Development of ghrelin transgenic mice for elucidation of clinical implication of ghrelin

Daisuke Aotani; Hiroyuki Ariyasu; Satoko Shimazu-Kuwahara; Yoshiyuki Shimizu; Hidenari Nomura; Yoshiteru Murofushi; Kentaro Kaneko; Ryota Izumi; Masaki Matsubara; Hajime Kanda; Michio Noguchi; Tomohiro Tanaka; Toru Kusakabe; Takashi Miyazawa; Kazuwa Nakao

doi:10.1507/endocrj.64.S31

Development of ghrelin transgenic mice for elucidation of clinical implication of ghrelin

Daisuke Aotani, Hiroyuki Ariyasu, Satoko Shimazu-Kuwahara, Yoshiyuki Shimizu, Hidenari Nomura, Yoshiteru Murofushi, Kentaro Kaneko, Ryota Izumi, Masaki Matsubara, Hajime Kanda, Michio Noguchi, Tomohiro Tanaka, Toru Kusakabe, Takashi Miyazawa, Kazuwa Nakao

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Abstract

To elucidate the clinical implication of ghrelin, we have been trying to generate variable models of transgenic (Tg) mice overexpressing ghrelin. We generated Tg mice overexpressing des-acyl ghrelin in a wide variety of tissues under the control of β-actin promoter. While plasma des-acyl ghrelin level in the Tg mice was 44-fold greater than that of control mice, there was no differences in the plasma ghrelin level between des-acyl ghrelin Tg and the control mice. The des-acyl ghrelin Tg mice exhibited the lower body weight and the shorter body length due to modulation of GH-IGF-1 axis. We tried to generate Tg mice expressing a ghrelin analog, which possessed ghrelin-like activity (Trp³-ghrelin Tg mice). The plasma Trp³-ghrelin concentration in Trp³-ghrelin Tg mice was approximately 85-fold higher than plasma ghrelin (acylated ghrelin) concentration seen in the control mice. Because Trp³-ghrelin is approximately 24-fold less potent than ghrelin, the plasma Trp³-ghrelin concentration in Trp³-ghrelin Tg mice was calculated to have approximately 3.5-fold biological activity greater than that of ghrelin (acylated ghrelin) in the control mice. Trp³-ghrelin Tg mice did not show any phenotypes except for reduced insulin sensitivity in 1-year old. After the identification of ghrelin O-acyltransferase (GOAT), we generated doubly Tg mice overexpressing both mouse des-acyl ghrelin and mouse GOAT in the liver by cross-mating the two kinds of Tg mice. The plasma ghrelin concentration of doubly Tg mice was approximately 2-fold higher than that of the control mice. No apparent phenotypic changes in body weight and food intake were observed in doubly Tg mice. Further studies are ongoing in our laboratory to generate Tg mice with the increased plasma ghrelin level to a greater extent. The better understanding of physiological and pathophysiological significance of ghrelin from experiments using an excellent animal model may provide a new therapeutic approach for human diseases.

Original language	English
Pages (from-to)	S31-S33
Journal	Endocrine Journal
Volume	64
DOIs	https://doi.org/10.1507/endocrj.64.S31
Publication status	Published - 2017
Externally published	Yes

All Science Journal Classification (ASJC) codes

Endocrinology, Diabetes and Metabolism
Endocrinology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1507/endocrj.64.S31

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Aotani, D., Ariyasu, H., Shimazu-Kuwahara, S., Shimizu, Y., Nomura, H., Murofushi, Y., Kaneko, K., Izumi, R., Matsubara, M., Kanda, H., Noguchi, M., Tanaka, T., Kusakabe, T., Miyazawa, T., & Nakao, K. (2017). Development of ghrelin transgenic mice for elucidation of clinical implication of ghrelin. Endocrine Journal, 64, S31-S33. https://doi.org/10.1507/endocrj.64.S31

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title = "Development of ghrelin transgenic mice for elucidation of clinical implication of ghrelin",

abstract = "To elucidate the clinical implication of ghrelin, we have been trying to generate variable models of transgenic (Tg) mice overexpressing ghrelin. We generated Tg mice overexpressing des-acyl ghrelin in a wide variety of tissues under the control of β-actin promoter. While plasma des-acyl ghrelin level in the Tg mice was 44-fold greater than that of control mice, there was no differences in the plasma ghrelin level between des-acyl ghrelin Tg and the control mice. The des-acyl ghrelin Tg mice exhibited the lower body weight and the shorter body length due to modulation of GH-IGF-1 axis. We tried to generate Tg mice expressing a ghrelin analog, which possessed ghrelin-like activity (Trp3-ghrelin Tg mice). The plasma Trp3-ghrelin concentration in Trp3-ghrelin Tg mice was approximately 85-fold higher than plasma ghrelin (acylated ghrelin) concentration seen in the control mice. Because Trp3-ghrelin is approximately 24-fold less potent than ghrelin, the plasma Trp3-ghrelin concentration in Trp3-ghrelin Tg mice was calculated to have approximately 3.5-fold biological activity greater than that of ghrelin (acylated ghrelin) in the control mice. Trp3-ghrelin Tg mice did not show any phenotypes except for reduced insulin sensitivity in 1-year old. After the identification of ghrelin O-acyltransferase (GOAT), we generated doubly Tg mice overexpressing both mouse des-acyl ghrelin and mouse GOAT in the liver by cross-mating the two kinds of Tg mice. The plasma ghrelin concentration of doubly Tg mice was approximately 2-fold higher than that of the control mice. No apparent phenotypic changes in body weight and food intake were observed in doubly Tg mice. Further studies are ongoing in our laboratory to generate Tg mice with the increased plasma ghrelin level to a greater extent. The better understanding of physiological and pathophysiological significance of ghrelin from experiments using an excellent animal model may provide a new therapeutic approach for human diseases.",

