Differential Nuclear Remodeling of Mammalian Somatic Cells by Xenopus Laevis Oocyte and Egg Cytoplasm

Overview

Journal Exp Cell Res

Specialty Cell Biology

Date 2005 Jun 1

PMID 15922733

Citations 26

Authors

Ramiro Alberio

Andrew D Johnson

Reimer Stick

Keith H S Campbell

Affiliations

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Abstract

The mechanisms governing nuclear reprogramming have not been fully elucidated yet; however, recent studies show a universally conserved ability of both oocyte and egg components to reprogram gene expression in somatic cells. The activation of genes associated with pluripotency by oocyte/egg components may require the remodeling of nuclear structures, such that they can acquire the features of early embryos and pluripotent cells. Here, we report on the remodeling of the nuclear lamina of mammalian cells by Xenopus oocyte and egg extracts. Lamin A/C is removed from somatic cells incubated in oocyte and egg extracts in an active process that requires permeable nuclear pores. Removal of lamin A/C is specific, since B-type lamins are not changed, and it is not dependent on the incorporation Xenopus egg specific lamin III. Moreover, transcriptional activity is differentially regulated in somatic cells incubated in the extracts. Pol I and II transcriptions are maintained in cells in oocyte extracts; however, both activities are abolished in egg extracts. Our study shows that components of oocyte and egg extracts can modify the nuclear lamina of somatic cells and that this nuclear remodeling induces a structural change in the nucleus which may have implications for transcriptional activity. These experiments suggest that modifications in the nuclear lamina structure by the removal of somatic proteins and the incorporation of oocyte/egg components may contribute to the reprogramming of somatic cell nuclei and may define a characteristic configuration of pluripotent cells.

Citing Articles

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Nuclear import of Xenopus egg extract components into cultured cells for reprogramming purposes: a case study on goldfish fin cells.

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Cancer reversion with oocyte extracts is mediated by cell cycle arrest and induction of tumour dormancy.

Saad N, Alberio R, Johnson A, Emes R, Giles T, Clarke P Oncotarget. 2018; 9(22):16008-16027.

PMID: 29662623 PMC: 5882314. DOI: 10.18632/oncotarget.24664.