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错配修复缺陷将干细胞转化为癌症干细胞及其治疗意义。

Mismatch repair deficiencies transforming stem cells into cancer stem cells and therapeutic implications.

作者信息

Vaish Minal

机构信息

Department of Biochemistry, University of Lucknow-226007, UP, India.

出版信息

Mol Cancer. 2007 Apr 2;6:26. doi: 10.1186/1476-4598-6-26.

Abstract

For the exceptional self-renewal capacity, regulated cell proliferation and differential potential to a wide variety of cell types, the stem cells must maintain the intact genome. The cells under continuous exogenous and endogenous genotoxic stress accumulate DNA errors, drive proliferative expansion and transform into cancer stem cells with a heterogeneous population of tumor cells. These cells are a common phenomenon for the hematological malignancies and solid tumors. In response to DNA damage, the complex cellular mechanisms including cell cycle arrest, transcription induction and DNA repair are activated. The cells when exposed to cytotoxic agents, the apoptosis lead to cell death. However, the absence of repair machinery makes the cells resistant to tumor sensitizing agents and result in malignant transformation. Mismatch repair gene defects are recently identified in hematopoietic malignancies, leukemia and lymphoma cell lines. This review emphasizes the importance of MMR systems in maintaining the stem cell functioning and its therapeutic implications in the eradication of cancer stem cells and differentiated tumor cells as well. The understanding of the biological functions of mismatch repair in the stem cells and its malignant counterparts could help in developing an effective novel therapies leaving residual non-tumorigenic population of cells resulting in potential cancer cures.

摘要

由于具有非凡的自我更新能力、受调控的细胞增殖以及向多种细胞类型分化的潜能,干细胞必须维持基因组的完整性。处于持续外源性和内源性基因毒性应激下的细胞会积累DNA错误,驱动增殖性扩增,并转化为具有异质性肿瘤细胞群体的癌症干细胞。这些细胞在血液系统恶性肿瘤和实体瘤中很常见。作为对DNA损伤的反应,包括细胞周期停滞、转录诱导和DNA修复在内的复杂细胞机制被激活。当细胞暴露于细胞毒性剂时,细胞凋亡会导致细胞死亡。然而,缺乏修复机制会使细胞对肿瘤致敏剂产生抗性,并导致恶性转化。错配修复基因缺陷最近在血液系统恶性肿瘤、白血病和淋巴瘤细胞系中被发现。本综述强调了错配修复系统在维持干细胞功能中的重要性及其在根除癌症干细胞和分化肿瘤细胞方面的治疗意义。了解错配修复在干细胞及其恶性对应物中的生物学功能,有助于开发有效的新型疗法,使残留的非致瘤细胞群体得以保留,从而实现潜在的癌症治愈。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0417/1851711/abe25f61facc/1476-4598-6-26-1.jpg

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