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Development, maturation, and maintenance of human prostate inferred from somatic mutations

Title: Development, maturation, and maintenance of human prostate inferred from somatic mutations
Authors: Grossmann S; Hooks Y; Wilson L; Moore L; O'Neill L; Martincorena I; Voet T; Stratton MR; Heer R; Campbell PJ
Source: Cell Stem Cell, 2021
Publisher Information: Cell Press
Publication Year: 2021
Collection: Newcastle University Library ePrints Service
Description: © 2021 The Authors. Clonal dynamics and mutation burden in healthy human prostate epithelium are relevant to prostate cancer. We sequenced whole genomes from 409 microdissections of normal prostate epithelium across 8 donors, using phylogenetic reconstruction with spatial mapping in a 59-year-old man's prostate to reconstruct tissue dynamics across the lifespan. Somatic mutations accumulate steadily at ∼16 mutations/year/clone, with higher rates in peripheral than peri-urethral regions. The 24–30 independent glandular subunits are established as rudimentary ductal structures during fetal development by 5–10 embryonic cells each. Puberty induces formation of further side and terminal branches by local stem cells disseminated throughout the rudimentary ducts during development. During adult tissue maintenance, clonal expansions have limited geographic scope and minimal migration. Driver mutations are rare in aging prostate epithelium, but the one driver we did observe generated a sizable intraepithelial clonal expansion. Leveraging unbiased clock-like mutations, we define prostate stem cell dynamics through fetal development, puberty, and aging. Using spontaneously occurring somatic mutations as lineage marks, Campbell, Heer, and colleagues define the stem cell dynamics of normal human prostate epithelium through fetal development, puberty, adulthood, and aging.
Document Type: article in journal/newspaper
File Description: application/pdf
Language: unknown
Relation: https://eprints.ncl.ac.uk/274232; https://eprints.ncl.ac.uk/fulltext.aspx?url=274232/274D07D8-CBA3-4630-9522-C009DEBC7374.pdf&pub_id=274232
Availability: https://eprints.ncl.ac.uk/274232
Rights: https://creativecommons.org/licenses/by/4.0/
Accession Number: edsbas.A29F43A3
Database: BASE