TY - JOUR
T1 - The p.L302P mutation in the lysosomal enzyme gene SMPD1 is a risk factor for Parkinson disease
AU - Gan-Or, Ziv
AU - Ozelius, Laurie J.
AU - Bar-Shira, Anat
AU - Saunders-Pullman, Rachel
AU - Mirelman, Anat
AU - Kornreich, Ruth
AU - Gana-Weisz, Mali
AU - Raymond, Deborah
AU - Rozenkrantz, Liron
AU - Deik, Andres
AU - Gurevich, Tanya
AU - Gross, Susan J.
AU - Schreiber-Agus, Nicole
AU - Giladi, Nir
AU - Bressman, Susan B.
AU - Orr-Urtreger, Avi
PY - 2013/4/23
Y1 - 2013/4/23
N2 - Objective: To study the possible association of founder mutations in the lysosomal storage disorder genes HEXA, SMPD1, and MCOLN1 (causing Tay-Sachs, Niemann-Pick A, and mucolipidosis type IV diseases, respectively) with Parkinson disease (PD). Methods: Two PD patient cohorts of Ashkenazi Jewish (AJ) ancestry, that included a total of 938 patients, were studied: a cohort of 654 patients from Tel Aviv, and a replication cohort of 284 patients from New York. Eight AJ founder mutations in the HEXA, SMPD 1, and MCOLN1 genes were analyzed. The frequencies of these mutations were compared to AJ control groups that included large published groups undergoing prenatal screening and 282 individuals matched for age and sex. Results: Mutation frequencies were similar in the 2 groups of patients with PD. The SMPD 1 p.L302P was strongly associated with a highly increased risk for PD (odds ratio 9.4, 95% confidence interval 3.9-22.8, p < 0.0001), as 9/938 patients with PD were carriers of this mutation compared to only 11/10,709 controls. Conclusions: The SMPD 1 p.L302P mutation is a novel risk factor for PD. Although it is rare on a population level, the identification of this mutation as a strong risk factor for PD may further elucidate PD pathogenesis and the role of lysosomal pathways in disease development.
AB - Objective: To study the possible association of founder mutations in the lysosomal storage disorder genes HEXA, SMPD1, and MCOLN1 (causing Tay-Sachs, Niemann-Pick A, and mucolipidosis type IV diseases, respectively) with Parkinson disease (PD). Methods: Two PD patient cohorts of Ashkenazi Jewish (AJ) ancestry, that included a total of 938 patients, were studied: a cohort of 654 patients from Tel Aviv, and a replication cohort of 284 patients from New York. Eight AJ founder mutations in the HEXA, SMPD 1, and MCOLN1 genes were analyzed. The frequencies of these mutations were compared to AJ control groups that included large published groups undergoing prenatal screening and 282 individuals matched for age and sex. Results: Mutation frequencies were similar in the 2 groups of patients with PD. The SMPD 1 p.L302P was strongly associated with a highly increased risk for PD (odds ratio 9.4, 95% confidence interval 3.9-22.8, p < 0.0001), as 9/938 patients with PD were carriers of this mutation compared to only 11/10,709 controls. Conclusions: The SMPD 1 p.L302P mutation is a novel risk factor for PD. Although it is rare on a population level, the identification of this mutation as a strong risk factor for PD may further elucidate PD pathogenesis and the role of lysosomal pathways in disease development.
UR - http://www.scopus.com/inward/record.url?scp=84878911804&partnerID=8YFLogxK
U2 - 10.1212/WNL.0b013e31828f180e
DO - 10.1212/WNL.0b013e31828f180e
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C2 - 23535491
AN - SCOPUS:84878911804
SN - 0028-3878
VL - 80
SP - 1606
EP - 1610
JO - Neurology
JF - Neurology
IS - 17
ER -