Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis

BACKGROUND & AIMS: The pathogenic mechanism of pancreatitis is poorly understood. Recent evidence implicates defective autophagy in pancreatitis responses; however, the pathways mediating impaired autophagy in pancreas remain largely unknown. Here, we investigate the role of lysosome associated...

Descripción completa

Detalles Bibliográficos
Autores principales: Mareninova, Olga A., Sendler, Matthias, Malla, Sudarshan Ravi, Yakubov, Iskandar, French, Samuel W., Tokhtaeva, Elmira, Vagin, Olga, Oorschot, Viola, Lüllmann-Rauch, Renate, Blanz, Judith, Dawson, David, Klumperman, Judith, Lerch, Markus M., Mayerle, Julia, Gukovsky, Ilya, Gukovskaya, Anna S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2015
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673685/
https://www.ncbi.nlm.nih.gov/pubmed/26693174
http://dx.doi.org/10.1016/j.jcmgh.2015.07.006
_version_ 1782404786035884032
author Mareninova, Olga A.
Sendler, Matthias
Malla, Sudarshan Ravi
Yakubov, Iskandar
French, Samuel W.
Tokhtaeva, Elmira
Vagin, Olga
Oorschot, Viola
Lüllmann-Rauch, Renate
Blanz, Judith
Dawson, David
Klumperman, Judith
Lerch, Markus M.
Mayerle, Julia
Gukovsky, Ilya
Gukovskaya, Anna S.
author_facet Mareninova, Olga A.
Sendler, Matthias
Malla, Sudarshan Ravi
Yakubov, Iskandar
French, Samuel W.
Tokhtaeva, Elmira
Vagin, Olga
Oorschot, Viola
Lüllmann-Rauch, Renate
Blanz, Judith
Dawson, David
Klumperman, Judith
Lerch, Markus M.
Mayerle, Julia
Gukovsky, Ilya
Gukovskaya, Anna S.
author_sort Mareninova, Olga A.
collection PubMed
description BACKGROUND & AIMS: The pathogenic mechanism of pancreatitis is poorly understood. Recent evidence implicates defective autophagy in pancreatitis responses; however, the pathways mediating impaired autophagy in pancreas remain largely unknown. Here, we investigate the role of lysosome associated membrane proteins (LAMPs) in pancreatitis. METHODS: We analyzed changes in LAMPs in experimental models and human pancreatitis, and the underlying mechanisms: LAMP deglycosylation and degradation. LAMP cleavage by cathepsin B (CatB) was analyzed by mass spectrometry. We used mice deficient in LAMP-2 to assess its role in pancreatitis. RESULTS: Pancreatic levels of LAMP-1 and LAMP-2 greatly decrease across various pancreatitis models and in human disease. Pancreatitis does not trigger the LAMPs’ bulk deglycosylation but induces their degradation via CatB-mediated cleavage of the LAMP molecule close to the boundary between luminal and transmembrane domains. LAMP-2 null mice spontaneously develop pancreatitis that begins with acinar cell vacuolization due to impaired autophagic flux, and progresses to severe pancreas damage characterized by trypsinogen activation, macrophage-driven inflammation, and acinar cell death. LAMP-2 deficiency causes a decrease in pancreatic digestive enzymes content, and stimulates the basal and inhibits cholecystokinin-induced amylase secretion by acinar cells. The effects of LAMP-2 knockout and acute cerulein pancreatitis overlap, which corroborates the pathogenic role of LAMP decrease in experimental pancreatitis models. CONCLUSIONS: The results indicate a critical role for LAMPs, particularly LAMP-2, in maintaining pancreatic acinar cell homeostasis and provide evidence that defective lysosomal function, resulting in impaired autophagy, leads to pancreatitis. Mice with LAMP-2 deficiency present a novel genetic model of human pancreatitis caused by lysosomal/autophagic dysfunction.
format Online
Article
Text
id pubmed-4673685
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-46736852016-11-01 Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis Mareninova, Olga A. Sendler, Matthias Malla, Sudarshan Ravi Yakubov, Iskandar French, Samuel W. Tokhtaeva, Elmira Vagin, Olga Oorschot, Viola Lüllmann-Rauch, Renate Blanz, Judith Dawson, David Klumperman, Judith Lerch, Markus M. Mayerle, Julia Gukovsky, Ilya Gukovskaya, Anna S. Cell Mol Gastroenterol Hepatol Original Research BACKGROUND & AIMS: The pathogenic mechanism of pancreatitis is poorly understood. Recent evidence implicates defective autophagy in pancreatitis responses; however, the pathways mediating