Omer Iqbal
Anschutz Medical Campus
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Expert Opinion on Emerging Drugs | 2002
Hazar Shadid; Salim Aziz; Sarfraz Ahmad; Jawed Fareed; Debra Hoppensteadt; Harry Messmore; William Wehrmacher; Mahmut Tobu; Omer Iqbal
Sepsis, a systemic inflammatory syndrome, is a response to infection and when associated with multiple organ dysfunction is termed severe sepsis. It remains a leading cause of mortality in the critically ill. The response to the invading microorganisms may be considered as a balance between a pro-inflammatory and an anti-inflammatory reaction. While an inadequate pro-inflammatory reaction and a strong anti-inflammatory response could lead to overwhelming infection and the death of the patient, a strong and uncontrolled pro-inflammatory response, manifested by the release of pro-inflammatory mediators may lead to microvascular thrombosis and multiple organ failure. Endotoxin triggers sepsis via the release of various mediators such as tumour necrosis factor-α and interleukin-1 (IL-1). These cytokines activate the complement and coagulation systems, release adhesion molecules, prostaglandins, leukotrienes, reactive oxygen species and nitric oxide. Other mediators involved in the sepsis syndrome include IL-1, -6 and -8; arachidonic acid metabolites; platelet activating factor; histamine; bradykinin; angiotensin; complement components and vasoactive intestinal peptide. These pro-inflammatory responses are counteracted by IL-10. Most of the trials targeting the different mediators of the pro-inflammatory response have failed due to a lack of correct definition of sepsis. Understanding the exact pathophysiology of the disease will enable more advanced treatment options. Targeting the coagulation system with various anticoagulant agents including, activated protein C, and tissue factor pathway inhibitor (TFPI) is a rational approach. Many clinical trials have been conducted to evaluate these agents in severe sepsis. While trials on antithrombin and TFPI were not so successful, the double-blind, placebo-controlled, Phase III trial of recombinant human activated Protein C Worldwide Evaluation in Severe Sepsis (PROWESS) was successful, creating a significant decrease in mortality when compared to the placebo group. A better understanding of the pathophysiologic mechanism of severe sepsis will provide better treatment options, and combination antithrombotic treatment may provide a multipronged approach for the treatment of severe sepsis.
Seminars in Thrombosis and Hemostasis | 1999
Walenga Jm; Fasanella Ar; Omer Iqbal; Debra Hoppensteadt; Sarfraz Ahmad; Wallis De; Mamdouh Bakhos
Archive | 2002
W. Jeske; Omer Iqbal; Jawed Fareed; Brigitte Kaiser
Hamostaseologie | 1993
Debra Hoppensteadt; Jeanine M. Walenga; Ahmad Ahsan; Omer Iqbal; W. Jeske; J. Fareed
Hamostaseologie | 2001
J. Fareed; Debra Hoppensteadt; Omer Iqbal; R. L. Bick
Blood | 2005
Jawed Fareed; D. Hoppensteadt; Josephine Cunanan; C. Patel; Jyothi Maddineni; Francis Baltasar; Daniel Fareed; Muzaffer Demir; M. Tobu; Omer Iqbal; Vinod Bansal; R. Greenfield
Seminars in Thrombosis and Hemostasis | 1993
Blazej Lojewski; P. Bacher; Omer Iqbal; Walenga Jm; D. Hoppensteadt; Fred Leya; Jawed Fareed
Archive | 2014
Jawed Fareed; Daneyal Syed; Omer Iqbal
Archive | 2012
Debra A. Hoppensteadt; Josephine Cunanan; Omer Iqbal; Angel Gray; Bruce E. Lewis; Walenga Jm; Jawed Fareed
Archive | 2007
Harry L. Messmore; Erwin Coyne; Meghan Businaro; Omer Iqbal; William H. Wehrmacher; W. Jeske