Regulation of DNA repair in serum-stimulated xeroderma pigmentosum cells.

Gupta, Pawan; Sirover, Michael A.

doi:10.1083/jcb.99.4.1275

Cited by 7 publications

(1 citation statement)

References 48 publications

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“…Like individuals with Bloom syndrome, those with ataxia telangiectasia and xeroderma pigmentosum are cancer prone (19). Further, xeroderma pigmentosum cells of complementation groups A, C, and D fail to enhance nucleotide-excision repair during the cell cycle (29). However, each complementation group regulates in a normal fashion both base-excision repair and the uracil DNA glycosylase.…”

Section: Resultsmentioning

confidence: 99%

Immunological lesions in human uracil DNA glycosylase: association with Bloom syndrome.

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Brech

Karp

et al. 1988

Proc. Natl. Acad. Sci. U.S.A.

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Three monoclonal antibodies that react with uracil DNA glycosylase of normal human placenta were tested to determine whether one of the antibodies could be used as a negative marker for Bloom syndrome. As defined by enzyme-linked immunosorbent assay, monoclonal antibody 40.10.09, which reacts with normal human glycosylase, neither recognized nor inhibited native uracil DNA glycosylase from any of five separate Bloom syndrome cell strains. Immunoblot analyses demonstrated that the denatured glycosylase protein from all five Bloom syndrome cell strains was immunoreactive with the 40.10.09 antibody. Further, each native enzyme was immunoreactive with two other anti-human placental uracil DNA glycosylase monoclonal antibodies. In contrast, ELISA reactivity was observed with all three monoclonal antibodies in reactions of glycosylases from 5 normal human cell types and 13 abnormal human cell strains. These results experimentally verify the specificity of the aberrant reactivity of the Bloom syndrome uracil DNA glycosylase. The possibility arises that determination of the lack of immunoreactivity with antibody 40.10.09 may have value in the early diagnosis of Bloom syndrome.

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Section: Resultsmentioning

confidence: 99%

Immunological lesions in human uracil DNA glycosylase: association with Bloom syndrome.

Seal

Brech

Karp

et al. 1988

Proc. Natl. Acad. Sci. U.S.A.

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Problems and paradigms: Fine tuning of DNA repair in transcribed genes: Mechanisms, prevalence and consequences

1993

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Cells fine-tune their DNA repair, selecting some regions of the genome in preference to others. In the paradigm case, excision of UV-induced pyrimidine dimers in mammalian cells, repair is concentrated in transcribed genes, especially in the transcribed strand. This is due both to chromatin structure being looser in transcribing domains, allowing more rapid repair, and to repair enzymes being coupled to RNA polymerases stalled at damage sites; possibly other factors are also involved. Some repair-defective diseases may involve repair-transcription coupling: three candidate genes have been suggested. However, preferential excision of pyrimidine dimers is not uniformly linked to transcription. In mammals it varies with species, and with cell differentiation. In Drosophila embryo cells it is absent, and in yeast, the determining factor is nucleosome stability rather than transcription. Repair of other damage departs further from the paradigm, even in some UV-mimetic lesions. No selectivity is known for repair of the very frequent minor forms of base damage. And the most interesting consequence of selective repair, selective mutagenesis, normally occurs for UV-induced, but not for spontaneous mutations. The temptation to extrapolate from mammalian UV repair should be resisted.

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Detection of Unique Antigenic Lesions in the Uracil DNA Glycosylase from Bloom’s Syndrome

Sirover

Seal

Vollberg

et al. 1989

DNA Repair Mechanisms and Their Biological Implications in Mammalian Cells

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Regulation of DNA repair in serum-stimulated xeroderma pigmentosum cells.

Cited by 7 publications

References 48 publications

Immunological lesions in human uracil DNA glycosylase: association with Bloom syndrome.

Immunological lesions in human uracil DNA glycosylase: association with Bloom syndrome.

Problems and paradigms: Fine tuning of DNA repair in transcribed genes: Mechanisms, prevalence and consequences

Detection of Unique Antigenic Lesions in the Uracil DNA Glycosylase from Bloom’s Syndrome

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