4.6 Article

Carboxylesterase 2 proteins are efficient diglyceride and monoglyceride lipases possibly implicated in metabolic disease

Journal

JOURNAL OF LIPID RESEARCH
Volume 62, Issue -, Pages -

Publisher

ELSEVIER
DOI: 10.1016/j.jlr.2021.100075

Keywords

carboxylesterase 2; lipolytic activity; triglycerides; diglycerides; monoglycerides; liver; small intestine; colon; NAFLD; colitis

Funding

  1. Austrian Science Fund, Austria (FWF) [SFB F73, P29253B28, P28882-B21, P31638-B34]
  2. DK MCD Metabolic and cardiovascular diseases [W 1226]
  3. docfund Molecular Metabolism [DOC 50]
  4. 'Land Steiermark'
  5. City of Graz
  6. DOC fellowship - Austrian Academy of Science, Austria (OeAW) [25049]
  7. Austrian Science Fund (FWF) [P28882, P31638] Funding Source: Austrian Science Fund (FWF)

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Research showed that CES2/Ces2 members are highly efficient DG and MG hydrolases, potentially playing an important role in liver and gut lipid signaling. In addition to TG hydrolysis, Ces2a, Ces2b, and Ces2e exhibited significant enzymatic activities towards DGs and MGs.
Carboxylesterase 2 (CES2/Ces2) proteins exert established roles in (pro)drug metabolism. Recently, human and murine CES2/Ces2c have been discovered as triglyceride (TG) hydrolases implicated in the development of obesity and fatty liver disease. The murine Ces2 family consists of seven homologous genes as opposed to a single CES2 gene in humans. However, the mechanistic role of Ces2 protein family members is not completely understood. In this study, we examined activities of all Ces2 members toward TGs, diglycerides (DGs), and monoglycerides (MGs) as the substrate. Besides CES2/Ces2c, we measured significant TG hydrolytic activities for Ces2a, Ces2b, and Ces2e. Notably, these Ces2 members and CES2 efficiently hydrolyzed DGs and MGs, and their activities even surpassed those measured for TG hydrolysis. The localization of CES2/Ces2c proteins at the ER may implicate a role of these lipases in lipid signaling pathways. We found divergent expression of Ces2 genes in the liver and intestine of mice on a high-fat diet, which could relate to changes in lipid signaling. Finally, we demonstrate reduced CES2 expression in the colon of patients with inflammatory bowel disease and a similar decline in Ces2 expression in the colon of a murine colitis model. Together, these results demonstrate that CES2/Ces2 members are highly efficient DG and MG hydrolases that may play an important role in liver and gut lipid signaling.

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