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Cardiovascular Diseases

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Title: Cardiovascular Diseases


1
Cardiovascular Diseases
  • Andrew Reisman, MD, ATC
  • PHYT-801
  • November 3, 2009

2
Objectives
  • Review pathophysiology
  • Discuss risk factors
  • Investigate hypertension
  • Exercise response
  • Exercise as treatment
  • Discuss cholesterol
  • Affects and treatment

3
Arteriosclerosis
  • Thickening and hardening of the arteries
  • Responsible for the majority of deaths in the
    United States
  • Atherosclerosis
  • Disorder of the larger arteries
  • Coronary artery disease (CAD)
  • Aortic aneurysm
  • Peripheral Vascular Occlusive Disease (PVOD)
  • Cerebrovascular Disease (CVD)

4
Mechanism of Injury
  • Fatty streaks develop along the intima (innermost
    layer of an artery)
  • A proliferation of smooth muscle cells ensues
    leading to a fibrous plaque
  • This plaque begins to decrease blood flow
    downstream

5
Mechanism of Injury
  • The plaque may then rupture
  • Sending a shower of plaque to the smaller vessels
    down stream leading to localized ischemia
  • Leading to a local reaction of platelet
    aggregation and clot formation causing regional
    ischemia

6
Categories of Risk Factors
  • Category I
  • Risk factors for which interventions have been
    proved to reduce the incidence of coronary artery
    disease (CAD) events
  • Category II
  • Risk factors for which interventions are likely,
    based on our current pathophysiological
    understanding and on epidemiologic and clinical
    trial evidence, to reduce the incidence of CAD
    events

7
Categories of Risk Factors
  • Category III
  • Risk factors clearly associated with an increase
    in CAD risk, and which, if modified, might lower
    the incidence of CAD events
  • Category IV
  • Risk factors associated with increased risk but
    which cannot be modified or whose modification
    would be unlikely to change the incidence of
    coronary disease events

8
Category I - Cigarette Smoking
  • A linear relationship exists between
    cardiovascular risk and of cigarettes consumed
  • Relative risk of a fatal cardiovascular event is
    5.5 times that of a non-smoker
  • Smoking accelerates the atherogenic process in
    both a duration- and dose-dependent fashion

9
Category I - Cigarette Smoking
  • An average smoker has a life expectancy 3 years
    less than a non-smoker
  • A smoker known to be at high risk for CAD has a
    life expectancy 10-15 years less than a
    comparable non-smoker
  • Smoking amplifies the effects of other risk
    factors
  • Thrombus formation, plaque instability and
    arrhythmias are all influenced by cigarette
    smoking

10
Category I - Cigarette Smoking
  • Clinical data accumulated over the last 20 years
    strongly suggests that smoking cessation reduces
    the risk of cardiovascular events
  • Risk of MI declines more rapidly than overall
    death from CV disease after smoking cessation
  • Greatest proportion of risk reduction occurs in
    the first several months after cessation

11
Category I - Cigarette Smoking
  • Patients who continue to smoke after acute MI
    have an increase in the risk of death and
    reinfarction (22 vs 47)
  • Continued smoking after bypass grafting is
    associated with a twofold increase in the
    relative risk of death and an increase in
    nonfatal MI and angina

12
Category I - Cigarette Smoking
  • Second hand smoke
  • Estimated that passive smoking causes almost
    40,000 heart disease deaths yearly in the US
  • Third leading cause of preventable death in this
    country

13
Category I - Low Density Lipoprotein (LDL)
Cholesterol
  • Total blood cholesterol is conclusively linked to
    the development of CAD
  • The majority of this risk is associated with LDL
    cholesterol concentration
  • For every increase of LDL by 1, the risk for CAD
    increases by 2-3

14
Category I - Low Density Lipoprotein (LDL)
Cholesterol
  • National Cholesterol Education Program (NCEP III)
    guidelines
  • Updated 2003
  • LDL gt 190 mg/dl very high risk
  • LDL 160 - 189 high risk
  • LDL 130-159 Borderline High
  • LDL 100-129 Above Optimal for CHD risk equivalent
  • LDL lt 100 optimal
  • Some studies have suggested that LDL levels as
    low as lt80 are recommended for those with a
    history of CAD

15
(No Transcript)
16
Category I - Low Density Lipoprotein (LDL)
Cholesterol
  • Increases in LDL associated with
  • Age
  • Weight gain
  • Diets high in saturated fat and cholesterol ?
  • Genetic factors
  • Chronic hypothyroidism
  • Estrogen deficiency

17
Category I - Low Density Lipoprotein (LDL)
Cholesterol
  • Recent studies indicate that therapeutic lowering
    of LDL is highly effective in secondary
    prevention
  • Angiographic studies showed delay in progression
    or coronary atherosclerosis and in some cases
    regression of the lesions

18
Category I - Low Density Lipoprotein (LDL)
Cholesterol
  • Scandinavian Simvastatin Survival Study (4S)
  • Simvastatin (Zocor) reduced coronary mortality
    by 42
  • Reduced total mortality by 30

