Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice

Kana Ikegami; Teppei Goto; Sho Nakamura; Youki Watanabe; Arisa Sugimoto; Sutisa Majarune; Kei Horihata; Mayuko Nagae; Junko Tomikawa; Takuya Imamura; Makoto Sanbo; Masumi Hirabayashi; Naoko Inoue; Kei Ichiro Maeda; Hiroko Tsukamura; Yoshihisa Uenoyama

doi:10.1262/jrd.2020-026

Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice

Kana Ikegami, Teppei Goto, Sho Nakamura, Youki Watanabe, Arisa Sugimoto, Sutisa Majarune, Kei Horihata, Mayuko Nagae, Junko Tomikawa, Takuya Imamura, Makoto Sanbo, Masumi Hirabayashi, Naoko Inoue, Kei Ichiro Maeda, Hiroko Tsukamura, Yoshihisa Uenoyama

Stem Cell Biology and Medicine

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21 Citations (Scopus)

Abstract

The present study aimed to evaluate whether novel conditional kisspeptin neuron-specific Kiss1 knockout (KO) mice utilizing the Cre-loxP system could recapitulate the infertility of global Kiss1 KO models, thereby providing further evidence for the fundamental role of hypothalamic kisspeptin neurons in regulating mammalian reproduction. We generated Kiss1-floxed mice and hypothalamic kisspeptin neuron-specific Cre-expressing transgenic mice and then crossed these two lines. The conditional Kiss1 KO mice showed pubertal failure along with a suppression of gonadotropin secretion and ovarian atrophy. These results indicate that newly-created hypothalamic Kiss1 KO mice obtained by the Cre-loxP system recapitulated the infertility of global Kiss1 KO models, suggesting that hypothalamic kisspeptin, but not peripheral kisspeptin, is critical for reproduction. Importantly, these Kiss1-floxed mice are now available and will be a valuable tool for detailed analyses of roles of each population of kisspeptin neurons in the brain and peripheral kisspeptin-producing cells by the spatiotemporal-specific manipulation of Cre expression.

Original language	English
Pages (from-to)	359-367
Number of pages	9
Journal	Journal of Reproduction and Development
Volume	66
Issue number	4
DOIs	https://doi.org/10.1262/jrd.2020-026
Publication status	Published - 2020

All Science Journal Classification (ASJC) codes

Animal Science and Zoology

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10.1262/jrd.2020-026

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Ikegami, K., Goto, T., Nakamura, S., Watanabe, Y., Sugimoto, A., Majarune, S., Horihata, K., Nagae, M., Tomikawa, J., Imamura, T., Sanbo, M., Hirabayashi, M., Inoue, N., Maeda, K. I., Tsukamura, H., & Uenoyama, Y. (2020). Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice. Journal of Reproduction and Development, 66(4), 359-367. https://doi.org/10.1262/jrd.2020-026

Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice. / Ikegami, Kana; Goto, Teppei; Nakamura, Sho et al.
In: Journal of Reproduction and Development, Vol. 66, No. 4, 2020, p. 359-367.

Research output: Contribution to journal › Article › peer-review

Ikegami, K, Goto, T, Nakamura, S, Watanabe, Y, Sugimoto, A, Majarune, S, Horihata, K, Nagae, M, Tomikawa, J, Imamura, T, Sanbo, M, Hirabayashi, M, Inoue, N, Maeda, KI, Tsukamura, H & Uenoyama, Y 2020, 'Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice', Journal of Reproduction and Development, vol. 66, no. 4, pp. 359-367. https://doi.org/10.1262/jrd.2020-026

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title = "Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice",

abstract = "The present study aimed to evaluate whether novel conditional kisspeptin neuron-specific Kiss1 knockout (KO) mice utilizing the Cre-loxP system could recapitulate the infertility of global Kiss1 KO models, thereby providing further evidence for the fundamental role of hypothalamic kisspeptin neurons in regulating mammalian reproduction. We generated Kiss1-floxed mice and hypothalamic kisspeptin neuron-specific Cre-expressing transgenic mice and then crossed these two lines. The conditional Kiss1 KO mice showed pubertal failure along with a suppression of gonadotropin secretion and ovarian atrophy. These results indicate that newly-created hypothalamic Kiss1 KO mice obtained by the Cre-loxP system recapitulated the infertility of global Kiss1 KO models, suggesting that hypothalamic kisspeptin, but not peripheral kisspeptin, is critical for reproduction. Importantly, these Kiss1-floxed mice are now available and will be a valuable tool for detailed analyses of roles of each population of kisspeptin neurons in the brain and peripheral kisspeptin-producing cells by the spatiotemporal-specific manipulation of Cre expression.",

author = "Kana Ikegami and Teppei Goto and Sho Nakamura and Youki Watanabe and Arisa Sugimoto and Sutisa Majarune and Kei Horihata and Mayuko Nagae and Junko Tomikawa and Takuya Imamura and Makoto Sanbo and Masumi Hirabayashi and Naoko Inoue and Maeda, {Kei Ichiro} and Hiroko Tsukamura and Yoshihisa Uenoyama",

