A rare sequence variant in intron 1 of thap1 is associated with primary dystonia

Satya R. Vemula; Jianfeng Xiao; Yu Zhao; Robert W. Bastian; Joel S. Perlmutter; Brad A. Racette; Randal C. Paniello; Zbigniew K. Wszolek; Ryan J. Uitti; Jay A. Van Gerpen; Peter Hedera; Daniel D. Truong; Andrew Blitzer; Monika Rudzinska; Dragana Momcilovic; Hyder A. Jinnah; Karen Frei; Ronald F. Pfeiffer; Mark S. Ledoux

doi:10.1002/mgg3.67

A rare sequence variant in intron 1 of thap1 is associated with primary dystonia

Satya R. Vemula, Jianfeng Xiao, Yu Zhao, Robert W. Bastian, Joel S. Perlmutter, Brad A. Racette, Randal C. Paniello, Zbigniew K. Wszolek, Ryan J. Uitti, Jay A. Van Gerpen, Peter Hedera, Daniel D. Truong, Andrew Blitzer, Monika Rudzinska, Dragana Momcilovic, Hyder A. Jinnah, Karen Frei, Ronald F. Pfeiffer, Mark S. Ledoux

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

18 Scopus citations

Abstract

Although coding variants in THAP1 have been causally associated with primary dystonia, the contribution of noncoding variants remains uncertain. Herein, we examine a previously identified Intron 1 variant (c.71+9C>A, rs200209986). Among 1672 subjects with mainly adult-onset primary dystonia, 12 harbored the variant in contrast to 1/1574 controls (P < 0.01). Dystonia classification included cervical dystonia (N = 3), laryngeal dystonia (adductor subtype, N = 3), jaw-opening oromandibular dystonia (N = 1), blepharospasm (N = 2), and unclassified (N = 3). Age of dystonia onset ranged from 25 to 69 years (mean = 54 years). In comparison to controls with no identified THAP1 sequence variants, the c.71+9C>A variant was associated with an elevated ratio of Isoform 1 (NM_018105) to Isoform 2 (NM_199003) in leukocytes. In silico and minigene analyses indicated that c.71+9C>A alters THAP1 splicing. Lymphoblastoid cells harboring the c.71+9C>A variant showed extensive apoptosis with relatively fewer cells in the G2 phase of the cell cycle. Differentially expressed genes from lymphoblastoid cells revealed that the c.71+9C>A variant exerts effects on DNA synthesis, cell growth and proliferation, cell survival, and cytotoxicity. In aggregate, these data indicate that THAP1 c.71+9C>A is a risk factor for adult-onset primary dystonia.

Original language	English (US)
Pages (from-to)	261-272
Number of pages	12
Journal	Molecular Genetics and Genomic Medicine
Volume	2
Issue number	3
DOIs	https://doi.org/10.1002/mgg3.67
State	Published - May 2014
Externally published	Yes

Keywords

DYT6
Dystonia
Intronic variant
Minigene assay
THAP1

ASJC Scopus subject areas

Molecular Biology
Genetics
Genetics(clinical)

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10.1002/mgg3.67

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Vemula, S. R., Xiao, J., Zhao, Y., Bastian, R. W., Perlmutter, J. S., Racette, B. A., Paniello, R. C., Wszolek, Z. K., Uitti, R. J., Van Gerpen, J. A., Hedera, P., Truong, D. D., Blitzer, A., Rudzinska, M., Momcilovic, D., Jinnah, H. A., Frei, K., Pfeiffer, R. F., & Ledoux, M. S. (2014). A rare sequence variant in intron 1 of thap1 is associated with primary dystonia. Molecular Genetics and Genomic Medicine, 2(3), 261-272. https://doi.org/10.1002/mgg3.67

Vemula, SR, Xiao, J, Zhao, Y, Bastian, RW, Perlmutter, JS, Racette, BA, Paniello, RC, Wszolek, ZK, Uitti, RJ, Van Gerpen, JA, Hedera, P, Truong, DD, Blitzer, A, Rudzinska, M, Momcilovic, D, Jinnah, HA, Frei, K, Pfeiffer, RF & Ledoux, MS 2014, 'A rare sequence variant in intron 1 of thap1 is associated with primary dystonia', Molecular Genetics and Genomic Medicine, vol. 2, no. 3, pp. 261-272. https://doi.org/10.1002/mgg3.67

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title = "A rare sequence variant in intron 1 of thap1 is associated with primary dystonia",

abstract = "Although coding variants in THAP1 have been causally associated with primary dystonia, the contribution of noncoding variants remains uncertain. Herein, we examine a previously identified Intron 1 variant (c.71+9C>A, rs200209986). Among 1672 subjects with mainly adult-onset primary dystonia, 12 harbored the variant in contrast to 1/1574 controls (P < 0.01). Dystonia classification included cervical dystonia (N = 3), laryngeal dystonia (adductor subtype, N = 3), jaw-opening oromandibular dystonia (N = 1), blepharospasm (N = 2), and unclassified (N = 3). Age of dystonia onset ranged from 25 to 69 years (mean = 54 years). In comparison to controls with no identified THAP1 sequence variants, the c.71+9C>A variant was associated with an elevated ratio of Isoform 1 (NM_018105) to Isoform 2 (NM_199003) in leukocytes. In silico and minigene analyses indicated that c.71+9C>A alters THAP1 splicing. Lymphoblastoid cells harboring the c.71+9C>A variant showed extensive apoptosis with relatively fewer cells in the G2 phase of the cell cycle. Differentially expressed genes from lymphoblastoid cells revealed that the c.71+9C>A variant exerts effects on DNA synthesis, cell growth and proliferation, cell survival, and cytotoxicity. In aggregate, these data indicate that THAP1 c.71+9C>A is a risk factor for adult-onset primary dystonia.",

