Investigating the role of common and rare variants in multiplex multiple sclerosis families reveals an increased burden of common risk variation

Everest, Elif; Ahangari, Mohammad; Uygunoğlu, Uğur; Tütüncü, Melih; Bulbul, Alper; Saıp, Sabahattin; Duman, Taşkın; Sezerman, Uğur; Reich, Daniel S.; Riley, Brien P.; Síva, Aksel; Turanlı, Eda Tahir

doi:10.1038/s41598-022-21484-x

Cited by 4 publications

(4 citation statements)

References 41 publications

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“…A limitation of these previous studies was that they were conducted prior to the latest MS GWAS and thus used fewer MS risk variants to compute their polygenic risk scores. Recent work in a Turkish cohort has suggested that population-based MS cases have a higher PRS than people with MS from multicase families; however, this comparison was not statistically significant, and not all HLA risk alleles were able to be imputed [32]. These conflicting results also reflect the heterogeneity of common genetic risk profiles for MS.…”

Section: Discussionmentioning

confidence: 90%

Multiple Sclerosis Polygenic Risk Is Not Enriched in Three Multicase Families in Comparison to Population-Based Cases

Chen,

Motyer,

Taylor

et al. 2024

Human Mutation

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Multiple sclerosis (MS) is a complex neurological and autoimmune disease with an established genetic component. Families with multiple cases of MS are rare but do occur. We hypothesised that multicase families may have a heightened polygenic risk for MS. In this work, we have determined whether polygenic risk for MS is enriched in multicase families in comparison to a case-control cohort. Using the findings from the largest MS genome-wide association study, we calculated a weighted polygenic risk score (wPRS) for MS. We applied this wPRS to study a population-based MS case-control cohort (3,252 people with MS and 5,725 controls) and three multicase MS families (9 individuals with MS, 10 unaffected family members). For both the population-based cohort and the three families, 167 of the 233 known genome-wide significant MS-associated variants were identified and used to calculate the wPRS. Within the population-based cohort, the wPRS was significantly higher in MS cases than controls (P=2.2×10−16). The wPRS of familial MS cases was not significantly different to population-based MS cases (P>0.05). Both affected and unaffected MS family members had higher wPRS than population controls. MS families have a higher polygenic risk for MS, but this did not differ to the polygenic risk of population-based MS cases. Only one family carried the established HLA-DRB1 15:01 MS risk allele, which was present in both affected and unaffected family members. Across families, unaffected family members had an elevated polygenic risk in comparison to population controls indicating that a higher polygenic risk does not fully explain the clustering of MS in families.

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Section: Discussionmentioning

confidence: 90%

Multiple Sclerosis Polygenic Risk Is Not Enriched in Three Multicase Families in Comparison to Population-Based Cases

Chen,

Motyer,

Taylor

et al. 2024

Human Mutation

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“…It is possible that PC could reinforce several gene loci associated with MS (39). In a study by Everest et al, FMS cases were signi cantly more likely to experience common rare risk variation than controls and control families (41).…”

Section: Discussionmentioning

confidence: 99%

The Role of Parental Consanguinity and Familial Aggregation in Development of Multiple Sclerosis: A Case-control Study

Vaheb,

Panah,

Afshari-Safavi

et al. 2024

Preprint

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Background Several studies pointed out the importance of genetic risk factors such as parental consanguinity (PC) and familial multiple sclerosis (FMS) in the risk of MS. This study aimed to investigate the PC and FMS among people with MS (pwMS) in Isfahan, Iran. Methods This case-control study was conducted on pwMS from the MS clinic of Kashani Hospital, Isfahan, Iran, between September 2022 and September 2023. Healthy controls (HC) were also recruited from the MS clinic. Data on demographic and clinical characteristics and history of PC and FMS were collected from participants. The relationships between PC, FMS, and developing MS were assessed using multinomial logistic regression analysis. The Odds ratio (OR) with a 95% confidence interval (CI) was computed. Results A total number of 4264 pwMS and 400 HCs were included. The prevalence of PC and FMS among pwMS were 29.3% and 24%, respectively. Multinomial logistic regression adjusted for age and sex indicated that the odds of developing MS were significantly associated with a history of PC (OR = 3.03, 95%CI: 2.23 to 4.13, p < 0.001) and FMS (OR = 5.42, 95%CI: 3.51 to 8.38, p < 0.001). Conclusion PC and FMS can increase the risk of developing MS. PC and FMS should be considered along with other risk factors for developing MS. A comprehensive conclusion requires further research.

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“…Despite the high prevalence of consanguinity among Emirati individuals, no significant differences in clinical and demographic characteristics were observed between those with familial and sporadic MS [ 42 ]. Previous studies have identified certain rare genetic risk variants that contribute to the heritability of MS, possibly explaining its occurrence in specific families [ 20 , 43 ], along with some hormonal contributors [ 44 ]. In contrast, additional studies have demonstrated a significant link between environmental factors and the development of MS, such as sunlight exposure, cigarette smoking, measles infection, Epstein-Barr virus (EBV) infection, and stressful events [ [45] , [46] , [47] ].…”

Section: Discussionmentioning

confidence: 99%

Consanguineous marriage among familial multiple sclerosis subjects: A national registry-based study

Salehi,

Naghizadeh,

Ezabadi

et al. 2024

Heliyon

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Investigating the role of common and rare variants in multiplex multiple sclerosis families reveals an increased burden of common risk variation

Cited by 4 publications

References 41 publications

Multiple Sclerosis Polygenic Risk Is Not Enriched in Three Multicase Families in Comparison to Population-Based Cases

Multiple Sclerosis Polygenic Risk Is Not Enriched in Three Multicase Families in Comparison to Population-Based Cases

The Role of Parental Consanguinity and Familial Aggregation in Development of Multiple Sclerosis: A Case-control Study

Consanguineous marriage among familial multiple sclerosis subjects: A national registry-based study

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