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寡毛纲纤毛虫新奥克草履虫大核染色质中的高阶DNA结构

Higher order DNA structure in macronuclear chromatin of the hypotrichous ciliate Oxytricha nova.

作者信息

Lipps H J, Gruissem W, Prescott D M

出版信息

Proc Natl Acad Sci U S A. 1982 Apr;79(8):2495-9. doi: 10.1073/pnas.79.8.2495.

Abstract

On lysis of macronuclei from the ciliated protozoan Oxytricha at 0.5-2 M NaCl, the DNA, which is normally found as discrete molecules ranging from 0.5 to 20 kilobases, appears in high molecular weight aggregates. Various treatments of the macronuclear lysate (i.e., nucleases, proteases, variation of salt, pH, and temperature) indicate that preservation of the aggregate structure depends on both nucleic acid-nucleic acid and nucleic acid-protein interactions. Purification of the DNA-protein complex after lysing the nuclei in 2 M NaCl shows that one major nuclear protein copurifies with the DNA. As shown by DNA-protein binding experiments, this protein has a high affinity for DNA; however, no evidence for sequence specificity of the protein binding was obtained. Chromatin reconstitution experiments suggest that the protein in itself is not sufficient for DNA aggregation in nuclei, but other factors, possibly the native chromatin structure, are required. Electron microscopy of the purified DNA-protein complex showed structures similar to those observed previously with in vitro-aggregated purified macronuclear DNA (14). A model is presented in which the terminal inverted repeat sequences found on all macronuclear DNA molecules interact with each other forming multistranded DNA complexes. The formation of these structures may be accelerated and stabilized by a protein in vivo.

摘要

在0.5 - 2M氯化钠溶液中对纤毛原生动物大草履虫的大核进行裂解时,通常以0.5至20千碱基的离散分子形式存在的DNA,会以高分子量聚集体的形式出现。对大核裂解物进行各种处理(即核酸酶、蛋白酶、盐、pH值和温度的变化)表明,聚集体结构的保留取决于核酸 - 核酸以及核酸 - 蛋白质相互作用。在2M氯化钠溶液中裂解细胞核后对DNA - 蛋白质复合物进行纯化,结果显示有一种主要的核蛋白与DNA共纯化。如DNA - 蛋白质结合实验所示,这种蛋白质对DNA具有高亲和力;然而,未获得该蛋白质结合具有序列特异性的证据。染色质重建实验表明,该蛋白质本身不足以使细胞核中的DNA聚集,还需要其他因素,可能是天然染色质结构。纯化的DNA - 蛋白质复合物的电子显微镜观察显示出与先前在体外聚集的纯化大核DNA中观察到的结构相似的结构(14)。本文提出了一个模型,其中在所有大核DNA分子上发现的末端反向重复序列相互作用形成多链DNA复合物。这些结构的形成在体内可能会被一种蛋白质加速并稳定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/774e/346225/3bf85f9be1a8/pnas00447-0077-a.jpg

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