نتایج جستجو برای: dna repair

تعداد نتایج: 607978  

Journal: :Mutagenesis 2007
Filipe V Jacinto Manel Esteller

Human cancers exhibit genomic instability and an increased mutation rate due to underlying defects in DNA repair genes. Hypermethylation of CpG islands in gene promoter regions is an important mechanism of gene inactivation in cancer. Many cellular pathways, including DNA repair, are inactivated by this type of epigenetic lesion, resulting in mutator pathways. In this review, we discuss the adv...

Journal: :Molecular carcinogenesis 2015
Jana Slyskova Francesca Cordero Barbara Pardini Vlasta Korenkova Veronika Vymetalkova Ludovit Bielik Ludmila Vodickova Pavel Pitule Vaclav Liska Vit Martin Matejka Miroslav Levy Tomas Buchler Mikael Kubista Alessio Naccarati Pavel Vodicka

DNA repair in blood cells was observed to be suboptimal in cancer patients at diagnosis, including colorectal cancer (CRC). To explore the causality of this phenomenon, we studied the dynamics of DNA repair from diagnosis to 1 yr follow-up, and with respect to CRC treatment. Systemic CRC therapy is targeted to DNA damage induction and DNA repair is thus of interest. CRC patients were blood-samp...

Journal: :Current Biology 1998
Richard D. Wood

Recent studies have investigated whether particular DNA repair pathways are involved in the somatic hypermutation mechanism that increases antibody diversity. The primary mutation mechanism still functions in mice carrying knockouts of all repair genes examined, but mismatch repair defects affect the final outcome.

Journal: :Cancer research 1991
J Hansson S M Keyse T Lindahl R D Wood

Whole cell extracts from human lymphoid cell lines can perform in vitro DNA repair synthesis in plasmids damaged by agents including UV or cis-diamminedichloroplatinum(II) (cis-DDP). Extracts from xeroderma pigmentosum (XP) cells are defective in repair synthesis. We have now studied in vitro DNA repair synthesis using extracts from lymphoblastoid cell lines representing four human hereditary s...

Journal: :Science 1998
B E Nelms R S Maser J F MacKay M G Lagally J H Petrini

A method was developed to examine DNA repair within the intact cell. Ultrasoft x-rays were used to induce DNA double-strand breaks (DSBs) in defined subnuclear volumes of human fibroblasts and DNA repair was visualized at those sites. The DSBs remained in a fixed position during the initial stages of DNA repair, and the DSB repair protein hMre11 migrated to the sites of damage within 30 minutes...

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