AI Article Synopsis

  • Mammalian genomes contain over 30 types of phospholipase A₂ (PLA₂) enzymes, classified into various categories like secreted, cytosolic, and lysosomal PLA₂s, with the cPLA₂, iPLA₂, and sPLA₂ families being the most significant.
  • The cPLA₂ family is crucial for arachidonic acid metabolism, while iPLA₂ supports membrane stability and energy processes, and sPLA₂ influences biological functions by changing the environment of extracellular phospholipids.
  • Recent research using knockout and transgenic mice has shed light on the roles of PLA₂s in diseases and health, revealing their significance in various biological processes.

Article Abstract

Mammalian genomes encode genes for more than 30 phospholipase A₂s (PLA₂s) or related enzymes, which are subdivided into several classes including low-molecular-weight secreted PLA₂s (sPLA₂s), Ca²+-dependent cytosolic PLA₂s (cPLA₂s), Ca²+-independent PLA₂s (iPLA₂s), platelet-activating factor acetylhydrolases (PAF-AHs), lysosomal PLA₂s, and a recently identified adipose-specific PLA. Of these, the intracellular cPLA₂ and iPLA₂ families and the extracellular sPLA₂ family are recognized as the "big three". From a general viewpoint, cPLA₂α (the prototypic cPLA₂ plays a major role in the initiation of arachidonic acid metabolism, the iPLA₂ family contributes to membrane homeostasis and energy metabolism, and the sPLA₂ family affects various biological events by modulating the extracellular phospholipid milieus. The cPLA₂ family evolved along with eicosanoid receptors when vertebrates first appeared, whereas the diverse branching of the iPLA₂ and sPLA₂ families during earlier eukaryote development suggests that they play fundamental roles in life-related processes. During the past decade, data concerning the unexplored roles of various PLA₂ enzymes in pathophysiology have emerged on the basis of studies using knockout and transgenic mice, the use of specific inhibitors, and information obtained from analysis of human diseases caused by mutations in PLA₂ genes. This review focuses on current understanding of the emerging biological functions of PLA₂s and related enzymes.

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Source
http://dx.doi.org/10.1016/j.plipres.2010.12.001DOI Listing

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