Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells

We describe here two novel endogenous variants of the human endoplasmic reticulum (ER) cargo receptor SEL1LA, designated p38 and p28. Biochemical and RNA interference studies in tumorigenic and non-tumorigenic cells indicate that p38 and p28 are N-terminal, ER-anchorless and more stable relative to...

Descripción completa

Detalles Bibliográficos
Autores principales: Cattaneo, Monica, Lotti, Lavinia Vittoria, Martino, Simone, Alessio, Massimo, Conti, Antonio, Bachi, Angela, Mariani-Costantini, Renato, Biunno, Ida
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3040770/
https://www.ncbi.nlm.nih.gov/pubmed/21359144
http://dx.doi.org/10.1371/journal.pone.0017206
_version_ 1782198374995329024
author Cattaneo, Monica
Lotti, Lavinia Vittoria
Martino, Simone
Alessio, Massimo
Conti, Antonio
Bachi, Angela
Mariani-Costantini, Renato
Biunno, Ida
author_facet Cattaneo, Monica
Lotti, Lavinia Vittoria
Martino, Simone
Alessio, Massimo
Conti, Antonio
Bachi, Angela
Mariani-Costantini, Renato
Biunno, Ida
author_sort Cattaneo, Monica
collection PubMed
description We describe here two novel endogenous variants of the human endoplasmic reticulum (ER) cargo receptor SEL1LA, designated p38 and p28. Biochemical and RNA interference studies in tumorigenic and non-tumorigenic cells indicate that p38 and p28 are N-terminal, ER-anchorless and more stable relative to the canonical transmembrane SEL1LA. P38 is expressed and constitutively secreted, with increase after ER stress, in the KMS11 myeloma line and in the breast cancer lines MCF7 and SKBr3, but not in the non-tumorigenic breast epithelial MCF10A line. P28 is detected only in the poorly differentiated SKBr3 cell line, where it is secreted after ER stress. Consistently with the presence of p38 and p28 in culture media, morphological studies of SKBr3 and KMS11 cells detect N-terminal SEL1L immunolabeling in secretory/degradative compartments and extracellularly-released membrane vesicles. Our findings suggest that the two new SEL1L variants are engaged in endosomal trafficking and secretion via vesicles, which could contribute to relieve ER stress in tumorigenic cells. P38 and p28 could therefore be relevant as diagnostic markers and/or therapeutic targets in cancer.
format Text
id pubmed-3040770
institution National Center for Biotechnology Information
language English
publishDate 2011
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-30407702011-02-25 Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells Cattaneo, Monica Lotti, Lavinia Vittoria Martino, Simone Alessio, Massimo Conti, Antonio Bachi, Angela Mariani-Costantini, Renato Biunno, Ida PLoS One Research Article We describe here two novel endogenous variants of the human endoplasmic reticulum (ER) cargo receptor SEL1LA, designated p38 and p28. Biochemical and RNA interference studies in tumorigenic and non-tumorigenic cells indicate that p38 and p28 are N-terminal, ER-anchorless and more stable relative to the canonical transmembrane SEL1LA. P38 is expressed and constitutively secreted, with increase after ER stress, in the KMS11 myeloma line and in the breast cancer lines MCF7 and SKBr3, but not in the non-tumorigenic breast epithelial MCF10A line. P28 is detected only in the poorly differentiated SKBr3 cell line, where it is secreted after ER stress. Consistently with the presence of p38 and p28 in culture media, morphological studies of SKBr3 and KMS11 cells detect N-terminal SEL1L immunolabeling in secretory/degradative compartments and extracellularly-released membrane vesicles. Our findings suggest that the two new SEL1L variants are engaged in endosomal trafficking and secretion via vesicles, which could contribute to relieve ER stress in tumorigenic cells. P38 and p28 could therefore be relevant as diagnostic markers and/or therapeutic targets in cancer. Public Library of Science 2011-02-17 /pmc/articles/PMC3040770/ /pubmed/21359144 http://dx.doi.org/10.1371/journal.pone.0017206 Text en Cattaneo et al. http://creativecommons.org/licenses/by/4.0/ 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 properly credited.
spellingShingle Research Article
Cattaneo, Monica
Lotti, Lavinia Vittoria
Martino, Simone
Alessio, Massimo
Conti, Antonio
Bachi, Angela
Mariani-Costantini, Renato
Biunno, Ida
Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells
title Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells
title_full Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells
title_fullStr Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells
title_full_unstemmed Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells
title_short Secretion of Novel SEL1L Endogenous Variants Is Promoted by ER Stress/UPR via Endosomes and Shed Vesicles in Human Cancer Cells
title_sort secretion of novel sel1l endogenous variants is promoted by er stress/upr via endosomes and shed vesicles in human cancer cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3040770/
https://www.ncbi.nlm.nih.gov/pubmed/21359144
http://dx.doi.org/10.1371/journal.pone.0017206
work_keys_str_mv AT cattaneomonica secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells
AT lottilaviniavittoria secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells
AT martinosimone secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells
AT alessiomassimo secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells
AT contiantonio secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells
AT bachiangela secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells
AT marianicostantinirenato secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells
AT biunnoida secretionofnovelsel1lendogenousvariantsispromotedbyerstressuprviaendosomesandshedvesiclesinhumancancercells

Ejemplares similares