| Literature DB >> 35122047 |
David Gallo1, Frédéric Racicot2,3, Lukas Tamayo-Orrego2,4,5, Amandine Bemmo2, Sushmetha Mohan2,4, Brandon Ho1, Samer Salameh2, Trang Hoang6, Andrew P Jackson5, Grant W Brown1, Frédéric Charron7,8,9,10.
Abstract
The mechanisms generating cancer-initiating mutations are not well understood. Sonic hedgehog (SHH) pathway activation is frequent in medulloblastoma (MB), with PTCH1 mutations being a common initiating event. Here we investigated the role of the developmental mitogen SHH in initiating carcinogenesis in the cells of origin: granule cell progenitors (GCPs). We delineate a molecular mechanism for tumor initiation in MB. Exposure of GCPs to Shh causes a distinct form of DNA replication stress, increasing both origin firing and fork velocity. Shh promotes DNA helicase loading and activation, with increased Cdc7-dependent origin firing. The S-phase duration is reduced and hyper-recombination occurs, causing copy number neutral loss of heterozygosity-a frequent event at the PTCH1/ptch1 locus. Moreover, Cdc7 inhibition to attenuate origin firing reduces recombination and preneoplastic tumor formation in mice. Therefore, tissue-specific replication stress induced by Shh promotes loss of heterozygosity, which in tumor-prone Ptch1+/- GCPs results in loss of this tumor suppressor-an early cancer-initiating event.Entities:
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Year: 2020 PMID: 35122047 DOI: 10.1038/s43018-020-0094-7
Source DB: PubMed Journal: Nat Cancer ISSN: 2662-1347