3. Low HDL cholesterol (45 yrs; women >55 yrs)

Question 20

Assessment of Risk
For persons without known CHD, other forms of atherosclerotic disease, or diabetes:
2

Answer 20

1. Count the number of risk factors.

2. Use Framingham scoring for persons with ≥2 risk factors* to determine the absolute 10-year CHD risk.

Question 21

Coronary heart disease (CHD) or CHD risk equivalent (10-year risk >20 percent):

LDL goal?

LDL level at which to initiate therapeutic lifestyle changes?

LDL level at which to consider drug therapy

Answer 21

LDL- less than100 mg/dL

Initiate therapy- greater than than 100 mg/dL

Drug therapy greater than 130 mg/dL; drug optional at 100 to 129 mg/dL

Question 22

Determining risk factor:
2 or more risk factors
(10-year risk less than 20%)

LDL goal?

LDL level at which to initiate therapeutic lifestyle changes?

LDL level at which to consider drug therapy

Answer 22

LDL- less than130 mg/dL

Initiate therapy- greater than than 130 mg/dL

Drug therapy: 10-year risk 10 to 20 percent: >130 mg/dL 10-year risk less than 10 percent: >160 mg/dL

Question 23

Determining risk factor:
0 to 1 risk factor
(10 year risk less than 10%)

LDL goal?

LDL level at which to initiate therapeutic lifestyle changes?

LDL level at which to consider drug therapy

Answer 23

LDL- less than 160 mg/dL

Initiate therapy- greater than than 160 mg/dL
Drug therapy: >190 mg/dL;

LDL-lowering drug optional at 160 to 189 mg/dL

Question 24

Data subsequent to ATP-III
Secondary Prevention Recommendations?
4

Answer 24

1. Intensive statin therapy in patients with acute coronary syndrome recommended as initial therapy
2. Patients at very high risk (very high risk patients are defined on the next slide) for CHD events should be targeted for LDL below 70 (if unable to achieve with statin alone, second agent should be added)
3. Usual risk patient with stable CHD unable to achieve LDL goal with statin alone should have second agent added
4. If they do not tolerate a statin, they should be treated with another lipid-lowering agent

Question 25

Who is at Very High Risk
for CHD Events?
4

Answer 25

Established coronary heart disease
PLUS
Multiple major risk factors (especially diabetes)

OR

Severe and poorly controlled risk factors (continued smoking)

OR

Multiple risk factors of metabolic syndrome (esp TGs> 200 plus non-HDL-C > 130 plus HDL

Question 26

Remember….very high risk patients!

What should we do?

Answer 26

More intensive lipid lowering therapy
LDL below 70 mg/dL
!!!!!!!!!!

Question 27

After Categorizing Patient
What should we do? 2

What is treating pts with hyerlipidemia based on? 2

Answer 27

1. Initiate Therapeutic Lifestyle Changes (TLC) alone
   OR
2. TLC and drug therapy
   —The decision to treat hyperlipidemia with drug therapy is based on LDL levels

Question 28

What are statins?

Answer 28

HMG-CoA Reductase Inhibitors

Question 29

Statins are excellent agents at lowering what?
4

What does it increase?

Answer 29

lowering

1. LDL
2. cholesterol and decreasing associated
3. TGs
4. morbidity and mortality rates for primary and secondary prevention of CAD

HDL

Question 30

What should our HDL to LDL ratio be?

Answer 30

1 to 4

Question 31

The Statins

7

Answer 31

1. Rosuvastatin (Crestor)
2. Atorvastatin (Lipitor)
3. Simvastatin (Zocor)
4. Lovastatin (Mevacor)
5. Pravastatin (Pravachol)
6. Fluvastatin (Lescol)
7. Simvastatin/Ezetimibe Combo (Vytorin)

Question 32

1. MOA of Statin Medications
2. What does it lead to an increase in?
3. What is more greatly taken up by the liver?
4. How does this affect LDL in the blood stream?
5. Is HDL affected?
6. Low density lipoprotein receptors are also involved with the uptake of what?
   What does this lead to an decrease in?

