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ASH 50th Anniversary Review: Bcl-2–family proteins and hematologic malignancies: history and future prospects

机译:ASH 50周年回顾:Bcl-2基因家族蛋白与血液系统恶性肿瘤的历史和未来展望

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摘要

BCL-2 was the first antideath gene dis-covered, a milestone that effectively launched a new era in cell death research. Since its discovery more than 2 decades ago, multiple members of the human Bcl-2 family of apoptosis-regulating proteins have been identified, including 6 antiapoptotic proteins, 3 structurally similar proapoptotic proteins, and several structurally diverse proapoptotic interacting proteins that operate as upstream agonists or antagonists. Bcl-2–family proteins regulate all major types of cell death, including apoptosis, necrosis, and autophagy. As such, they operate as nodal points at the convergence of multiple pathways with broad relevance to biology and medicine. Bcl-2 derives its name from its original discovery in the context of B-cell lymphomas, where chromosomal translocations commonly activate the BCL-2 protooncogene, endowing B cells with a selective survival advantage that promotes their neoplastic expansion. The concept that defective programmed cell death contributes to malignancy was established by studies of Bcl-2, representing a major step forward in current understanding of tumorigenesis. Experimental therapies targeting Bcl-2 family mRNAs or proteins are currently in clinical testing, raising hopes that a new class of anticancer drugs may be near.
机译:BCL-2是第一个发现的抗死亡基因,这一里程碑有效地开启了细胞死亡研究的新纪元。自二十多年前发现以来,已鉴定出人类Bcl-2家族的凋亡调节蛋白成员,包括6种抗凋亡蛋白,3种结构相似的促凋亡蛋白以及几种结构多样的促凋亡相互作用蛋白,它们均起着上游激动剂的作用。或拮抗剂。 Bcl-2家族蛋白调节细胞死亡的所有主要类型,包括凋亡,坏死和自噬。因此,它们在与生物学和医学广泛相关的多种途径的融合中充当节点。 Bcl-2因其在B细胞淋巴瘤中的最初发现而得名,在B细胞淋巴瘤中,染色体易位通常激活BCL-2原癌基因,赋予B细胞以选择性生存优势,从而促进其肿瘤的扩展。 Bcl-2的研究确立了缺陷性程序性细胞死亡导致恶性肿瘤的概念,这代表了当前对肿瘤发生的认识上的重大进步。针对Bcl-2家族mRNA或蛋白质的实验疗法目前正在临床测试中,这使人们希望新型抗癌药物即将问世。

著录项

  • 期刊名称 Blood
  • 作者

    John C. Reed;

  • 作者单位
  • 年(卷),期 -1(111),7
  • 年度 -1
  • 页码 3322–3330
  • 总页数 4
  • 原文格式 PDF
  • 正文语种
  • 中图分类 血液学检验;
  • 关键词

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