Involvement of Pancreatic Stellate Cells in Regeneration of Remnant Pancreas after Partial Pancreatectomy

Ota, Shigenori; Nishimura, Miyuki; Murakami, Yuya; Kubo Birukawa, Naoko; Yoneda, Akihiro; Nishita, Hiroki; Fujita, Ryosuke; Sato, Yasushi; Minomi, Kenjiro; Kajiwara, Keiko; Miyazaki, Miyono; Uchiumi, Maki; Mikuni, Shintaro; Tamura, Yasuaki; Mizuguchi, Toru; Imamura, Masafumi; Meguro, Makoto; Kimura, Yasutoshi; Hirata, Koichi; Niitsu, Yoshiro

doi:10.1371/journal.pone.0165747

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ID	112310
タイトル別表記	Role of PSCs in Regeneration of Remnant Pancreas after PX
著者	Ota, Shigenori Sapporo Medical University Nishimura, Miyuki Sapporo Medical University Murakami, Yuya Sapporo Medical University Kubo Birukawa, Naoko Sapporo Medical University Yoneda, Akihiro Sapporo Medical University\|Hokkaido University Nishita, Hiroki Sapporo Medical University\|Nitto Denko Corporation Fujita, Ryosuke Sapporo Medical University 佐藤, 康史 Sapporo Medical University 徳島大学教育研究者総覧 Minomi, Kenjiro Sapporo Medical University\|Nitto Denko Corporation Kajiwara, Keiko Sapporo Medical University\|Nitto Denko Corporation Miyazaki, Miyono Sapporo Medical University\|Nitto Denko Corporation Uchiumi, Maki Hokkaido University Mikuni, Shintaro Hokkaido University Tamura, Yasuaki Hokkaido University Mizuguchi, Toru Sapporo Medical University Imamura, Masafumi Sapporo Medical University Meguro, Makoto Sapporo Medical University Kimura, Yasutoshi Sapporo Medical University Hirata, Koichi Sapporo Medical University Niitsu, Yoshiro Sapporo Medical University
資料タイプ	学術雑誌論文
抄録	Background and objectives Mechanism of regeneration of remnant pancreas after partial pancreatectomy (PX) is still unknown. In this study, effect of siRNA against the collagen specific chaperone, HSP47, which inhibits collagen secretion from activated pancreas stellate cells (aPSCs), and induces their apoptosis, on regeneration of remnant pancreas was determined. Methods Pancreatectomy was performed according to established methods. Proliferation of cells was assessed by BrdU incorporation. Immunostaining of HSP47 was employed to identify PSCs. Progenitor cells were identified by SOX9 staining. Acinar cells were immunostained for amylase. Co-culture of acinar cells with aPSCs were carried out in a double chamber with a cell culture insert. siRNA HSP47 encapsulated in vitamin A-coupled liposome (VA-lip siRNA HSP47) was delivered to aPSCs by iv injection. Results In remnant pancreas of 90% PX rat, new areas of foci were located separately from duodenal areas with normal pancreatic features. After PX, BrdU uptake of acinar cells and islet cells significantly increased, but was suppressed by treatment with VA-lip siRNA HSP47. BrdU uptake by acinar cells was augmented by co-culturing with aPSCs and the augmentation was nullified by siRNA HSP47. BrdU uptake by progenitor cells in foci area was slightly enhanced by the same treatment. New area which exhibited intermediate features between those of duodenal and area of foci, emerged after the treatment. Conclusion aPSCs play a crucial role in regeneration of remnant pancreas, proliferation of acinar and islet cells after PX through the activity of secreted collagen. Characterization of new area emerged by siRNA HSP47 treatment as to its origin is a future task.
掲載誌名	PLOS ONE
ISSN	19326203
出版者	PLOS
巻	11
号	12
開始ページ	e0165747
発行日	2016-12-09
権利情報	Copyright: © 2016 Ota et al. 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 credited.
EDB ID	324992
出版社版DOI	10.1371/journal.pone.0165747
出版社版URL	https://doi.org/10.1371/journal.pone.0165747
フルテキストファイル	pone_11_12_e0165747.pdf 4.96 MB
言語	eng
著者版フラグ	出版社版
部局	医学系