| Literature DB >> 28077876 |
Nadja S Katheder1,2, Rojyar Khezri1,2, Fergal O'Farrell1,2, Sebastian W Schultz1,2, Ashish Jain1,2,3, Mohammed M Rahman1,2, Kay O Schink1,2, Theodossis A Theodossiou4, Terje Johansen3, Gábor Juhász5,6, David Bilder7, Andreas Brech1,2, Harald Stenmark1,2, Tor Erik Rusten1,2.
Abstract
As malignant tumours develop, they interact intimately with their microenvironment and can activate autophagy, a catabolic process which provides nutrients during starvation. How tumours regulate autophagy in vivo and whether autophagy affects tumour growth is controversial. Here we demonstrate, using a well characterized Drosophila melanogaster malignant tumour model, that non-cell-autonomous autophagy is induced both in the tumour microenvironment and systemically in distant tissues. Tumour growth can be pharmacologically restrained using autophagy inhibitors, and early-stage tumour growth and invasion are genetically dependent on autophagy within the local tumour microenvironment. Induction of autophagy is mediated by Drosophila tumour necrosis factor and interleukin-6-like signalling from metabolically stressed tumour cells, whereas tumour growth depends on active amino acid transport. We show that dormant growth-impaired tumours from autophagy-deficient animals reactivate tumorous growth when transplanted into autophagy-proficient hosts. We conclude that transformed cells engage surrounding normal cells as active and essential microenvironmental contributors to early tumour growth through nutrient-generating autophagy.Entities:
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Year: 2017 PMID: 28077876 PMCID: PMC5612666 DOI: 10.1038/nature20815
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962