keywords = "DYT6, Dystonia, Intronic variant, Minigene assay, THAP1",

author = "Vemula, {Satya R.} and Jianfeng Xiao and Yu Zhao and Bastian, {Robert W.} and Perlmutter, {Joel S.} and Racette, {Brad A.} and Paniello, {Randal C.} and Wszolek, {Zbigniew K.} and Uitti, {Ryan J.} and {Van Gerpen}, {Jay A.} and Peter Hedera and Truong, {Daniel D.} and Andrew Blitzer and Monika Rudzinska and Dragana Momcilovic and Jinnah, {Hyder A.} and Karen Frei and Pfeiffer, {Ronald F.} and Ledoux, {Mark S.}",

note = "Publisher Copyright: {\textcopyright} 2014 The Authors.",

year = "2014",

month = may,

doi = "10.1002/mgg3.67",

language = "English (US)",

volume = "2",

pages = "261--272",

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T1 - A rare sequence variant in intron 1 of thap1 is associated with primary dystonia

AU - Vemula, Satya R.

AU - Xiao, Jianfeng

AU - Zhao, Yu

AU - Bastian, Robert W.

AU - Perlmutter, Joel S.

AU - Racette, Brad A.

AU - Paniello, Randal C.

AU - Wszolek, Zbigniew K.

AU - Uitti, Ryan J.

AU - Van Gerpen, Jay A.

AU - Hedera, Peter

AU - Truong, Daniel D.

AU - Blitzer, Andrew

AU - Rudzinska, Monika

AU - Momcilovic, Dragana

AU - Jinnah, Hyder A.

AU - Frei, Karen

AU - Pfeiffer, Ronald F.

AU - Ledoux, Mark S.

PY - 2014/5

Y1 - 2014/5

N2 - Although coding variants in THAP1 have been causally associated with primary dystonia, the contribution of noncoding variants remains uncertain. Herein, we examine a previously identified Intron 1 variant (c.71+9C>A, rs200209986). Among 1672 subjects with mainly adult-onset primary dystonia, 12 harbored the variant in contrast to 1/1574 controls (P < 0.01). Dystonia classification included cervical dystonia (N = 3), laryngeal dystonia (adductor subtype, N = 3), jaw-opening oromandibular dystonia (N = 1), blepharospasm (N = 2), and unclassified (N = 3). Age of dystonia onset ranged from 25 to 69 years (mean = 54 years). In comparison to controls with no identified THAP1 sequence variants, the c.71+9C>A variant was associated with an elevated ratio of Isoform 1 (NM_018105) to Isoform 2 (NM_199003) in leukocytes. In silico and minigene analyses indicated that c.71+9C>A alters THAP1 splicing. Lymphoblastoid cells harboring the c.71+9C>A variant showed extensive apoptosis with relatively fewer cells in the G2 phase of the cell cycle. Differentially expressed genes from lymphoblastoid cells revealed that the c.71+9C>A variant exerts effects on DNA synthesis, cell growth and proliferation, cell survival, and cytotoxicity. In aggregate, these data indicate that THAP1 c.71+9C>A is a risk factor for adult-onset primary dystonia.

AB - Although coding variants in THAP1 have been causally associated with primary dystonia, the contribution of noncoding variants remains uncertain. Herein, we examine a previously identified Intron 1 variant (c.71+9C>A, rs200209986). Among 1672 subjects with mainly adult-onset primary dystonia, 12 harbored the variant in contrast to 1/1574 controls (P < 0.01). Dystonia classification included cervical dystonia (N = 3), laryngeal dystonia (adductor subtype, N = 3), jaw-opening oromandibular dystonia (N = 1), blepharospasm (N = 2), and unclassified (N = 3). Age of dystonia onset ranged from 25 to 69 years (mean = 54 years). In comparison to controls with no identified THAP1 sequence variants, the c.71+9C>A variant was associated with an elevated ratio of Isoform 1 (NM_018105) to Isoform 2 (NM_199003) in leukocytes. In silico and minigene analyses indicated that c.71+9C>A alters THAP1 splicing. Lymphoblastoid cells harboring the c.71+9C>A variant showed extensive apoptosis with relatively fewer cells in the G2 phase of the cell cycle. Differentially expressed genes from lymphoblastoid cells revealed that the c.71+9C>A variant exerts effects on DNA synthesis, cell growth and proliferation, cell survival, and cytotoxicity. In aggregate, these data indicate that THAP1 c.71+9C>A is a risk factor for adult-onset primary dystonia.

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KW - Minigene assay

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A rare sequence variant in intron 1 of thap1 is associated with primary dystonia

Abstract

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