Macrophage capping protein CapG is a putative oncogene involved in migration and invasiveness in ovarian carcinoma.
J GlaserM H D NeumannQi MeiB BetzN SeierI BeyerT FehmH NeubauerD NiederacherM C FleischPublished in: BioMed research international (2014)
The actin binding protein CapG modulates cell motility by interacting with the cytoskeleton. CapG is associated with tumor progression in different nongynecologic tumor entities and overexpression in breast cancer cell lines correlates with a more invasive phenotype in vitro. Here, we report a significant CapG overexpression in 18/47 (38%) of ovarian carcinomas (OC) analyzed by qRealTime-PCR analyses. Functional analyses in OC cell lines through siRNA mediated CapG knockdown and CapG overexpression showed CapG-dependent cell migration and invasiveness. A single nucleotide polymorphism rs6886 inside the CapG gene was identified, affecting a CapG phosphorylation site and thus potentially modifying CapG function. The minor allele frequency (MAF) of SNP rs6886 (c.1004A/G) was higher and the homozygous (A/A, His335) genotype was significantly more prevalent in patients with fallopian tube carcinomas (50%) as in controls (10%). With OC being one of the most lethal cancer diseases, the detection of novel biomarkers such as CapG could reveal new diagnostic and therapeutic targets. Moreover, in-depth analyses of SNP rs6886 related to FTC and OC will contribute to a better understanding of carcinogenesis and progression of OC.
Keyphrases
- cell migration
- genome wide
- binding protein
- cell proliferation
- transcription factor
- single cell
- high grade
- poor prognosis
- gene expression
- staphylococcus aureus
- real time pcr
- mesenchymal stem cells
- drug delivery
- cystic fibrosis
- cell therapy
- biofilm formation
- long non coding rna
- genome wide identification
- protein kinase
- drug induced
- amino acid