Nuclear retention of full-length HTT RNA is mediated by splicing factors MBNL1 and U2AF65

Xin Sun; Pan P. Li; Shanshan Zhu; Rachael Cohen; Leonard O. Marque; Christopher A. Ross; Stefan M. Pulst; Ho Yin Edwin Chan; Russell L. Margolis; Dobrila D. Rudnicki

doi:10.1038/srep12521

Nuclear retention of full-length HTT RNA is mediated by splicing factors MBNL1 and U2AF65

Xin Sun, Pan P. Li, Shanshan Zhu, Rachael Cohen, Leonard O. Marque, Christopher A. Ross, Stefan M. Pulst, Ho Yin Edwin Chan, Russell L. Margolis, Dobrila D. Rudnicki

School of Medicine

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

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Abstract

Huntington's disease (HD) is caused by a CAG repeat expansion in the huntingtin (HTT) gene. Recent evidence suggests that HD is a consequence of multimodal, non-mutually exclusive mechanisms of pathogenesis that involve both HTT protein- and HTT RNA-triggered mechanisms. Here we provide further evidence for the role of expanded HTT (expHTT) RNA in HD by demonstrating that a fragment of expHTT is cytotoxic in the absence of any translation and that the extent of cytotoxicity is similar to the cytotoxicity of an expHTT protein fragment encoded by a transcript of similar length and with a similar repeat size. In addition, full-length (FL) expHTT is retained in the nucleus. Overexpression of the splicing factor muscleblind-like 1 (MBNL1) increases nuclear retention of expHTT and decreases the expression of expHTT protein in the cytosol. The splicing and nuclear export factor U2AF65 has the opposite effect, decreasing expHTT nuclear retention and increasing expression of expHTT protein. This suggests that MBNL1 and U2AF65 play a role in nuclear export of expHTT RNA.

Original language	English (US)
Article number	12521
Journal	Scientific reports
Volume	5
DOIs	https://doi.org/10.1038/srep12521
State	Published - Jul 28 2015

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@article{85bf31c9df1d4b7b89b791a9f7678f89,

title = "Nuclear retention of full-length HTT RNA is mediated by splicing factors MBNL1 and U2AF65",

abstract = "Huntington's disease (HD) is caused by a CAG repeat expansion in the huntingtin (HTT) gene. Recent evidence suggests that HD is a consequence of multimodal, non-mutually exclusive mechanisms of pathogenesis that involve both HTT protein- and HTT RNA-triggered mechanisms. Here we provide further evidence for the role of expanded HTT (expHTT) RNA in HD by demonstrating that a fragment of expHTT is cytotoxic in the absence of any translation and that the extent of cytotoxicity is similar to the cytotoxicity of an expHTT protein fragment encoded by a transcript of similar length and with a similar repeat size. In addition, full-length (FL) expHTT is retained in the nucleus. Overexpression of the splicing factor muscleblind-like 1 (MBNL1) increases nuclear retention of expHTT and decreases the expression of expHTT protein in the cytosol. The splicing and nuclear export factor U2AF65 has the opposite effect, decreasing expHTT nuclear retention and increasing expression of expHTT protein. This suggests that MBNL1 and U2AF65 play a role in nuclear export of expHTT RNA.",

author = "Xin Sun and Li, {Pan P.} and Shanshan Zhu and Rachael Cohen and Marque, {Leonard O.} and Ross, {Christopher A.} and Pulst, {Stefan M.} and Chan, {Ho Yin Edwin} and Margolis, {Russell L.} and Rudnicki, {Dobrila D.}",

note = "Funding Information: The authors thank Dr. Ramee Lee for helpful discussions; Dr. Laura P.L. Ranum for helpful comments and suggestions, as well as for the kind gift of the A8(*KKQEXP)-3Tf1 construct; and Dr. Charles A. Thornton for the kind gift of the GFP-MBNL1 construct. This work was supported by the National Institutes of Health (NS064138 to D.D.R.), the CHDI Foundation (Early Discovery Initiative to D.D.R.), and the Hereditary Disease Foundation (to D.D.R.).",

year = "2015",

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doi = "10.1038/srep12521",

language = "English (US)",

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journal = "Scientific reports",

issn = "2045-2322",

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AU - Sun, Xin

AU - Li, Pan P.

AU - Zhu, Shanshan

AU - Cohen, Rachael

AU - Marque, Leonard O.

AU - Ross, Christopher A.

AU - Pulst, Stefan M.

AU - Chan, Ho Yin Edwin

AU - Margolis, Russell L.

AU - Rudnicki, Dobrila D.

N1 - Funding Information: The authors thank Dr. Ramee Lee for helpful discussions; Dr. Laura P.L. Ranum for helpful comments and suggestions, as well as for the kind gift of the A8(*KKQEXP)-3Tf1 construct; and Dr. Charles A. Thornton for the kind gift of the GFP-MBNL1 construct. This work was supported by the National Institutes of Health (NS064138 to D.D.R.), the CHDI Foundation (Early Discovery Initiative to D.D.R.), and the Hereditary Disease Foundation (to D.D.R.).

PY - 2015/7/28

Y1 - 2015/7/28

N2 - Huntington's disease (HD) is caused by a CAG repeat expansion in the huntingtin (HTT) gene. Recent evidence suggests that HD is a consequence of multimodal, non-mutually exclusive mechanisms of pathogenesis that involve both HTT protein- and HTT RNA-triggered mechanisms. Here we provide further evidence for the role of expanded HTT (expHTT) RNA in HD by demonstrating that a fragment of expHTT is cytotoxic in the absence of any translation and that the extent of cytotoxicity is similar to the cytotoxicity of an expHTT protein fragment encoded by a transcript of similar length and with a similar repeat size. In addition, full-length (FL) expHTT is retained in the nucleus. Overexpression of the splicing factor muscleblind-like 1 (MBNL1) increases nuclear retention of expHTT and decreases the expression of expHTT protein in the cytosol. The splicing and nuclear export factor U2AF65 has the opposite effect, decreasing expHTT nuclear retention and increasing expression of expHTT protein. This suggests that MBNL1 and U2AF65 play a role in nuclear export of expHTT RNA.

AB - Huntington's disease (HD) is caused by a CAG repeat expansion in the huntingtin (HTT) gene. Recent evidence suggests that HD is a consequence of multimodal, non-mutually exclusive mechanisms of pathogenesis that involve both HTT protein- and HTT RNA-triggered mechanisms. Here we provide further evidence for the role of expanded HTT (expHTT) RNA in HD by demonstrating that a fragment of expHTT is cytotoxic in the absence of any translation and that the extent of cytotoxicity is similar to the cytotoxicity of an expHTT protein fragment encoded by a transcript of similar length and with a similar repeat size. In addition, full-length (FL) expHTT is retained in the nucleus. Overexpression of the splicing factor muscleblind-like 1 (MBNL1) increases nuclear retention of expHTT and decreases the expression of expHTT protein in the cytosol. The splicing and nuclear export factor U2AF65 has the opposite effect, decreasing expHTT nuclear retention and increasing expression of expHTT protein. This suggests that MBNL1 and U2AF65 play a role in nuclear export of expHTT RNA.

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Nuclear retention of full-length HTT RNA is mediated by splicing factors MBNL1 and U2AF65

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