Literature DB >> 8423773

Defective replication of psoralen adducts detected at the gene-specific level in xeroderma pigmentosum variant cells.

R R Misra1, J M Vos.   

Abstract

Replication of damaged DNA is suspected to play an important role in cell cycle, genetic stability, and survival pathways. Using psoralen photoaddition as prototype DNA damage and the renaturing agarose gel electrophoresis technique to measure DNA cross-linking in individual genes, Vos and Hanawalt previously observed efficient bypass replication of psoralen monoadducts in human genes (J.-M. H. Vos and P. C. Hanawalt, Cell 50:789-799, 1987). To understand the mechanism of bypass replication in human cells, mutants affected in such a process would be useful. We now report that cells from individuals suffering from the hereditary recessive syndrome xeroderma pigmentosum variant (XPV) are hypersensitive to killing induced by photoactivated psoralen. In addition, analysis of psoralen-mediated DNA cross-linking in the rRNA genes indicated that although repair of psoralen adducts was similar to that of normal individuals, XPV cells were markedly deficient in the ability to bypass psoralen adducts during replication; in comparison with normal cells, approximately half as many monoadducts were bypassed during replication in XPV cells. Furthermore, in contrast to normal cells, replication of interstrand cross-links was not detected in XPV. This is the first demonstration of a deficiency in bypass replication detected at the gene-specific level in vivo. A model involving a strand-specific defect in recombinational bypass in XPV is proposed.

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Year:  1993        PMID: 8423773      PMCID: PMC358985          DOI: 10.1128/mcb.13.2.1002-1012.1993

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  31 in total

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3.  Postreplication repair: questions of its definition and possible alteration in xeroderma pigmentosum cell strains.

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9.  Defective and enhanced postreplication repair in classical and variant xeroderma pigmentosum cells treated with N-acetoxy-2-acetylaminofluorene.

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Authors:  A N Moshell; R E Tarone; S A Newfield; A D Andrews; J H Robbins
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  16 in total

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6.  Human HMGB1 directly facilitates interactions between nucleotide excision repair proteins on triplex-directed psoralen interstrand crosslinks.

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7.  Strand specificity of mutagenic bypass replication of DNA containing psoralen monoadducts in a human cell extract.

Authors:  D C Thomas; D L Svoboda; J M Vos; T A Kunkel
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8.  DNA polymerase eta reduces the gamma-H2AX response to psoralen interstrand crosslinks in human cells.

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9.  Effect of cross-link structure on DNA interstrand cross-link repair synthesis.

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