AI Article Synopsis

  • - The study found that progesterone, U18666A, and the phospholipase inhibitor MAFP significantly reduced HIV production (70%-90%) in specific immune cells known as THP-1 monocytes and macrophages, while also impacting macropinocytosis and lipid balance in the cells.
  • - In the experiments, MAFP, U18666A, and progesterone increased the amount of a specific lipid (BMP) in the cells, with MAFP showing the ability to inhibit BMP breakdown by an enzyme (PLRP2).
  • - The results suggest that the accumulation of BMP due to these compounds may prevent the formation and uptake of HIV particles, indicating that BMP levels might be useful as a biomarker

Article Abstract

Progesterone, the cationic amphiphile U18666A and a phospholipase inhibitor (Methyl Arachidonyl Fluoro Phosphonate, MAFP) inhibited by 70%-90% HIV production in viral reservoir cells, i.e. human THP-1 monocytes and monocyte-derived macrophages (MDM). These compounds triggered an inhibition of fluid phase endocytosis (macropinocytosis) and modified cellular lipid homeostasis since endosomes accumulated filipin-stained sterols and Bis(Monoacylglycero)Phosphate (BMP). BMP was quantified using a new cytometry procedure and was increased by 1.25 times with MAFP, 1.7 times with U18666A and 2.5 times with progesterone. MAFP but not progesterone or U18666A inhibited the hydrolysis of BMP by the Pancreatic Lipase Related Protein 2 (PLRP2) as shown by in-vitro experiments. The possible role of sterol transporters in steroid-mediated BMP increase is discussed. Electron microscopy showed the accumulation of viral particles either into large intracellular viral-containing compartments or outside the cells, indicating that endosomal accumulation of BMP could block intracellular biogenesis of viral particles while inhibition of macropinocytosis would prevent viral particle uptake. This is the first report linking BMP metabolism with a natural steroid such as progesterone or with involvement of a phospholipase A1 activity. BMP cellular content could be used as a biomarker for efficient anti-viral drugs.

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Source
http://dx.doi.org/10.1016/j.biochi.2013.05.019DOI Listing

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