Answer 32

1. Blocks the conversion of HMG-CoA to mevalonate, which is the rate limiting step in the production of cholesterol in the liver ( the first statin is called Mevacor)
2. Leads to an increase in the number of LDL receptors in the liver
3. Larger amounts of LDL cholesterol is taken up by the liver and digested, thereby
4. decreasing the amount of LDL in the bloodstream
5. It usually tends to increase
6. VLDL and IDL
   This leads to a decrease in triglyceride levels

Question 33

What are main
side effects of Statins?
7

Answer 33

1. Hepatotoxicity
2. Myalgias
3. Myopathy
4. Myositis
5. GI Upset
6. Headache
7. Asymptomatic elevation in LFTs
   - They should be checked at baseline, at 6-12 weeks after starting or titrating, and every 6 months after

Question 34

Statin Contraindications?

4

Answer 34

1. Pregnant women
2. Patient with active / chronic liver disease
3. Patient with unexplained elevated aminotransferase levels (ALT’s)
4. CAUTION in patient who consume large amounts of alcohol or a history of liver disease

Question 35

Statins and Myopathy

1. Check ____ if patient complains of myalgias
2. Definition of myalgias?
3. Definition of myopathy?

Answer 35

CPK
pain
more breakdown

Question 36

If myopathy occurs with statins what should we do?

Answer 36

Change statin and rechallenge

Question 37

When rhabdomyolysis occurs what should we do?

2

Answer 37

1. stop statin use,

2. begin IV fluid hydration to prevent renal failure – usually CKs > 15,000 to cause ARF

Question 38

Meds that increase statin myopathy:

7

Answer 38

• gemfibrozil
• clarithryomycin
• verapamil
• erythromycin
• amiodarone
• ketoconazole
• protease inhibitors

Question 39

1. Statins and Liver Issues
   Generally well tolerated but some experience elevation in what?
2. What is it dependant on?
3. How can it be reversed?
4. How can we fix this?
5. When should we stop statin?

Answer 39

1. • liver transaminases (0.5 – 2.0% of pts)
2. • Are dose dependent
3. • Usually reversed with lower doses
4. • Can change statin and rechallenge
5. • Stop statin if LTFs > 3 times baseline

Question 40

Statins and Liver Issues teach pts to report what?
4

When should we monitor LFTs?
4

Answer 40

1. jaundice,
2. malaise,
3. fatigue,
4. lethargy

Monitor LFTs

1. prior to statin initiation,
2. at 3 months,
3. 6 months,
4. then every year

Question 41

Statins and Renal Issues:

What are they most specific to?

What are we testing? 2

Answer 41

Most specific to Rosuvastatin (Crestor)

- Cr at baseline	
- Renal function monitored at dose of 40 mg

Question 42

Take statins in evening or bedtime

- Exception?

Answer 42

Atorvastatin

Question 43

What’s the difference in the statins:

1. All statins have what?
2. Which are more effective at lowering TG? 2
3. Which is more effective in raising HDL? 1

Answer 43

1. • -All statins have an anti-inflammatory effect
   • -All are more potent by 10-15% with evening dosing

Despite same MOA, there are differences between the agents, including their ability to lower cholesterol

2. Per UpToDate, Atorvastatin and Rosuvastatin have more effective ability to lower TGs
3. Per UpToDate, Rosuvastatin is more effective in raising HDL-C than atorvastatin, simvastatin, or pravastatin

Question 44

Atorvastatin (Lipitor)

has good effects on what?

Answer 44

Lowers LDL 47-65%
Raises HDL 2-9%
Lowers triglycerides 20%

TG

Question 45

Rosuvastatin (Crestor)
has good effects on what?
2

Answer 45

Lowers LDL 39-60%
Raises HDL 5-9%
Lowers triglycerides 19-35%

TG
HDL

Question 46

Lovastatin (Mevacor)

compared to the others?

Answer 46

Lowers LDL 24-28%
Raises HDL 7%
Lowers triglycerides 10-14%

Not as good

Question 47

Pravastatin (Pravachol)

Compared to other?

Answer 47

Lowers LDL 22-34%
Raises HDL 2-12%
Lower triglycerides 11-24%

Not as good

Question 48

Simvastatin (Zocor)

compared to others?

Answer 48

Lowers LDL 30-40%
Raises HDL 5-7%
Lowers Triglicerides 10-30%

Still commonly used

Question 49

Elevated transaminases on statins (unless reaching 3x normal) are a reason or not a reason to stop a statin?

Statin side effects are often agent or class specific?

Unexplained myalgias may occur on statins without CK elevation. What should we do?

