Mutation of the insulin receptor at tyrosine 960 inhibits signal transmission but does not affect its tyrosine kinase activity

Morris F. White; James N. Livingston; Jonathan M. Backer; Vilma Lauris; Thomas J. Dull; Axel Ullrich; C. Ronald Kahn

doi:10.1016/S0092-8674(88)80008-4

Mutation of the insulin receptor at tyrosine 960 inhibits signal transmission but does not affect its tyrosine kinase activity

Morris F. White, James N. Livingston, Jonathan M. Backer, Vilma Lauris, Thomas J. Dull, Axel Ullrich, C. Ronald Kahn

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

341 Scopus citations

Abstract

Tyrosyl phosphorylation is implicated in the mechanism of insulin action. Mutation of the β-subunit of the insulin receptor by substitution of tyrosyl residue 960 with phenylalanine had no effect on insulin-stimulated autophosphorylation or phosphotransferase activity of the purified receptor. However, unlike the normal receptor, this mutant was not biologically active in Chinese hamster ovary cells. Furthermore, insulin-stimulated tyrosyl phosphorylation of at least one endogenous substrate (pp185) was increased significantly in cells expressing the normal receptor but was barely detected in cells expressing the mutant. Therefore, β-subunit autophosphorylation was not sufficient for the insulin response, and a region of the insulin receptor around Tyr-960 may facilitate phosphorylation of cellular substrates required for transmission of the insulin signal.

Original language	English (US)
Pages (from-to)	641-649
Number of pages	9
Journal	Cell
Volume	54
Issue number	5
DOIs	https://doi.org/10.1016/S0092-8674(88)80008-4
State	Published - Aug 26 1988
Externally published	Yes

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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10.1016/S0092-8674(88)80008-4

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title = "Mutation of the insulin receptor at tyrosine 960 inhibits signal transmission but does not affect its tyrosine kinase activity",

abstract = "Tyrosyl phosphorylation is implicated in the mechanism of insulin action. Mutation of the β-subunit of the insulin receptor by substitution of tyrosyl residue 960 with phenylalanine had no effect on insulin-stimulated autophosphorylation or phosphotransferase activity of the purified receptor. However, unlike the normal receptor, this mutant was not biologically active in Chinese hamster ovary cells. Furthermore, insulin-stimulated tyrosyl phosphorylation of at least one endogenous substrate (pp185) was increased significantly in cells expressing the normal receptor but was barely detected in cells expressing the mutant. Therefore, β-subunit autophosphorylation was not sufficient for the insulin response, and a region of the insulin receptor around Tyr-960 may facilitate phosphorylation of cellular substrates required for transmission of the insulin signal.",

author = "White, {Morris F.} and Livingston, {James N.} and Backer, {Jonathan M.} and Vilma Lauris and Dull, {Thomas J.} and Axel Ullrich and Kahn, {C. Ronald}",

note = "Funding Information: This work was supported in part by a Research and Development Award from the American Diabetes Association, National Institutes of Health grants DK35988 and DK38712 to M. E W., and NIH grants AM31036 and AM33201 to C. R. K. M. E W. is a scholar of the Pew Foundation, Philadelphia. The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked {"}advertisement{"} in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.",

year = "1988",

month = aug,

day = "26",

doi = "10.1016/S0092-8674(88)80008-4",

language = "English (US)",

volume = "54",

pages = "641--649",

journal = "Cell",

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T1 - Mutation of the insulin receptor at tyrosine 960 inhibits signal transmission but does not affect its tyrosine kinase activity

AU - White, Morris F.

AU - Livingston, James N.

AU - Backer, Jonathan M.

AU - Lauris, Vilma

AU - Dull, Thomas J.

AU - Ullrich, Axel

AU - Kahn, C. Ronald

N1 - Funding Information: This work was supported in part by a Research and Development Award from the American Diabetes Association, National Institutes of Health grants DK35988 and DK38712 to M. E W., and NIH grants AM31036 and AM33201 to C. R. K. M. E W. is a scholar of the Pew Foundation, Philadelphia. The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

PY - 1988/8/26

Y1 - 1988/8/26

N2 - Tyrosyl phosphorylation is implicated in the mechanism of insulin action. Mutation of the β-subunit of the insulin receptor by substitution of tyrosyl residue 960 with phenylalanine had no effect on insulin-stimulated autophosphorylation or phosphotransferase activity of the purified receptor. However, unlike the normal receptor, this mutant was not biologically active in Chinese hamster ovary cells. Furthermore, insulin-stimulated tyrosyl phosphorylation of at least one endogenous substrate (pp185) was increased significantly in cells expressing the normal receptor but was barely detected in cells expressing the mutant. Therefore, β-subunit autophosphorylation was not sufficient for the insulin response, and a region of the insulin receptor around Tyr-960 may facilitate phosphorylation of cellular substrates required for transmission of the insulin signal.

AB - Tyrosyl phosphorylation is implicated in the mechanism of insulin action. Mutation of the β-subunit of the insulin receptor by substitution of tyrosyl residue 960 with phenylalanine had no effect on insulin-stimulated autophosphorylation or phosphotransferase activity of the purified receptor. However, unlike the normal receptor, this mutant was not biologically active in Chinese hamster ovary cells. Furthermore, insulin-stimulated tyrosyl phosphorylation of at least one endogenous substrate (pp185) was increased significantly in cells expressing the normal receptor but was barely detected in cells expressing the mutant. Therefore, β-subunit autophosphorylation was not sufficient for the insulin response, and a region of the insulin receptor around Tyr-960 may facilitate phosphorylation of cellular substrates required for transmission of the insulin signal.

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JO - Cell

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Mutation of the insulin receptor at tyrosine 960 inhibits signal transmission but does not affect its tyrosine kinase activity

Abstract

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