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Two-stage association study and meta-analysis of mitochondrial DNA variants in Parkinson disease [Article]

Hudson, G., Nalls, M., Evans, J. R., Breen, D. P., Winder-Rhodes, S., Morrison, K. E., Morris, H. R., Williams-Gray, C. H., Barker, R. A., Singleton, A. B., Hardy, J., Wood, N. E., Burn, D. J. and Chinnery, P. F. 2013. Two-stage association study and meta-analysis of mitochondrial DNA variants in Parkinson disease [Article]. Neurology 80 (22) , pp. 2042-2048. 10.1212/WNL.0b013e318294b434

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Official URL: http://dx.doi.org/10.1212/WNL.0b013e318294b434

Abstract

Objectives: Previous associations between mitochondrial DNA (mtDNA) and idiopathic Parkinson disease (PD) have been inconsistent and contradictory. Our aim was to resolve these inconsistencies and determine whether mtDNA has a significant role in the risk of developing PD. Methods: Two-stage genetic association study of 138 common mtDNA variants in 3,074 PD cases and 5,659 ethnically matched controls followed by meta-analysis of 6,140 PD cases and 13,280 controls. Results: In the association study, m.2158T>C and m.11251A>G were associated with a reduced risk of PD in both the discovery and replication cohorts. None of the common European mtDNA haplogroups were consistently associated with PD, but pooling of discovery and replication cohorts revealed a protective association with “super-haplogroup” JT. In the meta-analysis, there was a reduced risk of PD with haplogroups J, K, and T and super-haplogroup JT, and an increase in the risk of PD with super-haplogroup H. Conclusions: In a 2-stage association study of mtDNA variants and PD, we confirm the reduced risk of PD with super-haplogroup JT and resolve this at the J1b level. Meta-analysis explains the previous inconsistent associations that likely arise through sampling effects. The reduced risk of PD with haplogroups J, K, and T is mirrored by an increased risk of PD in super-haplogroup HV, which increases survival after sepsis. Antagonistic pleiotropy between mtDNA haplogroups may thus be shaping the genetic landscape in humans, leading to an increased risk of PD in later life.

Item Type:	Article
Status:	Published
Schools:	Medicine MRC Centre for Neuropsychiatric Genetics and Genomics (CNGG)
Subjects:	R Medicine > R Medicine (General)
Publisher:	American Academy of Neurology (AAN)
ISSN:	0028-3878
Last Modified:	10 Jan 2018 06:48
URI:	https://orca.cardiff.ac.uk/id/eprint/75706

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