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M期哺乳动物高尔基体拆卸与重新组装的分子机制

Molecular mechanisms in the disassembly and reassembly of the mammalian Golgi apparatus during M-phase.

作者信息

Misteli T

机构信息

Cold Spring Harbor Laboratory, NY 11724, USA.

出版信息

FEBS Lett. 1996 Jun 24;389(1):66-9. doi: 10.1016/0014-5793(96)00518-2.

Abstract

The mitotic disassembly and reassembly of the mammalian Golgi apparatus is an ideal system to study the molecular mechanisms involved in biogenesis and maintenance of membranous organelles. As cells enter M-phase, Golgi stacks are converted into Golgi clusters of small membrane fragments, which are dispersed throughout the cytoplasmic space during metaphase. Disassembly is dependent on the action of cdc2-kinase and at least two distinct pathways contribute to the fragmentation: one involves the budding of COP I-coated vesicles from Golgi cisternae, the other is a less well characterised COP I-independent pathway. During telophase, the Golgi fragments reassemble and fuse into a fully functional Golgi stack, using at least two distinct ATPase-mediated fusion pathways.

摘要

哺乳动物高尔基体的有丝分裂解体和重新组装是研究膜性细胞器生物发生和维持所涉及分子机制的理想系统。当细胞进入M期时,高尔基体堆叠会转变为小膜片段的高尔基体簇,这些簇在中期分散于整个细胞质空间。解体依赖于cdc2激酶的作用,至少有两条不同的途径导致碎片化:一条涉及从高尔基体潴泡出芽形成COP I被膜小泡,另一条是特征不太明确的不依赖COP I的途径。在末期,高尔基体片段重新组装并融合成一个功能完整的高尔基体堆叠,至少使用两条不同的由ATP酶介导的融合途径。

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