| Literature DB >> 32165588 |
Sampath K Loganathan1, Krista Schleicher1,2, Ahmad Malik1,2, Rene Quevedo3,4, Ellen Langille1,2, Katie Teng1, Robin H Oh1,2, Bhavisha Rathod1, Ricky Tsai1, Payman Samavarchi-Tehrani1, Trevor J Pugh3,4,5, Anne-Claude Gingras1,2, Daniel Schramek6,2.
Abstract
In most human cancers, only a few genes are mutated at high frequencies; most are mutated at low frequencies. The functional consequences of these recurrent but infrequent "long tail" mutations are often unknown. We focused on 484 long tail genes in head and neck squamous cell carcinoma (HNSCC) and used in vivo CRISPR to screen for genes that, upon mutation, trigger tumor development in mice. Of the 15 tumor-suppressor genes identified, ADAM10 and AJUBA suppressed HNSCC in a haploinsufficient manner by promoting NOTCH receptor signaling. ADAM10 and AJUBA mutations or monoallelic loss occur in 28% of human HNSCC cases and are mutually exclusive with NOTCH receptor mutations. Our results show that oncogenic mutations in 67% of human HNSCC cases converge onto the NOTCH signaling pathway, making NOTCH inactivation a hallmark of HNSCC.Entities:
Year: 2020 PMID: 32165588 DOI: 10.1126/science.aax0902
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728