AGGRASTAT(R) Strategy Trial Data Presented At American Heart Association Annual Meeting
November 12 2004 - 9:58AM
PR Newswire (US)
AGGRASTAT(R) Strategy Trial Data Presented At American Heart
Association Annual Meeting Guilford's Phase III Development Plan
Progresses; Enrollment in AGGRASTAT(R) Phase III TENACITY Trial
Begins BALTIMORE, Nov. 12 /PRNewswire-FirstCall/ -- Guilford
Pharmaceuticals Inc. (NASDAQ:GLFD) today announced the presentation
of data from the STRATEGY trial of AGGRASTAT(R) Injection
(tirofiban hydrochloride) at the 2004 Scientific Sessions of the
American Heart Association Annual Meeting in New Orleans. The study
found that a combination of AGGRASTAT(R) and a drug- eluting stent
(DES; Sirolimus eluting stent) resulted in a significantly lower
rate of death, MI, stroke, and binary restenosis at six months,
while also providing a similar cost of care when compared to
abciximab used in combination with a bare metal stent. Marco
Valgimigli, M.D., Chair of Cardiology, University of Ferrara, and
principal investigator for the STRATEGY trial, commented, "The use
of GP IIb- IIIa inhibitor therapy has been the standard of care for
patients undergoing coronary stent procedures. However, increasing
costs have prevented the adoption of approaches such as DES that
have been shown to reduce the incidence of binary restenosis and
target vessel revascularization. A new, cost-saving strategy for
using DES with a GP IIb-IIIa inhibitor will help us improve
outcomes in the cath lab without increasing costs for the health
care system." "Today's data add to a growing body of evidence
regarding the use of AGGRASTAT(R) both in and outside the cardiac
cath lab," commented Craig R. Smith, M.D., President and Chief
Executive Officer of Guilford. "Including the results from
STRATEGY, eight trials involving more than a thousand patients have
now been completed using the new single high-dose bolus
AGGRASTAT(R) regimen in various clinical settings." Dr. Smith
continued, "Our Phase III clinical development program will employ
a single high-dose bolus regimen of AGGRASTAT(R) followed by a
maintenance infusion in two separate Phase III trials in over
10,000 patients, comparing AGGRASTAT(R) to current standard of care
or placebo. The first trial to begin, TENACITY, which has recently
started patient enrollment, will evaluate whether the 30-day
efficacy of a single high-dose bolus regimen of AGGRASTAT(R)
retains at least 50% of the treatment benefit of abciximab in
patients undergoing PCI with coronary stent placement. In addition,
TENACITY will, for the first time, evaluate the 30-day safety and
efficacy of bivalirudin (Angiomax(R)) versus heparin with a single
high-dose bolus regimen of tirofiban or abciximab." Guilford plans
to conduct a superiority trial outside the United States. The trial
will be a multi-center, double-blind, placebo-controlled trial
evaluating the 30-day efficacy of the single high-dose bolus
regimen of AGGRASTAT(R) compared to placebo in high-risk patients
undergoing PCI with coronary stent placement. The trial is expected
to enroll approximately 2000 patients in 100 centers. All patients
will receive background treatment including heparin, aspirin and
clopidogrel (Plavix(R)), if not contraindicated. The results of
this trial are expected to provide a basis for seeking FDA approval
to expand the present indication of AGGRASTAT(R) to include a new
dosing regimen for treatment with AGGRASTAT(R) in the cardiac cath
laboratory at the time of PCI. STRATEGY Trial: High-Dose BoluS
TiRofibAn and Sirolimus Eluting STEnt versus Abiciximab and Bare
Metal Stent in Acute MYocardial Infarction (STRATEGY) Study The
six-month study included 175 patients with myocardial infarction
who had persistent ST segment elevation on their electrocardiogram
(STEMI) who were randomized to receive either the single high-dose
bolus (SHDB) tirofiban regimen (N=87; bolus of 25 mcg/Kg/3-min,
followed by an infusion of 0.15 mcg/Kg/min for 18-24 h) plus DES,
or abciximab (N=88; standard regimen) and bare metal stent (BMS).
