Lysosomal acid lipase regulates VLDL synthesis and insulin sensitivity in mice

Radović, Branislav; Vujić, Nemanja; Leopold, Christina; Schlager, Stefanie; Goeritzer, Madeleine; Patankar, Jay V.; Korbelius, Melanie; Kolb, Dagmar; Reindl, Julia; Wegscheider, Martin; Tomin, Tamara; Birner‐Gruenberger, Ruth; Schittmayer, Matthias; Groschner, Lukas N.; Magnes, Christoph; Frank, Saša; Steyrer, Ernst; Du, Hong; Graier, Wolfgang F.; Madl, Tobias; Kratky, Dagmar

doi:10.1007/s00125-016-3968-6

Cited by 38 publications

(77 citation statements)

References 40 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Within enterocytes, cLD catabolism can also be conducted by lysosomal lipolysis. Because LAL affects VLDL synthesis in the liver (Radović et al, 2016), lysosomal acid lipase (LAL) might be a potential candidate for supplying lipid precursors for CM synthesis, rather than ATGL and CGI-58.…”

Section: Discussionmentioning

confidence: 99%

ATGL/CGI-58-Dependent Hydrolysis of a Lipid Storage Pool in Murine Enterocytes

et al. 2019

Self Cite

View full text Add to dashboard Cite

Summary As circulating lipid levels are balanced by the rate of lipoprotein release and clearance from the plasma, lipid absorption in the small intestine critically contributes to the maintenance of whole-body lipid homeostasis. Within enterocytes, excessive triglycerides are transiently stored as cytosolic lipid droplets (cLDs), and their mobilization sustains lipid supply during interprandial periods. Using mice lacking adipose triglyceride lipase (ATGL) and its coactivator comparative gene identification-58 (CGI-58) exclusively in the intestine (intestine-specific double KO [iDKO]), we show that ATGL/CGI-58 are not involved in providing substrates for chylomicron synthesis. Massive intestinal cLD accumulation in iDKO mice independent of dietary lipids together with inefficient lipid incorporation into cLDs in the early absorption phase demonstrate the existence of a secretion/re-uptake cycle, corroborating the availability of two diverse cLD pools. This study identified ATGL/CGI-58 as critical players in the catabolism of basolaterally (blood) derived lipids and highlights the necessity to modify the current model of intestinal lipid metabolism.

show abstract

Section: Discussionmentioning

confidence: 99%

ATGL/CGI-58-Dependent Hydrolysis of a Lipid Storage Pool in Murine Enterocytes

et al. 2019

Self Cite

View full text Add to dashboard Cite

show abstract

“…500 μl of NMR buffer in D 2 O were added to the dried samples, redissolved, and transferred to 5-mm NMR tubes. Metabolites were measured as described previously (95, 96) and detailed below. All NMR experiments were performed at 310 K on a Bruker Avance III 500-MHz spectrometer equipped with a TXI probe head.…”

Section: Methodsmentioning

confidence: 99%

Acetyl-CoA carboxylase 1–dependent lipogenesis promotes autophagy downstream of AMPK

Gross

Zimmermann

Pendl

et al. 2019

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

Autophagy, a membrane-dependent catabolic process, ensures survival of aging cells and depends on the cellular energetic status. Acetyl-CoA carboxylase 1 (Acc1) connects central energy metabolism to lipid biosynthesis and is rate-limiting for the de novo synthesis of lipids. However, it is unclear how de novo lipogenesis and its metabolic consequences affect autophagic activity. Here, we show that in aging yeast, autophagy levels highly depend on the activity of Acc1. Constitutively active Acc1 ( acc1 S/A ) or a deletion of the Acc1 negative regulator, Snf1 (yeast AMPK), shows elevated autophagy levels, which can be reversed by the Acc1 inhibitor soraphen A. Vice versa, pharmacological inhibition of Acc1 drastically reduces cell survival and results in the accumulation of Atg8-positive structures at the vacuolar membrane, suggesting late defects in the autophagic cascade. As expected, acc1 S/A cells exhibit a reduction in acetate/acetyl-CoA availability along with elevated cellular lipid content. However, concomitant administration of acetate fails to fully revert the increase in autophagy exerted by acc1 S/A . Instead, administration of oleate, while mimicking constitutively active Acc1 in WT cells, alleviates the vacuolar fusion defects induced by Acc1 inhibition. Our results argue for a largely lipid-dependent process of autophagy regulation downstream of Acc1. We present a versatile genetic model to investigate the complex relationship between acetate metabolism, lipid homeostasis, and autophagy and propose Acc1-dependent lipogenesis as a fundamental metabolic path downstream of Snf1 to maintain autophagy and survival during cellular aging.

show abstract

“…Lal -/mice present with a massive accumulation of TG and CE in the liver, the spleen, the small intestine and the adrenals, which is associated to the loss of white (WAT) and brown adipose tissues (BAT) [30]. Despite the appearance of hepatic foamy lysosomes, lal -/mice show an improved insulin sensitivity and glucose metabolism [31], paralleled by a shift of lipid storage from hepatocytes to Kupffer cells over time [30]. This profile mirrors the observations in hepatic biopsies of LAL deficient patients (discussed below) [11].…”

Section: Expression and Role Of Lal In Cell Lipid Metabolismmentioning

confidence: 99%

Lysosomal Acid Lipase: From Cellular Lipid Handler to Immunometabolic Target

Gomaraschi

Bonacina

Norata

2019

Trends in Pharmacological Sciences

View full text Add to dashboard Cite

Lysosomal acid lipase (LAL) hydrolyzes cholesterol esters and triglycerides to free cholesterol and fatty acids,that are then used for the metabolic purposes in the cell. The process also occurs in immune cells which adapt their metabolic machinery to cope with the different energetic requirements associated to cell activation, proliferation and/or polarization. Deficiency of LAL not only causes severe lipid accumulation, but also impacts the immunometabolic signature in animal models. In humans, LAL deficiency has been recently associated with a peculiar clinical immune phenotype, secondary hemophagocytic lymphohistiocytosis. These observations indicate that LAL represents a critical player for cellular immunometabolic modulation and the availability of an effective enzyme replacement strategy makes LAL an attractive target to rewire the immunometabolic machinery of immune cells beyond its role in controlling cellular lipid metabolism.

show abstract

Lysosomal acid lipase regulates VLDL synthesis and insulin sensitivity in mice

Cited by 38 publications

References 40 publications

ATGL/CGI-58-Dependent Hydrolysis of a Lipid Storage Pool in Murine Enterocytes

ATGL/CGI-58-Dependent Hydrolysis of a Lipid Storage Pool in Murine Enterocytes

Acetyl-CoA carboxylase 1–dependent lipogenesis promotes autophagy downstream of AMPK

Lysosomal Acid Lipase: From Cellular Lipid Handler to Immunometabolic Target

Contact Info

Product

Resources

About