Answer 49

not

Agent

Try a different statin

Question 50

Rhabdomyolysis is uncommon unless what?

Answer 50

CK is elevated to 10 x normal. Usually occurs in patients with multiple co-morbidities.

Question 51

Bile Acid Resins MOA?
(what pathway and what do they bind to?)

What does this do to cholesterol return?

Are they absorbed in the Gi tract?

Answer 51

1. Decrease cholesterol absorption through exogenous pathway
2. These agents bind bile acids in the intestines, forming an insoluble complex that is excreted in the feces

This decreases the return of cholesterol to the liver.

NO

Question 52

How does your body respond to BAR?

What does this process interrupt?
this can cause an increase in what?

Answer 52

Body responds by increasing LDL receptors on the liver, which in turn decreases the amount of LDL cholesterol level in the bloodstream

This process interrupts enterohepatic recirculation of bile acids and affects enzyme systems – which can cause an increase in TGs

Question 53

Bile Acid Resins:

What kind of therapy is it commonly used for?
Pregnancy cat?

Max effects seen when?

Effects are related to what?

Taken with or without food?

Answer 53

Adjunct therapy

Safe in pregnancy and pediatrics

Maximum effects are seen in approx 3 weeks

Effects are dose related

Should be taken with meals
Meds should be taken at least 1 hr before or 4 hours after the bile acid resin

Question 54

Bile Acid Resin – Side Effects 4

Which one is less likely to cause GI effects?

Answer 54

Use is often limited by side effects
1. Nausea, 
2. bloating, 
3. cramping
4. Increase in liver enzymes
Colesevalam is better – less likely to cause GI effects

Question 55

Bile Acid Resins
2

Which one has better numbers?

Answer 55

1. Cholestyramine (Questran)
   Lowers LDL 15-30%
   Raises HDL 3-5%
   Lowers triglycerides 0-15%
2. Colestipol (Colstid)
   Lowers LDL 12-25%
   Raises HDL 0-1%
   Triglycerides 0-24%

Question 56

What is Niacin?

Can improve cholesterol levels when used at doses how many times the recommended daily dose?

What kind of effects on LDL?
HDL?
TG?

Answer 56

Naturally occurring B vitamin (B3)
(BEST DRUG TO INCREASE HDL)

100-300 times

Lowers LDL 15-25%
Raises HDL 35%
Lowers triglycerides 50%

Question 57

MOA for Niacin?

Answer 57

Uncertain

Appears to decrease VLDL synthesis in liver and increase lipoprotein lipase activity

Question 58

Absolute Contraindications for Niacin?

2

Answer 58

• Hepatic dysfunction

- Severe gout

Question 59

Relative Contraindications for niacin?

3

Answer 59

• Peptic ulcer disease
• Gout - can elevate uric acid levels
• Diabetes - can worsen glucose control

Question 60

Niacin side effects? 7

What might help certain side effects? 2

Answer 60

1. Increased prostaglandin activity leading to pruritis and flushing to the face and neck
   A dose of ASA taken 30 - 60 minutes before the Niacin may help
   Niaspan, an extended release, may help
2. Hepatotoxicity – monitor LFTs
3. Uric acid and
4. glucose increases – get baseline labs
5. Orthostatic hypotension
6. Dyspepsia,
7. GI side effects

Question 61

Cholesterol Absorption Inhibitors
1

MOA:

1. Where does it act?
2. What does it inhibit and what does this lead to?
3. What does it cause a reduction of and an increase of?
4. This mechanism is complementary to that of the what?

Answer 61

Ezetimibe (Zetia)

1. Appears to act at the brush border of the small intestine
2. Inhibits the absorption of cholesterol leading to a decrease in the delivery of intestinal cholesterol to the liver
3. Causes a reduction of hepatic cholesterol store and an increase in clearance of cholesterol from the blood
4. This mechanism is complementary to that of the STATINS

Question 62

Cholesterol Absorption Inhibitors
affects on LDL used on mono therapy?
In combination with statin?

Contraindications?2

Side effects? 3

Answer 62

Lowers LDL up to 18% (monotherapy)
Lowers LDL up to 35% with a statin

Contraindications
If used with a statin
1. Active hepatic disease
2. Elevated ALT’s

Side effects
Headache
Diarrhea
Abdominal pain

Question 63

Fibric Acid Derivatives
2 drugs?

