Exome-Sequence Analyses of Four Multi-Incident Multiple Sclerosis Families

Zrzavy, Tobias; Leutmezer, Fritz; Kristoferitsch, Wolfgang; Kornek, Barbara; Schneider, Christine; Berger, Thomas; Zimprich, Alexander

doi:10.3390/genes11090988

Cited by 7 publications

(8 citation statements)

References 38 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Additionally, class I/II human leukocyte antigen (HLA) genes contribute to an individual’s susceptibility for developing MS. A recent study analysed variants of 16 HLA genes and identified alleles associated with MS risk [ 97 ]. However, similar to other studies, an exome-sequence analysis of four multi-incident MS families did not identify individual disease-causing gene variants [ 98 , 99 , 100 , 101 ]. These results highlight the complex genetic aetiology of MS, and the possibility of a multigenic origin.…”

Section: Application Of Next-generation Sequencing In Neurogenetic Diseasessupporting

confidence: 76%

Next-Generation Sequencing Technologies and Neurogenetic Diseases

Sun

Shen

Fang

et al. 2021

Life

View full text Add to dashboard Cite

Next-generation sequencing (NGS) technology has led to great advances in understanding the causes of Mendelian and complex neurological diseases. Owing to the complexity of genetic diseases, the genetic factors contributing to many rare and common neurological diseases remain poorly understood. Selecting the correct genetic test based on cost-effectiveness, coverage area, and sequencing range can improve diagnosis, treatments, and prevention. Whole-exome sequencing and whole-genome sequencing are suitable methods for finding new mutations, and gene panels are suitable for exploring the roles of specific genes in neurogenetic diseases. Here, we provide an overview of the classifications, applications, advantages, and limitations of NGS in research on neurological diseases. We further provide examples of NGS-based explorations and insights of the genetic causes of neurogenetic diseases, including Charcot–Marie–Tooth disease, spinocerebellar ataxias, epilepsy, and multiple sclerosis. In addition, we focus on issues related to NGS-based analyses, including interpretations of variants of uncertain significance, de novo mutations, congenital genetic diseases with complex phenotypes, and single-molecule real-time approaches.

show abstract

Section: Application Of Next-generation Sequencing In Neurogenetic Diseasessupporting

confidence: 76%

Next-Generation Sequencing Technologies and Neurogenetic Diseases

Sun

Shen

Fang

et al. 2021

Life

View full text Add to dashboard Cite

show abstract

“…One cannot argue against the contribution of genetic factors to MS susceptibility, as studies regarding the genetics of MS have come a long way in the last few years, and quite a few loci have been unequivocally identified [ 2 , 28 , 29 , 30 , 31 ]. Results from candidate-gene association studies and genome-wide association studies (GWAS) suggest that both common, low-frequency, and rare variants contribute to MS susceptibility [ 4 , 8 ].…”

Section: Discussionmentioning

confidence: 99%

Multiple Sclerosis: Shall We Target CD33?

