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首页> 外文期刊>Human Immunology: Official Journal of the American Society for Histocompatibility and Immunogenetics >Janus kinase inhibition for immunosuppression in solid organ transplantation: Is there a role in complex immunologic challenges?
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Janus kinase inhibition for immunosuppression in solid organ transplantation: Is there a role in complex immunologic challenges?

机译:janus激酶抑制固体器官移植中的免疫抑制作用:是否存在复杂免疫挑战中的作用?

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Inhibition of the Janus kinase-signal transducer and activator of transcription (JAM-STAT) pathway for immunosuppression in solid organ transplantation is appealing due to its specificity for immune cell function, particularly for JAK3. This is due to its unique association with only the common gamma chain (gamma(c)). The gamma(c), is an appealing immunosuppression target in transplantation because of the critically important lymphokines that act at it, including IL-2, IL-4, IL-7, IL-9, IL-15, and IL-21. Tofacitinib was initially purported to selectively inhibit solely JAK3, but subsequent analyses have also demonstrated its activity at the other members of the JAM family. Clinical outcomes have validated tofacitinib's pan-JAK activity in kidney transplantation after demonstrating an increased risk of infection and malignancy as compared to CNI-based regimens. After these trials, tofacitinib investigation for use in transplantation has effectively ceased. However, a post-hoc analysis has shed new light on the monitoring of tofacitinib exposure in order to predict infection and oncologic events. With new methods to monitor tofacitinib exposure, clinicians may be able to effectively reduce toxicities while providing a high level of immunosuppression. The purpose of this review to identify when, and for whom, JAR inhibitors may provide benefit in solid organ transplantation. (C) 2016 American Society for Histocompatibility and Immunogenetics. Published by Elsevier Inc. All rights reserved.
机译:由于其对免疫细胞功能的特异性,特别是对于jak3,在固体器官移植中的免疫抑制抑制janus激酶 - 信号传感器和转录的活化剂这是由于其独特的伽马链(γ(c))。 γ(c)是一种吸引人的免疫抑制靶标,因其作用的危重重要淋巴因子,包括IL-2,IL-4,IL-7,IL-9,IL-15和IL-21。 Tofacitinib最初声称选择性地抑制JAK3,但随后的分析还证明了果酱家族的其他成员的活性。与基于CNI的方案相比,临床结果验证了在肾移植的肾移植方面验证了TOFACITINIB的PAN-JAK活性。在这些试验之后,Tofacitinib用于移植的调查已有效停止。然而,HOC后分析对Tofacitinib暴露的监测进行了新的光线,以预测感染和肿瘤事件。通过新方法监测TOFACITINIB暴露,临床医生可能能够有效减少毒性,同时提供高水平的免疫抑制。本次审查的目的是鉴定何时,罐抑制剂可以在固体器官移植中提供益处。 (c)2016年美国组织合作和免疫因素的美国学会。由elsevier Inc.保留所有权利发布。

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