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前列腺癌与免疫蛋白质组:唤醒并重新编程守护天使。

Prostate cancer and immunoproteome: awakening and reprogramming the guardian angels.

机构信息

Laboratory for Translational Oncology and Personalized Medicine, Rashid Latif Medical College (RLMC), Lahore, Pakistan.

出版信息

Arch Immunol Ther Exp (Warsz). 2012 Jun;60(3):191-8. doi: 10.1007/s00005-012-0169-y. Epub 2012 Apr 8.

Abstract

Prostate cancer is a life-threatening molecular disorder that is undruggable to date because of stumbling blocks in the standardization of therapy. An emerging framework of research is addressing how pathways that are derailed during tumorigenesis are linked to immunological responses, which are instrumental in immunosurveillance of cancer. However, interestingly, cancer cells circumvent such immunosurveillance through development of poorly immunogenic tumor cell variants (immunoselection) and through subversion of the immunological nanomachinery (immunosubversion). Detailed mechanistic insights of molecular specificities that regulate natural killer (NK) cell function suggest that it might be promising to design NK cell-based immunotherapeutic interventions against prostate cancer. Here, we elucidate evidence for NK cell targeting of prostate cancer proteome and address critical questions that, in our view, need thoughtfulness for the development of successful NK cell-based therapies. This review also disproves our contemporary understanding of the versatile regulators of DNA damage repair (ATM, ATR) that trigger cell surface expression of NKG2D ligands and consequent elimination of the tumor cells by NK cells and other lymphocytes that express NK cell receptors. Substantial fraction of information has been generated that guarantees productive future for this technology as more optimized constructs, better trial designs, and improved platforms are being brought from benchtop to bedside.

摘要

前列腺癌是一种危及生命的分子疾病,由于治疗标准化方面存在障碍,目前尚无药可医。一个新兴的研究框架正在研究肿瘤发生过程中发生故障的途径如何与免疫反应联系起来,免疫反应在癌症的免疫监视中起着重要作用。然而,有趣的是,癌细胞通过产生免疫原性差的肿瘤细胞变体(免疫选择)以及颠覆免疫的纳米机械(免疫抑制)来规避这种免疫监视。对调节自然杀伤 (NK) 细胞功能的分子特异性的详细机制见解表明,设计基于 NK 细胞的免疫治疗干预前列腺癌可能是有希望的。在这里,我们阐明了 NK 细胞针对前列腺癌蛋白质组的靶向证据,并解决了我们认为需要深思熟虑的关键问题,以开发成功的基于 NK 细胞的疗法。这篇综述还反驳了我们对触发 NK 细胞和其他表达 NK 细胞受体的淋巴细胞表面表达 NKG2D 配体并随后消除肿瘤细胞的 DNA 损伤修复(ATM、ATR)多功能调节剂的当代理解。已经产生了大量信息,为这项技术的未来提供了保证,因为更多优化的构建体、更好的试验设计和改进的平台正在从实验室走向临床。

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