Project description:Rhodocollybia butyracea AH 40177 - Standard Draft genome sequencing

Project description:Rhodocollybia butyracea overview

Project description:Rhodocollybia butyracea CCBAS 279 Transcriptome - RHO

Project description:Rhodocollybia butyracea CCBAS 279 Standard Draft genome sequencing

Project description:Cyathus striatus AH 40144 - Transcriptome

Project description:Agrocybe pediades AH 40210 Transcriptome

Project description:Gymnopilus junonius AH 44721 Transcriptome

Project description:Pholiota alnicola AH 47727 Transcriptome

Project description:Flavobacterium covae strain:AH-01 | isolate:AH-01 Genome sequencing and assembly

Project description:Objective: Alcoholic hepatitis (AH) is characterized by the expansion of ductular reaction (DR) cells and expression of liver progenitor cell (LPC) markers. The aim of this study was to identify the gene expression profile and associated genes of DR cells and to evaluate its weight in alcoholic disease progression. Design: KRT7+, KRT7- and total liver fractions were laser microdissected from liver biopsies (n=6) of patients with AH and whole transcriptome was sequenced. Gene signature was assessed in transcriptomic data from 41 patients with alcoholic liver disease. Pro-inflammatory profile was evaluated in tissue and serum samples and in human LPC organoids. Results: Transcriptome analysis of KRT7+ DR cells uncovered intrinsic gene pathways of DR and allowed identifying genes associated with DR expressed in AH. In addition, DR gene signature and associated genes correlated with disease progression and poor outcome in AH patients. Importantly, DR presented a pro-inflammatory profile with expression of CXC and CCL chemokines and was associated with infiltrating neutrophils. Moreover, LPC markers correlated with liver expression and circulating levels of inflammatory mediators. In vitro, human LPC organoids mimicked ductular reaction gene expression profile and produced chemokines. Moreover, LPC promoted neutrophil migration and enhanced their inflammatory profile. Conclusions: Here we report for the first time the gene expression signature of DR in AH and its association with disease progression. Functional and experimental analysis demonstrates that DR cells have a pro-inflammatory profile, and suggest their involvement in neutrophil recruitment and liver inflammatory response.