Loss of CAPS2/Cadps2 leads to exocrine pancreatic cell injury and intracellular accumulation of secretory granules in mice

Yotaroh Sato; Miho Tsuyusaki; Hiromi Takahashi-Iwanaga; Rena Fujisawa; Atsushi Masamune; Shin Hamada; Ryotaro Matsumoto; Yu Tanaka; Yoichi Kakuta; Yumi Yamaguchi-Kabata; Tamio Furuse; Shigeharu Wakana; Takuya Shimura; Rika Kobayashi; Yo Shinoda; Ryo Goitsuka; So Maezawa; Tetsushi Sadakata; Yoshitake Sano; Teiichi Furuichi

doi:10.3389/fmolb.2022.1040237

Loss of CAPS2/Cadps2 leads to exocrine pancreatic cell injury and intracellular accumulation of secretory granules in mice

Yotaroh Sato, Miho Tsuyusaki, Hiromi Takahashi-Iwanaga, Rena Fujisawa, Atsushi Masamune, Shin Hamada, Ryotaro Matsumoto, Yu Tanaka, Yoichi Kakuta, Yumi Yamaguchi-Kabata, Tamio Furuse, Shigeharu Wakana, Takuya Shimura, Rika Kobayashi, Yo Shinoda, Ryo Goitsuka, So Maezawa, Tetsushi Sadakata, Yoshitake Sano, Teiichi Furuichi

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Abstract

The type 2 Ca²⁺-dependent activator protein for secretion (CAPS2/CADPS2) regulates dense-core vesicle trafficking and exocytosis and is involved in the regulated release of catecholamines, peptidergic hormones, and neuromodulators. CAPS2 is expressed in the pancreatic exocrine acinar cells that produce and secrete digestive enzymes. However, the functional role of CAPS2 in vesicular trafficking and/or exocytosis of non-regulatory proteins in the exocrine pancreas remains to be determined. Here, we analyzed the morpho-pathological indicators of the pancreatic exocrine pathway in Cadps2-deficient mouse models using histochemistry, biochemistry, and electron microscopy. We used whole exosome sequencing to identify CADPS2 variants in patients with chronic pancreatitis (CP). Caps2/Cadps2-knockout (KO) mice exhibited morphophysiological abnormalities in the exocrine pancreas, including excessive accumulation of secretory granules (zymogen granules) and their amylase content in the cytoplasm, deterioration of the fine intracellular membrane structures (disorganized rough endoplasmic reticulum, dilated Golgi cisternae, and the appearance of empty vesicles and autophagic-like vacuoles), as well as exocrine pancreatic cell injury, including acinar cell atrophy, increased fibrosis, and inflammatory cell infiltration. Pancreas-specific Cadps2 conditional KO mice exhibited pathological abnormalities in the exocrine pancreas similar to the global Cadps2 KO mice, indicating that these phenotypes were caused either directly or indirectly by CAPS2 deficiency in the pancreas. Furthermore, we identified a rare variant in the exon3 coding region of CADPS2 in a non-alcoholic patient with CP and showed that Cadps2-dex3 mice lacking CAPS2 exon3 exhibited symptoms similar to those exhibited by the Cadps2 KO and cKO mice. These results suggest that CAPS2 is critical for the proper functioning of the pancreatic exocrine pathway, and its deficiency is associated with a risk of pancreatic acinar cell pathology.

Original language	English
Article number	1040237
Journal	Frontiers in Molecular Biosciences
Volume	9
DOIs	https://doi.org/10.3389/fmolb.2022.1040237
Publication status	Published - 7 Nov 2022

Keywords

CAPS2
Cadps2
amylase
exocrine pancreas
pancreatic acinar cells
secretory granules

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10.3389/fmolb.2022.1040237

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Sato, Y., Tsuyusaki, M., Takahashi-Iwanaga, H., Fujisawa, R., Masamune, A., Hamada, S., Matsumoto, R., Tanaka, Y., Kakuta, Y., Yamaguchi-Kabata, Y., Furuse, T., Wakana, S., Shimura, T., Kobayashi, R., Shinoda, Y., Goitsuka, R., Maezawa, S., Sadakata, T., Sano, Y., & Furuichi, T. (2022). Loss of CAPS2/Cadps2 leads to exocrine pancreatic cell injury and intracellular accumulation of secretory granules in mice. Frontiers in Molecular Biosciences, 9, Article 1040237. https://doi.org/10.3389/fmolb.2022.1040237