At six months, clinical and angiographic follow-up was conducted in
144 patients. The primary end-point, a composite of death,
myocardial infarction (MI), stroke and binary restenosis rate,
occurred in 23% of patients receiving SHDB tirofiban-DES and 48% of
patients receiving abciximab-BMS (p=0.003). There was also a
statistically significant reduction of 6-month MACE for patients
treated with single high-dose bolus tirofiban-DES (15%) compared to
those treated with abciximab-BMS (23%), p=0.04. There was a trend
towards reduction in all bleeding events for patients treated with
SHDB tirofiban-DES compared to abciximab-BMS (16 patients vs. 9
patients, P=0.3). Moreover, there was a significant reduction in
thrombocytopenia in patients treated with SHDB tirofiban-DES versus
abciximab-BMS (9 patients versus 1 patients, p=0.03). Follow-up for
these patients is ongoing. About GP IIb/IIIa Antagonists Platelets
are blood cells that provide an early defense from the potential
complications of vascular injury. When a blood vessel is damaged,
platelets adhere to the site and promote blood clot formation. Clot
formation prevents bleeding and recruits other cells to help heal
the damage. While usually a beneficial process, these effects can
be harmful when a clot forms on a ruptured lipid plaque within the
coronary vasculature. GP IIb/IIIa antagonists block the ability of
platelets to aggregate, inhibiting clot formation and reducing the
potential for cardiac ischemia. Over the last 8-10 years, several
large-scale, placebo-controlled clinical trials have established
the efficacy of intravenous GP IIb/IIIa inhibitors for patients
with acute coronary syndrome who are medically managed or go to the
cath lab. Important Information About AGGRASTAT(R) Injection
AGGRASTAT(R) was approved by the Food and Drug Administration (FDA)
on May 14, 1998. AGGRASTAT(R), in combination with heparin, and
aspirin, if not contraindicated, is indicated for the treatment of
ACS including patients who are to be managed medically and those
undergoing PTCA or atherectomy. In this setting, AGGRASTAT(R) has
been shown to decrease the rate of a combined endpoint of death,
new myocardial infarction or refractory ischemia/repeat cardiac
procedure. In most patients, AGGRASTAT(R) should be administered
intravenously, at an initial rate of 0.4 mcg/kg/min for 30 minutes
and then continued at 0.1 mcg/kg/min. For complete information,
please refer to the product's prescribing information. AGGRASTAT(R)
(tirofiban hydrochloride) is contraindicated in patients with known
hypersensitivity to any component of the product; active internal
bleeding or a history of bleeding diathesis within the previous 30
days; or a history of intracranial hemorrhage, intracranial
neoplasm, arteriovenous malformation, or aneurysm. Other
contraindications to AGGRASTAT(R) include: a history of
thrombocytopenia following prior exposure to AGGRASTAT(R); history
of stroke within 30 days or any history of hemorrhagic stroke;
major surgical procedure or severe physical trauma within the
previous month; or history, symptoms, or findings suggestive of
aortic dissection. AGGRASTAT(R) is also contraindicated in patients
with: severe hypertension (systolic blood pressure >180 mmHg
and/or diastolic blood pressure >110 mmHg); concomitant use of
another parenteral GP IIb/IIIa inhibitor; or acute pericarditis.
Bleeding is the most common complication encountered during therapy
with AGGRASTAT(R). Administration of AGGRASTAT(R) is associated
with an increase in bleeding events classified as both major and
minor bleeding events, by criteria developed by the Thrombolysis in
Myocardial Infarction Study group (TIMI). Most major bleeding
associated with AGGRASTAT(R) occurs at the arterial access site for
cardiac catheterization. Fatal bleedings have been reported.
AGGRASTAT(R) should be used with caution in patients with platelet
count
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