Journal of Lipid Research (Feb 2008)

Biogenesis of HDL by SAA is dependent on ABCA1 in the liver in vivos⃞

  • Wei Hu,
  • Sumiko Abe-Dohmae,
  • Maki Tsujita,
  • Noriyuki Iwamoto,
  • Osamu Ogikubo,
  • Takanobu Otsuka,
  • Yositaka Kumon,
  • Shinji Yokoyama

Journal volume & issue
Vol. 49, no. 2
pp. 386 – 393

Abstract

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Serum amyloid A (SAA) was markedly increased in the plasma and in the liver upon acute inflammation induced by intraperitoneal injection of lipopolysaccharide (LPS) in mice, and SAA in the plasma was exclusively associated with HDL. In contrast, no HDL was present in the plasma and only a small amount of SAA was found in the VLDL/LDL fraction (d 1.21 g/ml. The behavior of apolipoprotein A-I (apoA-I) was the same as that of SAA in HDL biogenesis by WT and ABCA1-KO mouse hepatocytes. Lipid-free SAA and apoA-I both stabilized ABCA1 and caused cellular lipid release in WT mouse-derived fibroblasts, but not in ABCA1-KO mouse-derived fibroblasts, in vitro when added exogenously. We conclude that both SAA and apoA-I generate HDL largely in hepatocytes only in the presence of ABCA1, likely being secreted in a lipid-free form to interact with cellular ABCA1. In the absence of ABCA1, nonlipidated SAA is seemingly removed rapidly from the extracellular space.

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