19
Category I - Low Density Lipoprotein (LDL)
Cholesterol
  • West of Scotland Coronary Prevention Study
    (WOSCOPS)
  • Demonstrated primary prevention benefits of LDL
    cholesterol reduction
  • LDL reduction by 1 mg/dl resulted in a 1-2
    decrease in relative risk for coronary artery
    disease

20
Category I - Hypertension
  • A continuous relationship between systolic and
    diastolic arterial pressure and cardiovascular
    risk exists
  • Mechanism
  • Direct vascular injury caused by increases in
    blood pressure
  • Effects on the myocardium, including increased
    wall stress and myocardial oxygen demand

21
Category I - Hypertension
  • Related to left ventricular hypertrophy (LVH)
  • an independent risk factor for CAD including MI,
    CHF, and sudden death
  • Framingham Heart Study showed that a regression
    of LVH associated with a substantial risk
    reduction for a cardiovascular event

22
Category I - Thrombogenic Factors
  • A number of prothrombogenic factors have been
    identified
  • Remember NSAIDs can inhibit platelet function
  • Aspirin has been documented to reduce both
    primary and secondary coronary heart disease
    events
  • The first medication given to someone having
    angina or an acute MI is ASA

23
Category II - Diabetes Mellitus
  • Both Insulin dependent and Type II DM are
    strongly linked with CAD
  • Atherosclerosis accounts for 80 of all diabetic
    mortality
  • Coronary mortality is increased 3-10X in
    diabetics compared to non-diabetic controls
  • 25 of all heart attacks in the US occur in
    patients with diabetes

24
Category II - Diabetes Mellitus
  • Diabetes linked to many other conditions so
    difficult to study the effect of diabetes as a
    lone factor
  • Coronary Artery Surgery Study (CASS)
  • Diabetics had a 57 increase in risk of death
    after controlling for other known factors
  • Higher risk of death and other complications noted

25
Category II - Physical Inactivity
  • Approximately 12 of all mortality in the US may
    be related to lack or regular physical activity
  • Associated with a twofold increase in risk for
    CAD events
  • Overall reduction in CAD events persists despite
    a small transient increase in the risk of MI or
    sudden death that occurs during physical activity

26
Category II - Physical Inactivity
  • Difficult to quantify the relationship between
    amount of exercise and CAD risk given multiple
    factors affected by exercise
  • Direct and indirect mechanism of actions
  • Improves myocardial supply/demand relationship
  • Lowers triglycerides and raises HDL cholesterol
    levels
  • Lowers blood pressure
  • Decreases platelet aggregation

27
Category II - High Density Lipoprotein (HDL)
Cholesterol
  • Strong inverse relationship between HDL levels
    and CAD risk
  • For every 1 mg/dl decrease in HDL there is a 2-3
    increase in relative risk for CAD events
  • High HDL levels associated with longevity
  • HDL goal gt 60mg/dl
  • Given inter-relationships, it has been difficult
    to establish HDL as an independent variable

28
Category II - Postmenopausal Status
  • CAD presents about a decade later in women
    compared with men
  • Cardiovascular disease is still the leading cause
    of death among US women
  • Observed that the protection conferred upon women
    appears to be lost after natural menopause
  • Coronary disease risk clearly increases after
    surgical menopause

29
Category II - Postmenopausal Status
  • Evidence of the beneficial effects of
    postmenopausal estrogen replacement were derived
    almost entirely from observational studies and
    recent prospective studies have showed an
    increased risk actually exists
  • Results of Womens Health Initiative were stopped
    early as increased cardiac risk was actually noted

30
Category II - Postmenopausal Status
  • Exogenous estrogen favorably effects both HDL and
    LDL cholesterol levels
  • Self selective population of women who choose
    HRT?

31
Category II - Obesity
  • Linear relationship between body mass and
    mortality
  • 20 of Americans between the ages of 25-34 are
    classified as obese
  • Approximate 10 of the population becomes obese
    with each succeeding decade to the age of 55

32
Category II - Obesity
  • Associated with multiple other risk factors
  • Hypertension
  • Glucose Intolerance
  • Decreased HDL
  • Increased Triglycerides
  • Hard to sort out effects of obesity vs
    association with other risk factors

33
Category III - Psychosocial Factors
  • A variety of psychosocial factors are associated
    with increased coronary heart disease risk
  • Given the multiplicity and diversity of these
    risk factors, it is difficult to establish a
    direct relationship between them and
    cardiovascular diseases

34
Category III - Psychosocial Factors
  • Type A personality
  • Efforts to change behavior have not convincingly
    demonstrated that it changes CAD risk
  • Other traits felt related to CAD in observational
    studies
  • Depression
  • Hostility
  • Social Isolation
  • Economic insecurity

35
Category III - Psychosocial Factors
  • Mechanisms
  • Directly through neuroendocrine effects
  • Brain catecholamine and serotonin levels
  • Indirectly through patients adherence to
    preventive recommendations and compliance with
    therapeutic strategies

36
Category III - Psychosocial Factors
  • Major depression after acute MI increases 6-month
    mortality
  • Patients without a social support system have a
    threefold increase in 6-month mortality after
    acute MI
  • Chronic stress doubles the risk of developing MI