Not considered a major class of lipid-lowering drugs because of what?

What is it good for?

What should be monitored?

Answer 63

Gemfibrozil (Lopid)- can cause rhabo!- dont use it
Fenofibrate (Tricor, Trilipix)

they have minimal effect on LDL.

Good for lowering triglycerides

LFT’s need to be monitored

Question 64

Fibric Acids / Fibrates MOA?

Affect on TGs?
Affect on HDL?
Affect on LDL?

Answer 64

Unclear
Principal effect of triglyceride lowering appears to result from the stimulation of lipoprotein lipase, which enhances the breakdown of VLDL to LDL
May inhibit hepatic VLDL production and triglyceride synthesis

Lower triglycerides up to 60%
Raise HDL up to 30%
Lowers LDL up to 20% (Tricor most effective at LDL reduction)

Question 65

Fibric Acid Derivatives
Contraindications?3
Adverse affects?6

Answer 65

Contraindications

1. History of gallstones
2. Severe hepatic or
3. renal dysfunction

Adverse effects
1. GI related
2. Myopathy chance increased if taken with statins
3. Jaundice
4. Increases the effects of 
Warfarin
5. Gallstones
6. Hepatotoxicity

Question 66

Hypertriglyceridemia
Borderline levels and treatment?
HIgh levels and treatment?

Answer 66

Borderline (150-199 mg/dL): calorie restriction and exercise

High (>200 mg/dL): diet and medications

Question 67

Hypertriglyceridema Therapy
Diet? 4
Limit what? 4
Supplement? 1
Pharm? 4

Answer 67

1. Low fat diet /
2. calorie restriction /
3. increase fiber
4. Exercise

Limit

1. alcohol,
2. simple sugars,
3. refined starches,
4. saturated and trans fatty acids

Omega 3 fatty acid (Lovaza) – fish oil:
2 – 4g/day recommended; higher dose can increase LDL

Pharm therapy with

1. niacin,
2. fibric acid derivative,
3. lovaza, or
4. statins

Question 68

Fish Oil Supplementation (Omega-3):

Limited by what?

FDA approval is limited to what?
why?

Answer 68

Use is often limited by metabolic and gastrointestinal side effects

The commercial preparation Lovaza, which has been available for many years in Europe and is now also available in the United States, is 90 percent omega-3 fatty acids.

US FDA limited approval for Lovaza to the treatment of severe hypertriglyceridemia (>500) because of concerns that it appears to increase LDL levels

Question 69

a

Answer 69

a

Question 70

Possible Benefits From Other Therapies. What are they?

4

Answer 70

1. Soluble fiber in diet (2–8 g/d) (oat bran, fruit, and vegetables)
2. Soy protein (20–30 g/d)
3. Stanol esters (1.5–4 g/d) (inhibit cholesterol absorption)
4. Fish oils (3–9 g/d)
   (n-3 fatty acids)

Question 71

Diabetes:
Remember, DM is considered what?

CARE trial and Heart Protection Study found significant improvement in outcomes with what?

Answer 71

Remember, DM is considered a CHD equivalent

CARE trial and Heart Protection Study found significant improvement in outcomes with statin therapy even at LDL-cholesterol values below 116 (Goal for LDL is less than 70)

Question 72

ACC/AHA: 4 Statin Benefit Groups Identified

Answer 72

1. Patients with clinical atherosclerotic disease
2. Patients with LDL > 190 (typically pt with FH)
3. Patients with diabetes 40-75 yo with LDL levels of 70 – 189 and without evidence of ASCVD
4. Patients without evidence of ASCVD or DM but who have LDL levels of 70 – 189 and a 10-year risk of ASCVD > 7.5%

Question 73

Statins reduce risk of what by 20%? 2

HOw should we think of statins as providers?
2

Answer 73

CV disease and stroke by about 20%, regardles of baseline lipid profile

1. Think of statins as risk-reduction meds the same way we consider aspirin
2. No longer treating to a target LDL level; we are treating to lower risk

Question 74

Why should we choose the lowest dosage that will get you the biggest LDL reduction?

Answer 74

Since statin harm is dose related

Question 75

In hyperlipidemia what should be the order of importance in treatment? 3

Answer 75

get LDLs down
Get HDLs up
Get TGs down