note = "Funding Information: The authors are grateful to the National Hormone and Peptide Program (HNPP), National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK), and Dr AF Parlow for providing the LH and FSH assay kit. The radioimmunoassays were performed at the Nagoya University Radioisotope Center. We wish to thank Dr Nicola Skoulding for editorial assistance and Takashi Hirashima, Tatsuya Fukanuma, Moe Yanagihara, Hitomi Abe, Yuhei Takaya-ma, Ren Ishigaki, Saki Okamoto and Koki Yamada for their technical support. This work was supported in part by a Grant-in-Aid for the JSPS Fellows (No. 26-4247 to KI); the Research Program on Innovative Technologies for Animal Breeding, Reproduction, and Vaccine Development Grant (REP2002 to HT); the Science and Technology Research Promotion Program for Agriculture, Forestry, Fisheries, and Food Industry (to HT); a Grants-in Aid from the Japan Society for the Promotion of Science (18H03973 and 18K19267 to HT); and the Cooperative Study Program of National Institute for Physiological Sciences. Publisher Copyright: {\textcopyright} 2020 by the Society for Reproduction and Development.",

year = "2020",

doi = "10.1262/jrd.2020-026",

language = "English",

volume = "66",

pages = "359--367",

journal = "Journal of Reproduction and Development",

issn = "0916-8818",

publisher = "Japanese Society of Animal Reproduction (JSAR)",

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T1 - Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice

AU - Ikegami, Kana

AU - Goto, Teppei

AU - Nakamura, Sho

AU - Watanabe, Youki

AU - Sugimoto, Arisa

AU - Majarune, Sutisa

AU - Horihata, Kei

AU - Nagae, Mayuko

AU - Tomikawa, Junko

AU - Imamura, Takuya

AU - Sanbo, Makoto

AU - Hirabayashi, Masumi

AU - Inoue, Naoko

AU - Maeda, Kei Ichiro

AU - Tsukamura, Hiroko

AU - Uenoyama, Yoshihisa

N1 - Funding Information: The authors are grateful to the National Hormone and Peptide Program (HNPP), National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK), and Dr AF Parlow for providing the LH and FSH assay kit. The radioimmunoassays were performed at the Nagoya University Radioisotope Center. We wish to thank Dr Nicola Skoulding for editorial assistance and Takashi Hirashima, Tatsuya Fukanuma, Moe Yanagihara, Hitomi Abe, Yuhei Takaya-ma, Ren Ishigaki, Saki Okamoto and Koki Yamada for their technical support. This work was supported in part by a Grant-in-Aid for the JSPS Fellows (No. 26-4247 to KI); the Research Program on Innovative Technologies for Animal Breeding, Reproduction, and Vaccine Development Grant (REP2002 to HT); the Science and Technology Research Promotion Program for Agriculture, Forestry, Fisheries, and Food Industry (to HT); a Grants-in Aid from the Japan Society for the Promotion of Science (18H03973 and 18K19267 to HT); and the Cooperative Study Program of National Institute for Physiological Sciences. Publisher Copyright: © 2020 by the Society for Reproduction and Development.

PY - 2020

Y1 - 2020

N2 - The present study aimed to evaluate whether novel conditional kisspeptin neuron-specific Kiss1 knockout (KO) mice utilizing the Cre-loxP system could recapitulate the infertility of global Kiss1 KO models, thereby providing further evidence for the fundamental role of hypothalamic kisspeptin neurons in regulating mammalian reproduction. We generated Kiss1-floxed mice and hypothalamic kisspeptin neuron-specific Cre-expressing transgenic mice and then crossed these two lines. The conditional Kiss1 KO mice showed pubertal failure along with a suppression of gonadotropin secretion and ovarian atrophy. These results indicate that newly-created hypothalamic Kiss1 KO mice obtained by the Cre-loxP system recapitulated the infertility of global Kiss1 KO models, suggesting that hypothalamic kisspeptin, but not peripheral kisspeptin, is critical for reproduction. Importantly, these Kiss1-floxed mice are now available and will be a valuable tool for detailed analyses of roles of each population of kisspeptin neurons in the brain and peripheral kisspeptin-producing cells by the spatiotemporal-specific manipulation of Cre expression.

AB - The present study aimed to evaluate whether novel conditional kisspeptin neuron-specific Kiss1 knockout (KO) mice utilizing the Cre-loxP system could recapitulate the infertility of global Kiss1 KO models, thereby providing further evidence for the fundamental role of hypothalamic kisspeptin neurons in regulating mammalian reproduction. We generated Kiss1-floxed mice and hypothalamic kisspeptin neuron-specific Cre-expressing transgenic mice and then crossed these two lines. The conditional Kiss1 KO mice showed pubertal failure along with a suppression of gonadotropin secretion and ovarian atrophy. These results indicate that newly-created hypothalamic Kiss1 KO mice obtained by the Cre-loxP system recapitulated the infertility of global Kiss1 KO models, suggesting that hypothalamic kisspeptin, but not peripheral kisspeptin, is critical for reproduction. Importantly, these Kiss1-floxed mice are now available and will be a valuable tool for detailed analyses of roles of each population of kisspeptin neurons in the brain and peripheral kisspeptin-producing cells by the spatiotemporal-specific manipulation of Cre expression.

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Conditional kisspeptin neuron-specific Kiss1 knockout with newly generated Kiss1-floxed and Kiss1-cre mice replicates a hypogonadal phenotype of global Kiss1 knockout mice

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