Author:
Robles Ana I.,Rodriguez-Puebla Marcelo L.,Glick Adam B.,Trempus Carol,Hansen Laura,Sicinski Piotr,Tennant Raymond W.,Weinberg Robert A.,Yuspa Stuart H.,Conti Claudio J.
Abstract
Cyclin D1 is part of a cell cycle control node consistently deregulated in most human cancers. However, studies with cyclin D1-null mice indicate that it is dispensable for normal mouse development as well as cell growth in culture. Here, we provide evidence thatras-mediated tumorigenesis depends on signaling pathways that act preferentially through cyclin D1. Cyclin D1 expression and the activity of its associated kinase are up-regulated in keratinocytes in response to oncogenic ras. Furthermore, cyclin D1 deficiency results in up to an 80% decrease in the development of squamous tumors generated through either grafting of retroviral ras-transduced keratinocytes, phorbol ester treatment of ras transgenic mice, or two-stage carcinogenesis.
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
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