????(?) -New Drugs of 2001-2004 Review-

About This Presentation

Title:

????(?) -New Drugs of 2001-2004 Review-

Description:

New agents for Dyslipidemia. Ezetimibe. Rosuvastatin. New Drugs for ... ( by adrenal gland, vasculature, and heart) Eplerenone. Eplerenone. Pharmacology (cont. ... – PowerPoint PPT presentation

Number of Views:160

Avg rating:3.0/5.0

Slides: 92

Provided by: tpa1

Category:

more less

Transcript and Presenter's Notes

Title: ????(?) -New Drugs of 2001-2004 Review-

1
????(?)-New Drugs of 2001-2004 Review-

?? ???
???????????

2
??

?????,??????
New Antihypertensive Agents
Olmesartan
Eplerenone
New agents for Dyslipidemia
Ezetimibe
Rosuvastatin
New Drugs for Treating Asthma/COPD
Formoterol

3
?????,?????

Part I
Antihypertensive agents
Antihyperlipidemic agents
Agents for asthma and COPD

Part II
Antihyperglycemics
Agents for migraine
Agents for impotence

4
?????,?????

Part III
Antimicrobials
Anticonvulsants
Agents for Parkinsons disease

Part IV
COX II inhibitors
Agent for treating psychosis
Agents for osteoporosis
Agents for peptic ulcer

5
?????,?????

Part V
Herbs or natural products that may cause cancer
and harm
Herbs that increase cancer growth and recurrence

Part VI
Cancer prevention
preventing tabacco-related cancer
Diet
chemopreventive agents
surgery
Cancer screening

6
New Antihypertensive Agents
7
Olmesartan

Olmesartan
Pharmacology
Angiotensin receptor blocker (ARB)
Selective antgonism of the angiotensin II type I
receptor (AT1)
Comparison chart
rapidly and completely de-esterified in the gut
active metabolite, olmesartan, in a reaction that
is not dependent on cytochrome P450
prolonged terminal elimination of 1218 hours,
which is longer than most other AT1 receptor
antagonists
T/P ratio
should have a troughpeak ratio that consistently
exceeds 60
the evidence suggests that blood pressure control
is sustained well beyond the dosage interval,
providing 'cover' for the poorly compliant
patient.

8
(No Transcript)
9
Olmesartan

Olmesartan
Adverse effects
The most commonly reported ADR
Headache (7.2 vs. 5.6 placebo)
Upper respiratory infection (4.9 vs. 3.3placebo)
Precautions
Unilateral or bilateral renal artety stenosis
have had increases in serum creatinine or BUN
after administration of drugs (ACEIs and ARBs)
Drug interactions
Antacids decrease olmesartans bioavailability
Dosage/administration
Initially, 20 mg QD
Dose increased to 40 mg if no response is seen in
the first 2 weeks
gt 40 mg, no additional benefit at higher doses

10
Olmesartan????ARB??????
11
(No Transcript)
12
Olmesartan

Comparison between ARBs
Blood pressure lowering effects
Olmesartangt irbesartangt losartangt valsartan
FDA approved indications
Losartan (Cozaar ?????)
Essential hypertension
Provides renoprotective effect in patients with
type 2 diabetes mellitus
hypertensive patients with left ventricular
hypertrophy for reduction of the risk of stroke

FDA approved indications (cont.)
Valsartan(Diovan ??)
CHF
Essential hypertension
Irbesartan (Aprovel???)
Essential hypertension
Provides renoprotective effect in patients with
type 2 diabetes mellitus
Candesartan (Blopress??)
Essential hypertension
Telmisartan (Micardis ??????)
Essential hypertension
Olmesartan (Olmetec ??)
Essential hypertension
Eprosartan (?????)
Essential hypertension

13
ARB ?ACEI??????
14
ACEIs vs. ARBs

Cardiovascular protection in high-risk
populations with cardiac disease and/or diabetes
ACEIARB
ARB are associated with less adverse side
effects and with higher compliance
Renoprotective in type 1 diabetes
Only ACEI