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title = "Loss of CAPS2/Cadps2 leads to exocrine pancreatic cell injury and intracellular accumulation of secretory granules in mice",

abstract = "The type 2 Ca2+-dependent activator protein for secretion (CAPS2/CADPS2) regulates dense-core vesicle trafficking and exocytosis and is involved in the regulated release of catecholamines, peptidergic hormones, and neuromodulators. CAPS2 is expressed in the pancreatic exocrine acinar cells that produce and secrete digestive enzymes. However, the functional role of CAPS2 in vesicular trafficking and/or exocytosis of non-regulatory proteins in the exocrine pancreas remains to be determined. Here, we analyzed the morpho-pathological indicators of the pancreatic exocrine pathway in Cadps2-deficient mouse models using histochemistry, biochemistry, and electron microscopy. We used whole exosome sequencing to identify CADPS2 variants in patients with chronic pancreatitis (CP). Caps2/Cadps2-knockout (KO) mice exhibited morphophysiological abnormalities in the exocrine pancreas, including excessive accumulation of secretory granules (zymogen granules) and their amylase content in the cytoplasm, deterioration of the fine intracellular membrane structures (disorganized rough endoplasmic reticulum, dilated Golgi cisternae, and the appearance of empty vesicles and autophagic-like vacuoles), as well as exocrine pancreatic cell injury, including acinar cell atrophy, increased fibrosis, and inflammatory cell infiltration. Pancreas-specific Cadps2 conditional KO mice exhibited pathological abnormalities in the exocrine pancreas similar to the global Cadps2 KO mice, indicating that these phenotypes were caused either directly or indirectly by CAPS2 deficiency in the pancreas. Furthermore, we identified a rare variant in the exon3 coding region of CADPS2 in a non-alcoholic patient with CP and showed that Cadps2-dex3 mice lacking CAPS2 exon3 exhibited symptoms similar to those exhibited by the Cadps2 KO and cKO mice. These results suggest that CAPS2 is critical for the proper functioning of the pancreatic exocrine pathway, and its deficiency is associated with a risk of pancreatic acinar cell pathology.",

keywords = "CAPS2, Cadps2, amylase, exocrine pancreas, pancreatic acinar cells, secretory granules",

author = "Yotaroh Sato and Miho Tsuyusaki and Hiromi Takahashi-Iwanaga and Rena Fujisawa and Atsushi Masamune and Shin Hamada and Ryotaro Matsumoto and Yu Tanaka and Yoichi Kakuta and Yumi Yamaguchi-Kabata and Tamio Furuse and Shigeharu Wakana and Takuya Shimura and Rika Kobayashi and Yo Shinoda and Ryo Goitsuka and So Maezawa and Tetsushi Sadakata and Yoshitake Sano and Teiichi Furuichi",

note = "Publisher Copyright: Copyright {\textcopyright} 2022 Sato, Tsuyusaki, Takahashi-Iwanaga, Fujisawa, Masamune, Hamada, Matsumoto, Tanaka, Kakuta, Yamaguchi-Kabata, Furuse, Wakana, Shimura, Kobayashi, Shinoda, Goitsuka, Maezawa, Sadakata, Sano and Furuichi.",

year = "2022",

month = nov,

day = "7",

doi = "10.3389/fmolb.2022.1040237",

language = "English",

volume = "9",

journal = "Frontiers in Molecular Biosciences",

issn = "2296-889X",

publisher = "Frontiers Media SA",

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Sato, Y, Tsuyusaki, M, Takahashi-Iwanaga, H, Fujisawa, R, Masamune, A, Hamada, S, Matsumoto, R, Tanaka, Y, Kakuta, Y, Yamaguchi-Kabata, Y, Furuse, T, Wakana, S, Shimura, T, Kobayashi, R, Shinoda, Y, Goitsuka, R, Maezawa, S, Sadakata, T, Sano, Y & Furuichi, T 2022, 'Loss of CAPS2/Cadps2 leads to exocrine pancreatic cell injury and intracellular accumulation of secretory granules in mice', Frontiers in Molecular Biosciences, vol. 9, 1040237. https://doi.org/10.3389/fmolb.2022.1040237

TY - JOUR

T1 - Loss of CAPS2/Cadps2 leads to exocrine pancreatic cell injury and intracellular accumulation of secretory granules in mice

AU - Sato, Yotaroh

AU - Tsuyusaki, Miho

AU - Takahashi-Iwanaga, Hiromi

AU - Fujisawa, Rena

AU - Masamune, Atsushi

AU - Hamada, Shin

AU - Matsumoto, Ryotaro

AU - Tanaka, Yu

AU - Kakuta, Yoichi

AU - Yamaguchi-Kabata, Yumi

AU - Furuse, Tamio

AU - Wakana, Shigeharu

AU - Shimura, Takuya

AU - Kobayashi, Rika

AU - Shinoda, Yo

AU - Goitsuka, Ryo

AU - Maezawa, So

AU - Sadakata, Tetsushi

AU - Sano, Yoshitake

AU - Furuichi, Teiichi

N1 - Publisher Copyright: Copyright © 2022 Sato, Tsuyusaki, Takahashi-Iwanaga, Fujisawa, Masamune, Hamada, Matsumoto, Tanaka, Kakuta, Yamaguchi-Kabata, Furuse, Wakana, Shimura, Kobayashi, Shinoda, Goitsuka, Maezawa, Sadakata, Sano and Furuichi.

