Differentiation of tumour-promoting stromal myofibroblasts by cancer exosomes

Activation of myofibroblast rich stroma is a rate-limiting step essential for cancer progression. The responsible factors are not fully understood, but TGFβ1 is probably critical. A proportion of TGFβ1 is associated with extracellular nano-vesicles termed exosomes, secreted by carcinoma cells, and t...

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Veröffentlicht in:Oncogene 2015-01, Vol.34 (3), p.290-302
Hauptverfasser: Webber, J P, Spary, L K, Sanders, A J, Chowdhury, R, Jiang, W G, Steadman, R, Wymant, J, Jones, A T, Kynaston, H, Mason, M D, Tabi, Z, Clayton, A
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Sprache:eng
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Zusammenfassung:Activation of myofibroblast rich stroma is a rate-limiting step essential for cancer progression. The responsible factors are not fully understood, but TGFβ1 is probably critical. A proportion of TGFβ1 is associated with extracellular nano-vesicles termed exosomes, secreted by carcinoma cells, and the relative importance of soluble and vesicular TGFβ in stromal activation is presented. Prostate cancer exosomes triggered TGFβ1-dependent fibroblast differentiation, to a distinctive myofibroblast phenotype resembling stromal cells isolated from cancerous prostate tissue; supporting angiogenesis in vitro and accelerating tumour growth in vivo . Myofibroblasts generated using soluble TGFβ1 were not pro-angiogenic or tumour-promoting. Cleaving heparan sulphate side chains from the exosome surface had no impact on TGFβ levels yet attenuated SMAD-dependent signalling and myofibroblastic differentiation. Eliminating exosomes from the cancer cell secretome, targeting Rab27a, abolished differentiation and lead to failure in stroma-assisted tumour growth in vivo . Exosomal TGFβ1 is therefore required for the formation of tumour-promoting stroma.
ISSN:0950-9232
1476-5594
DOI:10.1038/onc.2013.560