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Nitric oxide-modulating agents for gastrointestinal disorders

机译:胃肠疾病的一氧化氮调节剂

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Almost 20 years after the identification of the biological role of nitric oxide(NO),the full therapeutic potential of novel agents that mimic the activity of NO or interfere with its synthesis has yet to be realised for utilities involving the gastrointestinal tract.New utilities for classical NO donors,which were used as vasodilators for decades,in the treatment of motility disorders have been explored and a product for treating anal fissure was recently launched.New classes of compounds incorporating a NO-donating moiety into standard non-steroidal anti-inflammatory drugs,the NO-non-steroidal anti-inflammatory drugs(NO-NSAIDs)or COX-inhibiting nitric oxide donors(CINODs)have also been developed.These have been shown to exhibit reduced gastrointestinal injury in experimental models,and reports on their efficacy and safety in Phase I and II studies are now available.Modulation of the inducible NO synthase isoform that generates excessive NO that can lead to subsequent cytotoxic moieties,such as peroxynitrite,may have therapeutic possibilities in a range of inflammatory diseases of the gut.Likewise,agents that promote the decomposition of peroxynitrite or removal of its other component,super-oxide,may also prove to be of use.Further targets for pharmaceutical exploitation are likely to come from both genomic and molecular insights into the processes that regulate the NO system.
机译:在确定一氧化氮(NO)的生物学作用后将近20年,对于涉及胃肠道的应用,模仿NO的活性或干扰其合成的新型药物的全部治疗潜力尚未实现。探索了用于运动性障碍治疗的传统NO供体(已用作血管扩张药数十年),最近还开发了一种治疗肛裂的产品。将NO供体部分纳入标准非甾体类抗炎剂的新型化合物还开发了非甾体类抗炎药(NO-NSAIDs)或抑制COX的一氧化氮供体(CINODs)。在实验模型中已证明这些药物可减轻胃肠道损伤,并报告其疗效现在已经可以进行一期和二期研究的安全性和可调节性。可诱导型一氧化氮合酶亚型的调节会产生过量的一氧化氮,从而导致随后的细胞毒性部分诸如过氧亚硝酸盐之类的药物在肠道的各种炎症疾病中可能具有治疗可能性。同样,促进过氧亚硝酸盐分解或去除其其他成分超氧化物的药物也可能被证明是有用的。用于药物开发的药物可能来自基因组和分子方面对调节NO系统过程的了解。

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