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The secretion and biological function of tumor suppressor maspin as an exosome cargo protein

Maspin is an epithelial-specific tumor suppressor shown to exert its biological effects as an intracellular, cell membrane-associated, and secreted free molecule. A recent study suggests that upon DNA-damaging g-irradiation, tumor cells can secrete maspin as an exosome-associated protein. To date, t...

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Autores principales: Dean, Ivory, Dzinic, Sijana H, Bernardo, M. Margarida, Zou, Yi, Kimler, Vickie, Li, Xiaohua, Kaplun, Alexander, Granneman, James, Mao, Guangzhao, Sheng, Shijie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5352381/
https://www.ncbi.nlm.nih.gov/pubmed/28009978
http://dx.doi.org/10.18632/oncotarget.13302
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author Dean, Ivory
Dzinic, Sijana H
Bernardo, M. Margarida
Zou, Yi
Kimler, Vickie
Li, Xiaohua
Kaplun, Alexander
Granneman, James
Mao, Guangzhao
Sheng, Shijie
author_facet Dean, Ivory
Dzinic, Sijana H
Bernardo, M. Margarida
Zou, Yi
Kimler, Vickie
Li, Xiaohua
Kaplun, Alexander
Granneman, James
Mao, Guangzhao
Sheng, Shijie
author_sort Dean, Ivory
collection PubMed
description Maspin is an epithelial-specific tumor suppressor shown to exert its biological effects as an intracellular, cell membrane-associated, and secreted free molecule. A recent study suggests that upon DNA-damaging g-irradiation, tumor cells can secrete maspin as an exosome-associated protein. To date, the biological significance of exosomal secretion of maspin is unknown. The current study aims at addressing whether maspin is spontaneously secreted as an exosomal protein to regulate tumor/stromal interactions. We prepared exosomes along with cell extracts and vesicle-depleted conditioned media (VDCM) from normal epithelial (CRL2221, MCF-10A and BEAS-2B) and cancer (LNCaP, PC3 and SUM149) cell lines. Atomic force microscopy and dynamic light scattering analysis revealed similar size distribution patterns and surface zeta potentials between the normal cells-derived and tumor cells-derived exosomes. Electron microscopy revealed that maspin was encapsulated by the exosomal membrane as a cargo protein. While western blotting revealed that the level of exosomal maspin from tumor cell lines was disproportionally lower relative to the levels of corresponding intracellular and VDCM maspin, as compared to that from normal cell lines, maspin knockdown in MCF-10A cells led to maspin-devoid exosomes, which exhibited significantly reduced suppressive effects on the chemotaxis activity of recipient NIH3T3 fibroblast cells. These data are the first to demonstrate the potential of maspin delivered by exosomes to block tumor-induced stromal response, and support the clinical application of exosomal maspin in cancer diagnosis and treatment.
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spelling pubmed-53523812017-04-14 The secretion and biological function of tumor suppressor maspin as an exosome cargo protein Dean, Ivory Dzinic, Sijana H Bernardo, M. Margarida Zou, Yi Kimler, Vickie Li, Xiaohua Kaplun, Alexander Granneman, James Mao, Guangzhao Sheng, Shijie Oncotarget Research Paper Maspin is an epithelial-specific tumor suppressor shown to exert its biological effects as an intracellular, cell membrane-associated, and secreted free molecule. A recent study suggests that upon DNA-damaging g-irradiation, tumor cells can secrete maspin as an exosome-associated protein. To date, the biological significance of exosomal secretion of maspin is unknown. The current study aims at addressing whether maspin is spontaneously secreted as an exosomal protein to regulate tumor/stromal interactions. We prepared exosomes along with cell extracts and vesicle-depleted conditioned media (VDCM) from normal epithelial (CRL2221, MCF-10A and BEAS-2B) and cancer (LNCaP, PC3 and SUM149) cell lines. Atomic force microscopy and dynamic light scattering analysis revealed similar size distribution patterns and surface zeta potentials between the normal cells-derived and tumor cells-derived exosomes. Electron microscopy revealed that maspin was encapsulated by the exosomal membrane as a cargo protein. While western blotting revealed that the level of exosomal maspin from tumor cell lines was disproportionally lower relative to the levels of corresponding intracellular and VDCM maspin, as compared to that from normal cell lines, maspin knockdown in MCF-10A cells led to maspin-devoid exosomes, which exhibited significantly reduced suppressive effects on the chemotaxis activity of recipient NIH3T3 fibroblast cells. These data are the first to demonstrate the potential of maspin delivered by exosomes to block tumor-induced stromal response, and support the clinical application of exosomal maspin in cancer diagnosis and treatment. Impact Journals LLC 2016-11-11 /pmc/articles/PMC5352381/ /pubmed/28009978 http://dx.doi.org/10.18632/oncotarget.13302 Text en Copyright: © 2017 Dean et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Dean, Ivory
Dzinic, Sijana H
Bernardo, M. Margarida
Zou, Yi
Kimler, Vickie
Li, Xiaohua
Kaplun, Alexander
Granneman, James
Mao, Guangzhao
Sheng, Shijie
The secretion and biological function of tumor suppressor maspin as an exosome cargo protein
title The secretion and biological function of tumor suppressor maspin as an exosome cargo protein
title_full The secretion and biological function of tumor suppressor maspin as an exosome cargo protein
title_fullStr The secretion and biological function of tumor suppressor maspin as an exosome cargo protein
title_full_unstemmed The secretion and biological function of tumor suppressor maspin as an exosome cargo protein
title_short The secretion and biological function of tumor suppressor maspin as an exosome cargo protein
title_sort secretion and biological function of tumor suppressor maspin as an exosome cargo protein
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5352381/
https://www.ncbi.nlm.nih.gov/pubmed/28009978
http://dx.doi.org/10.18632/oncotarget.13302
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