Background Autophagy is critical for cellular homeostasis.Autophagy related 14(ATG14)is a key regulator of autophagy initiation;however,its role in hepatocyte survival remains poorly understood.This study aimed to inv...Background Autophagy is critical for cellular homeostasis.Autophagy related 14(ATG14)is a key regulator of autophagy initiation;however,its role in hepatocyte survival remains poorly understood.This study aimed to investigate the hepatocyte-specific function of ATG14 in vivo.Methods We generated Atg14 hepatocyte-specific knockout(HepKO)mice using adeno-associated virus to deliver thyroxine-binding globulin gene promoter-driven Cre into Atg14 floxed mice at an adult age and fed control and knockout mice with either normal chow or a Western diet.Blood and tissue samples were collected for biochemical and histological analyses.Results Atg14 HepKO mice develop severe hepatomegaly under normal dietary conditions.ATG14 deficiency leads to hepatic injury,inflammation and fibrosis.Multiple forms of cell death,including apoptosis and pyroptosis,increase significantly.When challenged with a Western diet for 4 weeks,Atg14 HepKO mice exhibit exacerbated hepatic injury,inflammation and fibrosis despite no significant lipid droplet accumulation in the liver.Transcriptomic analysis reveals upregulation of several cell death pathways,including pyroptosis,apoptosis and necroptosis.Further biochemical and microscopic analyses validate the induction of multiple cell death pathways.In addition,NLR family pyrin domain containing 3 inflammasome-mediated pyroptosis is significantly elevated in Atg14 HepKO mouse livers and ATG14-deficient hepatocytes.Conclusion Our data suggest that ATG14 is required for maintaining hepatocyte identity,survival and function and that hepatic ATG14 deficiency may lead to hepatomegaly,tissue injury,inflammation and fibrosis.展开更多
基金the National Institute of Diabetes and Digestive and Kidney Diseases(R01DK120689,R01DK121925,P30DK097512)the National Institute on Alcohol Abuse and Alcoholism(R01AA028506),the National Institute on Aging(R21AG072288)the National Cancer Institute(P30CA082709 and P30CA023168),the Walther Cancer Foundation and the Ricks Family Foundation.
文摘Background Autophagy is critical for cellular homeostasis.Autophagy related 14(ATG14)is a key regulator of autophagy initiation;however,its role in hepatocyte survival remains poorly understood.This study aimed to investigate the hepatocyte-specific function of ATG14 in vivo.Methods We generated Atg14 hepatocyte-specific knockout(HepKO)mice using adeno-associated virus to deliver thyroxine-binding globulin gene promoter-driven Cre into Atg14 floxed mice at an adult age and fed control and knockout mice with either normal chow or a Western diet.Blood and tissue samples were collected for biochemical and histological analyses.Results Atg14 HepKO mice develop severe hepatomegaly under normal dietary conditions.ATG14 deficiency leads to hepatic injury,inflammation and fibrosis.Multiple forms of cell death,including apoptosis and pyroptosis,increase significantly.When challenged with a Western diet for 4 weeks,Atg14 HepKO mice exhibit exacerbated hepatic injury,inflammation and fibrosis despite no significant lipid droplet accumulation in the liver.Transcriptomic analysis reveals upregulation of several cell death pathways,including pyroptosis,apoptosis and necroptosis.Further biochemical and microscopic analyses validate the induction of multiple cell death pathways.In addition,NLR family pyrin domain containing 3 inflammasome-mediated pyroptosis is significantly elevated in Atg14 HepKO mouse livers and ATG14-deficient hepatocytes.Conclusion Our data suggest that ATG14 is required for maintaining hepatocyte identity,survival and function and that hepatic ATG14 deficiency may lead to hepatomegaly,tissue injury,inflammation and fibrosis.
