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Phosphodiesterase inhibitors in inflammatory bowel disease

机译:磷酸二酯酶抑制剂在炎症性肠病中

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Inflammatory bowel disease (IBD) is fundamentally a relapsing and remitting disease appearing in forms of ulcerative colitis (UC) or Crohn's disease (CD) with a non-well-known etiology. With the hope to prevent adverse drug events and to increase the efficacy of therapies for IBD, in the recent years, other than new monoclonal antibodies such as infliximab, the novel phosphodiesterase inhibitors (PDEIs) have been introduced. Among PDE4Is, rolipram, OPC-6535, mesopram, roflumilast and tetomilast have shown beneficial effects in experimental colitis. Unfortunately until now, human studies have not been successful in showing significant superiority of PDE4Is in the treatment of IBD. Parallel with discovery of PDE4Is and their anti-inflammatory properties, inhibiting other PDE isoenzymes in immune and proinflammatory cells is on the way. PDE7Is have shown synergistic effect with PDE4Is and they may act similar to PDE3Is in experimental settings. Sildenafil as the PDE5I has shown good effects in experimental colitis by balancing oxidantantioxidant status. Although the present data about PDE superfamily and their specific roles in gastrointestinal tract is limited but inhibitors of PDE4, PDE5 and PDE7 seem good candidates as the next generation of effective drugs. The synergistic anti-inflammatory effect of PDE4Is and PDE7Is is also important.
机译:炎症性肠病(IBD)基本上是一种复发性和缓解性疾病,以溃疡性结肠炎(UC)或克罗恩氏病(CD)的形式出现,病因不明。为了防止药物不良事件并提高IBD疗法的疗效,近年来,除了新的单克隆抗体如英夫利昔单抗以外,还引入了新型的磷酸二酯酶抑制剂(PDEI)。在PDE4I中,咯利普兰,OPC-6535,美索普兰,鲁氟司特和替托司特在实验性结肠炎中显示出有益作用。不幸的是,到目前为止,人体研究尚未成功显示PDE4Is在IBD的治疗中具有明显的优势。与PDE4Is及其抗炎特性的发现并行,抑制免疫和促炎细胞中其他PDE同工酶的方法也在不断发展。 PDE7I已显示出与PDE4I的协同作用,并且在实验环境中其作用可能类似于PDE3I。西地那非作为PDE5I可通过平衡氧化剂和抗氧化剂的状态在实验性结肠炎中显示出良好的效果。尽管目前有关PDE超家族及其在胃肠道中的特殊作用的数据有限,但PDE4,PDE5和PDE7抑制剂似乎是下一代有效药物的良好候选者。 PDE4Is和PDE7Is的协同抗炎作用也很重要。

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