Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine

Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine

Reports have suggested that the two Notch ligands, Dll1 and Dll4, are indispensable to maintain the homeostasis of the intestinal epithelium. However, within the intestinal epithelium, the precise distribution of the cells that express those ligands at the protein level remains largely unknown. Here...

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Main Authors: Hiromichi Shimizu, Ryuichi Okamoto, Go Ito, Satoru Fujii, Toru Nakata, Kohei Suzuki, Tatsuro Murano, Tomohiro Mizutani, Kiichiro Tsuchiya, Tetsuya Nakamura, Katsuto Hozumi, Mamoru Watanabe
Format: Article
Language:English
Published: PeerJ Inc. 2014-05-01
Series:PeerJ
Subjects:
Dll1
Dll4
Hes1
ATOH1
Notch signaling
Intestinal epithelial cells
Online Access:https://peerj.com/articles/370.pdf
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spelling doaj-a6f339f7ef0a41d0b2d097098f897f532020-11-24T22:51:09ZengPeerJ Inc.PeerJ2167-83592014-05-012e37010.7717/peerj.370370Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestineHiromichi Shimizu0Ryuichi Okamoto1Go Ito2Satoru Fujii3Toru Nakata4Kohei Suzuki5Tatsuro Murano6Tomohiro Mizutani7Kiichiro Tsuchiya8Tetsuya Nakamura9Katsuto Hozumi10Mamoru Watanabe11Department of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanDepartment of Immunology, Tokai University School of Medicine, Isehara, JapanDepartment of Gastroenterology and Hepatology, Tokyo Medical and Dental University, Tokyo, JapanReports have suggested that the two Notch ligands, Dll1 and Dll4, are indispensable to maintain the homeostasis of the intestinal epithelium. However, within the intestinal epithelium, the precise distribution of the cells that express those ligands at the protein level remains largely unknown. Here, we show a series of immunohistochemical analysis through which we successfully identified mice intestinal epithelial cells (IECs) that endogenously express Dll1 or Dll4. Results showed that Dll1-positive (Dll1+ve) IECs reside exclusively within the crypt, whereas Dll4-positive (Dll4+ve) IECs can locate both in the crypt and in the villus of the small intestine. Also in the colon, Dll1+ve IECs resided at the lower part of the crypt, whereas Dll4+ve IECs resided at both upper and lower part of the crypt, including the surface epithelium. Both Dll1+ve and Dll4+ve IECs were ATOH1-positive, but Hes1-negative cells, and located adjacent to Hes1-positive cells within the crypts. A sub-population of both Dll1+ve and Dll4+ve IECs appeared to co-express Muc2, but rarely co-expressed other secretory lineage markers. However, as compared to Dll1+ve IECs, Dll4+ve IECs included larger number of Muc2-postive IECs, suggesting that Dll4 is more preferentially expressed by goblet cells. Also, we identified that Dll4 is expressed in the Paneth cells of the small intestine, whereas Dll1 and Dll4 is expressed in the c-kit-positive IECs of the colon, indicating that Dll1+ve and Dll4+ve IECs may contribute to constitute the intestinal stem cell niche. Compared to the normal colon, analysis of DSS-colitis showed that number of Dll1+ve IECs significantly decrease in the elongated crypts of the inflamed colonic mucosa. In sharp contrast, number of Dll4+ve IECs showed a significant increase in those crypts, which was accompanied by the increase in number of Hes1-positive IECs. Those Dll4+ve IECs were mostly found adjacent to the Hes1-positive IECs, suggesting that Dll4 may act as a major Notch ligand in the crypts of the inflamed colonic mucosa. Our results illustrate distinct expression patterns of Dll1 and Dll4 within the intestinal epithelium, and suggest that these two ligands may have different roles in normal and inflamed mucosa.https://peerj.com/articles/370.pdfDll1Dll4Hes1ATOH1Notch signalingIntestinal epithelial cells
