Heterozygous PINK1 p.G411S increases risk of Parkinson's disease via a dominant-negative mechanism

Andreas Puschmann; Fabienne C Fiesel; Thomas R Caulfield; Roman Hudec; Maya Ando; Dominika Truban; Xu Hou; Kotaro Ogaki; Michael G Heckman; Elle D James; Maria Swanberg; Itzia Jimenez-Ferrer; Oskar Hansson; Grzegorz Opala; Joanna Siuda; Magdalena Boczarska-Jedynak; Andrzej Friedman; Dariusz Koziorowski; Monika Rudzińska-Bar; Jan O Aasly; Timothy Lynch; George D Mellick; Megha Mohan; Peter A Silburn; Yanosh Sanotsky; Carles Vilariño-Güell; Matthew J Farrer; Li Chen; Valina L Dawson; Ted M Dawson; Zbigniew K Wszolek; Owen A Ross; Wolfdieter Springer

doi:10.1093/brain/aww261

Heterozygous PINK1 p.G411S increases risk of Parkinson's disease via a dominant-negative mechanism

Brain. 2017 Jan;140(1):98-117. doi: 10.1093/brain/aww261. Epub 2016 Nov 2.

Authors

Andreas Puschmann^{1

2

3}, Fabienne C Fiesel³, Thomas R Caulfield³, Roman Hudec³, Maya Ando³, Dominika Truban³, Xu Hou³, Kotaro Ogaki³, Michael G Heckman⁴, Elle D James³, Maria Swanberg⁵, Itzia Jimenez-Ferrer⁵, Oskar Hansson^{6

7}, Grzegorz Opala⁸, Joanna Siuda⁸, Magdalena Boczarska-Jedynak⁸, Andrzej Friedman⁹, Dariusz Koziorowski⁹, Monika Rudzińska-Bar, Jan O Aasly¹⁰, Timothy Lynch¹¹, George D Mellick¹², Megha Mohan¹², Peter A Silburn^{12

13}, Yanosh Sanotsky¹⁴, Carles Vilariño-Güell^{3

15}, Matthew J Farrer^{3

15}, Li Chen^{16

17

18}, Valina L Dawson^{16

17

18

19

20}, Ted M Dawson^{16

17

18

19

21}, Zbigniew K Wszolek²², Owen A Ross^{3

23

24}, Wolfdieter Springer^{25

24}

Affiliations

¹ 1 Lund University, Department of Clinical Sciences Lund, Neurology, Sweden Springer.Wolfdieter@mayo.edu Andreas.Puschmann@med.lu.se.
² 2 Department of Neurology, Skåne University Hospital, Sweden.
³ 3 Department of Neuroscience, Mayo Clinic, Jacksonville, FL 32224, USA.
⁴ 4 Division of Biomedical Statistics and Informatics, Mayo Clinic, Jacksonville, FL 32224, USA.
⁵ 5 Lund University, Department of Experimental Medical Science, Lund, Sweden.
⁶ 6 Clinical Memory Research Unit, Department of Clinical Sciences Malmö, Lund University, Sweden.
⁷ 7 Memory Clinic, Skåne University Hospital, Malmö, Sweden.
⁸ 8 Department of Neurology, School of Medicine in Katowice, Medical University of Silesia, Katowice, Poland.
⁹ 9 Department of Neurology, Medical University of Warsaw, Poland.
¹⁰ 10 Department of Neurology, St. Olav's Hospital, and Department of Neuroscience, Norwegian University of Science and Technology, Trondheim, Norway.
¹¹ 11 Dublin Neurological Institute at the Mater Misericordiae University Hospital, Conway Institute of Biomolecular and Biomedical Research, University College Dublin, Dublin, Ireland.
¹² 12 Eskitis Institute for Drug Discovery, Griffith University, Nathan, Queensland, Australia.
¹³ 13 University of Queensland, Asia-Pacific Centre for Neuromodulation, Centre for Clinical Research, Brisbane, Queensland, Australia.
¹⁴ 14 Lviv Regional Clinical Hospital, Lviv, Ukraine.
¹⁵ 15 Department of Medical Genetics, University of British Columbia, Vancouver, BC, Canada.
¹⁶ 16 Neuroregeneration and Stem Cell Programs, Institute for Cell Engineering, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.
¹⁷ 17 Solomon H Snyder Department of Neuroscience, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.
¹⁸ 18 Adrienne Helis Malvin Medical Research Foundation, New Orleans, LA 70130-2685, USA.
¹⁹ 19 Department of Neurology, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.
²⁰ 20 Department of Physiology, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.
²¹ 21 Department of Pharmacology and Molecular Sciences, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.
²² 22 Department of Neurology, Mayo Clinic, Jacksonville, FL 32224, USA.
²³ 23 School of Medicine and Medical Science, University College Dublin, Dublin, Ireland.
²⁴ 24 Mayo Graduate School, Neurobiology of Disease, Mayo Clinic, Jacksonville, FL 32224, USA.
²⁵ 3 Department of Neuroscience, Mayo Clinic, Jacksonville, FL 32224, USA Springer.Wolfdieter@mayo.edu Andreas.Puschmann@med.lu.se.