PY - 2022/11/7

Y1 - 2022/11/7

N2 - The type 2 Ca2+-dependent activator protein for secretion (CAPS2/CADPS2) regulates dense-core vesicle trafficking and exocytosis and is involved in the regulated release of catecholamines, peptidergic hormones, and neuromodulators. CAPS2 is expressed in the pancreatic exocrine acinar cells that produce and secrete digestive enzymes. However, the functional role of CAPS2 in vesicular trafficking and/or exocytosis of non-regulatory proteins in the exocrine pancreas remains to be determined. Here, we analyzed the morpho-pathological indicators of the pancreatic exocrine pathway in Cadps2-deficient mouse models using histochemistry, biochemistry, and electron microscopy. We used whole exosome sequencing to identify CADPS2 variants in patients with chronic pancreatitis (CP). Caps2/Cadps2-knockout (KO) mice exhibited morphophysiological abnormalities in the exocrine pancreas, including excessive accumulation of secretory granules (zymogen granules) and their amylase content in the cytoplasm, deterioration of the fine intracellular membrane structures (disorganized rough endoplasmic reticulum, dilated Golgi cisternae, and the appearance of empty vesicles and autophagic-like vacuoles), as well as exocrine pancreatic cell injury, including acinar cell atrophy, increased fibrosis, and inflammatory cell infiltration. Pancreas-specific Cadps2 conditional KO mice exhibited pathological abnormalities in the exocrine pancreas similar to the global Cadps2 KO mice, indicating that these phenotypes were caused either directly or indirectly by CAPS2 deficiency in the pancreas. Furthermore, we identified a rare variant in the exon3 coding region of CADPS2 in a non-alcoholic patient with CP and showed that Cadps2-dex3 mice lacking CAPS2 exon3 exhibited symptoms similar to those exhibited by the Cadps2 KO and cKO mice. These results suggest that CAPS2 is critical for the proper functioning of the pancreatic exocrine pathway, and its deficiency is associated with a risk of pancreatic acinar cell pathology.

AB - The type 2 Ca2+-dependent activator protein for secretion (CAPS2/CADPS2) regulates dense-core vesicle trafficking and exocytosis and is involved in the regulated release of catecholamines, peptidergic hormones, and neuromodulators. CAPS2 is expressed in the pancreatic exocrine acinar cells that produce and secrete digestive enzymes. However, the functional role of CAPS2 in vesicular trafficking and/or exocytosis of non-regulatory proteins in the exocrine pancreas remains to be determined. Here, we analyzed the morpho-pathological indicators of the pancreatic exocrine pathway in Cadps2-deficient mouse models using histochemistry, biochemistry, and electron microscopy. We used whole exosome sequencing to identify CADPS2 variants in patients with chronic pancreatitis (CP). Caps2/Cadps2-knockout (KO) mice exhibited morphophysiological abnormalities in the exocrine pancreas, including excessive accumulation of secretory granules (zymogen granules) and their amylase content in the cytoplasm, deterioration of the fine intracellular membrane structures (disorganized rough endoplasmic reticulum, dilated Golgi cisternae, and the appearance of empty vesicles and autophagic-like vacuoles), as well as exocrine pancreatic cell injury, including acinar cell atrophy, increased fibrosis, and inflammatory cell infiltration. Pancreas-specific Cadps2 conditional KO mice exhibited pathological abnormalities in the exocrine pancreas similar to the global Cadps2 KO mice, indicating that these phenotypes were caused either directly or indirectly by CAPS2 deficiency in the pancreas. Furthermore, we identified a rare variant in the exon3 coding region of CADPS2 in a non-alcoholic patient with CP and showed that Cadps2-dex3 mice lacking CAPS2 exon3 exhibited symptoms similar to those exhibited by the Cadps2 KO and cKO mice. These results suggest that CAPS2 is critical for the proper functioning of the pancreatic exocrine pathway, and its deficiency is associated with a risk of pancreatic acinar cell pathology.

KW - CAPS2

KW - Cadps2

KW - amylase

KW - exocrine pancreas

KW - pancreatic acinar cells

KW - secretory granules

UR - http://www.scopus.com/inward/record.url?scp=85142220920&partnerID=8YFLogxK

U2 - 10.3389/fmolb.2022.1040237

DO - 10.3389/fmolb.2022.1040237

M3 - Article

AN - SCOPUS:85142220920

SN - 2296-889X

VL - 9

JO - Frontiers in Molecular Biosciences

JF - Frontiers in Molecular Biosciences

M1 - 1040237

ER -

Loss of CAPS2/Cadps2 leads to exocrine pancreatic cell injury and intracellular accumulation of secretory granules in mice

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