# Recurrent & non-recurrent copy number variants in Native Americans and a cosmopolitan sample in relation to Alcohol Use Disorder and other psychiatric diseases

**Authors:** Salma M Wakil, Keita Morisaki, Pei-Hong Shen, Dylan G Sucich, Melanie Schwandt, Fielding Hejtmancik, Cheryl Marietta, Qiaoping Yuan, Nancy Diazgranados, Colin A Hodgkinson, David Goldman

PMC · DOI: 10.21203/rs.3.rs-8108448/v1 · 2025-12-11

## TL;DR

The study explores how copy number variants in Native American populations may be linked to psychiatric disorders like alcohol use disorder.

## Contribution

The study identifies specific recurrent CNVs in Native Americans that may increase psychiatric disease risk, despite overall CNV burden not predicting these conditions.

## Key findings

- Recurrent CNVs are common in Native Americans and some span multiple tribes.
- A specific CNV in the 22q11.2 region is associated with higher odds of alcohol use disorder and psychiatric diagnoses.
- Ancient CNVs persist in Native American populations for hundreds of generations.

## Abstract

Copy Number Variants (CNVs) can alter disease susceptibility by gene deletion, duplication and other mechanisms. CNVs are implicated in neuropsychiatric diseases. However, their rarity or de novo nature impedes linkage analysis. Therefore, we identified recurrent CNVs (rCNVs) in Native Americans with low genetic admixture and high prevalence of Alcohol Use Disorder (AUD) and other psychiatric disorders.

Large (> 200 kb) rCNVs were abundant in PI and SWI, almost all carrying at least one rCNV, and with some CNVs found in both geographically and linguistically distinct tribes. In patients carrying rCNVs, gene deletions led to haploinsufficiency, and duplications overexpression. Haplotype analysis revealed a common chromosome 6p21.33 rCNV that persisted in Native Americans for at least 750 generations, leading to haploinsufficiency of at least two genes. Gene-based CNV burden did not predict AUD or other psychiatric disorders. However, an rCNV, found in PI and duplicating three genes within the 22q11.2 Velocardiofacial Syndrome region, may be associated with psychiatric disease. Among 27 heterozygotes, 22 had AUD (OR = 3.18 [1.18–8.59], p = 0.01), and 24 had a psychiatric diagnosis (OR = 4.8 [1.4–16], p = 0.006, FDR 0.07 adjusted for 13 common rCNVs tested).

Recurrent CNVs are prevalent in Native American populations and have ancient origins. While gene-based CNV burden did not predict AUD or other psychiatric disorders, specific rCNVs, such as those within 22q11.2 region, may confer higher risk for psychiatric conditions. Other less abundant rCNVs and non-recurrent CNVs might also alter risk, the effects of such CNVs being undetectable via genome-wide association studies with single SNPs.

## Linked entities

- **Diseases:** Velocardiofacial Syndrome (MONDO:0008644)

## Full-text entities

- **Diseases:** AUD (MESH:D000437), neuropsychiatric diseases (MESH:D004194), Velocardiofacial Syndrome (MESH:D004062), psychiatric (MESH:D001523)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

6 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12776451/full.md

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Source: https://tomesphere.com/paper/PMC12776451