37
Category III - Triglycerides (TGs)
  • TG levels uniformly predict coronary heart
    disease in univariate analyses but often lose
    their predictive power when other risk factors
    are added in a multivariate analysis
  • HDL levels inversely related to TG levels so some
    feel these should be linked

38
Category III - Triglycerides (TGs)
  • Two important nonlipid associations of high TG
    levels
  • Abnormalities in various clotting factors
  • Syndrome X (Familial dyslipidemic hypertension)
  • High TG levels
  • Low HDL
  • Insulin resistance
  • Abdominal adiposity
  • Hypertension

39
Category III - Triglycerides (TGs)
  • Factors which decrease TG levels
  • Weight loss
  • Dietary changes
  • Decreased ETOH consumption
  • Smoking cessation
  • Increased physical activity
  • Difficult to determine if decreasing TG levels
    act independently from above factors

40
Category III - Triglycerides (TGs)
  • Triglyceride levels
  • lt200 Normal
  • 200-399 Borderline high
  • 400-1000 High
  • gt1000 Very high
  • Some recent advances in targeting TG levels with
    pharmacotherapy

41
Category III - Lipoprotein(a)
  • Elevated levels of Lipo(a) recently recognized as
    a potentially significant CAD risk factor
  • Acts as a potential inhibitor of fibrinolysis
    allowing for narrowing of vessel walls
  • Levels are largely determined through autosomal
    dominant inheritance
  • Among patients with premature CAD, 15-20 have
    elevated Lipo(a) levels

42
Category III - Lipoprotein(a)
  • Lipoprotein(a) levels increase with
  • Age
  • African-American heritage
  • Female sex
  • Levels may possibly be reduced be Niacin
  • No prospective interventional trial information
    is available

43
Category III - Homocysteine
  • Increased homocysteine levels are associated with
    increased risk of both CAD and peripheral
    arterial disease
  • Increased levels of homocysteine associated with
  • Deficiency of the catabolic enzyme cystathionine
    B-synthase
  • Vitamin B6 and Vitamin B12 (Folate) deficiency
  • Aging

44
Category III - Homocysteine
  • Homocysteine-induced vascular damage may occur as
    a consequence of the amino acids procoagulant
    activities or by direct injury of vascular
    endothelium
  • Appears to be unrelated to other CAD risk factors
  • The risk of premature occlusive vascular disease
    is 30X greater for those with elevated
    homocysteine levels
  • Clinical trials underway to further study
    homocysteine

45
Category III - Oxidative Stress
  • Oxidative modification of LDL cholesterol,
    particularly in the vessel wall, accelerates the
    atherogenic process
  • Oxidized LDL recruits monocyte macrophages,
    stimulating auto-antibodies, stimulating LDL
    uptake by macrophages and increasing
    intravascular tone and coagulability

46
Category III - Oxidative Stress
  • Antioxidants can increase LDL resistance to
    oxidation and are associated with lower CAD risk
  • Cambridge Heart Antioxidant Study (CHAOS)
  • Vitamin E therapy in patients with CAD reduced
    the rate of no-fatal MI
  • Vitamin E, Vitamin C and beta-carotene felt to be
    protective against CAD?
  • ? Wrong isomer in pill form Allhope study
  • Results inconsistent from various studies and
    more recent data shows increased CAD risk with
    use of antioxidants

47
Category III C- Reactive Protein
  • Marker of inflammation
  • It is felt that inflammatory changes cause
    rupture of plaque
  • Those with borderline cholesterol levels and
    increased CRP levels should be treated more
    aggressively

48
Category III - Alcoholic Beverage Consumption
  • Individuals reporting moderate amounts of alcohol
    intake (1-2 drinks daily) have a 40-50 reduction
    in CAD risk compared to individuals who are
    abstinent
  • Excessive consumption (gt2 drinks daily)
    associated with increased risk of CAD

49
Category III - Alcoholic Beverage Consumption
  • Increased risk may be associated with alcoholic
    cardiomyopathy
  • Alcohol also associated with
  • Hypertension
  • Cardiac arrhythmias
  • Alcohol (particularly red wine) associated with
    increased HDL levels
  • Only observational studies done to date

50
Category IV- Non-Modifiable Risks
  • Age
  • CAD increases nearly linearly with age
  • Male Sex
  • MaleFemale Risk equalizes at age 75
  • Incidence of CAD 3X greater in men below age of
    55
  • Family History/Genetic predisposition

51
Hypertension
52
  • The maintenance of health lies in forsaking the
    disinclination to exertion. Nothing is found
    that can substitute for exercise in any way,
    because in exercise the natural heat flames up
    and all the superfluities are engendered in the
    body, even though the food is of the very best
    quality and is moderate in quantity. And
    exercise will expel the harm done by most of the
    bad regimens that most men follow. Hippocrates
    420BC

53
Hypertension
  • Blood pressure is determined by two factors
    Cardiac Output (CO) and Total Peripheral
    resistance (TPR)
  • BP CO x TPR
  • CO HR X SV
  • Note - TPR sometimes referred to as SVR (Systemic
    Vascular Resistance)
  • Normal BP lt130/lt85