impaired autophagy in pancreas remain largely unknown. Here, we investigate the role of lysosome associated membrane proteins (LAMPs) in pancreatitis. METHODS: We analyzed changes in LAMPs in experimental models and human pancreatitis, and the underlying mechanisms: LAMP deglycosylation and degradation. LAMP cleavage by cathepsin B (CatB) was analyzed by mass spectrometry. We used mice deficient in LAMP-2 to assess its role in pancreatitis. RESULTS: Pancreatic levels of LAMP-1 and LAMP-2 greatly decrease across various pancreatitis models and in human disease. Pancreatitis does not trigger the LAMPs’ bulk deglycosylation but induces their degradation via CatB-mediated cleavage of the LAMP molecule close to the boundary between luminal and transmembrane domains. LAMP-2 null mice spontaneously develop pancreatitis that begins with acinar cell vacuolization due to impaired autophagic flux, and progresses to severe pancreas damage characterized by trypsinogen activation, macrophage-driven inflammation, and acinar cell death. LAMP-2 deficiency causes a decrease in pancreatic digestive enzymes content, and stimulates the basal and inhibits cholecystokinin-induced amylase secretion by acinar cells. The effects of LAMP-2 knockout and acute cerulein pancreatitis overlap, which corroborates the pathogenic role of LAMP decrease in experimental pancreatitis models. CONCLUSIONS: The results indicate a critical role for LAMPs, particularly LAMP-2, in maintaining pancreatic acinar cell homeostasis and provide evidence that defective lysosomal function, resulting in impaired autophagy, leads to pancreatitis. Mice with LAMP-2 deficiency present a novel genetic model of human pancreatitis caused by lysosomal/autophagic dysfunction. Elsevier 2015-07-22 /pmc/articles/PMC4673685/ /pubmed/26693174 http://dx.doi.org/10.1016/j.jcmgh.2015.07.006 Text en © 2015 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Research
Mareninova, Olga A.
Sendler, Matthias
Malla, Sudarshan Ravi
Yakubov, Iskandar
French, Samuel W.
Tokhtaeva, Elmira
Vagin, Olga
Oorschot, Viola
Lüllmann-Rauch, Renate
Blanz, Judith
Dawson, David
Klumperman, Judith
Lerch, Markus M.
Mayerle, Julia
Gukovsky, Ilya
Gukovskaya, Anna S.
Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis
title Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis
title_full Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis
title_fullStr Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis
title_full_unstemmed Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis
title_short Lysosome-Associated Membrane Proteins (LAMP) Maintain Pancreatic Acinar Cell Homeostasis: LAMP-2–Deficient Mice Develop Pancreatitis
title_sort lysosome-associated membrane proteins (lamp) maintain pancreatic acinar cell homeostasis: lamp-2–deficient mice develop pancreatitis
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673685/
https://www.ncbi.nlm.nih.gov/pubmed/26693174
http://dx.doi.org/10.1016/j.jcmgh.2015.07.006
work_keys_str_mv AT mareninovaolgaa lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT sendlermatthias lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT mallasudarshanravi lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT yakuboviskandar lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT frenchsamuelw lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT tokhtaevaelmira lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT vaginolga lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT oorschotviola lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT lullmannrauchrenate lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT blanzjudith lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT dawsondavid lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT klumpermanjudith lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT lerchmarkusm lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT mayerlejulia lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT gukovskyilya lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis
AT gukovskayaannas lysosomeassociatedmembraneproteinslampmaintainpancreaticacinarcellhomeostasislamp2deficientmicedeveloppancreatitis

Ejemplares similares