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米托蒽醌作为一种抗癌药物对肝细胞核和染色质的影响:组蛋白的选择性释放。

The effect of mitoxantrone as an anticancer drug on hepatocytes nuclei and chromatin: Selective release of histone proteins.

机构信息

Department of Biochemistry, Institute of Biochemistry and Biophysics, University of Tehran, Tehran, Iran.

出版信息

Indian J Pharmacol. 2011 Apr;43(2):187-91. doi: 10.4103/0253-7613.77362.

Abstract

OBJECTIVES

Mitoxantrone is an anticancer drug widely used in the treatment of various cancers. In the present study the effect of mitoxantrone on chromatin proteins of intact hepatocytes nuclei was investigated and compared with soluble chromatin.

MATERIALS AND METHODS

UV/Vis spectroscopy, SDS polyacrylamide gel electrophoresis, and western bolting were used.

RESULTS

The results show that exposure of intact nuclei to various concentrations of mitoxantrone resulted in the release of histone H1 family proteins, H1 and H1°, in a dose-dependent manner but not core histones and high mobility group proteins. Western blot analysis using antiserum against histones H1 and H1° revealed cross-reactivity and confirmed the result. Spectroscopy results showed that mitoxantrone binds to nuclear components and reduces the absorbances at 608 and 400 nm. The binding isotherms revealed cooperative binding with one binding site.

CONCLUSION

From the results it is suggested that mitoxantrone binds to intact nuclei and chromatin with different affinities and linker DNA can be considered as a main binding site for mitoxantrone at the nuclei level.

摘要

目的

米托蒽醌是一种广泛用于治疗各种癌症的抗癌药物。本研究旨在研究米托蒽醌对完整肝细胞核染色质蛋白的影响,并与可溶染色质进行比较。

材料与方法

采用紫外/可见光谱法、SDS 聚丙烯酰胺凝胶电泳和 Western blot 法。

结果

结果表明,暴露于各种浓度米托蒽醌的完整核会导致组蛋白 H1 家族蛋白 H1 和 H1°以剂量依赖的方式释放,但不释放核心组蛋白和高迁移率族蛋白。使用针对组蛋白 H1 和 H1°的抗血清进行的 Western blot 分析显示交叉反应并证实了这一结果。光谱结果表明,米托蒽醌与核成分结合,并降低了 608nm 和 400nm 处的吸光度。结合等温线显示具有一个结合位点的协同结合。

结论

从结果来看,米托蒽醌以不同的亲和力与完整细胞核和染色质结合,并且可以认为连接 DNA 是米托蒽醌在核水平上的主要结合位点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b9f/3081460/4ef74e57666d/IJPharm-43-187-g001.jpg

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