posted on 2023-03-31, 03:10authored byK Mackenzie, NJ Foot, Sushma Anand, HE Dalton, N Chaudhary, BM Collins, Suresh MathivananSuresh Mathivanan, S Kumar
The release of extracellular vesicles (EVs) is important for both normal physiology and disease. However, a basic understanding of the targeting of EV cargoes, composition and mechanism of release is lacking. Here we present evidence that the divalent metal ion transporter (DMT1) is unexpectedly regulated through release in EVs. This process involves the Nedd4-2 ubiquitin ligase, and the adaptor proteins Arrdc1 and Arrdc4 via different budding mechanisms. We show that mouse gut explants release endogenous DMT1 in EVs. Although we observed no change in the relative amount of DMT1 released in EVs from gut explants in Arrdc1 or Arrdc4 deficient mice, the extent of EVs released was significantly reduced indicating an adaptor role in biogenesis. Furthermore, using Arrdc1 or Arrdc4 knockout mouse embryonic fibroblasts, we show that both Arrdc1 and Arrdc4 are non-redundant positive regulators of EV release. Our results suggest that DMT1 release from the plasma membrane into EVs may represent a novel mechanism for the maintenance of iron homeostasis, which may also be important for the regulation of other membrane proteins.
Funding
This work was supported by the National Health and Medical Research Council (NHMRC) project grants (1059393) and a NHMRC Senior Principal Research Fellowship (1103006) to SK. BMC is supported by a NHMRC Career Development Fellowship (1061574).
History
Publication Date
2016-06-21
Journal
Cell Discovery
Volume
2
Issue
1
Article Number
16011
Pagination
14p. (p. 1-14)
Publisher
Springer Nature
ISSN
2056-5968
Rights Statement
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