| Literature DB >> 31406347 |
Sahar Nissim1,2,3,4, Ignaty Leshchiner2,5, Joseph D Mancias3,6, Matthew B Greenblatt7, Ophélia Maertens2, Christopher A Cassa2, Jill A Rosenfeld8, Andrew G Cox9,10, John Hedgepeth2, Julia I Wucherpfennig2, Andrew J Kim2, Jake E Henderson2, Patrick Gonyo11, Anthony Brandt11, Ellen Lorimer11, Bethany Unger11, Jeremy W Prokop12, Jerry R Heidel13, Xiao-Xu Wang3, Chinedu I Ukaegbu3, Benjamin C Jennings14, Joao A Paulo6, Sebastian Gableske3, Carol A Fierke14, Gad Getz5,15, Shamil R Sunyaev2,16, J Wade Harper6, Karen Cichowski2,3, Alec C Kimmelman17, Yariv Houvras18, Sapna Syngal1,3, Carol Williams11, Wolfram Goessling19,20,21,22,23,24.
Abstract
Pancreatic ductal adenocarcinoma is an aggressive cancer with limited treatment options1. Approximately 10% of cases exhibit familial predisposition, but causative genes are not known in most families2. We perform whole-genome sequence analysis in a family with multiple cases of pancreatic ductal adenocarcinoma and identify a germline truncating mutation in the member of the RAS oncogene family-like 3 (RABL3) gene. Heterozygous rabl3 mutant zebrafish show increased susceptibility to cancer formation. Transcriptomic and mass spectrometry approaches implicate RABL3 in RAS pathway regulation and identify an interaction with RAP1GDS1 (SmgGDS), a chaperone regulating prenylation of RAS GTPases3. Indeed, the truncated mutant RABL3 protein accelerates KRAS prenylation and requires RAS proteins to promote cell proliferation. Finally, evidence in patient cohorts with developmental disorders implicates germline RABL3 mutations in RASopathy syndromes. Our studies identify RABL3 mutations as a target for genetic testing in cancer families and uncover a mechanism for dysregulated RAS activity in development and cancer.Entities:
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Year: 2019 PMID: 31406347 PMCID: PMC7159804 DOI: 10.1038/s41588-019-0475-y
Source DB: PubMed Journal: Nat Genet ISSN: 1061-4036 Impact factor: 38.330