Hydrogen sulfide induces serum-independent cell cycle entry in nontransformed rat intestinal epithelial cells

Hydrogen sulfide (H2S), produced by commensal sulfate-reducing bacteria, is an environmental insult that potentially contributes to chronic intestinal epithelial disorders. We tested the hypothesis that exposure of nontransformed intestinal epithelial cells (IEC-18) to the reducing agent sodium hydrogen sulfide (NaHS) activates molecular pathways that underlie epithelial hyperplasia, a phenotype common to both ulcerative colitis (UC) and colorectal cancer. Exposure of IEC-18 cells to NaHS rapidly increased the NADPH/NADP ratio, reduced the intracellular redox environment, and inhibited mitochondrial respiratory activity. The addition of 0.2-5 mM NaHS for 4 h increased the IEC-18 proliferative cell fraction (P

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Hydrogen sulfide induces serum-independent cell cycle entry in nontransformed rat intestinal epithelial cells

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Transposable elements mediate genetic effects altering the expression of nearby genes in colorectal cancer

Regulation and function of a hemicleaved Activin-A processing intermediate in melanoma

Gallocin A, an Atypical Two-Peptide Bacteriocin with Intramolecular Disulfide Bonds Required for Activity

Regulation and function of a hemicleaved Activin-A processing intermediate in melanoma

Gallocin A, an Atypical Two-Peptide Bacteriocin with Intramolecular Disulfide Bonds Required for Activity

Transposable elements mediate genetic effects altering the expression of nearby genes in colorectal cancer