Siokas

Tsouris

Aloizou

et al. 2020

Genes

View full text Add to dashboard Cite

Background: Multiple sclerosis (MS) is a chronic disease of the central nervous system (CNS). Myeloid lineage cells (microglia and macrophages) may participate in the pathogenic mechanisms leading to MS. CD33 is a transmembrane receptor, mainly expressed by myeloid lineage cells. CD33 rs3865444 is a promoter variant previously associated with Alzheimer’s disease, whose role in MS remains obscure. Objective: To assess the role of CD33 rs3865444 in MS risk. Methods: We genotyped 1396 patients with MS and 400 healthy controls for the presence of the CD33 rs3865444 variant. Odds ratios (ORs) with the respective 95% confidence intervals (CIs), were calculated with the SNPStats software, assuming five genetic models (co-dominant, dominant, recessive, over-dominant, and log-additive), with the G allele as the reference allele. The value of 0.05 was set as the threshold for statistical significance. Results: CD33 rs3865444 was associated with MS risk in the dominant (GG vs. GT + TT; OR (95% C.I.) = 0.79 (0.63–0.99), p = 0.041) and the over-dominant (GG + TT vs. GT; OR (95% C.I.) = 0.77 (0.61–0.97), p = 0.03) modes of inheritance. Given that the GG genotype was more frequent and the GT genotype was less frequent in MS patients compared to controls—while the observed frequency of the TT genotype did not differ between the two groups—the observed difference in MS risk may be stemming from either the GG (as a risk factor) or the GT (as a protective factor) genotype of CD33 rs3865444. Conclusions: Our preliminary results suggest a possible contribution of CD33 rs3865444 to MS. Therefore, larger multiethnic studies should be conducted, investigating the role of CD33 rs3865444 in MS.

show abstract

“…Interestingly, in the most recently reported WES study of MS, a missense variant in MBP was found in four MS patients from the same family 32 , further pointing towards a role of rare variants in MBP in MS susceptibility. The product of PLK1 is a kinase that phosphorylates and regulates the activity of MTHFR, an enzyme is involved in the synthesis of methionine and its product S-adenosylmethionine (SAM) 49,50 .…”

Section: Discussionmentioning

confidence: 83%

“…This makes multi-incident MS families of interest for identifying and studying rare variants involved in the disease. In the past 10 years, a number of studies have reported rare, putatively pathogenic genetic variants in MS patients from multi-incident families through WES 22,[27][28][29][30][31][32] . Most of these family studies, however, only involved a small number of families, analyses were sometimes targeted exclusively at known MS loci, and the vast majority of the identified variants were not studied in replication studies or did not replicate 27,29,[33][34][35][36] .…”

Section: Introductionmentioning

confidence: 99%

Whole exome sequencing in multi-incident families identifies novel candidate genes for multiple sclerosis

Horjus

Banda

Heerings

et al. 2022

Preprint

View full text Add to dashboard Cite

Multiple sclerosis (MS) is a degenerative disease of the central nervous system in which auto-immunity-induced demyelination occurs. MS is thought to be caused by a complex interplay of environmental and genetic risk factors. While most genetic studies have focused on identifying common genetic variants for MS through genome-wide association studies, the objective of the present study was to identify rare genetic variants contributing to MS susceptibility. We used whole exome sequencing (WES) followed by co-segregation analyses in nine multi-incident families with 2 to 4 affected individuals. WES was performed in 31 family members with and without MS. After applying a suite of selection criteria, co-segregation analyses for a number of rare variants selected from the WES results were performed, adding 24 family members. This approach resulted in 12 exonic rare variants that showed acceptable co-segregation with MS within the nine families, implicating the genes MBP, PLK1, MECP2, MTMR7, TOX3, CPT1A, SORCS1, TRIM66, ITPR3, TTC28, CACNA1F, and PRAM1. Of these, three genes (MBP, MECP2, and CPT1A) have been previously reported as carrying MS-related rare variants. Six additional genes (MTMR7, TOX3, SORCS1, ITPR3, TTC28, and PRAM1) have also been implicated in MS through common genetic variants. The proteins encoded by all twelve genes containing rare variants interact in a molecular framework that points to biological processes involved in (de-/re-)myelination and auto-immunity. Our approach provides clues to possible molecular mechanisms underlying MS that should be further studied in cellular and/or animal models.

show abstract

Exome-Sequence Analyses of Four Multi-Incident Multiple Sclerosis Families

Cited by 7 publications

References 38 publications

Next-Generation Sequencing Technologies and Neurogenetic Diseases

Next-Generation Sequencing Technologies and Neurogenetic Diseases

Multiple Sclerosis: Shall We Target CD33?

Whole exome sequencing in multi-incident families identifies novel candidate genes for multiple sclerosis

Contact Info

Product

Resources

About