Whole-genome sequencing identifies variants inANK1,LRRN1,HAS1,and other genes and regulatory regions for stroke in type 1 diabetes-Reference-Cited by-同舟云学术

Whole-genome sequencing identifies variants inANK1,LRRN1,HAS1,and other genes and regulatory regions for stroke in type 1 diabetes

Published:2022-12-01 Issue: Volume: Page:
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Antikainen Anni A.^ORCID,Haukka Jani K.^ORCID,Kumar Anmol^ORCID,Syreeni Anna^ORCID,Hägg-Holmberg Stefanie^ORCID,Ylinen Anni^ORCID,Kilpeläinen Elina,Kytölä Anastasia,Palotie Aarno^ORCID,Putaala Jukka^ORCID,Thorn Lena M.^ORCID,Harjutsalo Valma^ORCID,Groop Per-Henrik^ORCID,Sandholm Niina^ORCID

Abstract

AbstractAimsIndividuals with type 1 diabetes (T1D) carry a markedly increased risk of stroke, with distinct clinical and neuroimaging characteristics as compared to those without diabetes. Using whole-genome sequencing (WGS) and whole-exome sequencing (WES), we aimed to find rare and low-frequency genomic variants associated with stroke in T1D. The lead findings were followed up in various datasets to replicate the findings and to assess their specificity to diabetes.Methods and ResultsWe studied stroke genetics in 1,051 individuals with T1D using WGS or WES. We analysed the genome with single-variant analyses, gene aggregate analyses, and aggregate analyses on genomic windows, enhancers and promoters. Furthermore, we attempted replication in T1D using a genome-wide association study (N=3,945) and direct genotyping (N=3,600), and in the general population from the FinnGen project and UK Biobank summary statistics. We identified a rare missense mutation onSREBF1associated with hemorrhagic stroke (rs114001633, p.Pro227Leu,p-value=8.96×10-9), which further replicated in T1D. Using gene aggregate analysis with protein altering or protein truncating variants, we identified exome-wide significant genes:ANK1andLRRN1displayed replication evidence in T1D, whileLRRN1,HAS1andUACAreplicated in the general population (UK Biobank). Furthermore, we performed sliding-window analyses and identified 14 genome-wide significant windows for stroke on 4q33-34.1, of which two replicated in T1D, and a suggestive genomic window onLINC01500, which replicated in T1D. Finally, with the regulatory region aggregate analyses, we identified a stroke-associatedTRPM2-ASpromoter (p-value=5.78×10-6), which we validated with an in vitro cell-based assay.TRPM2has been previously linked to ischemic stroke.ConclusionsHere, we report the first genome-wide analysis on stroke in individuals with diabetes. We identified multiple stroke risk loci with evidence of replication: 4q33-34.1,SREBF1, andANK1for stroke in T1D; andHAS1,UACA,LRRN1,LINC01500, andTRPM2-ASpromoter for stroke potentially generalizable to the non-diabetic population.

Publisher

Cold Spring Harbor Laboratory

Reference50 articles.

1. Presence and Determinants of Cardiovascular Disease and Mortality in Individuals With Type 1 Diabetes of Long Duration: The FinnDiane 50 Years of Diabetes Study

2. Sun H , Saeedi P , Karuranga S , Pinkepank M , Ogurtsova K , Duncan BB , Stein C , Basit A , Chan JCN , Mbanya JC , et al. IDF Diabetes Atlas: Global, regional and country-level diabetes prevalence estimates for 2021 and projections for 2045. Diabetes Res. Clin. Pract. 2022;183.

3. The epidemic of type 1 diabetes

4. Glycaemic control and excess risk of ischaemic and haemorrhagic stroke in patients with type 1 diabetes: a cohort study of 33 453 patients;J. Intern. Med,2017

5. Prospective Study of Type 1 and Type 2 Diabetes and Risk of Stroke Subtypes