Preventing progression from microalbuminuria to
overt albuminuria in type 2 diabetes
Both ACEI and ARB
ARB can prevent loss of GFR
ACEI can prevent loss of GFR?
Side effects
ARBs cause less cough
ARBs cuase less angioedema

15
Eplerenone

Eplerenone
Pharmacology
A competitive antagonist of the aldosterone
receptor (potassium sparing diuretic)
A chemical derivative of spironolactone
enhance selective binding to the
mineralocorticoid receptor
minimizing binding to progesterone and androgen
receptors, which may lead to adverse effects

16
Eplerenone

Eplerenone
Pharmacology
Aldosterone and cardiovascular injury
Renin-angiotensin-aldosterone system (RAAS)
regulates cardiovascular homeotasis
Activation of RAAS
Increases risk of ischemic cardiovascular events
Drugs interrupt the RAAS
Reduce the risk of cardiovascular events
Preventing angiotensin IIs effects on
cellular growth and proliferation
vascular superoxide radical formation
thrombotic pathway

17
Eplerenone

Eplerenone
Pharmacology (cont.)
Heart failure and Aldosterone
a decrease in cardiac output
an ischemic or non-ischemic insult to myocardial
tissue
activation of the RAAS and SNS
in the short term for restoring cardiac output
prolonged RAAS and SNS activation
the progression of heart failure by increasing
cardiac workload
Chronic neurohormonal stimulation promotes
ventricular hypertrophy and remodeling.
Increases in circulating catecholamines and
angiotensin II promote synthesis and release of
aldosterone. (by adrenal gland, vasculature, and
heart)

18
Eplerenone

Eplerenone
Pharmacology (cont.)
Elevated aldosterone plasma concentration
Endothelial dysfunction
Myocardial infarction
Left ventricular hypertrophy
Death
ACEI and AT1 antagonist
initially reduce aldosterone concentration,
the aldosterone concentration return to baseline
with chronic therapy
Coadministration of spironolactone enhances the
beneficial effects of ACEI on mortality in
patient with CHF
Aldosterone contributes to cardiovascular
toxicity independent of the effects of
angiotensin II

19
(No Transcript)
20
Eplerenone

Eplerenone vs. spironolactone
Advantages of eplerenone
the lack of altered absorption with food
the absence of active metabolites.
Disadvantage of eplerenone
metabolism via the CYP3A4 pathway (potential for
drug interactions)
Adverse effects (chart)
Drug interactions
Hyperkalemia
Potassium supplements
ACEI or ARB
Enzyme inhibitors or inducers
Decrease antihypertensive effects
NSAIDs

21
(No Transcript)
22
The Seventh Report of the JointNational
Committee on Prevention, Detection,Evaluation,
and Treatment of High BloodPressure (JNC 7)

JAMA. 2003 May 21289(19)2560-72 (express
version)
Hypertension. 2003 Dec42(6)1206-52 (complete
version)

23
Outline of JNC 7

Introduction
Lifetime risk of hypertension
Blood pressure and cardiovascular risk
Basis for reclassification of blood pressure
Importance of systolic blood pressure
Calibration, maintenance, and use of blood
pressure measuring devises

Patient evaluation
Identifiable causes of hypertension
Genetics of hypertension
Treatment
Special situation in hypertension management
Drugs and other agents affecting blood pressure
Improving hypertension control

24
Introduction

Worldwide prevalence estimates for hypertension
may be as much as 1 billion individuals, and
approximately 7.1 million deaths per year may be
attributable to hypertension
The World Health Organization reports that
suboptimal BP (gt115 mmHg SBP) is responsible for
62 percent of cerebrovascular disease and 49
percent of ischemic heart disease

25
?????????
26
Introduction
27
Introduction
28
Introduction
29
Introduction
30
?????????????
31
Lifetime risk of hypertension
32
Lifetime risk of hypertension

Remaining lifetime risks of hypertension
women 8690
men 8183
4-year rates of progression to hypertension
65 years and older with BP in the 130139/8589
mmHg range 50
65 years and older with BP between 120129/8084
mmHg 26

