TY - JOUR
T1 - Phenotypic variability associated with progranulin haploinsufficiency in patients with the common 1477C→T (Arg493X) mutation
T2 - an international initiative
AU - Rademakers, Rosa
AU - Baker, Matt
AU - Gass, Jennifer
AU - Adamson, Jennifer
AU - Huey, Edward D.
AU - Momeni, Parastoo
AU - Spina, Salvatore
AU - Coppola, Giovanni
AU - Karydas, Anna M.
AU - Stewart, Heather
AU - Johnson, Nancy
AU - Hsiung, Ging Yuek
AU - Kelley, Brendan
AU - Kuntz, Karen
AU - Steinbart, Ellen
AU - Wood, Elisabeth Mc Carty
AU - Yu, Chang En
AU - Josephs, Keith
AU - Sorenson, Eric
AU - Womack, Kyle B.
AU - Weintraub, Sandra
AU - Pickering-Brown, Stuart M.
AU - Schofield, Peter R.
AU - Brooks, William S.
AU - Van Deerlin, Vivianna M.
AU - Snowden, Julie
AU - Clark, Christopher M.
AU - Kertesz, Andrew
AU - Boylan, Kevin
AU - Ghetti, Bernardino
AU - Neary, David
AU - Schellenberg, Gerard D.
AU - Beach, Thomas G.
AU - Mesulam, Marsel
AU - Mann, David
AU - Grafman, Jordan
AU - Mackenzie, Ian R.
AU - Feldman, Howard
AU - Bird, Thomas
AU - Petersen, Ron
AU - Knopman, David
AU - Boeve, Bradley
AU - Geschwind, Dan H.
AU - Miller, Bruce
AU - Wszolek, Zbigniew
AU - Lippa, Carol
AU - Bigio, Eileen H.
AU - Dickson, Dennis
AU - Graff-Radford, Neill
AU - Hutton, Mike
N1 - Funding Information:
We thank the families who contributed samples that were crucial to this study. This work was supported by NIH grants P01 AG017216 and R01 AG026251 (to MH), R01 AG026938 (to DHG), P50 NS40256 (to DD and ZW), the Mayo Clinic ADRC (P50 AG16574, RP PI; to MH, BB, and RP), P30 AG10133 (to SS and BG), P30 AG13854 (to MM, SW, NJ, and EHB), P30 AG12300 (to KBW), P01 AG17586 (to VMVD and GDS), P50 AG05136 (to GDS), P50 AG03006 and P01 AG019724 (to BM), the California DHS #04-35522 (to DHG), the Mayo Clinic Research Foundation (to MH and DD), and the Robert and Clarice Smith Fellowship program (to RR). EDH and JG were supported by the intramural research program of the Institute of Neurological Disorders and Stroke (NINDS). The work of TGB at the Sun Health Research Institute is supported by the National Institute on Aging (P30 AG19610 Arizona Alzheimer's Disease Core Center) and the Arizona Department of Health Services contract 211002. IRM and HF were funded by the Canadian Institutes of Health Research Operating Grant number 74580. CL was supported by the Potamkin Foundation. Our work was also supported by the Veterans Affairs Research Funds, the ACCORD study (to AK), the Pacific Alzheimer Research Foundation, the Medical Research Council (to SMPB), and the National Health and Medical Research Council (Australia) grants 282933, 300400, and 276401. This study used samples from patients with amyotrophic lateral sclerosis from the NINDS Human Genetics Resource Center DNA and Cell Line Repository ( http://ccr.coriell.org/ninds ). RR is a postdoctoral fellow of the Fund for Scientific Research Flanders. SS is in part supported by, and is a PhD student of, the Department of Neurological and Behavioral Sciences, University of Siena, Siena, Italy. We thank Richard Caselli for providing us with FTLD patients for this study. His work is supported by the NIH P30 AG19610 grant. We also thank Jillian J Kril, Glenda M Halliday, Clement Loy, and Ralph N Martins for their study and ascertainment of the family with FTLD in Sydney.
