Genetic landscape of early-onset dementia in Hungary

Csaban, Dora and Illes, Anett and Renata, Toth-Bencsik and Balicza, Peter and Pentelenyi, Klara and Molnar, Viktor and Gezsi, Andras and Grosz, Zoltan and Gal, Aniko and Kovacs, Tibor and Klivenyi, Peter and Molnar, Maria Judit (2022) Genetic landscape of early-onset dementia in Hungary. NEUROLOGICAL SCIENCES, 43 (9). pp. 5289-5300. ISSN 1590-1874

Preview

Text
csaban2022_Genetic landscape of early-onset dementia in Hungary.pdf
Download (726kB) | Preview

Official URL: http://doi.org/10.1007/s10072-022-06168-8

Abstract

Introduction: Early-onset dementias (EOD) are predominantly genetically determined, but the underlying disease-causing alterations are often unknown. The most frequent forms of EODs are early-onset Alzheimer's disease (EOAD) and frontotemporal dementia (FTD). Patients: This study included 120 Hungarian patients with EOD (48 familial and 72 sporadic) which had a diagnosis of EOAD (n = 49), FTD (n = 49), or atypical dementia (n = 22). Results: Monogenic dementia was detected in 15.8% of the patients. A pathogenic hexanucleotide repeat expansion in the C9ORF72 gene was present in 6.7% of cases and disease-causing variants were detected in other known AD or FTD genes in 6.7% of cases (APP, PSEN1, PSEN2, GRN). A compound heterozygous alteration of the TREM2 gene was identified in one patient and heterozygous damaging variants in the CSF1R and PRNP genes were detected in two other cases. In two patients, the coexistence of several heterozygous damaging rare variants associated with neurodegeneration was detected (1.7%). The APOE genotype had a high odds ratio for both the APOE ɛ4/3 and the ɛ4/4 genotype (OR = 2.7 (95%CI = 1.3-5.9) and OR = 6.5 (95%CI = 1.4-29.2), respectively). In TREM2, SORL1, and ABCA7 genes, 5 different rare damaging variants were detected as genetic risk factors. These alterations were not present in the control group. Conclusion: Based on our observations, a comprehensive, targeted panel of next-generation sequencing (NGS) testing investigating several neurodegeneration-associated genes may accelerate the path to achieve the proper genetic diagnosis since phenotypes are present on a spectrum. This can also reveal hidden correlations and overlaps in neurodegenerative diseases that would remain concealed in separated genetic testing.

Item Type:	Article
Subjects:	R Medicine / orvostudomány > RZ Other systems of medicine / orvostudomány egyéb területei
Depositing User:	Dr András Gézsi
Date Deposited:	28 Sep 2022 10:57
Last Modified:	28 Sep 2022 10:57
URI:	http://real.mtak.hu/id/eprint/150295

Actions (login required)

Edit Item