A potential role for p15Ink4b and p57Kip2 in liver development

Abstract

Hepatocytes undergo marked changes in proliferation during normal liver development. In order to elucidate the mechanism for these changes, we examined the ontogeny of expression for the known cyclin‐dependent kinase inhibitors (CKIs), p15^Ink4b, p16^Ink4a, p18^Ink4c, p19^Ink4d, p21^Cip1, p27^Kip1 and p57^Kip2. All except p16^Ink4a were expressed at some time between late gestation and adulthood. The mRNA and protein expression patterns for p15^Ink4b and p57^Kip2 were consistent with a role for these CKIs in the regulation of hepatocyte proliferation. Specifically, p57^Kip2 may contribute to hepatocyte growth arrest that occurs in term fetuses, while p15^Ink4b may contribute to the maintenance of adult hepatocytes in a quiescent state. These results assign a possible role to two CKIs not previously identified as involved in hepatocyte cell cycle control.