Defective Lipid Droplet-Lysosome Interaction Causes Fatty Liver Disease as Evidenced by Human Mutations in TMEM199 and CCDC115

Lars E Larsen; Marjolein A W van den Boogert; Wilson A Rios-Ocampo; Jos C Jansen; Donna Conlon; Patrick L E Chong; J Han M Levels; Roos E Eilers; Vinay V Sachdev; Noam Zelcer; Tobias Raabe; Miao He; Nicholas J Hand; Joost P H Drenth; David J Rader; Eric S G Stroes; Dirk J Lefeber; Johan W Jonker; Adriaan G Holleboom

doi:10.1016/j.jcmgh.2021.09.013

Defective Lipid Droplet-Lysosome Interaction Causes Fatty Liver Disease as Evidenced by Human Mutations in TMEM199 and CCDC115

Cell Mol Gastroenterol Hepatol. 2022;13(2):583-597. doi: 10.1016/j.jcmgh.2021.09.013. Epub 2021 Oct 7.

Authors

Lars E Larsen¹, Marjolein A W van den Boogert², Wilson A Rios-Ocampo³, Jos C Jansen⁴, Donna Conlon⁵, Patrick L E Chong², J Han M Levels², Roos E Eilers³, Vinay V Sachdev⁶, Noam Zelcer⁶, Tobias Raabe⁵, Miao He⁷, Nicholas J Hand⁸, Joost P H Drenth⁴, David J Rader⁹, Eric S G Stroes², Dirk J Lefeber¹⁰, Johan W Jonker³, Adriaan G Holleboom¹¹

Affiliations

¹ Department of Vascular Medicine, Amsterdam UMC, location AMC, Amsterdam, The Netherlands; Department of Pediatrics, Section Molecular Metabolism and Nutrition, University Medical Center Groningen, University of Groningen, The Netherlands.
² Department of Vascular Medicine, Amsterdam UMC, location AMC, Amsterdam, The Netherlands.
³ Department of Pediatrics, Section Molecular Metabolism and Nutrition, University Medical Center Groningen, University of Groningen, The Netherlands.
⁴ Department of Gastroenterology and Hepatology, Radboud University Medical Center, Nijmegen, The Netherlands.
⁵ Department of Medicine, Perelman School of Medicine at the University of Pennsylvania, Philadelphia, Pennsylvania.
⁶ Department of Medical Biochemistry, Amsterdam University Medical Centers, location AMC, Amsterdam, The Netherlands.
⁷ Department of Pathology and Laboratory Medicine, Perelman School of Medicine at the University of Pennsylvania, Philadelphia, Pennsylvania; Division of Laboratory Medicine, The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania.
⁸ Department of Genetics, Perelman School of Medicine at the University of Pennsylvania, Philadelphia, Pennsylvania.
⁹ Department of Medicine, Perelman School of Medicine at the University of Pennsylvania, Philadelphia, Pennsylvania; Division of Laboratory Medicine, The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania.
¹⁰ Department of Laboratory Medicine, Translational Metabolic Laboratory, Radboud University Medical Center, Nijmegen, The Netherlands.
¹¹ Department of Vascular Medicine, Amsterdam UMC, location AMC, Amsterdam, The Netherlands. Electronic address: a.g.holleboom@amsterdamumc.nl.

Abstract

Background & aims: Recently, novel inborn errors of metabolism were identified because of mutations in V-ATPase assembly factors TMEM199 and CCDC115. Patients are characterized by generalized protein glycosylation defects, hypercholesterolemia, and fatty liver disease. Here, we set out to characterize the lipid and fatty liver phenotype in human plasma, cell models, and a mouse model.

Methods and results: Patients with TMEM199 and CCDC115 mutations displayed hyperlipidemia, characterized by increased levels of lipoproteins in the very low density lipoprotein range. HepG2 hepatoma cells, in which the expression of TMEM199 and CCDC115 was silenced, and induced pluripotent stem cell (iPSC)-derived hepatocyte-like cells from patients with TMEM199 mutations showed markedly increased secretion of apolipoprotein B (apoB) compared with controls. A mouse model for TMEM199 deficiency with a CRISPR/Cas9-mediated knock-in of the human A7E mutation had marked hepatic steatosis on chow diet. Plasma N-glycans were hypogalactosylated, consistent with the patient phenotype, but no clear plasma lipid abnormalities were observed in the mouse model. In the siTMEM199 and siCCDC115 HepG2 hepatocyte models, increased numbers and size of lipid droplets were observed, including abnormally large lipid droplets, which colocalized with lysosomes. Excessive de novo lipogenesis, failing oxidative capacity, and elevated lipid uptake were not observed. Further investigation of lysosomal function revealed impaired acidification combined with impaired autophagic capacity.

Conclusions: Our data suggest that the hypercholesterolemia in TMEM199 and CCDC115 deficiency is due to increased secretion of apoB-containing particles. This may in turn be secondary to the hepatic steatosis observed in these patients as well as in the mouse model. Mechanistically, we observed impaired lysosomal function characterized by reduced acidification, autophagy, and increased lysosomal lipid accumulation. These findings could explain the hepatic steatosis seen in patients and highlight the importance of lipophagy in fatty liver disease. Because this pathway remains understudied and its regulation is largely untargeted, further exploration of this pathway may offer novel strategies for therapeutic interventions to reduce lipotoxicity in fatty liver disease.

Keywords: Fatty liver disease; Hyperlipidemia; Lipid droplet; Lipophagy; Mutations in TMEM199 and in CCDC115; NAFLD; V-ATPase assembly defects.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Fatty Liver* / genetics
Fatty Liver* / metabolism
Hepatocytes / metabolism
Humans
Lipid Droplets* / metabolism
Lysosomes / metabolism
Membrane Proteins / genetics
Membrane Proteins / metabolism
Mice
Mutation / genetics
Nerve Tissue Proteins / genetics

Substances

Ccdc115 protein, human
Membrane Proteins
Nerve Tissue Proteins
TMEM199 protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding