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Citations to this article

Apical secretion of lysosomal enzymes in rabbit pancreas occurs via a secretagogue regulated pathway and is increased after pancreatic duct obstruction.
T Hirano, … , M Saluja, M L Steer
T Hirano, … , M Saluja, M L Steer
Published March 1, 1991
Citation Information: J Clin Invest. 1991;87(3):865-869. https://doi.org/10.1172/JCI115091.
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Research Article

Apical secretion of lysosomal enzymes in rabbit pancreas occurs via a secretagogue regulated pathway and is increased after pancreatic duct obstruction.

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Abstract

Lysosomal hydrolases such as cathepsin B are apically secreted from rabbit pancreatic acinar cells via a regulated as opposed to a constitutive pathway. Intravenous infusion of the cholecystokinin analogue caerulein results in highly correlated apical secretion of digestive and lysosomal enzymes, suggesting that they are discharged from the same presecretory compartment (zymogen granules). Lysosomal enzymes appear to enter that compartment as a result of missorting. After 7 h of duct obstruction is relieved, caerulein-stimulated apical secretion of cathepsin B and amylase is increased, but the ratio of cathepsin B to amylase secretion is not different than that following caerulein stimulation of animals never obstructed. These findings indicate that duct obstruction causes an increased amount of both lysosomal and digestive enzymes to accumulate within the secretagogue releasable compartment but that duct obstruction does not increase the degree of lysosomal enzyme missorting into that compartment. Pancreatic duct obstruction causes lysosomal hydrolases to become colocalized with digestive enzymes in organelles that, in size and distribution, resemble zymogen granules but that are not subject to secretion in response to secretagogue stimulation. These organelles may be of importance in the development of pancreatitis.

Authors

T Hirano, A Saluja, P Ramarao, M M Lerch, M Saluja, M L Steer

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Citations to this article (58)

Title and authors Publication Year
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Cellular and molecular life sciences : CMLS 2024
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Gut 2020
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Early trypsin activation develops independently of autophagy in caerulein-induced pancreatitis in mice
SR Malla, B Krueger, T Wartmann, M Sendler, UM Mahajan, FU Weiss, FG Thiel, CD Boni, FS Gorelick, W Halangk, AA Aghdassi, T Reinheckel, AS Gukovskaya, MM Lerch, J Mayerle
Cellular and Molecular Life Sciences 2019
A Tribute to Michael L. Steer (1939–2019)
MM Lerch, G Perides, AK Saluja
Pancreas 2019
A tribute to Michael L. Steer (1939–2019)
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Pancreatology 2019
The shaping, making and baking of a pancreatologist
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Pancreatology 2018
Cathepsin B-Mediated Activation of Trypsinogen in Endocytosing Macrophages Increases Severity of Pancreatitis in Mice
M Sendler, FU Weiss, J Golchert, G Homuth, C van den Brandt, UM Mahajan, LI Partecke, P Döring, I Gukovsky, AS Gukovskaya, PR Wagh, MM Lerch, J Mayerle
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FU Weiss, ME Skube, MM Lerch
Current Opinion in Gastroenterology 2018
Do Animal Models of Acute Pancreatitis Reproduce Human Disease?
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Lysosomes - Associated Diseases and Methods to Study Their Function
PD Sharma
Lysosomes - Associated Diseases and Methods to Study Their Function 2017
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M Sendler, S Maertin, D John, M Persike, FU Weiss, B Krüger, T Wartmann, P Wagh, W Halangk, N Schaschke, J Mayerle, MM Lerch
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Necrosis, Apoptosis, Necroptosis, Pyroptosis: It Matters How Acinar Cells Die During Pancreatitis
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CMGH Cellular and Molecular Gastroenterology and Hepatology 2016
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SR Malla, CK Mårdh, A Günther, UM Mahajan, M Sendler, J D'Haese, FU Weiss, MM Lerch, MB Hansen, J Mayerle
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Gastroenterology 2014
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2013
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HG Beger, MW Büchler, H Dralle, MM Lerch, P Malfertheiner, J Mössner, JF Riemann
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Animal models for investigating chronic pancreatitis
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Molecular Pathology 2009
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HG Beger, S Matsuno, JL Cameron, BM Rau, M Sunamura, RD Schulick
2008
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NAADP, cADPR and IP3 all release Ca2+ from the endoplasmic reticulum and an acidic store in the secretory granule area
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Glutathione and ATP levels, subcellular distribution of enzymes, and permeability of duct system in rabbit pancreas following intravenous administration of alcohol and cerulein
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Lysosomes
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