TY - JOUR
T1 - Genome wide association study of clinical duration and age at onset of sporadic CJD
AU - Hummerich, Holger
AU - Speedy, Helen
AU - Campbell, Tracy
AU - Darwent, Lee
AU - Hill, Elizabeth
AU - Collins, Steven
AU - Stehmann, Christiane
AU - Kovacs, Gabor G.
AU - Geschwind, Michael D.
AU - Frontzek, Karl
AU - Budka, Herbert
AU - Gelpi, Ellen
AU - Aguzzi, Adriano
AU - van der Lee, Sven J.
AU - van Duijn, Cornelia M.
AU - Liberski, Pawel P.
AU - Calero, Miguel
AU - Sanchez-Juan, Pascual
AU - Bouaziz-Amar, Elodie
AU - Laplanche, Jean Louis
AU - Haïk, Stéphane
AU - Brandel, Jean Phillipe
AU - Mammana, Angela
AU - Capellari, Sabina
AU - Poleggi, Anna
AU - Ladogana, Anna
AU - Pocchiari, Maurizio
AU - Zafar, Saima
AU - Booth, Stephanie
AU - Jansen, Gerard H.
AU - Areškevičiūtė, Aušrinė
AU - Lund, Eva Løbner
AU - Glisic, Katie
AU - Parchi, Piero
AU - Hermann, Peter
AU - Zerr, Inga
AU - Appleby, Brian S.
AU - Safar, Jiri
AU - Gambetti, Pierluigi
AU - Collinge, John
AU - Mead, Simon
N1 - Publisher Copyright:
© 2024 Hummerich et al.
PY - 2024/7/26
Y1 - 2024/7/26
N2 - Human prion diseases are rare, transmissible and often rapidly progressive dementias. The most common type, sporadic Creutzfeldt-Jakob disease (sCJD), is highly variable in clinical duration and age at onset. Genetic determinants of late onset or slower progression might suggest new targets for research and therapeutics. We assembled and array genotyped sCJD cases diagnosed in life or at autopsy. Clinical duration (median:4, interquartile range (IQR):2.5–9 (months)) was available in 3,773 and age at onset (median:67, IQR:61–73 (years)) in 3,767 cases. Phenotypes were successfully transformed to approximate normal distributions allowing genome-wide analysis without statistical inflation. 53 SNPs achieved genome-wide significance for the clinical duration phenotype; all of which were located at chromosome 20 (top SNP rs1799990, pvalue = 3.45x10-36, beta = 0.34 for an additive model; rs1799990, pvalue = 9.92x10-67, beta = 0.84 for a heterozygous model). Fine mapping, conditional and expression analysis suggests that the well-known non-synonymous variant at codon 129 is the obvious outstanding genome-wide determinant of clinical duration. Pathway analysis and suggestive loci are described. No genome-wide significant SNP determinants of age at onset were found, but the HS6ST3 gene was significant (pvalue = 1.93 x 10−6) in a gene-based test. We found no evidence of genome-wide genetic correlation between case-control (disease risk factors) and case-only (determinants of phenotypes) studies. Relative to other common genetic variants, PRNP codon 129 is by far the outstanding modifier of CJD survival suggesting only modest or rare variant effects at other genetic loci.
AB - Human prion diseases are rare, transmissible and often rapidly progressive dementias. The most common type, sporadic Creutzfeldt-Jakob disease (sCJD), is highly variable in clinical duration and age at onset. Genetic determinants of late onset or slower progression might suggest new targets for research and therapeutics. We assembled and array genotyped sCJD cases diagnosed in life or at autopsy. Clinical duration (median:4, interquartile range (IQR):2.5–9 (months)) was available in 3,773 and age at onset (median:67, IQR:61–73 (years)) in 3,767 cases. Phenotypes were successfully transformed to approximate normal distributions allowing genome-wide analysis without statistical inflation. 53 SNPs achieved genome-wide significance for the clinical duration phenotype; all of which were located at chromosome 20 (top SNP rs1799990, pvalue = 3.45x10-36, beta = 0.34 for an additive model; rs1799990, pvalue = 9.92x10-67, beta = 0.84 for a heterozygous model). Fine mapping, conditional and expression analysis suggests that the well-known non-synonymous variant at codon 129 is the obvious outstanding genome-wide determinant of clinical duration. Pathway analysis and suggestive loci are described. No genome-wide significant SNP determinants of age at onset were found, but the HS6ST3 gene was significant (pvalue = 1.93 x 10−6) in a gene-based test. We found no evidence of genome-wide genetic correlation between case-control (disease risk factors) and case-only (determinants of phenotypes) studies. Relative to other common genetic variants, PRNP codon 129 is by far the outstanding modifier of CJD survival suggesting only modest or rare variant effects at other genetic loci.
UR - http://www.scopus.com/inward/record.url?scp=85200111842&partnerID=8YFLogxK
U2 - 10.1371/journal.pone.0304528
DO - 10.1371/journal.pone.0304528
M3 - Article
C2 - 39079175
AN - SCOPUS:85200111842
SN - 1932-6203
VL - 19
JO - PLoS ONE
JF - PLoS ONE
IS - 7 July
M1 - e0304528
ER -