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顺铂即使在高浓度的氯离子存在下也能使染色质不可逆地固定。

Cisplatin fastens chromatin irreversibly even at a high chloride concentration.

机构信息

Center for Molecular Spectroscopy and Dynamics, Institute for Basic Science, Seoul 02841, Korea.

Department of Physics, Korea University, Seoul 02841, Korea.

出版信息

Nucleic Acids Res. 2021 Dec 2;49(21):12035-12047. doi: 10.1093/nar/gkab922.

Abstract

Cisplatin is one of the most potent anti-cancer drugs developed so far. Recent studies highlighted several intriguing roles of histones in cisplatin's anti-cancer effect. Thus, the effect of nucleosome formation should be considered to give a better account of the anti-cancer effect of cisplatin. Here we investigated this important issue via single-molecule measurements. Surprisingly, the reduced activity of cisplatin under [NaCl] = 180 mM, corresponding to the total concentration of cellular ionic species, is still sufficient to impair the integrity of a nucleosome by retaining its condensed structure firmly, even against severe mechanical and chemical disturbances. Our finding suggests that such cisplatin-induced fastening of chromatin can inhibit nucleosome remodelling required for normal biological functions. The in vitro chromatin transcription assay indeed revealed that the transcription activity was effectively suppressed in the presence of cisplatin. Our direct physical measurements on cisplatin-nucleosome adducts suggest that the formation of such adducts be the key to the anti-cancer effect by cisplatin.

摘要

顺铂是迄今为止开发的最有效的抗癌药物之一。最近的研究强调了组蛋白在顺铂抗癌作用中的几个有趣作用。因此,应该考虑核小体形成的影响,以便更好地解释顺铂的抗癌作用。在这里,我们通过单分子测量研究了这个重要问题。令人惊讶的是,在[NaCl] = 180 mM 下,即细胞离子种类的总浓度下,顺铂的活性降低,仍然足以通过牢固地保持其浓缩结构来损害核小体的完整性,即使受到严重的机械和化学干扰。我们的发现表明,这种顺铂诱导的染色质紧固可以抑制正常生物学功能所需的核小体重塑。体外染色质转录实验确实表明,在顺铂存在的情况下,转录活性被有效抑制。我们对顺铂-核小体加合物的直接物理测量表明,这种加合物的形成是顺铂抗癌作用的关键。

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