Persistence of p53 mutations and resistance of keratinocytes to apoptosis are associated with the increased susceptibility of mice lacking the XPC gene to UV carcinogenesis. - Wikidata - wikimedia - TriplyDB

Persistence of p53 mutations and resistance of keratinocytes to apoptosis are associated with the increased susceptibility of mice lacking the XPC gene to UV carcinogenesis.

Persistence of p53 mutations and resistance of keratinocytes to apoptosis are associated with the increased susceptibility of mice lacking the XPC gene to UV carcinogenesis.

http://www.wikidata.org/entity/Q30827983

about

Differential role of transcription-coupled repair in UVB-induced G2 arrest and apoptosis in mouse epidermis Error-prone translesion replication of damaged DNA suppresses skin carcinogenesis by controlling inflammatory hyperplasia The DNA damage-binding protein XPC is a frequent target for inactivation in squamous cell carcinomas XPC silencing in normal human keratinocytes triggers metabolic alterations that drive the formation of squamous cell carcinomas.p53 suppression overwhelms DNA polymerase eta deficiency in determining the cellular UV DNA damage response Reduced XPC DNA repair gene mRNA levels in clinically normal parents of xeroderma pigmentosum patients.Catalase overexpression reduces UVB-induced apoptosis in a human xeroderma pigmentosum reconstructed epidermis.

P2860

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P2860

Persistence of p53 mutations and resistance of keratinocytes to apoptosis are associated with the increased susceptibility of mice lacking the XPC gene to UV carcinogenesis.

http://www.wikidata.org/entity/Q30827983

description

1999 nî lūn-bûn

@nan

1999 թուականի Դեկտեմբերին հրատարակուած գիտական յօդուած

@hyw

1999 թվականի դեկտեմբերին հրատարակված գիտական հոդված

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1999年の論文

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1999年論文

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1999年論文

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1999年論文

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1999年論文

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1999年論文

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1999年论文

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Persistence of p53 mutations a ...... XPC gene to UV carcinogenesis.

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Persistence of p53 mutations a ...... XPC gene to UV carcinogenesis.

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Persistence of p53 mutations a ...... XPC gene to UV carcinogenesis.

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Persistence of p53 mutations a ...... XPC gene to UV carcinogenesis.

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Persistence of p53 mutations a ...... XPC gene to UV carcinogenesis.

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Ananthaswamy HN

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Conti CJ

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Evans RL

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Khaskina P

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P2860

p53 modulation of TFIIH-associated nucleotide excision repair activity

p53 mutations in human cancers

XPA-deficiency in hairless mice causes a shift in skin tumor types and mutational target genes after exposure to low doses of U.V.B.

Defective repair replication of DNA in xeroderma pigmentosum.

Structure and function of the p53 tumor suppressor gene: clues for rational cancer therapeutic strategies.

p53 function and dysfunction.

The residual repair capacity of xeroderma pigmentosum complementation group C fibroblasts is highly specific for transcriptionally active DNA

Evidence that xeroderma pigmentosum cells do not perform the first step in the repair of ultraviolet damage to their DNA.

High incidence of ultraviolet-B-or chemical-carcinogen-induced skin tumours in mice lacking the xeroderma pigmentosum group A gene.

Increased susceptibility to ultraviolet-B and carcinogens of mice lacking the DNA excision repair gene XPA.

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10.1038/SJ.ONC.1203147

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51

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18

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1999-12-01T00:00:00Z

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10602497

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