33
Blood pressure and cardiovascular risk

The increased risks are present in individuals
ranging from 40 to 89 years of age.
For every 20 mmHg systolic or 10 mmHg diastolic
increase in BP, there is a doubling of mortality
from both IHD and stroke

34
????????
35
Blood pressure and cardiovascular risk
36
Basis for reclassification of blood pressure
37
Classification of blood pressure

Prehypertension
is not a disease category
identify individuals at high risk of developing
hypertension
encouraged to intervene and prevent or delay the
disease from developing.
not candidates for drug therapy
advised to practice lifestyle modification in
order to reduce their risk of developing
hypertension in the future
Prehypertension diabetes or kidney disease
should be considered candidates for appropriate
drug therapy if a trial of lifestyle modification
fails to reduce their BP to 130/80 mmHg or less.
All people with hypertension (stages 1 and 2) be
treated

38
???????????
39
Importance of systolic blood pressure

The rise in SBP continues throughout life
DBP rises until approximately age 50, tends to
level off over the next decade, and may remain
the same or fall later in life.
DBP is a more potent cardiovascular risk factor
than SBP until age 50 thereafter, SBP is more
important.

40
(No Transcript)
41
Importance of systolic blood pressure
42
??????????
43
Calibration, maintenance, and use of blood
pressure measuring devise

Persons should be seated quietly for at least 5
minutes
in a chair (rather than on an exam table),
with feet on the floor
arm supported at heart level
Caffeine, exercise, and smoking should be avoided
for at least 30 minutes prior to measurement
An appropriately sized cuff (cuff bladder
encircling at least 80 percent of the arm) should
be used to ensure accuracy

At least two measurements should be made and the
average recorded.
The cuff deflation rate for auscultatory readings
should be 2 mmHg per second.
SBP is the point at which the first of two or
more Korotkoff sounds is heard (onset of phase 1)
The disappearance of Korotkoff sound (onset of
phase 5) is used to define DBP.

44
(No Transcript)
45
?????????
46
Patient Evaluation

To assess lifestyle and identify other
cardiovascular risk factors or concomitant
disorders that may affect prognosis and guide
treatment
To reveal identifiable causes of high BP
To assess the presence or absence of target organ
damage and CVD.

47
Patient Evaluation
48
Treatment

In the majority of patients, reducing SBP has
been considerably more difficult than lowering
DBP.
The majority will require two or more
antihypertensive drugs.
The causes of BP control failure
failure to prescribe lifestyle modifications,
inadequate antihypertensive drug doses,
or inappropriate drug combination

49
Treatment

Goal of therapy
Reaching the DBP goal once the SBP goal is
achieved
the primary focus should be on attaining the SBP
goal.
Treating SBP and DBP to targets that are lt140/90
mmHg is associated with a decrease in CVD
complications.
In patients with hypertension and diabetes or
renal disease, the BP goal is lt130/80 mmHg

50
Treatment
51
(No Transcript)
52
Treatment
53
Drugs and other agents affecting blood pressure
54
New agents for Dyslipidemia
55
Ezetimibe

2-azetidinones (2-aze)
Interfere with cholesterol absorption (similar to
bile acid sequestrant)
provide enhanced cholesterol lowering when used
concomitantly with statins
do not interfere with the absorption of
concurrently administered medications

56
Ezetimibe

Mechanism of action
Absorption of cholesterol
Ingestion and delivery into the intestinal lumen,
Dietary cholesterol is absorbed predominantly in
the duodenum and jejunum, in an unesterified form
Upon entry into the intestines, cholesterol is
esterified by acyl-CoAcholesterol
acyltransferase (ACAT)
ACATis incorporated into chylomicrons conjointly
with triglycerides.
Chylomicrons are then delivered to the
circulation through the lymphatic system.

