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本文引用的文献

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Induction of cancerous stem cells during embryonic stem cell differentiation.胚胎干细胞分化过程中癌症干细胞的诱导。
J Biol Chem. 2012 Oct 26;287(44):36777-91. doi: 10.1074/jbc.M112.372557. Epub 2012 Sep 7.
2
The quiescent cellular state is Arf/p53-dependent and associated with H2AX downregulation and genome stability.静止细胞状态依赖于Arf/p53,并与H2AX下调和基因组稳定性相关。
Int J Mol Sci. 2012;13(5):6492-6506. doi: 10.3390/ijms13056492. Epub 2012 May 24.
3
Tumor suppression in the absence of p53-mediated cell-cycle arrest, apoptosis, and senescence.在没有 p53 介导的细胞周期阻滞、细胞凋亡和衰老的情况下抑制肿瘤。
Cell. 2012 Jun 8;149(6):1269-83. doi: 10.1016/j.cell.2012.04.026.
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Combining immunotherapy and targeted therapies in cancer treatment.将免疫疗法和靶向疗法相结合用于癌症治疗。
Nat Rev Cancer. 2012 Mar 22;12(4):237-51. doi: 10.1038/nrc3237.
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Topoisomerase I poisoning results in PARP-mediated replication fork reversal.拓扑异构酶 I 中毒导致 PARP 介导的复制叉反转。
Nat Struct Mol Biol. 2012 Mar 4;19(4):417-23. doi: 10.1038/nsmb.2258.
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Onset of quiescence following p53 mediated down-regulation of H2AX in normal cells.正常细胞中 p53 介导的 H2AX 下调后进入静止期。
PLoS One. 2011;6(8):e23432. doi: 10.1371/journal.pone.0023432. Epub 2011 Aug 12.
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Distinct p53 transcriptional programs dictate acute DNA-damage responses and tumor suppression.不同的 p53 转录程序决定了急性 DNA 损伤反应和肿瘤抑制。
Cell. 2011 May 13;145(4):571-83. doi: 10.1016/j.cell.2011.03.035.
8
Poly(ADP-ribose) polymerase and XPF-ERCC1 participate in distinct pathways for the repair of topoisomerase I-induced DNA damage in mammalian cells.聚(ADP-核糖)聚合酶和 XPF-ERCC1 参与修复哺乳动物细胞中拓扑异构酶 I 诱导的 DNA 损伤的不同途径。
Nucleic Acids Res. 2011 May;39(9):3607-20. doi: 10.1093/nar/gkq1304. Epub 2011 Jan 11.
9
Histone gammaH2AX and poly(ADP-ribose) as clinical pharmacodynamic biomarkers.组蛋白 γH2AX 和聚(ADP-核糖)作为临床药效动力学生物标志物。
Clin Cancer Res. 2010 Sep 15;16(18):4532-42. doi: 10.1158/1078-0432.CCR-10-0523. Epub 2010 Sep 7.
10
DNA topoisomerases and their poisoning by anticancer and antibacterial drugs.DNA拓扑异构酶及其被抗癌和抗菌药物抑制的情况。
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Arf/p53 蛋白模块诱导细胞凋亡,下调组蛋白 H2AX 水平,使正常细胞能够在抗癌药物存在的情况下存活。

The Arf/p53 protein module, which induces apoptosis, down-regulates histone H2AX to allow normal cells to survive in the presence of anti-cancer drugs.

机构信息

Division of Genome Stability Research, National Cancer Center, 5-1-1 Tsukiji, Chuo-ku, Tokyo 104-0045, Japan.

出版信息

J Biol Chem. 2013 May 10;288(19):13269-77. doi: 10.1074/jbc.M112.402560. Epub 2013 Mar 27.

DOI:10.1074/jbc.M112.402560
PMID:23536184
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3650366/
Abstract

BACKGROUND

It is unclear how DNA-damaging agents target cancer cells over normal somatic cells.

RESULTS

Arf/p53-dependent down-regulation of H2AX enables normal cells to survive after DNA damage.

CONCLUSION

Transformed cells, which harbor mutations in either Arf or p53, are more sensitive to DNA-damaging agents.

SIGNIFICANCE

Cellular transformation renders cells more susceptible to some DNA-damaging agents. Anti-cancer drugs generally target cancer cells rather than normal somatic cells. However, the factors that determine this differential sensitivity are poorly understood. Here we show that Arf/p53-dependent down-regulation of H2AX induced the selective survival of normal cells after drug treatment, resulting in the preferential targeting of cancer cells. Treatment with camptothecin, a topoisomerase I inhibitor, caused normal cells to down-regulate H2AX and become quiescent, a process mediated by both Arf and p53. In contrast, transformed cells that harbor mutations in either Arf or p53 do not down-regulate H2AX and are more sensitive to drugs unless they have developed drug resistance. Such transformation-associated changes in H2AX expression rendered cancer cells more susceptible to drug-induced damage (by two orders of magnitude). Thus, the expression of H2AX and γH2AX (phosphorylated form of H2AX at Ser-139) is a critical factor that determines drug sensitivity and should be considered when administering chemotherapy.

摘要

背景

目前尚不清楚 DNA 损伤剂如何靶向癌细胞而不是正常体细胞。

结果

Arf/p53 依赖性下调 H2AX 使正常细胞在 DNA 损伤后能够存活。

结论

携带 Arf 或 p53 突变的转化细胞对 DNA 损伤剂更为敏感。

意义

细胞转化使细胞更容易受到某些 DNA 损伤剂的影响。抗癌药物通常靶向癌细胞而不是正常体细胞。然而,决定这种差异敏感性的因素知之甚少。在这里,我们表明,Arf/p53 依赖性下调 H2AX 诱导药物治疗后正常细胞的选择性存活,从而导致癌细胞的优先靶向。用拓扑异构酶 I 抑制剂喜树碱处理会导致正常细胞下调 H2AX 并进入静止状态,该过程由 Arf 和 p53 介导。相比之下,携带 Arf 或 p53 突变的转化细胞不会下调 H2AX,除非它们已经产生耐药性,否则对药物更敏感。H2AX 表达的这种与转化相关的变化使癌细胞更容易受到药物引起的损伤(相差两个数量级)。因此,H2AX 和 γH2AX(H2AX 在 Ser-139 位磷酸化形式)的表达是决定药物敏感性的关键因素,在进行化疗时应予以考虑。