Increase in proliferative markers after inhibition of transglutaminase.

Abstract

Cystamine inhibited transglutaminase activity of proliferating WI-38 [human lung] cells in a dose-dependent manner over the concentration range 0.005-0.25 mM when added to the culture medium. The .epsilon.-(.gamma.-glutamyl)lysine content in the cells was decreased and several proliferation markers were enhanced. Non-mitotic cells were stimulated by cystamine (about 25% of that observed with 10% fetal bovine serum) to undergo DNA synthesis with subsequent increases in nuclei number. Numerous other disulfides, thiols and amines were ineffective when added to culture medium. The findings are supportive of the concept that growth control involves a relationship between isopeptide crosslinks and proliferation.