Common Mitochondrial Deletions in RNA-Seq: Evaluation of Bulk, Single-cell, and Spatial Transcriptomic Datasets

Overview

Journal Commun Biol

Specialty Biology

Date 2024 Feb 17

PMID 38368460

Authors

Audrey A Omidsalar

Carmel G McCullough

Lili Xu

Stanley Boedijono

Daniel Gerke

Michelle G Webb

Zarko Manojlovic

Adolfo Sequeira

Mark F Lew

Marco Santorelli

Geidy E Serrano

Thomas G Beach

Agenor Limon

Marquis P Vawter

Brooke E Hjelm

Affiliations

Soon will be listed here.

Abstract

Common mitochondrial DNA (mtDNA) deletions are large structural variants in the mitochondrial genome that accumulate in metabolically active tissues with age and have been investigated in various diseases. We applied the Splice-Break2 pipeline (designed for high-throughput quantification of mtDNA deletions) to human RNA-Seq datasets and describe the methodological considerations for evaluating common deletions in bulk, single-cell, and spatial transcriptomics datasets. A robust evaluation of 1570 samples from 14 RNA-Seq studies showed: (i) the abundance of some common deletions detected in PCR-amplified mtDNA correlates with levels observed in RNA-Seq data; (ii) RNA-Seq library preparation method has a strong effect on deletion detection; (iii) deletions had a significant, positive correlation with age in brain and muscle; (iv) deletions were enriched in cortical grey matter, specifically in layers 3 and 5; and (v) brain regions with dopaminergic neurons (i.e., substantia nigra, ventral tegmental area, and caudate nucleus) had remarkable enrichment of common mtDNA deletions.

Citing Articles

Increased Rate of Unique Mitochondrial DNA Deletion Breakpoints in Young Adults With Early-Life Stress.

Daniels T, Hjelm B, Lewis-de Los Angeles W, Smith E, Omidsalar A, Rollins B Biol Psychiatry Glob Open Sci. 2025; 5(2):100422.

PMID: 39845127 PMC: 11751525. DOI: 10.1016/j.bpsgos.2024.100422.

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