| Literature DB >> 27974362 |
Emilia Peuhu1, Riina Kaukonen2, Martina Lerche2, Markku Saari2, Camilo Guzmán2, Pia Rantakari3,4, Nicola De Franceschi2, Anni Wärri2, Maria Georgiadou2, Guillaume Jacquemet2, Elina Mattila2, Reetta Virtakoivu2, Yuming Liu5, Youmna Attieh6, Kathleen A Silva7, Timo Betz6,8, John P Sundberg7, Marko Salmi3,4, Marie-Ange Deugnier6,9, Kevin W Eliceiri5, Johanna Ivaska1,10.
Abstract
SHARPIN is a widely expressed multifunctional protein implicated in cancer, inflammation, linear ubiquitination and integrin activity inhibition; however, its contribution to epithelial homeostasis remains poorly understood. Here, we examined the role of SHARPIN in mammary gland development, a process strongly regulated by epithelial-stromal interactions. Mice lacking SHARPIN expression in all cells (Sharpincpdm), and mice with a stromal (S100a4-Cre) deletion of Sharpin, have reduced mammary ductal outgrowth during puberty. In contrast, Sharpincpdm mammary epithelial cells transplanted in vivo into wild-type stroma, fully repopulate the mammary gland fat pad, undergo unperturbed ductal outgrowth and terminal differentiation. Thus, SHARPIN is required in mammary gland stroma during development. Accordingly, stroma adjacent to invading mammary ducts of Sharpincpdm mice displayed reduced collagen arrangement and extracellular matrix (ECM) stiffness. Moreover, Sharpincpdm mammary gland stromal fibroblasts demonstrated defects in collagen fibre assembly, collagen contraction and degradation in vitro Together, these data imply that SHARPIN regulates the normal invasive mammary gland branching morphogenesis in an epithelial cell extrinsic manner by controlling the organisation of the stromal ECM.Entities:
Keywords: zzm321990SHARPINzzm321990; collagen; ductal morphogenesis; fibroblast; mammary gland
Mesh:
Substances:
Year: 2016 PMID: 27974362 PMCID: PMC5239997 DOI: 10.15252/embj.201694387
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598