54
Hypertension
  • Hypertension is present in 17-20 of adults
  • Prevalence rises with age
  • More common in men then women
  • More common in African Americans than European
    Americans
  • Most cases of hypertension are idiopathic (i.e.
    We dont know why)

55
Hypertension
  • Potential identifiable causes of hypertension
  • Adrenal tumors (pheochromocytoma)
  • Excessive production of glucocorticoids
  • ETOH abuse
  • Vascular abnormalities
  • Pregnancy (Pre-eclampsia/Eclampsia)
  • CNS disturbances (CVA)
  • Renovascular diseases

56
Health Risks Associated with Hypertension
  • Coronary Artery Disease
  • Renal disease
  • Stroke
  • Peripheral Vascular Disease
  • Retinopathy
  • Death

57
JNC7 ClassificationTreatment Recommendations
Prehypertension SBP 120-139/ DBP 80-89 Stage 1
140-159/90-99 Stage 2 gt 160/gt100
Exercise and Hypertension Position Statement.
MSSE March 2004. 36(3) P. 534.
58
Stages of Hypertension
  • Prehypertension
  • TPR fails to compensate for changes in CO (should
    decrease)
  • Usually due to impaired baroreceptor function
  • Systolic BP 120-139
  • Diastolic BP 80-89

59
Stages of Hypertension
  • Stage I (mild)
  • Most common form
  • Increased CO and decreased TPR
  • Systolic BP 140-159
  • Diastolic BP 90-99

60
Stages of Hypertension
  • Stage II (Moderate)
  • Decreased CO and increased TPR
  • Increased afterload leads to LVH
  • Systolic BP 160-179
  • Diastolic BP 100-109

61
Stages of Hypertension
  • Stage III (Severe)
  • Development of diastolic dysfunction
  • Systolic BP 180-209
  • Diastolic BP 110-119

62
Stages of Hypertension
  • Stage IV (very severe)
  • CO can no longer respond to exercise or other
    demands
  • Marked LVH exists
  • CHF and peripheral edema common
  • Systolic BP gt210
  • Diastolic BP gt120

63
Acute Effects of Dynamic Exercise
  • Initial response is a linear increase in SBP
    secondary to an increase in cardiac output
  • TPR decreases as blood vessels in exercising
    muscles dilate
  • SBP increases less than expected due to decrease
    TPR
  • DBP stays constant or may even decrease

64
Chronic Effects of Dynamic Exercise
  • Reduction of SBP by 7-12 mmHG
  • Reduction of DBP by 5-10 mmHG
  • Increase in LV diameter
  • Thickening of ventricular walls
  • Higher VO2 Max

65
Acute Effects of Isometric Exercise
  • Dramatic Increase in Systolic and Diastolic Blood
    Pressure
  • Increased CO due to Increase HR
  • Increased TPR due to compression of blood vessels
    in exercising muscle
  • Increase of SBP to 200-300 mmHG have been observed

66
Chronic Effects of Isometric Exercises
  • Concentric LVH
  • Decreased CO
  • Diastolic Function remains preserved
  • No long term effect on BP

67
Searching for an answer
  • Lifestyle interventions
  • Exercise
  • Weight Reduction
  • Sodium restriction
  • Alcohol restriction
  • Relaxation Techniques

68
The Devils in the Details
  • For people with labile or mild hypertension,
    review whether they are using any natural or
    herbal supplements
  • Ephedrine is a frequent ingredient in power or
    anti-allergy supplements and this may increase
    BP
  • Check for use of anabolic steroids, particularly
    in an adolescent population

69
In Support of Exercise
  • Multiple studies have confirmed that exercise
    decreases SBP and DBP as an independent variable
  • Unfortunately, this change lasts only as long as
    the subject continues to exercise with return to
    baseline over the course of 3-6 months of
    inactivity.

70
Mechanism of Effect
  • Decreased sympathetic tone
  • direct measurement of efferent postganglionic
    muscle sympathetic nerve activity before and
    after a 10 week endurance training activity
    showed a reduction in sympathetic nerve activity.
  • Reduction in Renin-Angiotensin Activity
  • Baroreceptor Sensitivity
  • Changes in myogenic structure

71
Which Exercises are Effective
  • Endurance exercise activities have proven to be
    most effective in reducing hypertension
  • Three sessions per week
  • Little further decrease in BP with workout
    frequency of 5-7 day per week
  • Duration from 30 - 90 minutes
  • 50-60 minutes most effective

72
Which Exercises are Effective
  • 40 - 60 of VO2 Max shown to be most effective
  • Actually had a better response than those who
    exercised at gt60 of VO2 Max
  • Involvement of large muscle groups through
    activities such as walking, jogging, cycling, and
    swimming

73
Which Exercises are Effective
  • Circuit training is also felt to be effective in
    lowering BP
  • Work loads should be between 40-50 of RM
  • 1 to 2 sets of each exercise with 1 minute rest
    between sets
  • 8-10 repetitions per set
  • Avoid holding breath (valsalva) during weight
    training
  • Some feel that data is inconclusive at this time

