Comparative Study

. 2009 Jan 27;72(4):310-6.

doi: 10.1212/01.wnl.0000327823.81237.d1. Epub 2008 Nov 5.

Mutations in GBA are associated with familial Parkinson disease susceptibility and age at onset

W C Nichols¹, N Pankratz, D K Marek, M W Pauciulo, V E Elsaesser, C A Halter, A Rudolph, J Wojcieszek, R F Pfeiffer, T Foroud; Parkinson Study Group-PROGENI Investigators

Collaborators, Affiliations

Collaborators

Parkinson Study Group-PROGENI Investigators:
R F Pfeiffer, F Marshall, D Oakes, A Rudolph, A Shinaman, K Marder, P M Conneally, T Foroud, C Halter, K Lyons, E Siemers, L Elmers, N Hermanowicz, S Factor, D Higgins, S Evans, H Shill, M Stacy, J Danielson, L Marlor, K Williamson, J Jankovic, C Hunter, D Simon, P Ryan, L Scollins, R Saunders-Pullman, K Boyar, C Costan-Toth, E Ohmann, L Sudarsky, C Joubert, J Friedman, K Chou, H Fernandez, M Lannon, N Galvez-Jimenez, A Podichetty, P Lewitt, M DeAngelis, C O'Brien, L Seeberger, C Dingmann, D Judd, K Marder, J Fraser, J Harris, J Bertoni, C Peterson, M Rezak, G Medalle, S Chouinard, M Panisset, J Hall, H Poiffaut, V Calabrese, P Roberge, J Wojcieszek, J Belden, C Halter, D Jennings, K Marek, S Mendick, S Reich, B Dunlop, M Jog, C Horn, J Rao, M Cook, R Uitti, M Turk, T Ajax, J Mannetter, M Panisset, J Hall, K Sethi, J Carpenter, B Dill, K Ligon, S Narayan, L Woodward, K Blindauer, K Abou-Samra, J Petit, L Elmer, E Aiken, K Davis, C Schell, S Wilson, M Velickovic, W Koller, S Phipps, A Feigin, M Gordon, J Hamann, E Licari, M Marotta-Kollarus, B Shannon, R Winnick, T Simuni, A Kaczmarek, K Williams, M Wolff, J Rao, M Cook, J Hubble, S Kostyk, A Campbell, C Reider, A Seward, J Nutt, R Camicioli, J Carter, P Andrews, S Morehouse, C Stone, T Mendis, C Alcorn-Costa, D Grimes, P Gray, K Haas, J Vendette, J Sutton, B Hutchinson, J Young, A Rajput, L Klassen, T Shirley, B Manyam, P Simpson, J Whetteckey, B Wulbrecht, D Truong, M Pathak, N Luong, T Tra, A Tran, J Vo, A Lang, L Johnston, G Kleiner-Fisman, A Nieves, J So, G Podskalny, L Giffin, P Atchison, C Allen, W Martin, M Wieler, O Suchowersky, M Klimek, N Hermanowicz, S Niswonger, C Shults, D Fontaine, M Aminoff, C Christine, M Diminno, J Hevezi, A Dalvi, U Kang, J Richman, S Uy, J Young, A Dalvi, M Gartner, A Sahay, D Schwieterman, B Wolthoff, D Hall, M Leehey, S Culver, T Derian, T Demarcaida, S Belber, R Rodnitzky, J Dobson, R Pahwa, K Lyons, T Gales, S Thomas, L Shulman, S Reich, W Weiner, K Dustin, C Singer, W Koller, K Lyons, W Weiner, L Zelaya, P Tuite, V Hagen, J Kosowicz, S Rolandelli, R Schacherer, P Gordon, J Werner, C Serrano, S Roque, R Kurlan, D Berry, I Gardiner, R Hauser, J Sanchez-Ramos, T Zesiewicz, H Delgado, K Price, P Rodriguez, S Wolfrath, L Davis, B Pfeiffer, R Dewey, B Estes, B Hayward, A Johnson, M Meacham, F Walker, V Hunt, C O'Neill, B Racette, L Good, M Rundle

Affiliation

¹ Associate Division of Human Genetics, Cincinnati Children's Hospital Medical Center, Cincinnati, OH 45229, USA. bill.nichols@cchmc.org

PMID: 18987351
PMCID: PMC2677501
DOI: 10.1212/01.wnl.0000327823.81237.d1

Comparative Study

Mutations in GBA are associated with familial Parkinson disease susceptibility and age at onset

W C Nichols et al. Neurology. 2009.

. 2009 Jan 27;72(4):310-6.

doi: 10.1212/01.wnl.0000327823.81237.d1. Epub 2008 Nov 5.

Authors

W C Nichols¹, N Pankratz, D K Marek, M W Pauciulo, V E Elsaesser, C A Halter, A Rudolph, J Wojcieszek, R F Pfeiffer, T Foroud; Parkinson Study Group-PROGENI Investigators

