Altres ajuts: NIH/HL-072925
Altres ajuts: NIH/CA-117990
Altres ajuts: MSPS/PI05/1723
The biogenesis of lipid droplets (LD) induced by serum depends on group IVA phospholipase A2 (cPLA2α). This work dissects the pathway leading to cPLA2α activation and LD biogenesis. Both processes were Ca2+-independent, as they took place after pharmacological blockade of Ca2+ transients elicited by serum or chelation with 1,2-bis(2-aminophenoxy)ethane-N,N,N',N'-tetraacetic acid tetrakis(acetoxymethyl ester). The single mutation D43N in cPLA2α, which abrogates its Ca2+ binding capacity and translocation to membranes, did not affect enzyme activation and formation of LD. In contrast, the mutation S505A did not affect membrane relocation of the enzyme in response to Ca2+ but prevented its phosphorylation, activation, and the appearance of LD. Expression of specific activators of different mitogen-activated protein kinases showed that phosphorylation of cPLA2α at Ser-505 is due to JNK. This was confirmed by pharmacological inhibition and expression of a dominant-negative form of the upstream activator MEKK1. LD biogenesis was accompanied by increased synthesis of ceramide 1-phosphate. Overexpression of its synthesizing enzyme ceramide kinase increased phosphorylation of cPLA2α at Ser-505 and formation of LD, and its down-regulation blocked the phosphorylation of cPLA2α and LD biogenesis. These results demonstrate that LD biogenesis induced by serum is regulated by JNK and ceramide kinase.
Article
English
Acetoxymethyl esters; Binding capacities; Ceramide 1-phosphate; Ceramides; Down-regulation; Enzyme activation; Lipid droplets; Mitogen activated protein kinase; Over-expression; Pharmacological blockade; Pharmacological inhibition; Phospholipase A; Single mutation; Tetraacetic acid; Tetrakis
Ministerio de Educación y Ciencia SAF2004-01698
Ministerio de Educación y Ciencia SAF2007-60055
Ministerio de Ciencia e Innovación BFU2009-07823
Journal of biological chemistry ; Vol. 284, Num. 47 (2009), p. 32359-32369
open access
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