Transcriptional profiling of pediatric cholestatic livers identifies three distinct macrophage populations.

Sarah A TaylorShang-Yang ChenGaurav GadhviLiang FengKyle D GromerHiam Abdala-ValenciaKiwon NamSalina T DominguezAnna B MontgomeryPaul A ReyfmanLorena OstillaJoshua B WechslerCarla M CudaRichard M GreenHarris PerlmanDeborah R Winter

Published in: PloS one (2021)

We are the first to perform single-cell RNA sequencing on human pediatric cholestatic liver and identified three macrophage subsets with distinct transcriptional signatures from healthy liver macrophages. Further analyses will identify similarities and differences in these macrophage sub-populations across etiologies of cholestatic liver disease. Taken together, these findings may allow for future development of targeted therapeutic strategies to reprogram macrophages to an immune regulatory phenotype and reduce cholestatic liver injury.

Keyphrases

liver injury
drug induced
single cell
rna seq
transcription factor
adipose tissue
gene expression
endothelial cells
genome wide
high throughput
peripheral blood
genetic diversity
heat shock
pluripotent stem cells
oxidative stress
drug delivery
young adults
childhood cancer