Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:2.4.2.8 (
hypoxanthine-guanine phosphoribosyltransferase
)
2,527
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Mutant huntingtin lowered steady-state levels of DARPP-32 mRNA in the brain but not kidney of R6 transgenic HD mice by repressing transcription from one of two promoters. The activity of DARPP-32 promoter deletion constructs were lower in the presence of mutant huntingtin in immortalized striatal cell lines but no difference in transcription factor binding to the promoter was detected. The activity of CMV, TK and
HPRT
promoters was also affected by mutant huntingtin in these cell lines. Transient transfection experiments demonstrated that short-term expression of mutant huntingtin exerted a cell- and promoter-specific transcriptional repression. In in vitro experiments, transcription of the CMV promoter was reduced in the presence of striatal proteins and mutant huntingtin. It is likely that select combinations of trans-acting factors, co-activators and components of the
Pol
II holoenzyme acting in concert provide the basis for both the gene- and tissue-specific effects of mutant huntingtin.
...
PMID:Brain-specific factors in combination with mutant huntingtin induce gene-specific transcriptional dysregulation. 1644 1
Genes coding for DNA polymerases eta, iota and zeta, or for both
Pol
eta and Pol iota have been inactivated by homologous recombination in the Burkitt's lymphoma BL2 cell line, thus providing for the first time the total suppression of these enzymes in a human context. The UV sensitivities and UV-induced mutagenesis on an irradiated shuttle vector have been analyzed for these deficient cell lines. The double
Pol
eta/iota deficient cell line was more UV sensitive than the
Pol
eta-deficient cell line and mutation hotspots specific to the
Pol
eta-deficient context appeared to require the presence of Pol iota, thus strengthening the view that Pol iota is involved in UV damage translesion synthesis and UV-induced mutagenesis. A role for
Pol
zeta in a damage repair process at late replicative stages is reported, which may explain the drastic UV-sensitivity phenotype observed when this polymerase is absent. A specific mutation pattern was observed for the UV-irradiated shuttle vector transfected in
Pol
zeta-deficient cell lines, which, in contrast to mutagenesis at the
HPRT
locus previously reported, strikingly resembled mutations observed in UV-induced skin cancers in humans. Finally, a
Pol
eta PIP-box mutant (without its PCNA binding domain) could completely restore the UV resistance in a
Pol
eta deficient cell line, in the absence of UV-induced foci, suggesting, as observed for Pol iota in a
Pol
eta-deficient background, that TLS may occur without the accumulation of microscopically visible repair factories.
...
PMID:Role of DNA polymerases eta, iota and zeta in UV resistance and UV-induced mutagenesis in a human cell line. 1858 18