74
Review of stages of Hypertension
  • High Normal BP
  • Systolic BP 130-139
  • Diastolic BP 85-89
  • Mild (Stage I)
  • Systolic BP 140-159
  • Diastolic BP 90-99
  • Moderate (stage II)
  • Systolic BP 160-179
  • Diastolic BP 100-109
  • Severe (stage III)
  • Systolic BP 180-209
  • Diastolic BP 110-119
  • Very Severe (stage IV)
  • Systolic gt210
  • Diastolic gt120

75
Exercise Prescriptions
  • For People with Pre-Hypertension and Stage I
    Hypertension
  • Dynamic exercises safe and effective as a first
    line attempt at controlling blood pressure
  • Work at 40-60 of VO2 Max for 50-60 minutes three
    times a week
  • May need to start at a shorter time and increase
    to 50-60 minutes over a few weeks

76
Exercise Prescriptions
  • Combine with other lifestyle modifications
  • Monitor blood pressure response over the next 2
    months and institute other therapy options as
    warranted
  • Avoid isometric activities

77
Exercise Prescriptions
  • For people with Stage II hypertension
  • Exercise can be used as an adjunct to
    pharmacological therapy
  • Make sure blood pressure is controlled prior to
    instituting an exercise regimen

78
Exercise Prescriptions
  • Once an exercise program has been instituted,
    monitor response regularly as the dose of
    antihypertensive medications may be able to be
    decreased
  • Again, avoid isometric exercises but dynamic
    exercises have been proven to be safe

79
Pharmacotherapy
  • There are many classes of medications which are
    used on a regular basis to treat hypertension and
    other cardiovascular conditions
  • All of these medications can have an effect on
    the exercise response

80
Pharmacotherapy
  • Diuretics
  • Medications which act directly upon the kidney to
    lead to an increased volume loss (diureses)
  • Diuretic therapy allows a near normal cardiac
    response to exercise
  • Acutely, there is a decreased plasma volume --gt
    decreased SV --gt decreased CO and therefore
    decrease BP without any effect on TPR
  • Short term use decreases maximal exercise
    performance and endurance

81
Pharmacotherapy
  • Diuretics (continued)
  • Need to watch for electrolyte imbalances which
    may lead to cramping, rhabdomyolysis (due to
    hypokalemia), or cardiac arrhythmias
  • Not recommended for endurance athletes who are
    prone to dehydration
  • Should be avoided in adolescent athletes as
    hypertension in this group generally due to
    increased sympathetic tone

82
Pharmacotherapy - Diuretics
  • Diuretics are generally inexpensive and well
    tolerated
  • Can increase triglyceride levels and interfere
    with glucose lowering medication

83
Pharmacotherapy - Diuretics
  • Thiazide Type
  • Chlorothiazide (Diuril)
  • Hydrochlorothiazide (HCTZ)
  • Chlorthalidone (Hygroton)
  • Metolazone (Zaroxolyn)
  • Carbonic Anhydrase Inhibitor
  • Acetazolamide ( Diamox)
  • Loop
  • Furosemide (Lasix)
  • Bumex ( Bumetanide)
  • Torsemide (Demadex)
  • Potassium Sparing
  • Amiloride ( Midamor)
  • Spironolactone (Aldactone)
  • Triamterene (Dyrenium)

Many times, different types are combined into one
pill
84
Pharmacotherapy
  • Central Alpha Agonists
  • Act centrally to block sympathetic stimulation
    leading to decreased plasma norepinephrine at
    rest and during exercise
  • Can blunt the sympathetic response during
    exercise
  • CO normalizes with chronic use allowing for
    normal cardiac response to exercise

85
Pharmacotherapy
  • Central alpha agonists (continued)
  • Excellent choice for young athletes as
    hypertension often due to increased sympathetic
    tone
  • Should be avoided in older patients as confusion
    can result
  • Side effects include sedation, dry mouth, and
    depression

86
Pharmacotherapy
  • Central alpha agonists (continued)
  • Clonidine (Catapres)
  • PO
  • Transdermal patch
  • guanabenz (Wytensin)
  • guanfacine (Tenex)
  • methyldopa (Aldomet)

87
Pharmacotherapy
  • Alpha1-receptor blockers
  • Decrease TPR by blocking postsynaptic alpha1
    arteriolar smooth muscle receptors
  • Allows for a normal physiologic response to
    exercise
  • Reduces afterload

88
Pharmacotherapy
  • Alpha1-receptor blockers (Continued)
  • Good choice for those involved with isometric
    activities
  • Can be used as an adjunct to nitrates in patients
    with heart failure
  • Frequently used in older men with Benign
    Prostatic Hypertrophy (BPH)
  • Orthostatic hypotension is a frequent
    complication

89
Pharmacotherapy
  • Alpha1-receptor blockers (Continued)
  • Prazosin (Minipress)
  • Terazosin (Hytrin)
  • Doxazosin (Cardura)

90
Pharmacotherapy
  • Beta-Blockers
  • Reduce Cardiac Output without effecting TPR (mild
    initial increase returns to baseline)
  • Useful in patients with
  • ASCVD
  • Increases exercise duration without anginal
    symptoms
  • fewer incidents of ST-segment depression
  • Hypertensive subjects with an excessive response
    to exercise
  • Intermittent exertion sports

