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当核小体在低离子强度下展开时,特定的组蛋白-组蛋白接触会破裂。

Specific histone-histone contacts are ruptured when nucleosomes unfold at low ionic strength.

作者信息

Martinson H G, True R J, Burch J B

出版信息

Biochemistry. 1979 Mar 20;18(6):1082-9. doi: 10.1021/bi00573a023.

Abstract

The ordered unfolding of the nucleosome core within chromatin at low ionic strengths has been studied. The results show that, when nuclei are lysed gently in solutions of very low ionic strength, their constituent nucleosomes rupture at a major H2B-H4 binding site but remain unperturbed at the site of the H2A-H2B interaction. These conclusions are based on data which show that at least four separate but closely spaced H2B-H4 contacts, identifiable by contact-site cross-linking in intact nuclei, are broken when nuclei are suspended in very dilute buffers. Appropriate controls on purified nucleosomes monomers demonstrate that the H2B-H4 contacts being broken are indeed intranucleosomal. Sedimentation of nucleosomes in the ultracentrifuge at various salt concentrations reveals that a significant conformational transition occurs in the range of ionic strength over which the H2B-H4 binding site ruptures.

摘要

已经研究了在低离子强度下染色质内核小体核心的有序展开。结果表明,当在极低离子强度的溶液中轻轻裂解细胞核时,其组成的核小体在主要的H2B - H4结合位点断裂,但在H2A - H2B相互作用位点保持未受干扰。这些结论基于的数据表明,当细胞核悬浮在非常稀的缓冲液中时,至少四个可通过完整细胞核中的接触位点交联识别的独立但紧密间隔的H2B - H4接触会断裂。对纯化的核小体单体进行的适当对照表明,被破坏的H2B - H4接触确实是核小体内的。在各种盐浓度下在超速离心机中对核小体进行沉降分析表明,在H2B - H4结合位点断裂的离子强度范围内发生了显著的构象转变。

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