Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4

Loretta L. Collins; Yi Fen Lee; Cynthia A. Heinlein; Ning Chun Liu; Yei Tsung Chen; Chih Rong Shyr; Charles K. Meshul; Hideo Uno; Kenneth A. Platt; Chawnshang Chang

doi:10.1073/pnas.0405700101

Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4

Loretta L. Collins, Yi Fen Lee, Cynthia A. Heinlein, Ning Chun Liu, Yei Tsung Chen, Chih Rong Shyr, Charles K. Meshul, Hideo Uno, Kenneth A. Platt, Chawnshang Chang^*

^*Corresponding author for this work

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

86 Scopus citations

Abstract

Testicular orphan nuclear receptor 4 (TR4) is a member of the nuclear receptor superfamily for which a ligand has not yet been found. In vitro data obtained from various cell lines suggest that TR4 functions as a master regulator to modulate many signaling pathways, yet the in vivo physiological roles of TR4 remain unclear. Here, we report the generation of mice lacking TR4 by means of targeted gene disruption (TR4^-/-). The number of TR4 ^-/- pups generated by the mating of TR4^+/- mice is well under that predicted by the normal Mendelian ratio, and TR4^-/- mice demonstrate high rates of early postnatal mortality, as well as significant growth retardation. Additionally, TR4^-/- females show defects in reproduction and maternal behavior, with pups of TR4^-/- dams dying soon after birth with no indication of milk intake. These results provide in vivo evidence that TR4 plays important roles in growth, embryonic and early postnatal pup survival, female reproductive function, and maternal behavior.

Original language	English
Pages (from-to)	15058-15063
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	101
Issue number	42
DOIs	https://doi.org/10.1073/pnas.0405700101
State	Published - 19 10 2004
Externally published	Yes

Keywords

Gene expression regulation
Knockout mice
Reproduction

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10.1073/pnas.0405700101

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Collins, L. L., Lee, Y. F., Heinlein, C. A., Liu, N. C., Chen, Y. T., Shyr, C. R., Meshul, C. K., Uno, H., Platt, K. A., & Chang, C. (2004). Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4. Proceedings of the National Academy of Sciences of the United States of America, 101(42), 15058-15063. https://doi.org/10.1073/pnas.0405700101

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title = "Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4",

abstract = "Testicular orphan nuclear receptor 4 (TR4) is a member of the nuclear receptor superfamily for which a ligand has not yet been found. In vitro data obtained from various cell lines suggest that TR4 functions as a master regulator to modulate many signaling pathways, yet the in vivo physiological roles of TR4 remain unclear. Here, we report the generation of mice lacking TR4 by means of targeted gene disruption (TR4-/-). The number of TR4 -/- pups generated by the mating of TR4+/- mice is well under that predicted by the normal Mendelian ratio, and TR4-/- mice demonstrate high rates of early postnatal mortality, as well as significant growth retardation. Additionally, TR4-/- females show defects in reproduction and maternal behavior, with pups of TR4-/- dams dying soon after birth with no indication of milk intake. These results provide in vivo evidence that TR4 plays important roles in growth, embryonic and early postnatal pup survival, female reproductive function, and maternal behavior.",

keywords = "Gene expression regulation, Knockout mice, Reproduction",

author = "Collins, {Loretta L.} and Lee, {Yi Fen} and Heinlein, {Cynthia A.} and Liu, {Ning Chun} and Chen, {Yei Tsung} and Shyr, {Chih Rong} and Meshul, {Charles K.} and Hideo Uno and Platt, {Kenneth A.} and Chawnshang Chang",

year = "2004",

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doi = "10.1073/pnas.0405700101",

language = "英语",

volume = "101",

pages = "15058--15063",

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Collins, LL, Lee, YF, Heinlein, CA, Liu, NC, Chen, YT, Shyr, CR, Meshul, CK, Uno, H, Platt, KA & Chang, C 2004, 'Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4', Proceedings of the National Academy of Sciences of the United States of America, vol. 101, no. 42, pp. 15058-15063. https://doi.org/10.1073/pnas.0405700101

Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4. / Collins, Loretta L.; Lee, Yi Fen; Heinlein, Cynthia A. et al.
In: Proceedings of the National Academy of Sciences of the United States of America, Vol. 101, No. 42, 19.10.2004, p. 15058-15063.

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

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T1 - Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4

AU - Collins, Loretta L.

AU - Lee, Yi Fen

AU - Heinlein, Cynthia A.

AU - Liu, Ning Chun

AU - Chen, Yei Tsung

AU - Shyr, Chih Rong

AU - Meshul, Charles K.

AU - Uno, Hideo

AU - Platt, Kenneth A.

AU - Chang, Chawnshang

PY - 2004/10/19

Y1 - 2004/10/19

N2 - Testicular orphan nuclear receptor 4 (TR4) is a member of the nuclear receptor superfamily for which a ligand has not yet been found. In vitro data obtained from various cell lines suggest that TR4 functions as a master regulator to modulate many signaling pathways, yet the in vivo physiological roles of TR4 remain unclear. Here, we report the generation of mice lacking TR4 by means of targeted gene disruption (TR4-/-). The number of TR4 -/- pups generated by the mating of TR4+/- mice is well under that predicted by the normal Mendelian ratio, and TR4-/- mice demonstrate high rates of early postnatal mortality, as well as significant growth retardation. Additionally, TR4-/- females show defects in reproduction and maternal behavior, with pups of TR4-/- dams dying soon after birth with no indication of milk intake. These results provide in vivo evidence that TR4 plays important roles in growth, embryonic and early postnatal pup survival, female reproductive function, and maternal behavior.

AB - Testicular orphan nuclear receptor 4 (TR4) is a member of the nuclear receptor superfamily for which a ligand has not yet been found. In vitro data obtained from various cell lines suggest that TR4 functions as a master regulator to modulate many signaling pathways, yet the in vivo physiological roles of TR4 remain unclear. Here, we report the generation of mice lacking TR4 by means of targeted gene disruption (TR4-/-). The number of TR4 -/- pups generated by the mating of TR4+/- mice is well under that predicted by the normal Mendelian ratio, and TR4-/- mice demonstrate high rates of early postnatal mortality, as well as significant growth retardation. Additionally, TR4-/- females show defects in reproduction and maternal behavior, with pups of TR4-/- dams dying soon after birth with no indication of milk intake. These results provide in vivo evidence that TR4 plays important roles in growth, embryonic and early postnatal pup survival, female reproductive function, and maternal behavior.

KW - Gene expression regulation

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JF - Proceedings of the National Academy of Sciences of the United States of America

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ER -

Growth retardation and abnormal maternal behavior in mice lacking testicular orphan nuclear receptor 4

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