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通过微核挤出从癌细胞中选择性消除无着丝粒双微体。

Selective elimination of acentric double minutes from cancer cells through the extrusion of micronuclei.

作者信息

Shimizu N, Shimura T, Tanaka T

机构信息

Faculty of Integrated Arts and Sciences, Hiroshima University, 1-7-1 Kagamiyama, Higashi-hiroshima, Hiroshima, Japan.

出版信息

Mutat Res. 2000 Mar 14;448(1):81-90. doi: 10.1016/s0027-5107(00)00003-8.

Abstract

Several lines of evidences from us or other authors had shown that tumor cells revert their phenotypes and differentiate by the elimination of oncogenes amplified on the acentric double minutes (DMs). The selective incorporation of DMs into the cytoplasmic micronuclei was thought to be involved in this elimination, however, the mechanism by which the content of micronuclei was eliminated from the cells remains to be discovered. In this report, we show the finding and the characterization of the extruded micronuclei in the culture fluid of human COLO 320DM tumor line, and suggest that the extrusion of micronuclei mediates the selective elimination of DMs. The extracellular micronuclei enriched with DMs had an apparently normal cytoplasmic membrane, decondensed chromatin and nuclear lamin protein, and their DNA did not suffer any extensive degradation. These characteristics were closely related to their cytoplasmic counterpart and clearly differentiated from the apoptotic bodies. We also developed a method for purifying the extracellular micronuclei. In this paper, the implications of the micronuclear extrusion are discussed.

摘要

我们或其他作者的多项证据表明,肿瘤细胞通过消除在无着丝粒双微体(DMs)上扩增的癌基因来恢复其表型并分化。DMs选择性地并入细胞质微核被认为与这种消除有关,然而,微核内容物从细胞中消除的机制仍有待发现。在本报告中,我们展示了在人COLO 320DM肿瘤细胞系培养液中挤出微核的发现及特征,并表明微核的挤出介导了DMs的选择性消除。富含DMs的细胞外微核具有明显正常的细胞质膜、解聚的染色质和核纤层蛋白,并且它们的DNA没有遭受任何广泛降解。这些特征与它们的细胞质对应物密切相关,并且明显不同于凋亡小体。我们还开发了一种纯化细胞外微核的方法。本文讨论了微核挤出的意义。

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