91
Pharmacotherapy
  • Beta-Blockers (continued)
  • Leads to an impairment of exercise tolerance in
    individuals without ASCVD
  • Blunts decrease in LDL cholesterol and increase
    in HDL cholesterol generally associated with
    exercise
  • Associated with and increase in serum K
  • Avoided in patients with susceptibility to
    reactive airway disease

92
Pharmacotherapy
  • Beta-Blockers (continued)
  • Muscle glycogenolysis decreased causing
    hypoglycemia with endurance events
  • Use of free fatty acids impaired
  • Can impair thermoregulation
  • Increased muscle fatigue early on in therapy
  • Impotence

93
Pharmacotherapy
  • Beta-Blockers (continued)
  • Non-selective beta-blockers relatively
    contraindicated in athletes
  • Cardioselective beta-blockers are slightly better
    tolerated but still dramatically blunt exercise
    response
  • Beta-blockers with intrinsic sympathomimetic
    activity (ISA) thought to be the best tolerated
    with a decreased effect on heart rate and TPR

94
Pharmacotherapy
Beta-Blocking Agents by Cardioselectivity and ISA
  • Cardioselective
  • Atenolol (Tenormin)
  • Metoprolol (Lopressor)
  • Carteolol (Cartrol)
  • Penbutolol (Levatol)
  • Betaxolol (Kerlone)
  • Bisoprolol (Zebeta)
  • With ISA
  • Acebutolol (Sectral)
  • Noncardioselective
  • Nadolol (Corgard)
  • Propranolol (Inderal)
  • Carvedilol (Coreg)
  • Sotalol (Sotacor)
  • Timolol (Blocadren)
  • With ISA
  • Alprenolol (Aptin)
  • Oxprenolol (Trasicor)
  • Pindolol (Visken)

95
Pharmacotherapy
  • ACE Inhibitors and ARBs
  • Angiotensin Converting Enzyme (ACE) inhibitor and
    Angiotensin Receptor Blockers
  • ACE produced by lung tissue
  • Drug of choice in many athletes as it has the
    lowest incidence of side effects
  • Does not impair hemodynamic response to exercise
  • Decreases TPR

96
Pharmacotherapy
  • ACE Inhibitors and ARBs (continued)
  • Mechanism of action
  • Angiotensinogen converted to angiotensinogen I
  • Conversion of angiotensinogen I to
    angiotensinogen II by angiotensin converting
    enzyme (ACE) inhibited
  • Angiotensinogen II is a potent vasoconstrictor
    and leads to production of aldosterone which
    leads to increased blood volume

97
Pharmacotherapy
  • ACE Inhibitors and ARBs (continued)
  • Need to watch for interactions with NSAIDs and
    hyperkalemia with theses classes of medications
    (i.e. Avoid additional potassium replacement in
    fluids)
  • Reports of postural hypotension in athletes
    following intense endurance exercises.
  • Most frequent side-effect is a chronic cough
  • Not found with ARBs

98
Pharmacotherapy
  • Examples of ACE inhibitors
  • Captopril (Capoten)
  • Enalapril (Vasotec)
  • Lisinopril (Prinivil/Zestril)
  • Fosinopril (Monopril)
  • Benazepril ( Lotensin)
  • Ramipril (Altace)
  • Examples of ARBs
  • Losartan (Cozaar)
  • Irbesartan (Avapro)
  • Telmisartan (Micardis)
  • Candesartan (Atacand)
  • Olmesartan (Benicar)
  • Valsartan (Diovan)
  • Eposartan (Teveten)

99
Pharmacotherapy
  • Calcium Channel Blockers
  • Decrease TPR by reducing Ca concentrations in
    smooth muscle causing vasodilation
  • Decreases HR by decreasing AV conduction but SV
    increases so CO maintained
  • Generally allow for a normal physiologic response
    to exercise

100
Pharmacotherapy
  • Calcium Channel Blockers (continued)
  • No decrease in maximal aerobic capacity noted
  • Extend cool down period as can get orthostatic
    from fluid pooling in LEs
  • Most frequent side effects
  • Reflex tachycardia
  • Pedal edema
  • Constipation
  • Headache

101
Pharmacotherapy - Ca Channel Blockers
  • Dihydropyridines
  • Nifedipine (Procardia)
  • Amlodipine (Norvasc)
  • Felodipine (Plendil)
  • Isradipine (DynaCirc)
  • Nicardipine (Cardene)
  • Nimodipine (Nimotop)
  • Nisoldipine (Sular)
  • Phenylalkylamines
  • Verapamil (Calan/Isoptin)
  • Benzothiazepines
  • Diltiazem (Cardizem)

102
Hypertension Recap
  • Dynamic exercise has been proven to reduce SBP by
    7-12 mmHg and DBP by 5-10mmHG
  • This effect is independent of weight loss, body
    fat percentage, age, sex, dietary changes, or race

103
Hypertension Recap
  • A dynamic exercise regimen involving large muscle
    groups 3 times a week for 50-60 minutes at 40-60
    VO2 Max has been shown to be the most effective
    at controlling hypertension
  • Use antihypertensive medications appropriately
    when necessary

104
Hypertension Recap
  • The benefits of exercise last only as long as
    people continue to exercise with return to
    baseline blood pressure responses over 3-6 months.

