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Steps in the assembly of replication-competent nuclei in a cell-free system from Xenopus eggs

机译:在非洲爪蟾卵的无细胞系统中组装具有复制能力的细胞核的步骤

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摘要

We have studied the pathway of nuclear assembly from demembranated sperm chromatin by fractionating a cell-free system from Xenopus eggs (Lohka, M. J., and Y. Masui. 1983. Science (Wash. DC). 220:719-721). Both the soluble fraction and a washed vesicular fraction are required for formation of normal nuclei that initiate replication in vitro. The soluble fraction alone decondenses chromatin and the vesicular fraction alone surrounds chromatin with membranes. Both fractions are required for formation of nuclear pore complexes. Recombining these two fractions recovers approximately 100% of the nuclear assembly and DNA replication activities. Restricting the proportion of the vesicular fraction slows acquisition of the nuclear membrane and allows observation of immature nuclear pores ("prepores"). These form as arrays around and within the chromatin mass before membranes form. Subsequently membrane vesicles bind to these prepores, linking them by a single membrane throughout the chromatin mass. At the periphery this single membrane is surrounded by an outer membrane. In mature nuclei all membranes are at the periphery, the two membranes are linked by pores, and no prepores are seen. Nuclear assembly and replication are inhibited by preincubating the chromatin with the vesicular fraction. However nuclear assembly is accelerated by preincubating the condensed chromatin with the soluble fraction. This also decreases the lag before DNA replication. Initiation of DNA replication is only observed after normal nuclei have fully reassembled, increasing the evidence that replication depends on nuclear structure. The pathway of nuclear assembly and its relationship to DNA replication are discussed.
机译:我们已经通过分离非洲爪蟾卵的无细胞系统研究了去膜的精子染色质的核装配途径(Lohka,M。J.和Y. Masui。1983. Science(Wash。DC)。220:719-721)。可溶级分和洗涤的水泡级分均是正常核形成所需的,而正常核在体外开始复制。单独的可溶性部分使染色质缩聚,而单独的囊泡部分用膜包围染色质。这两个部分都是形成核孔复合物所必需的。重组这两个部分可以回收大约100%的核装配和DNA复制活性。限制囊泡部分的比例减慢了核膜的获取,并允许观察未成熟的核孔(“孔前”)。这些在膜形成之前以染色质块周围和之内的阵列形式形成。随后,膜囊泡与这些前孔结合,在整个染色质团中通过单个膜将它们连接起来。在外围,该单个膜被外膜包围。在成熟的细胞核中,所有膜都在外围,两个膜通过孔连接,没有预孔。通过将染色质与水泡级分预孵育来抑制核装配和复制。但是,通过将浓缩的染色质与可溶级分预孵育,可以加速核装配。这也减少了DNA复制之前的延迟。仅在正常核完全重组后才能观察到DNA复制的启动,这增加了复制取决于核结构的证据。讨论了核组装的途径及其与DNA复制的关系。

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