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Sulfisoxazole inhibits the secretion of small extracellular vesicles by targeting the endothelin receptor A.

Eun-Ju ImChan-Hyeong LeePyong-Gon MoonGunassekaran Gowri RangaswamyByungheon LeeJae Man LeeJae-Chul LeeJun-Goo JeeJong-Sup BaeTaeg-Kyu KwonKeon-Wook KangMyeong-Seon JeongJoo-Eun LeeHyun-Suk JungHyun-Joo RoSangmi JunWonku KangSeung-Yong SeoYoung-Eun ChoByoung-Joon SongMoon-Chang Baek
Published in: Nature communications (2019)
Inhibitors of the secretion of cancer exosomes, which promote cancer progression and metastasis, may not only accelerate exosome biology research but also offer therapeutic benefits for cancer patients. Here we identify sulfisoxazole (SFX) as an inhibitor of small extracellular vesicles (sEV) secretion from breast cancer cells through interference with endothelin receptor A (ETA). SFX, an FDA-approved oral antibiotic, showed significant anti-tumor and anti-metastatic effects in mouse models of breast cancer xenografts, the reduced expression of proteins involved in biogenesis and secretion of sEV, and triggered co-localization of multivesicular endosomes with lysosomes for degradation. We demonstrate the important role of ETA, as target of SFX, by gain- and loss-of-function studies of the ETA protein, through a direct binding assay, and pharmacological and genetic approaches. These findings may provide a foundation for sEV-targeted cancer therapies and the mechanistic studies on sEV biology.
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