PY - 2007/10
Y1 - 2007/10
N2 - Background: The progranulin gene (GRN) is mutated in 5-10% of patients with frontotemporal lobar degeneration (FTLD) and in about 20% of patients with familial FTLD. The most common mutation in GRN is Arg493X. We aimed to establish the contribution of this mutation to FTLD and related disorders. Methods: We measured the frequency of Arg493X in 3405 unrelated patients with various neurodegenerative diseases using Taqman single-nucleotide polymorphism (SNP) genotyping. Clinicopathological characterisation and shared haplotype analysis were done for 30 families with FTLD who carry Arg493X. To investigate the effect of potential modifying loci, we did linear regression analyses with onset age as the covariate for GRN variants, for genotypes of the apolipoprotein E gene (APOE), and for haplotypes of the microtubule-associated protein tau gene (MAPT). Findings: Of 731 patients with FTLD, 16 (2%) carried Arg493X. This mutation was not detected in 2674 patients who did not have FTLD. In 37 patients with Arg493X from 30 families with FTLD, clinical diagnoses included frontotemporal dementia, primary progressive aphasia, corticobasal syndrome, and Alzheimer's disease. Range of onset age was 44-69 years. In all patients who came to autopsy (n=13), the pathological diagnosis was FTLD with neuronal inclusions that contained TAR DNA-binding protein or ubiquitin, but not tau. Neurofibrillary tangle pathology in the form of Braak staging correlated with overall neuropathology in the Arg493X carriers. Haplotype analyses suggested that Arg493X arose twice, with a single founder for 27 families. Linear regression analyses suggested that patients with SNP rs9897528 on their wild-type GRN allele have delayed symptom onset. Onset ages were not associated with the MAPT H1 or H2 haplotypes or APOE genotypes, but early memory deficits were associated with the presence of an APOE ε4 allele. Interpretation: Clinical heterogeneity is associated with GRN haploinsufficiency, and genetic variability on the wild-type GRN allele might have a role in the age-related disease penetrance of GRN mutations.
AB - Background: The progranulin gene (GRN) is mutated in 5-10% of patients with frontotemporal lobar degeneration (FTLD) and in about 20% of patients with familial FTLD. The most common mutation in GRN is Arg493X. We aimed to establish the contribution of this mutation to FTLD and related disorders. Methods: We measured the frequency of Arg493X in 3405 unrelated patients with various neurodegenerative diseases using Taqman single-nucleotide polymorphism (SNP) genotyping. Clinicopathological characterisation and shared haplotype analysis were done for 30 families with FTLD who carry Arg493X. To investigate the effect of potential modifying loci, we did linear regression analyses with onset age as the covariate for GRN variants, for genotypes of the apolipoprotein E gene (APOE), and for haplotypes of the microtubule-associated protein tau gene (MAPT). Findings: Of 731 patients with FTLD, 16 (2%) carried Arg493X. This mutation was not detected in 2674 patients who did not have FTLD. In 37 patients with Arg493X from 30 families with FTLD, clinical diagnoses included frontotemporal dementia, primary progressive aphasia, corticobasal syndrome, and Alzheimer's disease. Range of onset age was 44-69 years. In all patients who came to autopsy (n=13), the pathological diagnosis was FTLD with neuronal inclusions that contained TAR DNA-binding protein or ubiquitin, but not tau. Neurofibrillary tangle pathology in the form of Braak staging correlated with overall neuropathology in the Arg493X carriers. Haplotype analyses suggested that Arg493X arose twice, with a single founder for 27 families. Linear regression analyses suggested that patients with SNP rs9897528 on their wild-type GRN allele have delayed symptom onset. Onset ages were not associated with the MAPT H1 or H2 haplotypes or APOE genotypes, but early memory deficits were associated with the presence of an APOE ε4 allele. Interpretation: Clinical heterogeneity is associated with GRN haploinsufficiency, and genetic variability on the wild-type GRN allele might have a role in the age-related disease penetrance of GRN mutations.
UR - http://www.scopus.com/inward/record.url?scp=34548633862&partnerID=8YFLogxK
U2 - 10.1016/S1474-4422(07)70221-1
DO - 10.1016/S1474-4422(07)70221-1
M3 - Article
C2 - 17826340
AN - SCOPUS:34548633862
SN - 1474-4422
VL - 6
SP - 857
EP - 868
JO - The Lancet Neurology
JF - The Lancet Neurology
IS - 10
ER -