Normal growth and development in the absence of hepatic insulin-like growth factor I

Shoshana Yakar; Jun L.I. Liu; Bethel Stannard; Andrew Butler; Domenici Accili; Brian Sauer; Derek Leroith

doi:10.1073/pnas.96.13.7324

Normal growth and development in the absence of hepatic insulin-like growth factor I

Shoshana Yakar, Jun L.I. Liu, Bethel Stannard, Andrew Butler, Domenici Accili, Brian Sauer, Derek Leroith

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Abstract

The somatomedin hypothesis proposed that insulin-like growth factor I (IGF-I) was a hepatically derived circulating mediator of growth hormone and is a crucial factor for postnatal growth and development. To reassess this hypothesis, we have used the Cre/loxP recombination system to delete the igf1 gene exclusively in the liver. igf1 gene deletion in the liver abrogated expression of igf1 mRNA and caused a dramatic reduction in circulating IGF-I levels. However, growth as determined by body weight, body length, and femoral length did not differ from wild-type littermates. Although our model proves that hepatic IGF-I is indeed the major contributor to circulating IGF-I levels in mice it challenges the concept that circulating IGF-I is crucial for normal postnatal growth. Rather, our model provides direct evidence for the importance of the autocrine/paracrine role of IGF-I.

Original language	English
Pages (from-to)	7324-7329
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	96
Issue number	13
DOIs	https://doi.org/10.1073/pnas.96.13.7324
State	Published - 22 Jun 1999
Externally published	Yes

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title = "Normal growth and development in the absence of hepatic insulin-like growth factor I",

abstract = "The somatomedin hypothesis proposed that insulin-like growth factor I (IGF-I) was a hepatically derived circulating mediator of growth hormone and is a crucial factor for postnatal growth and development. To reassess this hypothesis, we have used the Cre/loxP recombination system to delete the igf1 gene exclusively in the liver. igf1 gene deletion in the liver abrogated expression of igf1 mRNA and caused a dramatic reduction in circulating IGF-I levels. However, growth as determined by body weight, body length, and femoral length did not differ from wild-type littermates. Although our model proves that hepatic IGF-I is indeed the major contributor to circulating IGF-I levels in mice it challenges the concept that circulating IGF-I is crucial for normal postnatal growth. Rather, our model provides direct evidence for the importance of the autocrine/paracrine role of IGF-I.",

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AU - Yakar, Shoshana

AU - Liu, Jun L.I.

AU - Stannard, Bethel

AU - Butler, Andrew

AU - Accili, Domenici

AU - Sauer, Brian

AU - Leroith, Derek

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AB - The somatomedin hypothesis proposed that insulin-like growth factor I (IGF-I) was a hepatically derived circulating mediator of growth hormone and is a crucial factor for postnatal growth and development. To reassess this hypothesis, we have used the Cre/loxP recombination system to delete the igf1 gene exclusively in the liver. igf1 gene deletion in the liver abrogated expression of igf1 mRNA and caused a dramatic reduction in circulating IGF-I levels. However, growth as determined by body weight, body length, and femoral length did not differ from wild-type littermates. Although our model proves that hepatic IGF-I is indeed the major contributor to circulating IGF-I levels in mice it challenges the concept that circulating IGF-I is crucial for normal postnatal growth. Rather, our model provides direct evidence for the importance of the autocrine/paracrine role of IGF-I.

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Normal growth and development in the absence of hepatic insulin-like growth factor I

Abstract

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