RAS-MAPK-MSK1 pathway modulates ataxin 1 protein levels and toxicity in SCA1

Jeehye Park; Ismael Al-Ramahi; Qiumin Tan; Nissa Mollema; Javier R. Diaz-Garcia; Tatiana Gallego-Flores; Hsiang Chih Lu; Sarita Lagalwar; Lisa Duvick; Hyojin Kang; Yoontae Lee; Paymaan Jafar-Nejad; Layal S. Sayegh; Ronald Richman; Xiuyun Liu; Yan Gao; Chad A. Shaw; J. Simon C Arthur; Harry T. Orr; Thomas F. Westbrook; Juan Botas; Huda Y. Zoghbi

doi:10.1038/nature12204

RAS-MAPK-MSK1 pathway modulates ataxin 1 protein levels and toxicity in SCA1

Jeehye Park, Ismael Al-Ramahi, Qiumin Tan, Nissa Mollema, Javier R. Diaz-Garcia, Tatiana Gallego-Flores, Hsiang Chih Lu, Sarita Lagalwar, Lisa Duvick, Hyojin Kang, Yoontae Lee, Paymaan Jafar-Nejad, Layal S. Sayegh, Ronald Richman, Xiuyun Liu, Yan Gao, Chad A. Shaw, J. Simon C Arthur, Harry T. Orr, Thomas F. WestbrookJuan Botas, Huda Y. Zoghbi

Laboratory Medicine and Pathology

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

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Abstract

Many neurodegenerative disorders, such as Alzheimer's, Parkinson's and polyglutamine diseases, share a common pathogenic mechanism: the abnormal accumulation of disease-causing proteins, due to either the mutant protein's resistance to degradation or overexpression of the wild-type protein. We have developed a strategy to identify therapeutic entry points for such neurodegenerative disorders by screening for genetic networks that influence the levels of disease-driving proteins. We applied this approach, which integrates parallel cell-based and Drosophila genetic screens, to spinocerebellar ataxia type 1 (SCA1), a disease caused by expansion of a polyglutamine tract in ataxin 1 (ATXN1). Our approach revealed that downregulation of several components of the RAS-MAPK-MSK1 pathway decreases ATXN1 levels and suppresses neurodegeneration in Drosophila and mice. Importantly, pharmacological inhibitors of components of this pathway also decrease ATXN1 levels, suggesting that these components represent new therapeutic targets in mitigating SCA1. Collectively, these data reveal new therapeutic entry points for SCA1 and provide a proof-of-principle for tackling other classes of intractable neurodegenerative diseases.

Original language	English (US)
Pages (from-to)	325-331
Number of pages	7
Journal	Nature
Volume	498
Issue number	7454
DOIs	https://doi.org/10.1038/nature12204
State	Published - 2013

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Park, J., Al-Ramahi, I., Tan, Q., Mollema, N., Diaz-Garcia, J. R., Gallego-Flores, T., Lu, H. C., Lagalwar, S., Duvick, L., Kang, H., Lee, Y., Jafar-Nejad, P., Sayegh, L. S., Richman, R., Liu, X., Gao, Y., Shaw, C. A., Arthur, J. S. C., Orr, H. T., ... Zoghbi, H. Y. (2013). RAS-MAPK-MSK1 pathway modulates ataxin 1 protein levels and toxicity in SCA1. Nature, 498(7454), 325-331. https://doi.org/10.1038/nature12204

Park, J, Al-Ramahi, I, Tan, Q, Mollema, N, Diaz-Garcia, JR, Gallego-Flores, T, Lu, HC, Lagalwar, S, Duvick, L, Kang, H, Lee, Y, Jafar-Nejad, P, Sayegh, LS, Richman, R, Liu, X, Gao, Y, Shaw, CA, Arthur, JSC, Orr, HT, Westbrook, TF, Botas, J & Zoghbi, HY 2013, 'RAS-MAPK-MSK1 pathway modulates ataxin 1 protein levels and toxicity in SCA1', Nature, vol. 498, no. 7454, pp. 325-331. https://doi.org/10.1038/nature12204

