Structural Variation Detection and Association Analysis of Whole-Genome-Sequence Data from 16,905 Alzheimer's Diseases Sequencing Project Subjects.

Structural variations (SVs) are important contributors to the genetics of numerous human diseases. However, their role in Alzheimer's disease (AD) remains largely unstudied due to challenges in accurately detecting SVs. Here, we analyzed whole-genome sequencing data from the Alzheimer's Disease Sequencing Project (ADSP, N=16,905 subjects) and identified 400,234 (168,223 high-quality) SVs. We found a significant burden of deletions and duplications in AD cases (OR=1.05, P =0.03), particularly for singletons (OR=1.12, P =0.0002) and homozygous events (OR=1.10, P <0.0004). On AD genes, the ultra-rare SVs, including protein-altering SVs in ABCA7 , APP , PLCG2 , and SORL1 , were associated with AD (SKAT-O P =0.004). Twenty-one SVs are in linkage disequilibrium (LD) with known AD-risk variants, e.g., a deletion (chr2:105731359-105736864) in complete LD (R ² =0.99) with rs143080277 (chr2:105749599) in NCK2 . We also identified 16 SVs associated with AD and 13 SVs associated with AD-related pathological/cognitive endophenotypes. Our findings demonstrate the broad impact of SVs on AD genetics.
Competing Interests: Competing interests The authors declare that they have no competing interests.