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人类白血病发展的概念。

Concepts of human leukemic development.

作者信息

Warner Jennifer K, Wang Jean C Y, Hope Kristin J, Jin Liqing, Dick John E

机构信息

Division of Cell and Molecular Biology, University Health Network, University of Toronto, 620 University Ave, ON M5G 2C1, Canada.

出版信息

Oncogene. 2004 Sep 20;23(43):7164-77. doi: 10.1038/sj.onc.1207933.

Abstract

Two fundamental problems in cancer research are identification of the normal cell within which cancer initiates and identification of the cell type capable of sustaining the growth of the neoplastic clone. There is overwhelming evidence that virtually all cancers are clonal and represent the progeny of a single cell. What is less clear for most cancers is which cells within the tumor clone possess tumorigenic or 'cancer stem cell' (CSC) properties and are capable of maintaining tumor growth. The concept that only a subpopulation of rare CSC is responsible for maintenance of the neoplasm emerged nearly 50 years ago. Testing of this hypothesis is most advanced for the hematopoietic system due to the establishment of functional in vitro and in vivo assays for stem and progenitor cells at all stages of development. This body of work led to conclusive proof for CSC with the identification and purification of leukemic stem cells capable of repopulating NOD/SCID mice. This review will focus on the historical development of the CSC hypothesis, the mechanisms necessary to subvert normal developmental programs, and the identification of the cell in which these leukemogenic events first occur.

摘要

癌症研究中的两个基本问题是确定癌症起源的正常细胞以及确定能够维持肿瘤克隆生长的细胞类型。有压倒性的证据表明,几乎所有癌症都是克隆性的,代表单个细胞的后代。对于大多数癌症来说,不太清楚的是肿瘤克隆中的哪些细胞具有致瘤性或“癌症干细胞”(CSC)特性并能够维持肿瘤生长。只有少数罕见的癌症干细胞亚群负责肿瘤维持的概念大约在50年前出现。由于建立了针对发育各个阶段的干细胞和祖细胞的功能性体外和体内检测方法,对造血系统而言,对这一假设的测试最为先进。这项工作通过鉴定和纯化能够使NOD/SCID小鼠重新增殖的白血病干细胞,为癌症干细胞提供了确凿的证据。本综述将重点关注癌症干细胞假说的历史发展、颠覆正常发育程序所需的机制,以及首次发生这些致白血病事件的细胞的鉴定。

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