author = "Daisuke Aotani and Hiroyuki Ariyasu and Satoko Shimazu-Kuwahara and Yoshiyuki Shimizu and Hidenari Nomura and Yoshiteru Murofushi and Kentaro Kaneko and Ryota Izumi and Masaki Matsubara and Hajime Kanda and Michio Noguchi and Tomohiro Tanaka and Toru Kusakabe and Takashi Miyazawa and Kazuwa Nakao",

note = "Publisher Copyright: {\textcopyright} 2017 The Japan Endocrine Society.",

year = "2017",

doi = "10.1507/endocrj.64.S31",

language = "English",

volume = "64",

pages = "S31--S33",

journal = "Endocrine Journal",

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T1 - Development of ghrelin transgenic mice for elucidation of clinical implication of ghrelin

AU - Aotani, Daisuke

AU - Ariyasu, Hiroyuki

AU - Shimazu-Kuwahara, Satoko

AU - Shimizu, Yoshiyuki

AU - Nomura, Hidenari

AU - Murofushi, Yoshiteru

AU - Kaneko, Kentaro

AU - Izumi, Ryota

AU - Matsubara, Masaki

AU - Kanda, Hajime

AU - Noguchi, Michio

AU - Tanaka, Tomohiro

AU - Kusakabe, Toru

AU - Miyazawa, Takashi

AU - Nakao, Kazuwa

PY - 2017

Y1 - 2017

N2 - To elucidate the clinical implication of ghrelin, we have been trying to generate variable models of transgenic (Tg) mice overexpressing ghrelin. We generated Tg mice overexpressing des-acyl ghrelin in a wide variety of tissues under the control of β-actin promoter. While plasma des-acyl ghrelin level in the Tg mice was 44-fold greater than that of control mice, there was no differences in the plasma ghrelin level between des-acyl ghrelin Tg and the control mice. The des-acyl ghrelin Tg mice exhibited the lower body weight and the shorter body length due to modulation of GH-IGF-1 axis. We tried to generate Tg mice expressing a ghrelin analog, which possessed ghrelin-like activity (Trp3-ghrelin Tg mice). The plasma Trp3-ghrelin concentration in Trp3-ghrelin Tg mice was approximately 85-fold higher than plasma ghrelin (acylated ghrelin) concentration seen in the control mice. Because Trp3-ghrelin is approximately 24-fold less potent than ghrelin, the plasma Trp3-ghrelin concentration in Trp3-ghrelin Tg mice was calculated to have approximately 3.5-fold biological activity greater than that of ghrelin (acylated ghrelin) in the control mice. Trp3-ghrelin Tg mice did not show any phenotypes except for reduced insulin sensitivity in 1-year old. After the identification of ghrelin O-acyltransferase (GOAT), we generated doubly Tg mice overexpressing both mouse des-acyl ghrelin and mouse GOAT in the liver by cross-mating the two kinds of Tg mice. The plasma ghrelin concentration of doubly Tg mice was approximately 2-fold higher than that of the control mice. No apparent phenotypic changes in body weight and food intake were observed in doubly Tg mice. Further studies are ongoing in our laboratory to generate Tg mice with the increased plasma ghrelin level to a greater extent. The better understanding of physiological and pathophysiological significance of ghrelin from experiments using an excellent animal model may provide a new therapeutic approach for human diseases.

AB - To elucidate the clinical implication of ghrelin, we have been trying to generate variable models of transgenic (Tg) mice overexpressing ghrelin. We generated Tg mice overexpressing des-acyl ghrelin in a wide variety of tissues under the control of β-actin promoter. While plasma des-acyl ghrelin level in the Tg mice was 44-fold greater than that of control mice, there was no differences in the plasma ghrelin level between des-acyl ghrelin Tg and the control mice. The des-acyl ghrelin Tg mice exhibited the lower body weight and the shorter body length due to modulation of GH-IGF-1 axis. We tried to generate Tg mice expressing a ghrelin analog, which possessed ghrelin-like activity (Trp3-ghrelin Tg mice). The plasma Trp3-ghrelin concentration in Trp3-ghrelin Tg mice was approximately 85-fold higher than plasma ghrelin (acylated ghrelin) concentration seen in the control mice. Because Trp3-ghrelin is approximately 24-fold less potent than ghrelin, the plasma Trp3-ghrelin concentration in Trp3-ghrelin Tg mice was calculated to have approximately 3.5-fold biological activity greater than that of ghrelin (acylated ghrelin) in the control mice. Trp3-ghrelin Tg mice did not show any phenotypes except for reduced insulin sensitivity in 1-year old. After the identification of ghrelin O-acyltransferase (GOAT), we generated doubly Tg mice overexpressing both mouse des-acyl ghrelin and mouse GOAT in the liver by cross-mating the two kinds of Tg mice. The plasma ghrelin concentration of doubly Tg mice was approximately 2-fold higher than that of the control mice. No apparent phenotypic changes in body weight and food intake were observed in doubly Tg mice. Further studies are ongoing in our laboratory to generate Tg mice with the increased plasma ghrelin level to a greater extent. The better understanding of physiological and pathophysiological significance of ghrelin from experiments using an excellent animal model may provide a new therapeutic approach for human diseases.

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Development of ghrelin transgenic mice for elucidation of clinical implication of ghrelin

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