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Can Electronegative LDL Act as a Multienzymatic Complex? | LitMetric

AI Article Synopsis

  • * It shows pro-atherogenic traits like inflammation and aggregation, but also possesses enzymatic properties that help break down certain lipids, suggesting a complex role in cholesterol management.
  • * The review proposes that LDL(-) may function as a multi-enzymatic complex, where different enzymatic activities could work together through structural changes in its protein, apoB-100, to influence its effects on cardiovascular health.

Article Abstract

Electronegative LDL (LDL(-)) is a minor form of LDL present in blood for which proportions are increased in pathologies with increased cardiovascular risk. In vitro studies have shown that LDL(-) presents pro-atherogenic properties, including a high susceptibility to aggregation, the ability to induce inflammation and apoptosis, and increased binding to arterial proteoglycans; however, it also shows some anti-atherogenic properties, which suggest a role in controlling the atherosclerotic process. One of the distinctive features of LDL(-) is that it has enzymatic activities with the ability to degrade different lipids. For example, LDL(-) transports platelet-activating factor acetylhydrolase (PAF-AH), which degrades oxidized phospholipids. In addition, two other enzymatic activities are exhibited by LDL(-). The first is type C phospholipase activity, which degrades both lysophosphatidylcholine (LysoPLC-like activity) and sphingomyelin (SMase-like activity). The second is ceramidase activity (CDase-like). Based on the complementarity of the products and substrates of these different activities, this review speculates on the possibility that LDL(-) may act as a sort of multienzymatic complex in which these enzymatic activities exert a concerted action. We hypothesize that LysoPLC/SMase and CDase activities could be generated by conformational changes in apoB-100 and that both activities occur in proximity to PAF-AH, making it feasible to discern a coordinated action among them.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10138509PMC
http://dx.doi.org/10.3390/ijms24087074DOI Listing

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