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一氧化氮供体在药理学研究中的应用。

The use of nitric oxide donors in pharmacological studies.

作者信息

Feelisch M

机构信息

The Wolfson Institute for Biomedical Research, University College London, UK.

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 1998 Jul;358(1):113-22. doi: 10.1007/pl00005231.

Abstract

A growing appreciation of the involvement of nitric oxide (NO) in numerous bioregulatory pathways has not only opened up new therapeutic avenues for organic nitrates and other NO donors but also led to an increased use of such compounds in pharmacological studies. By definition, all NO donors produce NO-related activity when applied to biological systems and are thus principally suited to either mimic an endogenous NO-related response or substitute for an endogenous NO deficiency. However, the pathways leading to enzymatic and/or non-enzymatic formation of NO differ greatly among individual compound classes, as do their chemical reactivities and kinetics of NO release. Moreover, since the reaction of NO with oxygen is a function of its concentration, the same absolute amounts of NO generated over different periods of time may lead to substantially different rates of NOx formation and, consequently, to varying extents of side reactions, such as nitration and/or nitrosation of biomolecules. Matters are further complicated by compound-specific formation of by-products, which may arise during decomposition or metabolism, sometimes in amounts far exceeding those of NO. The term "NO donor" implies that the compound releases the active mediator, NO. Ultimately, this may be true for many different chemical classes of compound, since the principal NO-related species generated may be converted to NO, if not directly released as such. However, in a biological system, the redox form of nitrogen monoxide (NO+, NO. or NO-) that is actually released makes a substantial difference to the NO donor's reactivity towards other biomolecules, the profile of by-products, and the bioresponse. Such considerations are likely to account for much of the discrepancy in experimental results obtained using the same cell or tissue preparation but different NO mimetics. Thus, compound selection is not a trivial issue and the investigator should be aware of the key properties and differences between various NO donor classes in order to avoid misinterpretation of experimental results.

摘要

人们越来越认识到一氧化氮(NO)参与众多生物调节途径,这不仅为有机硝酸盐和其他NO供体开辟了新的治疗途径,也导致此类化合物在药理学研究中的使用增加。根据定义,所有NO供体在应用于生物系统时都会产生与NO相关的活性,因此主要适用于模拟内源性NO相关反应或替代内源性NO缺乏。然而,不同化合物类别中导致NO酶促和/或非酶促形成的途径差异很大,其化学反应性和NO释放动力学也是如此。此外,由于NO与氧气的反应是其浓度的函数,在不同时间段内产生的相同绝对量的NO可能导致NOx形成速率有很大差异,进而导致副反应的程度不同,例如生物分子的硝化和/或亚硝化。化合物特异性副产物的形成使情况更加复杂,这些副产物可能在分解或代谢过程中产生,有时其数量远远超过NO。术语“NO供体”意味着该化合物释放活性介质NO。最终,对于许多不同化学类别的化合物来说可能都是如此,因为产生的主要与NO相关的物种即使不是直接以这种形式释放,也可能转化为NO。然而,在生物系统中,实际释放的一氧化氮的氧化还原形式(NO+、NO·或NO-)对NO供体与其他生物分子的反应性、副产物谱和生物反应有很大影响。这些考虑因素可能是导致使用相同细胞或组织制剂但不同NO模拟物获得的实验结果存在差异的主要原因。因此,化合物的选择并非小事,研究人员应了解各种NO供体类别的关键特性和差异,以避免对实验结果的误解。

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