AI Article Synopsis

  • E-Cadherin (CDH1) gene variations may affect cancer invasion and metastasis by changing transcriptional activity in epithelial cells, but studies on its link to cancer risk are inconsistent due to differing lifestyles and genetics.
  • A meta-analysis of 57 studies found that three specific CDH1 polymorphisms (-160 C>A, -347 G>GA, and 3'-UTR +54 C>T) were significantly associated with cancer risk, with varying effects depending on the type of cancer.
  • Results indicated that the -160 A allele increases prostate cancer risk, while it may decrease colorectal cancer risk; the -347 GAGA genotype heightens overall cancer risk, particularly in colorectal cancer among Asians, while the +

Article Abstract

E-Cadherin (CDH1) genetic variations may be involved in invasion and metastasis of various cancers by altering gene transcriptional activity of epithelial cells. However, published studies on the association of CDH1 gene polymorphisms and cancer risk remain contradictory, owing to differences in living habits and genetic backgrounds. To derive a more better and comprehensive conclusion, the present meta-analysis was performed including 57 eligible studies of the association between polymorphisms of CDH1 gene promoter -160 C>A, -347 G>GA and 3'-UTR +54 C>T and cancer risk. Results showed that these three polymorphisms of CDH1 were significantly associated with cancer risk. For -160 C>A polymorphism, -160A allele carriers (CA and CA+AA) had an increased risk of cancer compared with the homozygotes (CC), and the similar result was discovered for the -160A allele in the overall analyses. In the subgroup analyses, obvious elevated risk was found with -160A allele carriers (AA, CA, CA+AA and A allele) for prostate cancer, while a decreased colorectal cancer risk was shown with the AA genotype. For the -347 G>GA polymorphism, the GAGA genotype was associated with increased cancer risk in the overall analysis with homozygous and recessive models. In addition, results of subgroup analysis indicated that the elevated risks were observed in colorectal cancer and Asian descendants. For +54 C>T polymorphism, a decreased risk of cancer was found in heterozygous, dominant and allele models. Moreover, +54T allele carriers (CT, CT+TT genotype and T allele) showed a potential protective factor in gastric cancer and Asian descendants.

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Source
http://dx.doi.org/10.7314/apjcp.2014.15.8.3705DOI Listing

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