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Coxibs, the Cardiologist’s Advice John Ducas Associate Professor of Medicine University of Manitoba
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Page 1: Coxibs, the Cardiologist’s Advice - in1touchmpha.in1touch.org/uploaded/38/web/documents/Dr. Ducas Coxibs Oct … · Coxibs, the Cardiologist’s Advice ... abundant watery sap,

Coxibs,

the Cardiologist’s Advice

John Ducas

Associate Professor of Medicine

University of Manitoba

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Disclosure

Have received honoraria for: – lectures

Have received payment for– Clinical trial participation

From: Pfizer, AstraZeneca, Merck/Schering Plough,

SanofiAventis, Servier, Boehringer-Ingelheim, Novartis

From: Pfizer, AstraZeneca, CSL Ltd, Servier,

Schering-Plough, GSK, Roche

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Conflict of Interest

• I am paid to give this talk

• Content has been determine by me, not sponsor

• Comments & content reflects my views, not the

University of Manitoba Faculty of Medicine

• My intent is to provide a fair & balanced

discussion of current science & treatment options

For feedback or questions:

[email protected]

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Agenda

At the end of this lecture you should

understand:

1. The mechanism of action of NSAIDs

2. The GI affects of NSAIDs

3. The CV effects of NSAIDs

4. The interaction between low dose ASA & NSAIDs

5. Some common misconceptions about NSAIDs

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The problem

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The problem

1. 1:4 adults have musc-skel pains

– nsNSAID & sNSAID are commonly Rx’ed

– nsNSAID are now OTC

2. nsNSAID & sNSAID have serious AE

– GI

– CV– Renal

– Hepatic

– Allergic

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The problem

3. Musc-skel pain pts have other problems &

risks:

Chronic inflammatory state

Immobility

- smoking

- hypertension

- dyslipidemia

- alcoholism

High GI risk

-previous GI bleed

-H pylori infection

-anticoagulants

-oral steroids

High CV risk

-elderly

-CV disease present

-multiple RF

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The problem

4. The Nomenclature

NSAID, nsNSAID, sNSAID, COX-2 inhibitors, COXIBS,

COX-2 selective

Generic Vs Brand

celecoxib (Celebrex®)

rofecoxib (Vioxx®), valdecoxib (Bextra®), lumiracoxib (Prexige®)

etoricoxib (Arcoxia®)

Older Drugs (some OTC)

Ibuprofen, diclofenac, aspirin, naproxen, indomethacin, sulindac,

ketorolac

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4. The Nomenclature simplified

All NSAID:

nsNSAID, = Mostly Older Drugs (aspirin, naproxen, etc)

sNSAID = celecoxib (Celebrex®)

The problem

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Salix sepulcralis - weeping willow

abundant watery sap, bark which is

heavily charged with salicylic acid

1700’s bark extract used for

effects on fever, pain and inflammation

1829, German chemists isolated

salicin from willow bark

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Charles Frederic Gerhardt

1853 ASA synthesized in an unstable and impure form

1897, scientists at the drug

and dye firm Bayer began

investigating acetylsalicylic

acid as a less-irritating

replacement for standard

common salicylate medicine

66 years later…

Indomethacin was discovered in 1963 and it was first approved

for use in the U.S. by the Food and Drug Administration in 1965

Efficacy unquestioned

Mechanism of action entirely unknown

Today there is no way this drug would have been approved

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Sir John Robert Vane (1927 – November 19, 2004)

won a Nobel Prize in Medicine in 1982

for his work 1971 on aspirin in which he discovered

it inhibited prostaglandin biosynthesis

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Prostaglandins

• found in virtually all tissues and organs

• lipid mediators or hormones

• potent

• short half-life inactivated rapidly after excretion

• paracrine (locally active)

• autocrine (acting on the same cells synthesizing it)

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Circulation 2005;112;759

BronchoconstrictionBronchoconstriction

Uteroconstriction

Multiple effectsBronchocodilation

Vasodilatation

Platelet inhibition

Platelet activation

Prostaglandins

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nsNSAID

Large Dose

Three different types of blockade

1

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Low dose

ASA

•Platelet irreversible

•Other sites intermittent

Three different types of blockade

2

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sNSAID

(coxib)

3

Three different types of blockade

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They have different T1/2

/ ASA

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A brief word on the GI effects…

Annals of Internal Medicine 85:299-303, 1976

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A brief word on the GI effects…

nsNSAIDS cause:

– 100,000 hospital stays USA per year

– 16,500 deaths per year

J Rheumatol 1999:26(Suppl 56):18

Incidence in Pts over 2 months:

2:3………….dyspepsia

1:5………….endoscopically demonstrable ulcer

1:40………...symptomatic ulcer

1:145……….bleeding ulcer

1:1,220…….dies from nsNSAID

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A brief word on the GI effects…

PUB

J Rheumatol 1999:26(Suppl 56):18

~1%

nsNSAIDS cause:Perforation

Ulcer

Bleeding

Annual

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A brief word on the GI effects…

10 X

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BMC Musculoskeletal Disorders 2007, 8:73

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N Engl J Med 2000;343:1520

VIGOR n=8076 with RA, rofecoxib 50 Vs naprosen 1000

overall & CV mortality rate were similar

(%)(%)

MI 12 (0.4) 4 (0.1)

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RofecoxibPoint Estimates and Summary Relative Risks for CV event With Rofecoxib

