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Publication : Prostate cancer sheds the αvβ3 integrin in vivo through exosomes.

First Author  Krishn SR Year  2019
Journal  Matrix Biol Volume  77
Pages  41-57 PubMed ID  30098419
Mgi Jnum  J:275732 Mgi Id  MGI:6313467
Doi  10.1016/j.matbio.2018.08.004 Citation  Krishn SR, et al. (2019) Prostate cancer sheds the alphavbeta3 integrin in vivo through exosomes. Matrix Biol 77:41-57
abstractText  The alphavbeta3 integrin has been shown to promote aggressive phenotypes in many types of cancers, including prostate cancer. We show that GFP-labeled alphavbeta3 derived from cancer cells circulates in the blood and is detected in distant lesions in NOD scid gamma (NSG) mice. We, therefore, hypothesized that alphavbeta3 travels through exosomes and tested its levels in pools of vesicles, which we designate extracellular vesicles highly enriched in exosomes (ExVs), and in exosomes isolated from the plasma of prostate cancer patients. Here, we show that the alphavbeta3 integrin is found in patient blood exosomes purified by sucrose or iodixanol density gradients. In addition, we provide evidence that the alphavbeta3 integrin is transferred through ExVs isolated from prostate cancer patient plasma to beta3-negative recipient cells. We also demonstrate the intracellular localization of beta3-GFP transferred via cancer cell-derived ExVs. We show that the ExVs present in plasma from prostate cancer patients contain higher levels of alphavbeta3 and CD9 as compared to plasma ExVs from age-matched subjects who are not affected by cancer. Furthermore, using PSMA antibody-bead mediated immunocapture, we show that the alphavbeta3 integrin is expressed in a subset of exosomes characterized by PSMA, CD9, CD63, and an epithelial-specific marker, Trop-2. Finally, we present evidence that the levels of alphavbeta3, CD63, and CD9 remain unaltered in ExVs isolated from the blood of prostate cancer patients treated with enzalutamide. Our results suggest that detecting exosomal alphavbeta3 integrin in prostate cancer patients could be a clinically useful and non-invasive biomarker to follow prostate cancer progression. Moreover, the ability of alphavbeta3 integrin to be transferred from ExVs to recipient cells provides a strong rationale for further investigating the role of alphavbeta3 integrin in the pathogenesis of prostate cancer and as a potential therapeutic target.
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