Apolipoprotein modulation of streptococcal serum opacity factor activity against human plasma high-density lipoproteins. Academic Article uri icon

Overview

abstract

  • Human plasma HDL are the target of streptococcal serum opacity factor (SOF), a virulence factor that clouds human plasma. Recombinant (r) SOF transfers cholesteryl esters (CE) from approximately 400,000 HDL particles to a CE-rich microemulsion (CERM), forms a cholesterol-poor HDL-like particle (neo HDL), and releases lipid-free (LF) apo A-I. Whereas the rSOF reaction requires labile apo A-I, the modulation effects of other apos are not known. We compared the products and rates of the rSOF reaction against human HDL and HDL from mice overexpressing apos A-I and A-II. Kinetic studies showed that the reactivity of various HDL species is apo-specific. LpA-I reacts faster than LpA-I/A-II. Adding apos A-I and A-II inhibited the SOF reaction, an effect that was more profound for apo A-II. The rate of SOF-mediated CERM formation was slower against HDL from mice expressing human apos A-I and A-II than against WT mice HDL and slowest against HDL from apo A-II overexpressing mice. The lower reactivity of SOF against HDL containing human apos is due to the higher hydropathy of human apo A-I, particularly its C-terminus relative to mouse apo A-I, and the higher lipophilicity of human apo A-II. The SOF-catalyzed reaction is the first to target HDL rather than its transporters and receptors in a way that enhances reverse cholesterol transport (RCT). Thus, effects of apos on the SOF reaction are highly relevant. Our studies show that the "humanized" apo A-I-expressing mouse is a good animal model for studies of rSOF effects on RCT in vivo.

publication date

  • August 25, 2009

Research

keywords

  • Apolipoprotein A-I
  • Apolipoprotein A-II
  • Lipoproteins, HDL
  • Peptide Hydrolases
  • Streptococcus pyogenes

Identity

PubMed Central ID

  • PMC3236702

Scopus Document Identifier

  • 69049092124

Digital Object Identifier (DOI)

  • 10.1021/bi901087z

PubMed ID

  • 19618959

Additional Document Info

volume

  • 48

issue

  • 33