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Apoptosis as a Therapeutic Tool in IBD?

机译:凋亡作为IBD的治疗工具?

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Defective apoptosis of mucosal cell populations seems to be a relevant pathogenetic mechanism in inflammatory bowel disease (IBD). It has been suggested that the induction of apoptosis in various effector cells may be a relevant therapeutic mechanism in IBD. Indeed, it was shown that different drugs used for treatment of IBD have the capacity to induce apoptosis in T cells or monocytes in vitro and in vivo. However, it remains unclear whether these observations are related to clinical efficacy of these agents. TNF-α is one of the most relevant proinflammatory mediators in IBD and anti-TNF treatment has been shown to be of particular benefit for patients with IBD. It could subsequently be shown that various anti-TNF-α agents, such as infliximab and adalimumab, can induce apoptosis in activated monocytes and lymphocytes in vitro and in vivo. This mechanism requires reverse signaling via transmembranous TNF, thereby eliciting a signal transduction cascade that results in programmed cell death. Although other mechanisms might also contribute to the clinical effect of anti-TNF-α, current data suggest that apoptosis is a relevant mechanism that is associated with clinical efficacy of anti-TNF agents. Induction of apoptosis in activated monocytes or T cells may be regarded as therapeutic tool not only for anti-TNF agents, but also for other drugs used in IBD. Future strategies should focus on identification of mechanisms that prevent apoptosis in the mucosa of patients with IBD and in targeting apoptotic pathways as a therapeutic strategy in IBD.
机译:粘膜细胞群体的凋亡性缺陷似乎是炎症性肠病(IBD)的相关致病机制。已经提出在各种效应细胞中诱导凋亡可能是IBD中的相关治疗机制。实际上,已表明用于治疗IBD的不同药物具有在体外和体内诱导T细胞或单核细胞凋亡的能力。但是,尚不清楚这些观察是否与这些药物的临床功效有关。 TNF-α是IBD中最相关的促炎介质之一,抗TNF治疗已被证明对IBD患者特别有益。随后可以证明,各种抗TNF-α剂,例如英夫利昔单抗和阿达木单抗,可以在体外和体内诱导活化的单核细胞和淋巴细胞中的凋亡。此机制需要通过跨膜TNF进行反向信号传导,从而引发信号转导级联反应,从而导致程序性细胞死亡。尽管其他机制也可能有助于抗TNF-α的临床作用,但目前的数据表明凋亡是与抗TNF药物的临床功效相关的相关机制。在活化的单核细胞或T细胞中诱导细胞凋亡不仅可以被认为是抗TNF药物的治疗工具,而且可以被认为是IBD中使用的其他药物的治疗工具。未来的策略应侧重于确定预防IBD患者黏膜细胞凋亡的机制,以及靶向凋亡途径作为IBD的治疗策略。

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