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Publication
BAd-CRISPR: Inducible gene knockout in interscapular brown adipose tissue of
adult mice.
Authors Romanelli SM, Lewis KT, Nishii A, Rupp AC, Li Z, Mori H, Schill RL, Learman BS,
Rhodes CJ, MacDougald OA
Submitted By Submitted Externally on 1/10/2022
Status Published
Journal The Journal of biological chemistry
Year 2021
Date Published 12/1/2021
Volume : Pages 297 : 101402
PubMed Reference 34774798
Abstract CRISPR/Cas9 has enabled inducible gene knockout in numerous tissues; however,
its use has not been reported in brown adipose tissue (BAT). Here, we developed
the brown adipocyte CRISPR (BAd-CRISPR) methodology to rapidly interrogate the
function of one or multiple genes. With BAd-CRISPR, an adeno-associated virus
(AAV8) expressing a single guide RNA (sgRNA) is administered directly to BAT of
mice expressing Cas9 in brown adipocytes. We show that the local administration
of AAV8-sgRNA to interscapular BAT of adult mice robustly transduced brown
adipocytes and ablated expression of adiponectin, adipose triglyceride lipase,
fatty acid synthase, perilipin 1, or stearoyl-CoA desaturase 1 by >90%.
Administration of multiple AAV8 sgRNAs led to simultaneous knockout of up to
three genes. BAd-CRISPR induced frameshift mutations and suppressed target gene
mRNA expression but did not lead to substantial accumulation of off-target
mutations in BAT. We used BAd-CRISPR to create an inducible uncoupling protein 1
(Ucp1) knockout mouse to assess the effects of UCP1 loss on adaptive
thermogenesis in adult mice. Inducible Ucp1 knockout did not alter core body
temperature; however, BAd-CRISPR Ucp1 mice had elevated circulating
concentrations of fibroblast growth factor 21 and changes in BAT gene expression
consistent with heat production through increased peroxisomal lipid oxidation.
Other molecular adaptations predict additional cellular inefficiencies with an
increase in both protein synthesis and turnover, and mitochondria with reduced
reliance on mitochondrial-encoded gene expression and increased expression of
nuclear-encoded mitochondrial genes. These data suggest that BAd-CRISPR is an
efficient tool to speed discoveries in adipose tissue biology.




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