105
Hypercholesterolemia
106
Cholesterol
  • A direct relationship exists between elevated
    total cholesterol levels and cardiovascular risk
  • Cholesterol plays an important role in cell
    membrane structure and cellular communication
  • Act to shuttle lipids through the plasma

107
Major Classes of Lipoproteins
  • Triglycerides
  • VLDL -Very low density lipid
  • IDL - Intermediate density lipid
  • Chylomicrons
  • LDL - Low density lipid
  • Bad cholesterol
  • Transfers lipids from liver to periphery
  • HDL - High density lipid
  • Good cholesterol
  • Transfers lipids from periphery to liver

108
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109
Cholesterol
  • When we get a lipid profile we look at
  • Total Cholesterol
  • LDL
  • HDL
  • Triglycerides

110
Adult Treatment Panel III (ATP III) Guidelines
  • National Cholesterol Education Program

111
Focus on Multiple Risk Factors
  • Diabetes CHD risk equivalent
  • Framingham projections of 10-year CHD risk
  • Identify certain patients with multiple risk
    factors for more intensive treatment
  • Multiple metabolic risk factors (metabolic
    syndrome)
  • Intensified therapeutic lifestyle changes

112
Modification of Lipid and Lipoprotein
Classification
  • LDL cholesterol lt100 mg/dLoptimal
  • HDL cholesterol gt40 mg/dL
  • The higher the better
  • Categorical risk factor
  • Lower triglyceride classification cut points
  • More attention to moderate elevations

113
Recommendation for Screening/Detection
  • Complete lipoprotein profile preferred
  • Fasting total cholesterol, LDL, HDL,
    triglycerides
  • Secondary option
  • Non-fasting total cholesterol and HDL
  • Proceed to lipoprotein profile if TC ?200 mg/dL
    or HDL lt40 mg/dL

114
More Intensive Lifestyle Intervention
(Therapeutic Lifestyle Changes TLC)
  • Therapeutic diet lowers saturated fat and
    cholesterol intakes to levels of previous Step II
  • Adds dietary options to enhance LDL lowering
  • Plant stanols/sterols (2 g/d)
  • Viscous (soluble) fiber (1025 g/d)
  • Increased emphasis on weight management and
    physical activity

115
Cost-Effectiveness Issues
  • Therapeutic lifestyle changes (TLC)
  • Most cost-effective therapy
  • Drug therapy
  • Dominant factor affecting costs
  • Cost effectiveness one factor in the decision
    for drug therapy
  • Declining price of drugs increases cost
    effectiveness

116
CHD Risk Equivalents
  • Other clinical forms of atherosclerotic disease
    (peripheral arterial disease, abdominal aortic
    aneurysm, and symptomatic carotid artery disease)
  • Diabetes
  • Multiple risk factors that confer a 10-year risk
    for CHD gt20

117
Three Categories of Risk that Modify
LDL-Cholesterol Goals
  • Risk Category
  • CHD and CHD riskequivalents
  • Multiple (2) risk factors
  • Zero to one risk factor
  • LDL Goal (mg/dL)
  • lt100
  • lt130
  • lt160

118
ATP III Lipid and Lipoprotein Classification
  • LDL Cholesterol (mg/dL)
  • lt100 Optimal
  • 100129 Near optimal/above optimal
  • 130159 Borderline high
  • 160189 High
  • ?190 Very high

119
ATP III Lipid and Lipoprotein Classification
(continued)
  • HDL Cholesterol (mg/dL)
  • lt40 Low
  • ?60 High

120
ATP III Lipid and Lipoprotein Classification
(continued)
  • Total Cholesterol (mg/dL)
  • lt200 Desirable
  • 200239 Borderline high
  • ?240 High

121
Causes of Secondary Dyslipidemia
  • Diabetes
  • Hypothyroidism
  • Obstructive liver disease
  • Chronic renal failure
  • Drugs that raise LDL cholesterol and lower HDL
    cholesterol (progestins, anabolic steroids, and
    corticosteroids)

122
LDL Cholesterol Goals and Cutpoints for
Therapeutic Lifestyle Changes (TLC)and Drug
Therapy in Different Risk Categories
123
Benefit Beyond LDL Lowering The Metabolic
Syndrome as a Secondary Target of Therapy
  • General Features of the Metabolic Syndrome
  • Abdominal obesity
  • Atherogenic dyslipidemia
  • Elevated triglycerides
  • Small LDL particles
  • Low HDL cholesterol
  • Raised blood pressure
  • Insulin resistance (? glucose intolerance)
  • Prothrombotic state
  • Proinflammatory state

124
Goals and TreatmentOverview
125
Therapeutic Lifestyle ChangesNutrient
Composition of TLC Diet
  • Nutrient Recommended Intake
  • Saturated fat Less than 7 of total calories
  • Polyunsaturated fat Up to 10 of total calories
  • Monounsaturated fat Up to 20 of total calories
  • Total fat 2535 of total calories
  • Carbohydrate 5060 of total calories
  • Fiber 2030 grams per day
  • Protein Approximately 15 of total calories
  • Cholesterol Less than 200 mg/day
  • Total calories (energy) Balance energy intake and
    expenditure to maintain desirable body
    weight/ prevent weight gain

