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Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly

Microvesicles are the body's most powerful intercellular communication system and cancer-initiating cell microvesicles (CIC-TEX) reprogram Non-CIC towards fortified malignancy. Claudin7, a CIC-biomarker in gastrointestinal tumors, is recovered in TEX. Recent evidence suggesting individual cells...

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Autores principales: Kyuno, Daisuke, Bauer, Nathalie, Schnölzer, Martina, Provaznik, Jan, Ryschich, Eduard, Hackert, Thilo, Zöller, Margot
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6775303/
https://www.ncbi.nlm.nih.gov/pubmed/31592143
http://dx.doi.org/10.7150/ijbs.35347
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author Kyuno, Daisuke
Bauer, Nathalie
Schnölzer, Martina
Provaznik, Jan
Ryschich, Eduard
Hackert, Thilo
Zöller, Margot
author_facet Kyuno, Daisuke
Bauer, Nathalie
Schnölzer, Martina
Provaznik, Jan
Ryschich, Eduard
Hackert, Thilo
Zöller, Margot
author_sort Kyuno, Daisuke
collection PubMed
description Microvesicles are the body's most powerful intercellular communication system and cancer-initiating cell microvesicles (CIC-TEX) reprogram Non-CIC towards fortified malignancy. Claudin7, a CIC-biomarker in gastrointestinal tumors, is recovered in TEX. Recent evidence suggesting individual cells delivering distinct microvesicles became of particular interest for claudin7, which is part of tight junctions (TJ) and glycolipid-enriched membrane domains (GEM), GEM-located claudin7 is palmitoylated. This offered the unique possibility of exploring the contribution of a CIC marker and its origin from distinct membrane domains on CIC-TEX biogenesis and activities. Proteome and miRNA analysis of wild-type, claudin7-knockdown and a rescue with claudin7 harboring a mutated palmitoylation site (mP) of a rat pancreatic and a human colon cancer line uncovered significant, only partly overlapping contributions of palmitoylated and non-palmitoylated claudin7 to TEX composition. Palmitoylated claudin7 facilitates GEM-integrated plasma membrane and associated signaling molecule recruitment; non-palmitoylated claudin7 supports recruitment of trafficking components, proteins engaged in fatty acid metabolism and TJ proteins into TEX. Claudin7mP also assists TEX recovery of selected miRNA. Thus, distinctly located claudin7 affects CIC-TEX composition and TJ-derived cld7 might play a unique role in equipping CIC-TEX with transporters and lipid metabolism-regulating molecules, awareness of distinct TEX populations being crucial facing therapeutic translation.
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spelling pubmed-67753032019-10-07 Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly Kyuno, Daisuke Bauer, Nathalie Schnölzer, Martina Provaznik, Jan Ryschich, Eduard Hackert, Thilo Zöller, Margot Int J Biol Sci Research Paper Microvesicles are the body's most powerful intercellular communication system and cancer-initiating cell microvesicles (CIC-TEX) reprogram Non-CIC towards fortified malignancy. Claudin7, a CIC-biomarker in gastrointestinal tumors, is recovered in TEX. Recent evidence suggesting individual cells delivering distinct microvesicles became of particular interest for claudin7, which is part of tight junctions (TJ) and glycolipid-enriched membrane domains (GEM), GEM-located claudin7 is palmitoylated. This offered the unique possibility of exploring the contribution of a CIC marker and its origin from distinct membrane domains on CIC-TEX biogenesis and activities. Proteome and miRNA analysis of wild-type, claudin7-knockdown and a rescue with claudin7 harboring a mutated palmitoylation site (mP) of a rat pancreatic and a human colon cancer line uncovered significant, only partly overlapping contributions of palmitoylated and non-palmitoylated claudin7 to TEX composition. Palmitoylated claudin7 facilitates GEM-integrated plasma membrane and associated signaling molecule recruitment; non-palmitoylated claudin7 supports recruitment of trafficking components, proteins engaged in fatty acid metabolism and TJ proteins into TEX. Claudin7mP also assists TEX recovery of selected miRNA. Thus, distinctly located claudin7 affects CIC-TEX composition and TJ-derived cld7 might play a unique role in equipping CIC-TEX with transporters and lipid metabolism-regulating molecules, awareness of distinct TEX populations being crucial facing therapeutic translation. Ivyspring International Publisher 2019-08-19 /pmc/articles/PMC6775303/ /pubmed/31592143 http://dx.doi.org/10.7150/ijbs.35347 Text en © The author(s) This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Kyuno, Daisuke
Bauer, Nathalie
Schnölzer, Martina
Provaznik, Jan
Ryschich, Eduard
Hackert, Thilo
Zöller, Margot
Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly
title Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly
title_full Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly
title_fullStr Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly
title_full_unstemmed Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly
title_short Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly
title_sort distinct origin of claudin7 in early tumor endosomes affects exosome assembly
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6775303/
https://www.ncbi.nlm.nih.gov/pubmed/31592143
http://dx.doi.org/10.7150/ijbs.35347
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