Guanhua Yu scite author profile

In synchronized rat or mouse cells infected with Moloney murine leukemia virus (MLV), integration of viral DNA and production of viral proteins occur only after the cells traverse mitosis. Integration is blocked when cells are prevented from progressing through mitosis. Viral nucleoprotein complexes isolated from arrested cells contain full‐length viral DNA and can integrate this viral DNA in vitro, showing that the block to integration in arrested cells is not due to a lack of mature integration machinery. When infected cells traverse mitosis, there is a sharp increase in nuclear accumulation of viral DNA. The dependence of integration on mitosis may therefore be due to a requirement for mitosis and nuclear envelope breakdown for entry of the viral integration complex into the nucleus.

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Origin-Specific Initiation of Mammalian Nuclear DNA Replication in aXenopusCell-Free System

Gilbert

1997

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Analysis of mammalian origin specification in ORC-depleted Xenopus egg extracts

Yu¹

1998

Genes Cells

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Xenopus embryonic ORC is clearly not required for random origin site selection in Xenopus egg extracts. We conclude that a modification of Chinese Hamster chromatin takes place shortly after metaphase that complements a lack of XORC activity. This modification most likely represents an interaction of mammalian ORC with chromatin that is required for replication but, that is not sufficient for origin specification.

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Guanhua Yu

Integration of murine leukemia virus DNA depends on mitosis.

Origin-Specific Initiation of Mammalian Nuclear DNA Replication in aXenopusCell-Free System

Analysis of mammalian origin specification in ORC-depleted Xenopus egg extracts

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