Dissection of artifactual and confounding glial signatures by single-cell sequencing of mouse and human brain

Marsh, Samuel E.; Walker, Alec J.; Kamath, Tushar; Dissing‐Olesen, Lasse; Hammond, Timothy R.; Soysa, T. Yvanka de; Young, Adam M. H.; Murphy, Sarah Louise; Abdulraouf, Abdulraouf; Nadaf, Naeem; Dufort, Connor; Walker, Alicia C.; Lucca, Liliana E.; Kozareva, Velina; Vanderburg, Charles; Hong, Soyon; Bulstrode, Harry; Hutchinson, Peter J.; Gaffney, Daniel J.; Hafler, David A.; Franklin, Robin J.M.; Macosko, Evan Z.; Stevens, Beth

doi:10.1038/s41593-022-01022-8

articleNature NeuroscienceMar 1, 2022HYBRID OA

Dissection of artifactual and confounding glial signatures by single-cell sequencing of mouse and human brain

SESamuel E. Marsh AJAlec J. Walker TKTushar Kamath LDLasse Dissing‐Olesen TRTimothy R. Hammond

Broad Institute · Boston Children's Hospital · +12 more institutions

PubMed

Indexed incrossrefpubmed

Abstract

A key aspect of nearly all single-cell sequencing experiments is dissociation of intact tissues into single-cell suspensions. While many protocols have been optimized for optimal cell yield, they have often overlooked the effects that dissociation can have on ex vivo gene expression. Here, we demonstrate that use of enzymatic dissociation on brain tissue induces an aberrant ex vivo gene expression signature, most prominently in microglia, which is prevalent in published literature and can substantially confound downstream analyses. To address this issue, we present a rigorously validated protocol that preserves both in vivo transcriptional profiles and cell-type diversity and yield across tissue types and…

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Topics

Keywords

Ex vivo
Biology
Human brain
Gene expression
Microglia
Cell
In vivo
Cell type

UN Sustainable Development Goals

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