57
Two Sources of Cholesterol
Dietary cholesterol(300700 mg/day)
Fecal bile acids and neutral sterols
Intestine
Biliarycholesterol(1000 mg/day)
700 mg/day
Liver
Synthesis(800 mg/day)
Extrahepatictissues
Adapted from Champe PC, Harvey RA. Biochemistry.
2nd ed. Philadelphia Lippincott Raven, 1994
Glew RH. In Textbook of Biochemistry with
Clinical Correlations. 5th ed. New York
Wiley-Liss, 2002728-777 Ginsberg HN, Goldberg
IJ. In Harrisons Principles of Internal
Medicine. 14th ed. New York McGraw-Hill,
19982138-2149 Shepherd J Eur Heart J Suppl
20013(suppl E)E2-E5 Hopfer U. In Textbook of
Biochemistry with Clinical Correlations. 5th ed.
New York Wiley-Liss, 20021082-1150.
58
Cholesterol Synthesis
Acetyl-CoA
Acetoacetyl-CoA
HMG-CoA
HMG-CoA reductase
Hepatocyte
Mevalonate
Cholesterol
Adapted from Dietschy JM Am J Clin Nutr
1997651581S-1589S.
59
Cholesterol Absorption
ABCA1
ABCA1adenosine triphosphatebinding cassette
protein ACATacyl-coenzyme Acholesterol
acyltransferase CMchylomicron Adapted from
Champe PC, Harvey RA. Lippincotts Illustrated
Reviews Biochemistry. 2nd ed. Philadelphia
Lippincott-Raven, 1994.
60
Ezetimibe

Mechanism of action
Cholesterol transit across intestinal cellular
walls uses a specific protein-mediated
transport system.
2-aze bind to a protein on or within the brush
border membrane of intestinal cells.
2-aze relatively specific for inhibits
cholesterol absorption by inhibiting the
transport system.
Ezetimibe had no impact on the absorption of
triglycerides,
ethinyl estradiol,
progesterone,
fatsoluble vitamins (e.g., vitamin A, vitamin D,
tocopherol, or carotenoid)

61
Ezetimibe

Pharmacokinetics
Ezetimibe is readily taken up by intestinal cells
primarily glucuronidated within the intestinal
wall to the pharmacologically active ezetimibe
glucuronide (SCH 60663)
SCH 60663
is delivered to the liver by the portal system
secreted back into the intestinal lumen via the
biliary system
binds to the intestinal wall.
minimal systemic distribution of unconjugated
ezetimibe or SCH 60663 occurs.
more potent in inhibiting cholesterol absorption
than ezetimibe

62
Ezetimibe

Pharmacokinetics
Enterohepatic recirculation
SCH 60663 being deconjugated back to ezetimibe,
which is then reabsorbed in the ileum.
This process appears to recur every 4 hours for
several cycles and corresponds with meals.
Due to enterohepatic recirculation, it is
difficult to truly determine an elimination
half-life.
The effective half-life of ezetimibe has been
estimated to be 2830 hours
Ezetimibe and its conjugate are gt90 bound to
plasma proteins.
80 of an ezetimibe dose is eliminated fecally,
with 10 eliminated renally.

63
Ezetimibe

Adverse drug reactions
occur slightly more frequentlywith ezetimibe than
with placebo
Chest pain,
arthralgia,
diarrhea,
dizziness,
headache
Liver or skeletal muscle dysfunction has not been
associated with ezetimibe when used alone or in
combination with other agents.

64
Ezetimibe

Drug interactions
no impact on CYP1A2, 2C8/9, 2D6, 3A4
Fenofibrate and gemfibrozil have increased total
ezetimibe concentrations by 50
Cholystyramine considerably decreased total
ezetimibe concentrations
Antacid ezetimibe the AUC for total ezetimibe
did not differ, although the rate of absorption
was reduced

65
Ezetimibe

Dosage and administration
10-mg tablet given once daily with or without
food
ingested at least 2 hours before or 4 hours after
a BAS
Peak LDL-C lowering is generally achieved after 2
weeks of therapy.
contraindicated in patients with active liver
disease or continuously elevated liver enzymes
Liver function monitoring is not required when
zetimibe is used alone
No dosage adjustment is recommended by the
manufacturer for elderly patients or patients
with renal insufficiency or mild liver
insufficiency.

