K. Blad scite author profile

The body growth of animals is regulated by growth hormone and IGF-I. The classical theory of this regulation is that most IGF-I in the blood originates in the liver and that body growth is controlled by the concentration of IGF-I in the blood. We have abolished IGF-I production in the livers of mice by using the Cre͞loxP recombination system. These mice demonstrated complete inactivation of the IGF-I gene in the hepatocytes. Although the liver accounts for less than 5% of body mass, the concentration of IGF-I in the serum was reduced by 75%. This finding confirms that the liver is the principal source of IGF-I in the blood. However, the reduction in serum IGF-I concentration had no discernible effect on postnatal body growth. We conclude that postnatal body growth is preserved despite complete absence of IGF-I production by the hepatocytes.

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Insulin-like growth factor signalling pathways in rat hepatic stellate cells: Effects on DNA synthesis and hepatocyte growth factor production

Skrtic¹,

Blad²,

Gressner³

et al. 1999

Growth Hormone & IGF Research

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Insulin-like growth factor signalling pathways inrat hepatic stellate cells are important for DNA synthesis and hepatocyte growth factor production

Skrtic¹,

Blad²,

Gressner³

et al. 2000

Growth Hormone & IGF Research

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K. Blad

Liver-derived insulin-like growth factor I (IGF-I) is the principal source of IGF-I in blood but is not required for postnatal body growth in mice

Insulin-like growth factor signalling pathways in rat hepatic stellate cells: Effects on DNA synthesis and hepatocyte growth factor production

Insulin-like growth factor signalling pathways inrat hepatic stellate cells are important for DNA synthesis and hepatocyte growth factor production

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