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: UMLS:C0476089 (
endometrial cancer
)
11,379
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The purpose of this study was to determine whether the human
APEX
and OGG1 genes, encoding proteins important in base excision repair (BER) of DNA, contain nucleotide sequence polymorphisms or are mutated somatically in tumors from women diagnosed with ovarian or
endometrial cancer
. Based upon the analysis of germline DNA from 83 individuals, 63 with ovarian cancer and 20 with
endometrial cancer
, we found two missense polymorphisms in
APEX
(Q51H and D 148E) and two missense (A3P and S326C) and one intronic (Exon 5-15 bp) polymorphism in OGG1. The frequencies of the various alleles (in the ovarian and
endometrial cancer
patients combined) were 4.8% for 51-His and 56.2% for 148-Glu in
APEX
, and 1.0% for 3-Pro and 20.0% for 326-Cys in OGG1. Somatic mutations in
APEX
(P112L, W188X and R237C) were identified in three of 20 endometrial tumors, but no mutations were identified in
APEX
in 43 ovarian tumors, or in OGG1 at either tumor site. Given the crucial role of the
APEX
and OGG1 proteins in BER of oxidative DNA damage, the identified polymorphisms are good candidates for genetic epidemiologic studies of cancer susceptibility, while the finding that three of 20 (15%) endometrial tumors have somatic mutations in
APEX
suggests that inactivation of the BER pathway is important for the development of
endometrial cancer
in at least a subset of cases.
...
PMID:Common polymorphisms and somatic mutations in human base excision repair genes in ovarian and endometrial cancers. 1146 42
Several polymorphisms in the DNA repair gene are thought to have significant effects on cancer risk. In this study, we investigated the association of the polymorphisms in the DNA repair genes, XRCC1 Arg399Gln, XRCC3 Thr241Met, XPD Lys751Gln, XPG Asp1104His,
APE1
Asp148Glu, and HOGG1 Ser326Cys, with endometrium cancer risk. Two hundred and sixty-two women were included in the study. Endometrial biopsy was performed, and on the basis of diagnosis and histological examination, women were divided into two groups: a control group (n=158) and an
endometrial cancer
group (n=104). Genotypes were determined by PCR-RFLP assays in
endometrial carcinoma
patients and age-matched controls. In this study, we found that the frequencies of Glu+ and Asp/Glu genotypes in APE, Gln/Gln genotype of XRCC1, Met/Met genotype of XRCC3, Cys+ and Ser/Cys genotypes of HOGG1, His+ and Asp/His genotypes of XPG, and Gln+ and Gln/Gln genotypes of XPD are more prevalent in patients than controls. Frequencies of Thr/Thr genotype in XRCC3 were increased in controls compared with patients and seem to be protected from
endometrial cancer
. Our findings suggest that XRCC1, XRCC3, XPD, XPG,
APE1
, and HOGG1 genetic variants may be associated with
endometrial cancer
in Turkish women.
...
PMID:DNA repair gene variants in endometrial carcinoma. 2227 35
Apurinic/apyrimidinic endonuclease 1 (APE1) is the predominant AP site repair enzyme in mammals. APE1 also maintains 3'-5' exonuclease and 3'-repair activities, and regulates transcription factor DNA binding through its
REF-1
function. Since complete or severe APE1 deficiency leads to embryonic lethality and cell death, it has been hypothesized that APE1 protein variants with slightly impaired function will contribute to disease etiology. Our data indicate that except for the
endometrial cancer
-associated APE1 variant R237C, the polymorphic variants Q51H, I64V and D148E, the rare population variants G241R, P311S and A317V, and the tumor-associated variant P112L exhibit normal thermodynamic stability of protein folding; abasic endonuclease, 3'-5' exonuclease and
REF-1
activities; coordination during the early steps of base excision repair; and intracellular distribution when expressed exogenously in HeLa cells. The R237C mutant displayed reduced AP-DNA complex stability, 3'-5' exonuclease activity and 3'-damage processing. Re-sequencing of the exonic regions of APE1 uncovered no novel amino acid substitutions in the 60 cancer cell lines of the NCI-60 panel, or in HeLa or T98G cancer cell lines; only the common D148E and Q51H variants were observed. Our results indicate that APE1 missense mutations are seemingly rare and that the cancer-associated R237C variant may represent a reduced-function susceptibility allele.
...
PMID:Functional assessment of population and tumor-associated APE1 protein variants. 2377 69