66
Ezetimibe

Role of therapy
Ezetimibe significantly lowers LDL-C
concentrations (gt 20) and modestly increases
HDL-C and lowers triglyceride concentrations.
most likely will be in combination with a statin
in patients who are unable to achieve target
LDL-C concentrations using a statin alone.
Homozygous form of familial hypercholesterolemia
Elevated sitosterol first-line treatment and
monotherapy

67
Bile acid sequestrants
68
Rosuvastatin

A hydroxymethylglutaryl coenzyme A (HMG-CoA)
reductase inhibitors
Competitively inhibition
the rate-limiting enzyme necessary for the
biosynthesis of cholesterol
are structural analogues of the half-reduced
intermediate of HMG-CoA

69
Rosuvastatin
70
Rosuvastatin
71
Rosuvastatin

Hepatocyte selectivity
Rosuvastatin and pravastatin are selective for
hepatocytes in vivo
This is consistent with the relatively
hydrophilic properties of both drugs
Drug interactions
Cyclosporine and rosuvastatin concomitantly
should be initiated on rosuvastatin 5 mg once
daily.
Warfarin and rosuvastatin warfarin therapy
should be monitored for international normalized
ratio changes

72
Rosuvastatin

Approximate equivalent doses for rosuvastatin
appear to be
one-half the atorvastatin dose
one-fourth the simvastatin dose
one-eighth the pravastatin dose (eg, substitute
rosuvastatin 5 mg for atorvastatin 10 mg,
simvastatin 20 mg, and pravastatin 40 mg).

73
Third Report of the Expert Panel on Detection,
Evaluation, and Treatment of High Blood
Cholesterol in Adults (Adult Treatment Panel
III)

Circulation. 2002 1063143-421

74
Revision and Addition of ATP III

Designation of a CHD risk equivalent category
identifying patients who require aggressive lipid
management
Recommendation of Framingham-based CHD risk
assessment in patients with multiple risk factors
Revised target levels for several of the lipids
and lipoproteins
Criteria for the identification of patients with
the metabolic syndrome

75
CHD risk equivalent
76
Target levels for several of the lipids and
lipoproteins
77
Therapeutic Goals
78
Detection of metabolic syndrome
79
Initiation of Drug Therapy
80
New Agents for Asthma/COPD
81
Formoterol

A ß2-selective adrenoceptor agonist
Has a rapid onset of action and maintains
a bronchodilatory effect for up to 12 hours.
Has minimal stimulating effects on
ß1-adrenoceptors and virtually no effect on
a-adrenoceptors

82
Formoterol

Dose and administration
The current recommended dosage of inhaled
formoterol for adults and children 6 years and
older
6mg twice daily via Turbuhaler, or
12mg (1 puff) twice daily via Aerolizer or
other dry powder devices or MDI.
If the recommended dosage does not sufficiently
control symptoms, it may be increased to 24mg
twice daily and subsequently be titrated
according to effect.

83
Formoterol

Dosage and administration
Formoterol should be administered in conjunction
with regular doses of inhaled or oral
corticosteroids.
The current recommendations for the use of
formoterol are as an alternative to increased
dosages of inhaled corticosteroids in patients
who remain symptomatic while receiving low to
moderate doses of inhaled corticosteroids.
Therapeutic role
is a long-acting b2-agonist currently recommended
for maintenance therapy
should not be used to treat acute exacerbations
of asthma.

84
Formoterol/Budesonide

Fixed-combination inhalers, such as
budesonide/formoterol formulation, are
recommended as a convenient way of administering
an inhaled corticosteroid plus a long-acting
ß2-agonist
Most of the antiinflammatory effect can be
achieved at lower dosage of steroids
The complementary bronchodilator effects of
additional long-acting ß2-agonists and the
possibility of positive interactions between the
two classes may make it possible to reduce the
dose of inhaled corticosteroids while maintaining
the same degree of asthma control

85
Guideline on the Diagnosis and Management of
Asthma