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abstract = "Many neurodegenerative disorders, such as Alzheimer's, Parkinson's and polyglutamine diseases, share a common pathogenic mechanism: the abnormal accumulation of disease-causing proteins, due to either the mutant protein's resistance to degradation or overexpression of the wild-type protein. We have developed a strategy to identify therapeutic entry points for such neurodegenerative disorders by screening for genetic networks that influence the levels of disease-driving proteins. We applied this approach, which integrates parallel cell-based and Drosophila genetic screens, to spinocerebellar ataxia type 1 (SCA1), a disease caused by expansion of a polyglutamine tract in ataxin 1 (ATXN1). Our approach revealed that downregulation of several components of the RAS-MAPK-MSK1 pathway decreases ATXN1 levels and suppresses neurodegeneration in Drosophila and mice. Importantly, pharmacological inhibitors of components of this pathway also decrease ATXN1 levels, suggesting that these components represent new therapeutic targets in mitigating SCA1. Collectively, these data reveal new therapeutic entry points for SCA1 and provide a proof-of-principle for tackling other classes of intractable neurodegenerative diseases.",

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AU - Park, Jeehye

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AU - Tan, Qiumin

AU - Mollema, Nissa

AU - Diaz-Garcia, Javier R.

AU - Gallego-Flores, Tatiana

AU - Lu, Hsiang Chih

AU - Lagalwar, Sarita

AU - Duvick, Lisa

AU - Kang, Hyojin

AU - Lee, Yoontae

AU - Jafar-Nejad, Paymaan

AU - Sayegh, Layal S.

AU - Richman, Ronald

AU - Liu, Xiuyun

AU - Gao, Yan

AU - Shaw, Chad A.

AU - Arthur, J. Simon C

AU - Orr, Harry T.

AU - Westbrook, Thomas F.

AU - Botas, Juan

AU - Zoghbi, Huda Y.

PY - 2013

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N2 - Many neurodegenerative disorders, such as Alzheimer's, Parkinson's and polyglutamine diseases, share a common pathogenic mechanism: the abnormal accumulation of disease-causing proteins, due to either the mutant protein's resistance to degradation or overexpression of the wild-type protein. We have developed a strategy to identify therapeutic entry points for such neurodegenerative disorders by screening for genetic networks that influence the levels of disease-driving proteins. We applied this approach, which integrates parallel cell-based and Drosophila genetic screens, to spinocerebellar ataxia type 1 (SCA1), a disease caused by expansion of a polyglutamine tract in ataxin 1 (ATXN1). Our approach revealed that downregulation of several components of the RAS-MAPK-MSK1 pathway decreases ATXN1 levels and suppresses neurodegeneration in Drosophila and mice. Importantly, pharmacological inhibitors of components of this pathway also decrease ATXN1 levels, suggesting that these components represent new therapeutic targets in mitigating SCA1. Collectively, these data reveal new therapeutic entry points for SCA1 and provide a proof-of-principle for tackling other classes of intractable neurodegenerative diseases.

AB - Many neurodegenerative disorders, such as Alzheimer's, Parkinson's and polyglutamine diseases, share a common pathogenic mechanism: the abnormal accumulation of disease-causing proteins, due to either the mutant protein's resistance to degradation or overexpression of the wild-type protein. We have developed a strategy to identify therapeutic entry points for such neurodegenerative disorders by screening for genetic networks that influence the levels of disease-driving proteins. We applied this approach, which integrates parallel cell-based and Drosophila genetic screens, to spinocerebellar ataxia type 1 (SCA1), a disease caused by expansion of a polyglutamine tract in ataxin 1 (ATXN1). Our approach revealed that downregulation of several components of the RAS-MAPK-MSK1 pathway decreases ATXN1 levels and suppresses neurodegeneration in Drosophila and mice. Importantly, pharmacological inhibitors of components of this pathway also decrease ATXN1 levels, suggesting that these components represent new therapeutic targets in mitigating SCA1. Collectively, these data reveal new therapeutic entry points for SCA1 and provide a proof-of-principle for tackling other classes of intractable neurodegenerative diseases.

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RAS-MAPK-MSK1 pathway modulates ataxin 1 protein levels and toxicity in SCA1

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