Abstract

SEE GANDHI AND PLUN-FAVREAU DOI101093/AWW320 FOR A SCIENTIFIC COMMENTARY ON THIS ARTICLE: It has been postulated that heterozygous mutations in recessive Parkinson's genes may increase the risk of developing the disease. In particular, the PTEN-induced putative kinase 1 (PINK1) p.G411S (c.1231G>A, rs45478900) mutation has been reported in families with dominant inheritance patterns of Parkinson's disease, suggesting that it might confer a sizeable disease risk when present on only one allele. We examined families with PINK1 p.G411S and conducted a genetic association study with 2560 patients with Parkinson's disease and 2145 control subjects. Heterozygous PINK1 p.G411S mutations markedly increased Parkinson's disease risk (odds ratio = 2.92, P = 0.032); significance remained when supplementing with results from previous studies on 4437 additional subjects (odds ratio = 2.89, P = 0.027). We analysed primary human skin fibroblasts and induced neurons from heterozygous PINK1 p.G411S carriers compared to PINK1 p.Q456X heterozygotes and PINK1 wild-type controls under endogenous conditions. While cells from PINK1 p.Q456X heterozygotes showed reduced levels of PINK1 protein and decreased initial kinase activity upon mitochondrial damage, stress-response was largely unaffected over time, as expected for a recessive loss-of-function mutation. By contrast, PINK1 p.G411S heterozygotes showed no decrease of PINK1 protein levels but a sustained, significant reduction in kinase activity. Molecular modelling and dynamics simulations as well as multiple functional assays revealed that the p.G411S mutation interferes with ubiquitin phosphorylation by wild-type PINK1 in a heterodimeric complex. This impairs the protective functions of the PINK1/parkin-mediated mitochondrial quality control. Based on genetic and clinical evaluation as well as functional and structural characterization, we established p.G411S as a rare genetic risk factor with a relatively large effect size conferred by a partial dominant-negative function phenotype.

Keywords: PINK1; Parkinson’s disease; heterozygous mutation; mitophagy; ubiquitin.

Publication types

Meta-Analysis

MeSH terms

Adolescent
Adult
Aged
Aged, 80 and over
Case-Control Studies
Female
Fibroblasts
Genetic Association Studies*
Genetic Predisposition to Disease / genetics*
Heterozygote
Humans
Male
Middle Aged
Models, Molecular*
Parkinson Disease / genetics*
Pedigree
Protein Kinases / genetics*
Risk
Young Adult

Substances

Protein Kinases
PTEN-induced putative kinase

Abstract

Publication types

MeSH terms

Substances

Grants and funding