collection DOAJ
language English
format Article
sources DOAJ
author Hiromichi Shimizu
Ryuichi Okamoto
Go Ito
Satoru Fujii
Toru Nakata
Kohei Suzuki
Tatsuro Murano
Tomohiro Mizutani
Kiichiro Tsuchiya
Tetsuya Nakamura
Katsuto Hozumi
Mamoru Watanabe
spellingShingle Hiromichi Shimizu
Ryuichi Okamoto
Go Ito
Satoru Fujii
Toru Nakata
Kohei Suzuki
Tatsuro Murano
Tomohiro Mizutani
Kiichiro Tsuchiya
Tetsuya Nakamura
Katsuto Hozumi
Mamoru Watanabe
Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine
PeerJ
Dll1
Dll4
Hes1
ATOH1
Notch signaling
Intestinal epithelial cells
author_facet Hiromichi Shimizu
Ryuichi Okamoto
Go Ito
Satoru Fujii
Toru Nakata
Kohei Suzuki
Tatsuro Murano
Tomohiro Mizutani
Kiichiro Tsuchiya
Tetsuya Nakamura
Katsuto Hozumi
Mamoru Watanabe
author_sort Hiromichi Shimizu
title Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine
title_short Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine
title_full Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine
title_fullStr Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine
title_full_unstemmed Distinct expression patterns of Notch ligands, Dll1 and Dll4, in normal and inflamed mice intestine
title_sort distinct expression patterns of notch ligands, dll1 and dll4, in normal and inflamed mice intestine
publisher PeerJ Inc.
series PeerJ
issn 2167-8359
publishDate 2014-05-01
description Reports have suggested that the two Notch ligands, Dll1 and Dll4, are indispensable to maintain the homeostasis of the intestinal epithelium. However, within the intestinal epithelium, the precise distribution of the cells that express those ligands at the protein level remains largely unknown. Here, we show a series of immunohistochemical analysis through which we successfully identified mice intestinal epithelial cells (IECs) that endogenously express Dll1 or Dll4. Results showed that Dll1-positive (Dll1+ve) IECs reside exclusively within the crypt, whereas Dll4-positive (Dll4+ve) IECs can locate both in the crypt and in the villus of the small intestine. Also in the colon, Dll1+ve IECs resided at the lower part of the crypt, whereas Dll4+ve IECs resided at both upper and lower part of the crypt, including the surface epithelium. Both Dll1+ve and Dll4+ve IECs were ATOH1-positive, but Hes1-negative cells, and located adjacent to Hes1-positive cells within the crypts. A sub-population of both Dll1+ve and Dll4+ve IECs appeared to co-express Muc2, but rarely co-expressed other secretory lineage markers. However, as compared to Dll1+ve IECs, Dll4+ve IECs included larger number of Muc2-postive IECs, suggesting that Dll4 is more preferentially expressed by goblet cells. Also, we identified that Dll4 is expressed in the Paneth cells of the small intestine, whereas Dll1 and Dll4 is expressed in the c-kit-positive IECs of the colon, indicating that Dll1+ve and Dll4+ve IECs may contribute to constitute the intestinal stem cell niche. Compared to the normal colon, analysis of DSS-colitis showed that number of Dll1+ve IECs significantly decrease in the elongated crypts of the inflamed colonic mucosa. In sharp contrast, number of Dll4+ve IECs showed a significant increase in those crypts, which was accompanied by the increase in number of Hes1-positive IECs. Those Dll4+ve IECs were mostly found adjacent to the Hes1-positive IECs, suggesting that Dll4 may act as a major Notch ligand in the crypts of the inflamed colonic mucosa. Our results illustrate distinct expression patterns of Dll1 and Dll4 within the intestinal epithelium, and suggest that these two ligands may have different roles in normal and inflamed mucosa.
topic Dll1
Dll4
Hes1
ATOH1
Notch signaling
Intestinal epithelial cells
url https://peerj.com/articles/370.pdf
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