JAMA. 2006;296:1633-1644

09/2004, Merck announced

a voluntary worldwide

withdrawal of Vioxx

(rofecoxib) because of

increased risk of MI & CVA

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Carol and Robert Ernst

Robert died 2001

ANGLETON, Tex., Aug. 19, 2005

- the first verdict involving Vioxx

- awarded $253.5 m

-10,000 cases & 180 class action suits

pending against Merck

09/2004, Merck announced

a voluntary worldwide

withdrawal of Vioxx

(rofecoxib) because of

increased risk of MI & CVA

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Cardiovascular Effects

• BP

• CHF

– Kidney

• ASA Blockade by NSAID

• Vessel Wall / Platelet

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Cardiovascular Effects

• BP

– rise averages 3 to 6 mmHg

– most prominent in Na & high Na diet

– less effect in pt on CCB

NSAIDs:

1. increase BP

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Cardiovascular Effects

EPIDEMIOLOGY 2003;14:240 –246

0

0.2

0.4

0.6

0.8

1

1.2

1.4

1.6

1.8

2

No NSAID

Current NSAID

Low Dose

High Dose

Rela

tive R

isk C

HF

N=5857

• CHFCohort study / case–control analysis from UK GP Research Database

1ST hospital admission for non-fatal CHF

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Cardiovascular Effects

• CHF

Heart 2006;92:1610

Cohort study / case–control analysis from UK GP Research Database

new hospital admission for non-fatal CHF

0

1

2

3

4

5

6

7

8

9

No CHF Prior CHF

No NSAID

Current NSAID

N=6396

Rela

tive R

isk C

HF

History

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Cardiovascular Effects

• CHF

BMJ 2005;330:1370

Databases of hospital discharge summaries & prescription drug

claims in Quebec

N=2256

NSAIDs:

1. increase BP

2. cause CHF

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Cardiovascular Effects

• Kidney

NSAIDs:

1. increase BP

2. cause CHF

3. cause ARF

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Cardiovascular Effects

• ASA Blockade by NSAID

N Engl J Med 2001;345:1809

nsNSAID

NSAIDs:

1. increase BP

2. cause CHF

3. cause ARF

4. Block LD ASA

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Cardiovascular Effects

• Vessel Wall / Platelet

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COX-1

COX-1

(No COX 2 induced)

Normally, Balance

platelet reactivity

vascular reactivity

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↑COX-1

atherosclerosis,

↑COX-1

↑COX 2 induced

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(Low Dose)

Low dose ASA prevents MI & CVA!

COX-1

↑COX-1

↑COX 2 induced

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sNSAID

sNSAID promotes MI & CVA!

↑COX-1

COX-1

COX 2 induced

NSAIDs:

1.increase BP

2.cause CHF

3.cause ARF

4.cause CV Events

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Myths

1. ASA is the only safe NSAID, use in high dose

2. Naproxen is the only safe NSAID

3. All sNSAID are dangerous

4. Just give a PPI with nsNSAID

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1. ASA is the only safe NSAID, use in high

dose

ACE Trial

n=2849 undergoing CEA, pre op ASA & x 3m

Death, MI, CVA 3m

– ASA 81

– ASA 325

– ASA 650

– ASA 1300

3.7%

8.2%

P=0.002

Lancet 1991;353:2179

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2. Naproxen is the only safe

NSAIDADAPT

>70 y with family history of AD n=2,528

PLoS Clin

Trials 2006;1(7): e33.

•celecoxib 200 b.i.d.

•naproxen sodium 220 b.i.d

•placebo

Cardiovascular Death, MI, Stroke, CHF, or TIA

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3. All sNSAID are dangerousPoint Estimates and Summary Relative Risks for CV With Rofecoxib & Celecoxib

JAMA. 2006;296:1633-1644

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3. All sNSAID are dangerous

Circulation. 2008;117:2104

CV Death, MI , CVA, CHF, or Thromboembolism

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4. Just give a PPI with nsNSAID

image, from: Rheumatol Int (2008) 28:1187, original study :

CLINICAL GASTROENTEROLOGY AND HEPATOLOGY 2005;3:133

video capsule endoscopy

Normal baseline

No ASA

N=120 celecoxib 200 BID

N=118 naproxen 500 BID + Losec 20 OD

N=118 naproxen 500 BID + placebo

2 weeks

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4. Just give a PPI with nsNSAID

CLINICAL GASTROENTEROLOGY AND HEPATOLOGY 2007;5:1167

N = 854, OA + CVD

•baseline endoscopy normal

•all ASA 81 or 325

blind randomization

celecoxib 200

naproxen 5002 +lansoprazole 30

•Endoscopy 12 w

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Meta-analysis

99,400 patient years of exposure

Take Home

BMC Musculoskeletal Disorders 2007, 8:73

*

**

*

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Take Home

sNSIAD (+PPI) nsNSAID

(FRS >10%)

Risk Factor Modification / Low Dose ASA / BP / Statin

nsNSAID + PPI

(FRS)

Low Risk (FRS <10%)

nsNSIAD* +PPI or

low dose sNSAID (+PPI)

* ??Naproxen preferred

nsNSIAD*

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Take Home

When starting NSAID Monitor:– BP

– CHF

– Cr

– GI

• Alter NSAID if necessary

• Use plain ASA not ecASA, 2 hours before nsNSAID

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H pylori

H pylori

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Agenda

At the end of this lecture you should

understand:

1. The mechanism of action of NSAIDs

2. The GI affects of NSAIDs

3. The CV effects of NSAIDs

4. The interaction between low dose ASA & NSAIDs

5. Some common misconceptions about NSAIDs

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THANK YOU

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