126
A Model of Steps in Therapeutic Lifestyle
Changes (TLC)
Visit N
6 wks
6 wks
Q 4-6 mo
MonitorAdherenceto TLC
  • Emphasizereduction insaturated fat
    cholesterol
  • Encouragemoderate physicalactivity
  • Consider referral toa dietitian
  • Reinforce reductionin saturated fat
    andcholesterol
  • Consider addingplant stanols/sterols
  • Increase fiber intake
  • Consider referral toa dietitian
  • Initiate Tx forMetabolicSyndrome
  • Intensify weightmanagement physical activity
  • Consider referral to a dietitian

127
Drug Therapy
  • HMG CoA Reductase Inhibitors (Statins)
  • Reduce LDL-C 1855 TG 730
  • Raise HDL-C 515
  • Major side effects
  • Myopathy/ myalgias
  • Increased liver enzymes
  • Contraindications
  • Absolute liver disease
  • Relative use with certain drugs

128
Pharmacology
  • HMG-CoA reductase (Contd)
  • HMG-CoA reductase is the rate limiting enzyme in
    cholesterol synthesis. Inhibition of this enzyme
    stimulates LDL receptor synthesis and increased
    uptake of LDL and VLDL
  • All work through Cytochrome P450 so need to
    monitor liver function tests and other drug
    levels
  • Potential for rhabdomyolysis
  • Used for elevated LDL and /- triglycerides

129
HMG CoA Reductase Inhibitors (Statins)
  • Statin Dose Range
  • Lovastatin (Mevacor, altoprev) 2080 mg
  • Pravastatin (Pravachol) 2040 mg
  • Simvastatin (zocor) 2080 mg
  • Fluvastatin (Lescol) 2080 mg
  • Atorvastatin (Lipitor) 1080 mg
  • Resuvastatin (Crestor) 5-40 mg
  • Baycol recently taken off market 2o to high rate
    of liver failure and death

130
HMG CoA Reductase Inhibitors (Statins)
(continued)
  • Demonstrated Therapeutic Benefits
  • Reduce major coronary events
  • Reduce CHD mortality
  • Reduce coronary procedures (PTCA/CABG)
  • Reduce stroke
  • Reduce total mortality

131
Drug Therapy
  • Bile Acid Sequestrants
  • Major actions
  • Reduce LDL-C 1530
  • Raise HDL-C 35
  • May increase TG
  • Side effects
  • GI distress/constipation
  • Decreased absorption of other drugs
  • Contraindications
  • Dysbetalipoproteinemia
  • Raised TG (especially gt400 mg/dL)

132
Bile Acid Sequestrants
  • Drug Dose Range
  • Cholestyramine 416 g
  • Colestipol 520 g
  • Colesevelam 2.63.8 g

133
Bile Acid Sequestrants (continued)
  • Demonstrated Therapeutic Benefits
  • Reduce major coronary events
  • Reduce CHD mortality

134
Drug Therapy
  • Nicotinic Acid
  • Major actions
  • Lowers LDL-C 525
  • Lowers TG 2050
  • Raises HDL-C 1535
  • Side effects flushing, hyperglycemia,
    hyperuricemia, upper GI distress, hepatotoxicity
  • Contraindications liver disease, severe gout,
    peptic ulcer

135
Nicotinic Acid
  • Drug Form Dose Range
  • Immediate release 1.53 g(crystalline)
  • Extended release 12 g
  • Sustained release 12 g

136
Nicotinic Acid (continued)
  • Demonstrated Therapeutic Benefits
  • Reduces major coronary events
  • Possible reduction in total mortality

137
Drug Therapy
  • Fibric Acids
  • Major actions
  • Lower LDL-C 520 (with normal TG)
  • May raise LDL-C (with high TG)
  • Lower TG 2050
  • Raise HDL-C 1020
  • Side effects dyspepsia, gallstones, myopathy
  • Contraindications Severe renal or hepatic disease

138
Fibric Acids
  • Drug Dose
  • Gemfibrozil (Lopid/Gemcor) 600 mg BID
  • Fenofibrate (Tricor) 200 mg QD

139
Fibric Acids (continued)
  • Demonstrated Therapeutic Benefits
  • Reduce progression of coronary lesions
  • Reduce major coronary events

140
Inhibitors of Absorption
  • Ezetimibe (Zetia)
  • New class of agent
  • Inhibits small intestine brush border absorption
  • Works in conjunction with other medications to
    lower cholesterol by additional 10
  • Allows lower doses of statins thereby reducing
    side-effect profile
  • Vytorin ezetimibe simvastatin

141
Patterns of Lipoprotein Elevation
Major elevations in Plasma levels
142
Familial Hyperlipoproteinemia
  • Many of these patterns are familial in nature
  • Familial lipoprotein lipase deficiency Type I
  • Familial apoprotein CII deficiency Type I or 5
  • Familial type 3 hyperlipoproteinemia 3,2a,2b,
    or 4
  • Familial hypercholesterolemia 2a (rarely 2b)
  • Familial hypertriglyceridemia 4 (rarely 5)
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