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Coxibs and Cardiovascular Side-Effects: From Light to Shadow

机译:考昔布和心血管的副作用:从光到影

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摘要

Since the discovery of COX-2, a second subtype of cyclooxygenase, selective inhibitors or "coxibs" were developed with the idea that this isoform was inducible at the site of inflammation whereas COX-1 was expressed constitutively in several tissues including gastric epithelium. This new class of non steroidal anti-inflammatory agents was though to be safer for ulcerations of the gastroinstestinal mucosa observed with non selective COX-2 inhibitors. Nevertheless, at the end of September 2004, Merck & Co announced the voluntary withdrawal of rofecoxib (Vioxx) worldwide because of an increased risk of cardiovascular events. This decision raised serious concerns about safety of selective COX-2 inhibitors which are actively marketed today, and the ones currently under development. The mechanism of this cardiovascular toxicity could lie in the inhibition of COX-2 itself, and thus be a class effect. On the other hand, these cardiovascular side effects could be limited on rofecoxib and be dependent on its chemical and/or pharmacological own properties. This hypothesis is undermined by the unexpected findings of one colon cancer study which has shown that celecoxib might also increase the chance of heart attack and stroke in some patients. In this review, we compared the different coxibs marketed to date on the basis of their clinical, pharmacological and chemical properties with the aim of providing some clues in the understanding of their potential or revealed "cardiovascular effects".
机译:自从发现COX-2后,便开发出环氧合酶的第二种亚型,选择性抑制剂或“ coxibs”,其想法是该同工型可在炎症部位诱导,而COX-1在包括胃上皮在内的多种组织中组成性表达。这类新的非甾体类抗炎药对于用非选择性COX-2抑制剂观察到的胃肠道粘膜溃疡更安全。但是,由于心血管事件的风险增加,默克公司(Merck&Co)于2004年9月宣布在全球范围内自愿停用罗非考昔(Vioxx)。该决定引起了人们对选择性COX-2抑制剂的安全性的严重关注,选择性COX-2抑制剂目前正在积极销售中,目前正在开发中。这种心血管毒性的机制可能在于抑制COX-2本身,因此是一种类效应。另一方面,这些心血管副作用可能仅限于罗非昔布,并取决于其化学和/或药理学性质。一项结肠癌研究的意外发现破坏了这一假设,该研究表明塞来昔布可能还会增加某些患者的心脏病和中风的机会。在这篇综述中,我们根据其临床,药理和化学特性比较了迄今上市的各种考昔布,目的是提供一些线索来了解它们的潜在作用或揭示的“心血管效应”。

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