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Abciximab

Abciximab (previously known as c7E3 Fab), manufactured by Centocor and distributed by Eli Lilly under the trade name ReoPro^®, is a platelet aggregation inhibitor mainly used during and after coronary artery procedures like angioplasty to prevent platelets from sticking together and causing thrombus (blood clot) formation within the coronary artery. Its mechanism of action is inhibition of glycoprotein IIb/IIIa. more...

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While Abciximab has a short plasma half life, due to its strong affinity for its receptor on the platelets, it may occupy some receptors for weeks. In practice, platelet aggregation gradually returns to normal about 24 to 48 hours after discontinuation of the drug.

Abciximab is made from the Fab fragments of an immunoglobulin that targets the glycoprotein IIb/IIIa receptor on the platelet membrane.

Indications for use

Abciximab is indicated for use in individuals undergoing percutaneous coronary intervention (angioplasty with or without stent placement). The use of abciximab in this setting is associated with a decreased incidence of ischemic complications due to the procedure¹ and a decreased need for repeated coronary artery revascularization in the first month following the procedure².

Pharmacokinetics

Abciximab has a plasma half life of about ten minutes, with a second phase half life of about 30 minutes. However, its effects on platelet function can be seen for up to 48 hours after the infusion has been terminated, and low levels of glycoprotein IIb/IIIa receptor blockade are present for up to 15 days after the infusion is terminated.

Side effects

Many of the side effects of abciximab are due to its anti-platelet effects. This includes an increased risk of bleeding. The most common type of bleeding due to abciximab is gastrointestinal hemorrhage. Thrombocytopenia is a rare but known serious risk.

Read more at Wikipedia.org

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Stenting Plus Abciximab Reduces Damage After MI - Brief Article
From American Family Physician, 6/15/02 by Anne D. Walling

Following myocardial infarction, one drawback of several reperfusion strategies is the potential to activate platelet and inflammatory mechanisms, which exacerbates microvascular dysfunction. Several studies have indicated that abciximab, a potent antiplatelet agent, can contribute to myocardial salvage. Kastrati and colleagues compared the two leading reperfusion strategies of stenting and fibrinolysis when each was combined with abciximab.

They studied patients presenting within 12 hours of onset of symptoms of proven myocardial infarction as demonstrated by ST segment changes of at least 0.1 mV in two or more limb leads, or at least 2.0 mV in two or more contiguous precordial leads, or complete left bundle branch block of new onset. Patients with contraindications to reperfusion or anticoagulation were excluded. More than 160 patients were randomly assigned to intravenous fibrinolysis or stenting, each plus abciximab. All patients also received aspirin and clopidogrel. Scintigraphy was performed on admission and repeated after seven to 14 days to document the extent of myocardial damage. The primary end point was the salvage index, defined as the proportion of the initial perfusion defect salvaged by reperfusion therapy. The study also monitored clinically significant events in patients for six months after the acute myocardial infarction.

The 81 patients assigned to stenting were similar in all significant variables to the 81 patients receiving alteplase. The initial perfusion defect was similar in size in the two groups. The stent was not necessary in three cases. The left anterior descending coronary artery was the target vessel in 48 percent of cases. Five patients assigned to fibrinolysis required rescue stenting, but no patients in the stenting group required more than one intervention. At discharge, the two groups of patients were receiving similar treatment based on aspirin, beta blockers, angiotensin-converting enzyme inhibitors, and statins. Follow-up scintigraphy was performed in 88 percent of patients in the stent group and 94 percent of those receiving alteplase. The salvage index was significantly greater in the stent group, and this group also had fewer deaths within six months (5 percent compared with 9 percent). The groups were similar in bleeding complications, but four alteplase patients experienced recurrent myocardial infarction, and three required urgent coronary artery surgery. At six months, the combined rate of death and recurrent myocardial infarction was 7.4 percent in the stent group compared with 17.3 percent in the fibrinolysis group.

The authors conclude that stenting plus abciximab resulted in greater myocardial salvage than alteplase plus abciximab. They call for larger studies to confirm this advantage.

2002;359:920-5.

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