A new era of secreted phospholipase A2

Makoto Murakami(Japan Science and Technology Agency), Hiroyasu Sato(Tokyo Metropolitan Institute of Medical Science), Yoshimi Miki(Tokyo Metropolitan Institute of Medical Science), Kei Yamamoto(Tokyo Metropolitan Institute of Medical Science), Yoshitaka Taketomi(Tokyo Metropolitan Institute of Medical Science)
Journal of Lipid Research
March 25, 2015
Cited by 222Open Access
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Abstract

Among more than 30 members of the phospholipase A2 (PLA2) superfamily, secreted PLA2 (sPLA2) enzymes represent the largest family, being Ca(2+)-dependent low-molecular-weight enzymes with a His-Asp catalytic dyad. Individual sPLA2s exhibit unique tissue and cellular distributions and enzymatic properties, suggesting their distinct biological roles. Recent studies using transgenic and knockout mice for nearly a full set of sPLA2 subtypes, in combination with sophisticated lipidomics as well as biochemical and cell biological studies, have revealed distinct contributions of individual sPLA2s to various pathophysiological events, including production of pro- and anti-inflammatory lipid mediators, regulation of membrane remodeling, degradation of foreign phospholipids in microbes or food, or modification of extracellular noncellular lipid components. In this review, we highlight the current understanding of the in vivo functions of sPLA2s and the underlying lipid pathways as revealed by a series of studies over the last decade.


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