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The Emerging Physiological Role of AGMO 10 Years after Its Gene Identification

期刊

LIFE-BASEL
卷 11, 期 2, 页码 -

出版社

MDPI
DOI: 10.3390/life11020088

关键词

AGMO; tetrahydrobiopterin; alkylglycerols; plasmalogens; neurodevelopment; autism; inflammation; macrophages; type 2 diabetes; energy homeostasis

资金

  1. National Bank of Austria [18001]
  2. Austrian Science Funds (FWF) [P-28769, P-30800]

向作者/读者索取更多资源

AGMO is the only known enzyme capable of catalyzing the breakdown of alkylglycerols and lyso-alkylglycerophospholipids, potentially contributing to various human pathologies. Its absence impacts lipid composition and may play a role in immunity, energy homeostasis, and development.
The gene encoding alkylglycerol monooxygenase (AGMO) was assigned 10 years ago. So far, AGMO is the only known enzyme capable of catalysing the breakdown of alkylglycerols and lyso-alkylglycerophospholipids. With the knowledge of the genetic information, it was possible to relate a potential contribution for mutations in the AGMO locus to human diseases by genome-wide association studies. A possible role for AGMO was implicated by genetic analyses in a variety of human pathologies such as type 2 diabetes, neurodevelopmental disorders, cancer, and immune defence. Deficient catabolism of stored lipids carrying an alkyl bond by an absence of AGMO was shown to impact on the overall lipid composition also outside the ether lipid pool. This review focuses on the current evidence of AGMO in human diseases and summarises experimental evidence for its role in immunity, energy homeostasis, and development in humans and several model organisms. With the progress in lipidomics platform and genetic identification of enzymes involved in ether lipid metabolism such as AGMO, it is now possible to study the consequence of gene ablation on the global lipid pool and further on certain signalling cascades in a variety of model organisms in more detail.

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