TY - JOUR
T1 - Revisiting the non-Gaucher-GBA-E326K carrier state
T2 - Is it sufficient to increase Parkinson's disease risk?
AU - Goldstein, Orly
AU - Gana-Weisz, Mali
AU - Cohen-Avinoam, Danielle
AU - Shiner, Tamara
AU - Thaler, Avner
AU - Cedarbaum, Jesse M.
AU - John, Sally
AU - Lalioti, Maria
AU - Gurevich, Tanya
AU - Bar-Shira, Anat
AU - Mirelman, Anat
AU - Giladi, Nir
AU - Orr-Urtreger, Avi
N1 - Funding Information:
Orly Goldstein, Mali Gana-Weisz, Danielle Cohen-Avinoam, Tamara Shiner, Anat Bar-Shira, and Anat Mirelman have no conflict of interest. Avner Thaler reports receiving honorary from ABBVIE. Maria Lalioti and Sally John are employees of Biogen. Jesse M. Cedarbaum is a former employee of and shareholder in Biogen. Tanya Gurevich reports advisory board membership with honoraria to her and to her Institution from AbbVie Israel, Neuroderm Ltd. and Allergan, research support from Phonetica Ltd., Israeli Innovation Authority, Sagol School of Neuroscience (Brain Boost) and Parkinson's Foundation. She received travel support for herself and her team from Abbvie, Allergan, Medisson, Medronic. Nir Giladi serves as a member of the Editorial Board for the Journal of Parkinson's Disease. He serves as consultant to Sionara, Accelmed, Teva, NeuroDerm, Intec Pharma, Pharma2B, Denali and Abbvie. He receives royalties from Lysosomal Therapeutics (LTI) and payment for lectures at Teva, UCB, Abbvie, Sanofi-Genzyme, Bial and Movement Disorder Society. He received research support from the Michael J Fox Foundation, the National Parkinson Foundation , the European Union 7th Framework Program and the Israel Science Foundation as well as from Teva NNE program, Biogen, LTI, and Pfizer. Avi Orr-Urtreger received research support from the Michael J Fox Foundation, Chaya Charitable Fund and Biogen, and receives payment for lectures from Sanofi Genzyme and Pfizer.
Funding Information:
Orly Goldstein, Mali Gana-Weisz, Danielle Cohen-Avinoam, Tamara Shiner, Anat Bar-Shira, and Anat Mirelman have no conflict of interest. Avner Thaler reports receiving honorary from ABBVIE. Maria Lalioti and Sally John are employees of Biogen. Jesse M. Cedarbaum is a former employee of and shareholder in Biogen. Tanya Gurevich reports advisory board membership with honoraria to her and to her Institution from AbbVie Israel, Neuroderm Ltd. and Allergan, research support from Phonetica Ltd., Israeli Innovation Authority, Sagol School of Neuroscience (Brain Boost) and Parkinson's Foundation. She received travel support for herself and her team from Abbvie, Allergan, Medisson, Medronic. Nir Giladi serves as a member of the Editorial Board for the Journal of Parkinson's Disease. He serves as consultant to Sionara, Accelmed, Teva, NeuroDerm, Intec Pharma, Pharma2B, Denali and Abbvie. He receives royalties from Lysosomal Therapeutics (LTI) and payment for lectures at Teva, UCB, Abbvie, Sanofi-Genzyme, Bial and Movement Disorder Society. He received research support from the Michael J Fox Foundation, the National Parkinson Foundation, the European Union 7th Framework Program and the Israel Science Foundation as well as from Teva NNE program, Biogen, LTI, and Pfizer. Avi Orr-Urtreger received research support from the Michael J Fox Foundation, Chaya Charitable Fund and Biogen, and receives payment for lectures from Sanofi Genzyme and Pfizer.
Funding Information:
This work was supported by Michael J Fox Foundation, and Kahn Foundation.
Publisher Copyright:
© 2019 Elsevier Inc.
