Spongiform degeneration in mahoganoid mutant mice

Lin He; Xin Yun Lu; Aaron F. Jolly; Adam G. Eldridge; Stanley J. Watson; Peter K. Jackson; Gregory S. Barsh; Teresa M. Gunn

doi:10.1126/science.1079694

Spongiform degeneration in mahoganoid mutant mice

Lin He, Xin Yun Lu, Aaron F. Jolly, Adam G. Eldridge, Stanley J. Watson, Peter K. Jackson, Gregory S. Barsh, Teresa M. Gunn

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Abstract

mahoganoid is a mouse coat-color mutation whose pigmentary phenotype and genetic interactions resemble those of Attractin (Atrn). Atrn mutations also cause spongiform neurodegeneration. Here, we show that a null mutation for mahoganoid causes a similar age-dependent neuropathology that includes many features of prion diseases but without accumulation of protease-resistant prion protein. The gene mutated in mahoganoid encodes a RING-containing protein with E3 ubiquitin ligase activity in vitro. Similarities in phenotype, expression, and genetic interactions suggest that mahoganoid and Atrn genes are part of a conserved pathway for regulated protein turnover whose function is essential for neuronal viability.

Original language	English (US)
Pages (from-to)	710-712
Number of pages	3
Journal	Science
Volume	299
Issue number	5607
DOIs	https://doi.org/10.1126/science.1079694
State	Published - Jan 31 2003
Externally published	Yes

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title = "Spongiform degeneration in mahoganoid mutant mice",

abstract = "mahoganoid is a mouse coat-color mutation whose pigmentary phenotype and genetic interactions resemble those of Attractin (Atrn). Atrn mutations also cause spongiform neurodegeneration. Here, we show that a null mutation for mahoganoid causes a similar age-dependent neuropathology that includes many features of prion diseases but without accumulation of protease-resistant prion protein. The gene mutated in mahoganoid encodes a RING-containing protein with E3 ubiquitin ligase activity in vitro. Similarities in phenotype, expression, and genetic interactions suggest that mahoganoid and Atrn genes are part of a conserved pathway for regulated protein turnover whose function is essential for neuronal viability.",

author = "Lin He and Lu, {Xin Yun} and Jolly, {Aaron F.} and Eldridge, {Adam G.} and Watson, {Stanley J.} and Jackson, {Peter K.} and Barsh, {Gregory S.} and Gunn, {Teresa M.}",

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T1 - Spongiform degeneration in mahoganoid mutant mice

AU - He, Lin

AU - Lu, Xin Yun

AU - Jolly, Aaron F.

AU - Eldridge, Adam G.

AU - Watson, Stanley J.

AU - Jackson, Peter K.

AU - Barsh, Gregory S.

AU - Gunn, Teresa M.

PY - 2003/1/31

Y1 - 2003/1/31

N2 - mahoganoid is a mouse coat-color mutation whose pigmentary phenotype and genetic interactions resemble those of Attractin (Atrn). Atrn mutations also cause spongiform neurodegeneration. Here, we show that a null mutation for mahoganoid causes a similar age-dependent neuropathology that includes many features of prion diseases but without accumulation of protease-resistant prion protein. The gene mutated in mahoganoid encodes a RING-containing protein with E3 ubiquitin ligase activity in vitro. Similarities in phenotype, expression, and genetic interactions suggest that mahoganoid and Atrn genes are part of a conserved pathway for regulated protein turnover whose function is essential for neuronal viability.

AB - mahoganoid is a mouse coat-color mutation whose pigmentary phenotype and genetic interactions resemble those of Attractin (Atrn). Atrn mutations also cause spongiform neurodegeneration. Here, we show that a null mutation for mahoganoid causes a similar age-dependent neuropathology that includes many features of prion diseases but without accumulation of protease-resistant prion protein. The gene mutated in mahoganoid encodes a RING-containing protein with E3 ubiquitin ligase activity in vitro. Similarities in phenotype, expression, and genetic interactions suggest that mahoganoid and Atrn genes are part of a conserved pathway for regulated protein turnover whose function is essential for neuronal viability.

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Spongiform degeneration in mahoganoid mutant mice

Abstract

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