Collaborators

Parkinson Study Group-PROGENI Investigators:
R F Pfeiffer, F Marshall, D Oakes, A Rudolph, A Shinaman, K Marder, P M Conneally, T Foroud, C Halter, K Lyons, E Siemers, L Elmers, N Hermanowicz, S Factor, D Higgins, S Evans, H Shill, M Stacy, J Danielson, L Marlor, K Williamson, J Jankovic, C Hunter, D Simon, P Ryan, L Scollins, R Saunders-Pullman, K Boyar, C Costan-Toth, E Ohmann, L Sudarsky, C Joubert, J Friedman, K Chou, H Fernandez, M Lannon, N Galvez-Jimenez, A Podichetty, P Lewitt, M DeAngelis, C O'Brien, L Seeberger, C Dingmann, D Judd, K Marder, J Fraser, J Harris, J Bertoni, C Peterson, M Rezak, G Medalle, S Chouinard, M Panisset, J Hall, H Poiffaut, V Calabrese, P Roberge, J Wojcieszek, J Belden, C Halter, D Jennings, K Marek, S Mendick, S Reich, B Dunlop, M Jog, C Horn, J Rao, M Cook, R Uitti, M Turk, T Ajax, J Mannetter, M Panisset, J Hall, K Sethi, J Carpenter, B Dill, K Ligon, S Narayan, L Woodward, K Blindauer, K Abou-Samra, J Petit, L Elmer, E Aiken, K Davis, C Schell, S Wilson, M Velickovic, W Koller, S Phipps, A Feigin, M Gordon, J Hamann, E Licari, M Marotta-Kollarus, B Shannon, R Winnick, T Simuni, A Kaczmarek, K Williams, M Wolff, J Rao, M Cook, J Hubble, S Kostyk, A Campbell, C Reider, A Seward, J Nutt, R Camicioli, J Carter, P Andrews, S Morehouse, C Stone, T Mendis, C Alcorn-Costa, D Grimes, P Gray, K Haas, J Vendette, J Sutton, B Hutchinson, J Young, A Rajput, L Klassen, T Shirley, B Manyam, P Simpson, J Whetteckey, B Wulbrecht, D Truong, M Pathak, N Luong, T Tra, A Tran, J Vo, A Lang, L Johnston, G Kleiner-Fisman, A Nieves, J So, G Podskalny, L Giffin, P Atchison, C Allen, W Martin, M Wieler, O Suchowersky, M Klimek, N Hermanowicz, S Niswonger, C Shults, D Fontaine, M Aminoff, C Christine, M Diminno, J Hevezi, A Dalvi, U Kang, J Richman, S Uy, J Young, A Dalvi, M Gartner, A Sahay, D Schwieterman, B Wolthoff, D Hall, M Leehey, S Culver, T Derian, T Demarcaida, S Belber, R Rodnitzky, J Dobson, R Pahwa, K Lyons, T Gales, S Thomas, L Shulman, S Reich, W Weiner, K Dustin, C Singer, W Koller, K Lyons, W Weiner, L Zelaya, P Tuite, V Hagen, J Kosowicz, S Rolandelli, R Schacherer, P Gordon, J Werner, C Serrano, S Roque, R Kurlan, D Berry, I Gardiner, R Hauser, J Sanchez-Ramos, T Zesiewicz, H Delgado, K Price, P Rodriguez, S Wolfrath, L Davis, B Pfeiffer, R Dewey, B Estes, B Hayward, A Johnson, M Meacham, F Walker, V Hunt, C O'Neill, B Racette, L Good, M Rundle

Affiliation

¹ Associate Division of Human Genetics, Cincinnati Children's Hospital Medical Center, Cincinnati, OH 45229, USA. bill.nichols@cchmc.org

PMID: 18987351
PMCID: PMC2677501
DOI: 10.1212/01.wnl.0000327823.81237.d1

Abstract

Objective: To characterize sequence variation within the glucocerebrosidase (GBA) gene in a select subset of our sample of patients with familial Parkinson disease (PD) and then to test in our full sample whether these sequence variants increased the risk for PD and were associated with an earlier onset of disease.

Methods: We performed a comprehensive study of all GBA exons in one patient with PD from each of 96 PD families, selected based on the family-specific lod scores at the GBA locus. Identified GBA variants were subsequently screened in all 1325 PD cases from 566 multiplex PD families and in 359 controls.

Results: Nine different GBA variants, five previously reported, were identified in 21 of the 96 PD cases sequenced. Screening for these variants in the full sample identified 161 variant carriers (12.2%) in 99 different PD families. An unbiased estimate of the frequency of the five previously reported GBA variants in the familial PD sample was 12.6% and in the control sample was 5.3% (odds ratio 2.6; 95% confidence interval 1.5-4.4). Presence of a GBA variant was associated with an earlier age at onset (p = 0.0001). On average, those patients carrying a GBA variant had onset with PD 6.04 years earlier than those without a GBA variant.

Conclusions: This study suggests that GBA is a susceptibility gene for familial Parkinson disease (PD) and patients with GBA variants have an earlier age at onset than patients with PD without GBA variants.

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Figures

None — **Figure** Cumulative incidence rates of Parkinson disease among carriers and noncarriers of *GBA* variants

See this image and copyright information in PMC

Comment in

Mutations in GBA are associated with familial Parkinson disease susceptibility and age at onset.
Sidransky E, Samaddar T, Tayebi N. Sidransky E, et al. Neurology. 2009 Oct 27;73(17):1424-5, author reply 1425-6. doi: 10.1212/WNL.0b013e3181b28601. Neurology. 2009. PMID: 19858467 No abstract available.

References

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1. Gasser T. Genetics of Parkinson’s disease. Curr Opin Neurol 2005;18:363–369. - PubMed
1. Zimprich A, Biskup S, Leitner P, et al. Mutations in LRRK2 cause autosomal-dominant parkinsonism with pleomorphic pathology. Neuron 2004;44:601–607. - PubMed
1. Paisan-Ruiz C, Jain S, Evans EW, et al. Cloning of the gene containing mutations that cause PARK8-linked Parkinson’s disease. Neuron 2004;44:595–600. - PubMed
1. Sidransky E. Gaucher disease: complexity in a “simple” disorder. Mol Genet Metab 2004;83:6–15. - PubMed

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Mutations in GBA are associated with familial Parkinson disease susceptibility and age at onset

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Mutations in GBA are associated with familial Parkinson disease susceptibility and age at onset

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