Litcius/Paper detail

Loss of SELENOF Induces the Transformed Phenotype in Human Immortalized Prostate Epithelial Cells

Lenny K. Hong, Shrinidhi Kadkol, Maria Sverdlov, Irida Kastrati, Mostafa Elhodaky, Ryan Deaton, Karen S. Sfanos, Heidi Wang, Li Liu, Alan M. Diamond

2021International Journal of Molecular Sciences10 citationsDOIOpen Access PDF

Abstract

SELENOF is a member of the class of selenoproteins in which the amino acid selenocysteine is co-translationally inserted into the elongating peptide in response to an in-frame UGA codon located in the 3'-untranslated (3'-UTR) region of the SELENOF mRNA. Polymorphisms in the 3'-UTR are associated with an increased risk of dying from prostate cancer and these variations are functional and 10 times more frequent in the genomes of African American men. SELENOF is dramatically reduced in prostate cancer compared to benign adjacent regions. Using a prostate cancer tissue microarray, it was previously established that the reduction of SELENOF in the cancers from African American men was significantly greater than in cancers from Caucasian men. When SELENOF levels in human prostate immortalized epithelial cells were reduced with an shRNA construct, those cells acquired the ability to grow in soft agar, increased the ability to migrate in a scratch assay and acquired features of energy metabolism associated with prostate cancer. These results support a role of SELENOF loss in prostate cancer progression and further indicate that SELENOF loss and genotype may contribute to the disparity in prostate cancer mortality experienced by African American men.

Topics & Concepts

Prostate cancerProstateCancerBiologyCancer researchPhenotypeSelenoproteinUntranslated regionGeneInternal medicineMedicineEndocrinologyGeneticsMessenger RNAOxidative stressSuperoxide dismutaseGlutathione peroxidaseSelenium in Biological SystemsTrace Elements in HealthGlutathione Transferases and Polymorphisms
Loss of SELENOF Induces the Transformed Phenotype in Human Immortalized Prostate Epithelial Cells | Litcius