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Molecular Pathways: Increased Susceptibility to Infection Is a Complication of mTOR Inhibitor Use in Cancer Therapy

机译:分子途径:对感染的易感性增加是mTOR抑制剂在癌症治疗中使用的并发症。

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As one of the earliest examples of "chemical biology," the Mechanistic Target of Rapamycin (mTOR) protein and its chemical inhibitors have been extensively studied across a spectrum of physiologic and pathologic processes at the molecular, organismal, and patient population levels. There are several FDA-approved mTOR inhibitors (sirolimus, everolimus, and temsir-olimus) with indications for cancer treatment and for prevention of solid organ rejection. Dozens of mTOR inhibitors are currently being evaluated in hundreds of ongoing clinical trials across a spectrum of diseases, including numerous cancer indications, autoimmune diseases, and a number of congenital disorders. As many of the approved and investigational indications for mTOR inhibitors require long-term treatment, the magnitude and incidence of particular side effects differ from those observed in shorter-term treatments. Here, we focus on the increased risk of infections in patients being treated with mTOR inhibitors. While increased infection rates might be expected from a class of drugs approved as posttransplant immunosuppres-sants, we review reports from clinical, mechanistic, and genetically engineered mouse model studies detailing a much more nuanced view of mTOR inhibitor drug action and target biology.
机译:作为“化学生物学”的最早例子之一,雷帕霉素(mTOR)蛋白及其化学抑制剂的机理靶点已在分子,生物和患者群体水平上的一系列生理和病理过程中得到了广泛研究。有几种FDA批准的mTOR抑制剂(西罗莫司,依维莫司和坦西米尔-奥利莫司)可用于癌症治疗和预防实体器官排斥。目前正在数十种正在进行的针对多种疾病的临床试验中评估数十种mTOR抑制剂,包括多种癌症适应症,自身免疫性疾病和许多先天性疾病。由于许多mTOR抑制剂的批准和研究适应症需要长期治疗,因此特定副作用的程度和发生率与短期治疗中观察到的不同。在这里,我们集中于接受mTOR抑制剂治疗的患者感染风险的增加。虽然批准作为移植后免疫抑制剂的一类药物可能会增加感染率,但我们回顾了来自临床,机制和基因工程小鼠模型研究的报告,这些报告详细介绍了mTOR抑制剂药物作用和靶标生物学的细微差别。

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