Your search keyword '"Miko Valori"' showing total 2 results

1. Oligogenic basis of sporadic ALS: The example of

Author

Liina, Kuuluvainen, Karri, Kaivola, Saana, Mönkäre, Hannu, Laaksovirta, Manu, Jokela, Bjarne, Udd, Miko, Valori, Petra, Pasanen, Anders, Paetau, Bryan J, Traynor, David J, Stone, Johanna, Schleutker, Minna, Pöyhönen, Pentti J, Tienari, and Liisa, Myllykangas

Subjects

Article

Abstract

Objective To characterize the clinical and neuropathologic features of patients with amyotrophic lateral sclerosis (ALS) with the superoxide dismutase 1 (SOD1) p.Ala90Val mutation, as well as the mutation frequency and the role of oligogenic mechanisms in disease penetrance. Methods An index patient with autopsy-proven ALS was discovered to have the SOD1 p.Ala90Val mutation, which was screened in 2 Finnish ALS cohorts (n = 453). Additional contributing variants were analyzed from whole-genome or whole-exome sequencing data. Results Seven screened patients (1.5%) were found to carry the SOD1 heterozygous mutation. Allele-sharing analysis suggested a common founder haplotype. Common clinical features included limb-onset, long disease course, and sensory symptoms. No TDP43 pathology was observed. All cases were apparently sporadic, and pedigree analysis demonstrated that the mutation has reduced penetrance. Analysis of other contributing genes revealed a unique set of additional variants in each patient. These included previously described rare ANG and SPG11 mutations. One patient was compound heterozygous for SOD1 p.Ala90Val and p.Asp91Ala. Conclusions Our data suggest that the penetrance of SOD1 p.Ala90Val is modulated by other genes and indicates highly individual oligogenic basis of apparently sporadic ALS. Additional genetic variants likely contributing to disease penetrance were very heterogeneous, even among Finnish patients carrying the SOD1 founder mutation.

Published

2019

2. Alzheimer risk loci and associated neuropathology in a population-based study (Vantaa 85+)

Author

Terhi Peuralinna, Tuomo Polvikoski, Andrew B. Singleton, Liisa Myllykangas, Miko Valori, David J. Stone, Bryan J. Traynor, Maarit Tanskanen, Mira Mäkelä, Anders Paetau, Karri Kaivola, Pentti J. Tienari, Department of Pathology, Medicum, Clinicum, Research Programme for Molecular Neurology, Research Programs Unit, University of Helsinki, Neurologian yksikkö, and HUS Neurocenter

Subjects

0301 basic medicine, education, Population, Single-nucleotide polymorphism, Locus (genetics), Neuropathology, Biology, 3124 Neurology and psychiatry, Article, 03 medical and health sciences, medicine, Genetics (clinical), Genetic association, Genetics, education.field_of_study, 3112 Neurosciences, Neurofibrillary tangle, Odds ratio, medicine.disease, 3. Good health, 030104 developmental biology, Neurology (clinical), Cerebral amyloid angiopathy

Abstract

ObjectiveTo test the association of distinct neuropathologic features of Alzheimer disease (AD) with risk loci identified in genome-wide association studies.MethodsVantaa 85+ is a population-based study that includes 601 participants aged ≥85 years, of which 256 were neuropathologically examined. We analyzed 29 AD risk loci in addition to APOE ε4, which was studied separately and used as a covariate. Genotyping was performed using a single nucleotide polymorphism (SNP) array (341 variants) and imputation (6,038 variants). Participants with Consortium to Establish a Registry for Alzheimer Disease (CERAD) (neuritic Aβ plaques) scores 0 (n = 65) vs score M + F (n = 171) and Braak (neurofibrillary tangle pathology) stages 0–II (n = 74) vs stages IV–VI (n = 119), and with capillary Aβ (CapAβ, n = 77) vs without (n = 179) were compared. Cerebral amyloid angiopathy (CAA) percentage was analyzed as a continuous variable.ResultsAltogether, 24 of the 29 loci were associated (at p < 0.05) with one or more AD-related neuropathologic features in either SNP array or imputation data. Fifteen loci associated with CERAD score, smallest p = 0.0002122, odds ratio (OR) 2.67 (1.58–4.49) at MEF2C locus. Fifteen loci associated with Braak stage, smallest p = 0.004372, OR 0.31 (0.14–0.69) at GAB2 locus. Twenty loci associated with CAA, smallest p = 7.17E-07, β 14.4 (8.88–20) at CR1 locus. Fifteen loci associated with CapAβ smallest p = 0.002594, OR 0.54 (0.37–0.81) at HLA-DRB1 locus. Certain loci associated with specific neuropathologic features. CASS4, CLU, and ZCWPW1 associated only with CAA, while TREM2 and HLA-DRB5 associated only with CapAβ.ConclusionsAD risk loci differ in their association with neuropathologic features, and we show for the first time distinct risk loci for CAA and CapAβ.

Published

2017