PY - 2019/12/1
Y1 - 2019/12/1
N2 - Background: GBA variants are the most common genetic risk factors for Parkinson's disease (PD) world-wide, and can be found in up to 20% of Ashkenazi PD patients. The E326K variant, which is not considered a Gaucher's disease causing mutation, was recently shown to increase the risk for PD. Since E326K is a common variant among Europeans, Finnish and Ashkenazi (2.4, 8.6 and 1.2% carrier rate, respectively), we aimed to refine its involvement in PD. Methods: 1200 consecutively recruited PD patients of a full Ashkenazi origin were genotyped for 10 GBA variants, the LRRK2-G2019S and the SMPD1-L302P. Alleles' frequencies were compared to controls, composed of 378 elderly healthy individuals and the non-neuro gnomAD Ashkenazi database. Odds-Ratio (OR) and age-at-motor-symptom-onset (AAO) were also calculated for all genotypes. Results: All allelic variations tested had significant allelic ORs, demonstrating a wide range (1.86–12.84). The lowest allelic OR was observed for E326K (p = .013). Forty-five patients (of 1200, 3.75%) had at least two mutations (of the 12 tested), compared to 2 (0.53%) among 378 controls (p = .0013). Of the E326K carrier patients, 37% (10/27) carried additional mutations and the genotypic OR for individuals who carried only the E326K variant was 1.07. It did not reach statistical significance even when simulating the expected carrier frequency of E326K in 100,000 Ashkenazi controls (p = .39). In addition, an additive effect was demonstrated for risk in carriers of two mutations, the LRRK2-G2019S and a mild-GBA mutation (N370S or R496H), compared to carriers of only one mutation in one of these genes (simulated OR 11.79 compared to 7.58 and 2.49, respectively). An additive effect was also suggested for earlier AAO (5.0 years earlier than in non-carriers, compared to 3.1 and 2.2 years, respectively). Conclusions: Compared to previous studies, we demonstrate here a higher frequency of PD patients that carry two mutations. The GBA-E326K is more likely to affect PD risk when accompanied by another mutation, and an additive effect on risk and earlier AAO was proposed for carriers of LRRK2/mild-GBA double mutations. Altogether, these data support an oligogenic approach to PD genetics.
AB - Background: GBA variants are the most common genetic risk factors for Parkinson's disease (PD) world-wide, and can be found in up to 20% of Ashkenazi PD patients. The E326K variant, which is not considered a Gaucher's disease causing mutation, was recently shown to increase the risk for PD. Since E326K is a common variant among Europeans, Finnish and Ashkenazi (2.4, 8.6 and 1.2% carrier rate, respectively), we aimed to refine its involvement in PD. Methods: 1200 consecutively recruited PD patients of a full Ashkenazi origin were genotyped for 10 GBA variants, the LRRK2-G2019S and the SMPD1-L302P. Alleles' frequencies were compared to controls, composed of 378 elderly healthy individuals and the non-neuro gnomAD Ashkenazi database. Odds-Ratio (OR) and age-at-motor-symptom-onset (AAO) were also calculated for all genotypes. Results: All allelic variations tested had significant allelic ORs, demonstrating a wide range (1.86–12.84). The lowest allelic OR was observed for E326K (p = .013). Forty-five patients (of 1200, 3.75%) had at least two mutations (of the 12 tested), compared to 2 (0.53%) among 378 controls (p = .0013). Of the E326K carrier patients, 37% (10/27) carried additional mutations and the genotypic OR for individuals who carried only the E326K variant was 1.07. It did not reach statistical significance even when simulating the expected carrier frequency of E326K in 100,000 Ashkenazi controls (p = .39). In addition, an additive effect was demonstrated for risk in carriers of two mutations, the LRRK2-G2019S and a mild-GBA mutation (N370S or R496H), compared to carriers of only one mutation in one of these genes (simulated OR 11.79 compared to 7.58 and 2.49, respectively). An additive effect was also suggested for earlier AAO (5.0 years earlier than in non-carriers, compared to 3.1 and 2.2 years, respectively). Conclusions: Compared to previous studies, we demonstrate here a higher frequency of PD patients that carry two mutations. The GBA-E326K is more likely to affect PD risk when accompanied by another mutation, and an additive effect on risk and earlier AAO was proposed for carriers of LRRK2/mild-GBA double mutations. Altogether, these data support an oligogenic approach to PD genetics.
KW - GBA
KW - Heterozygous mutation carrier
KW - LRRK2
KW - Oligogenic
KW - Parkinson's disease
UR - http://www.scopus.com/inward/record.url?scp=85074434242&partnerID=8YFLogxK
U2 - 10.1016/j.ymgme.2019.10.001
DO - 10.1016/j.ymgme.2019.10.001
M3 - Article
AN - SCOPUS:85074434242
SN - 1096-7192
VL - 128
SP - 470
EP - 475
JO - Molecular Genetics and Metabolism
JF - Molecular Genetics and Metabolism
IS - 4
ER -
