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Citations to this article

Orphan Gpr182 suppresses ERK-mediated intestinal proliferation during regeneration and adenoma formation
Daniel O. Kechele, … , P. Kay Lund, Kathleen M. Caron
Daniel O. Kechele, … , P. Kay Lund, Kathleen M. Caron
Published January 17, 2017
Citation Information: J Clin Invest. 2017;127(2):593-607. https://doi.org/10.1172/JCI87588.
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Research Article Gastroenterology Article has an altmetric score of 51

Orphan Gpr182 suppresses ERK-mediated intestinal proliferation during regeneration and adenoma formation

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Abstract

Orphan GPCRs provide an opportunity to identify potential pharmacological targets, yet their expression patterns and physiological functions remain challenging to elucidate. Here, we have used a genetically engineered knockin reporter mouse to map the expression pattern of the Gpr182 during development and adulthood. We observed that Gpr182 is expressed at the crypt base throughout the small intestine, where it is enriched in crypt base columnar stem cells, one of the most active stem cell populations in the body. Gpr182 knockdown had no effect on homeostatic intestinal proliferation in vivo, but led to marked increases in proliferation during intestinal regeneration following irradiation-induced injury. In the ApcMin mouse model, which forms spontaneous intestinal adenomas, reductions in Gpr182 led to more adenomas and decreased survival. Loss of Gpr182 enhanced organoid growth efficiency ex vivo in an EGF-dependent manner. Gpr182 reduction led to increased activation of ERK1/2 in basal and challenge models, demonstrating a potential role for this orphan GPCR in regulating the proliferative capacity of the intestine. Importantly, GPR182 expression was profoundly reduced in numerous human carcinomas, including colon adenocarcinoma. Together, these results implicate Gpr182 as a negative regulator of intestinal MAPK signaling–induced proliferation, particularly during regeneration and adenoma formation.

Authors

Daniel O. Kechele, R. Eric Blue, Bailey Zwarycz, Scott T. Espenschied, Amanda T. Mah, Marni B. Siegel, Charles M. Perou, Shengli Ding, Scott T. Magness, P. Kay Lund, Kathleen M. Caron

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Total citations by year

Year: 2024 2023 2022 2021 2020 2018 Total
Citations: 1 4 3 3 1 1 13
Citation information
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Citations to this article (13)

Title and authors Publication Year
Prevention and treatment of peri-implant fibrosis by functionally inhibiting skeletal cells expressing the leptin receptor.
Suhardi VJ, Oktarina A, Hammad M, Niu Y, Li Q, Thomson A, Lopez J, McCormick J, Ayturk UM, Greenblatt MB, Ivashkiv LB, Bostrom MPG, Yang X
Nature Biomedical Engineering 2024
New pairings and deorphanization among the atypical chemokine receptor family — physiological and clinical relevance
Szpakowska M, D\u2019Uonnolo G, Luís R, Alonso Bartolomé A, Thelen M, Legler DF, Chevigné A
Frontiers in immunology 2023
Atlas of the anatomical localization of atypical chemokine receptors in healthy mice.
Melgrati S, Radice E, Ameti R, Hub E, Thelen S, Pelczar P, Jarrossay D, Rot A, Thelen M
PLoS Biology 2023
GPR182 is a broadly scavenging atypical chemokine receptor influencing T-independent immunity
Melgrati S, Gerken OJ, Artinger M, Radice E, Szpakowska M, Chevigné A, D\u2019Uonnolo G, Antonello P, Thelen S, Pelczar P, Legler DF, Thelen M
Frontiers in immunology 2023
Development of a novel tumor microenvironment-related radiogenomics model for prognosis prediction in hepatocellular carcinoma
Wang Y, Gao B, Xia C, Peng X, Liu H, Wu S
Quantitative imaging in medicine and surgery 2023
GPR182 limits antitumor immunity via chemokine scavenging in mouse melanoma models
R Torphy, Y Sun, R Lin, A Caffrey-Carr, Y Fujiwara, F Ho, E Miller, M McCarter, T Lyons, R Schulick, R Kedl, Y Zhu
Nature Communications 2022
Suppression of CCL2 angiocrine function by adrenomedullin promotes tumor growth
Nakayama A, Roquid KA, Iring A, Strilic B, Günther S, Chen M, Weinstein LS, Offermanns S
Journal of Experimental Medicine 2022
Atypical chemokine receptors: Emerging therapeutic targets in cancer
Torphy RJ, Yee EJ, Schulick RD, Zhu Y
Trends in Pharmacological Sciences 2022
Constitutive G protein coupling profiles of understudied orphan GPCRs
S Lu, W Jang, A Inoue, NA Lambert, EC Johnson
PloS one 2021
GPR182 is an endothelium-specific atypical chemokine receptor that maintains hematopoietic stem cell homeostasis
AL Mercier, R Bonnavion, W Yu, MW Alnouri, S Ramas, Y Zhang, Y Jäger, KA Roquid, HW Jeong, KK Sivaraj, H Cho, X Chen, B Strilic, T Sijmonsma, R Adams, T Schroeder, MA Rieger, S Offermanns
Proceedings of the National Academy of Sciences 2021
Deciphering keys genes in Cardio-renal Syndrome using network analysis
R Ishrat
Bioinformation 2021
The orphan G-protein coupled receptor 182 is a negative regulator of definitive hematopoiesis through leukotriene B4 signaling
H Kwon, DI Mackie, R Bonnavion, A Le-Mercier, CS Helker, T Son, S Guenter, DS Serafin, K Kim, S Offermanns, KM Caron, DY Stainier
2020
Evidence for a direct effect of the autonomic nervous system on intestinal epithelial stem cell proliferation
EA Davis, W Zhou, MJ Dailey
Physiological Reports 2018

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