Selective delipidation of plasma HDL enhances reverse cholesterol transport in vivo.

نویسندگان

  • Frank M Sacks
  • Lawrence L Rudel
  • Adam Conner
  • Hassibullah Akeefe
  • Gerhard Kostner
  • Talal Baki
  • George Rothblat
  • Margarita de la Llera-Moya
  • Bela Asztalos
  • Timothy Perlman
  • Chunyu Zheng
  • Petar Alaupovic
  • Jo-Ann B Maltais
  • H Bryan Brewer
چکیده

Uptake of cholesterol from peripheral cells by nascent small HDL circulating in plasma is necessary to prevent atherosclerosis. This process, termed reverse cholesterol transport, produces larger cholesterol-rich HDL that transfers its cholesterol to the liver facilitating excretion. Most HDL in plasma is cholesterol-rich. We demonstrate that treating plasma with a novel selective delipidation procedure converts large to small HDL [HDL-selectively delipidated (HDL-sdl)]. HDL-sdl contains several cholesterol-depleted species resembling small alpha, prebeta-1, and other prebeta forms. Selective delipidation markedly increases efficacy of plasma to stimulate ABCA1-mediated cholesterol transfer from monocytic cells to HDL. Plasma from African Green monkeys underwent selective HDL delipidation. The delipidated plasma was reinfused into five monkeys. Prebeta-1-like HDL had a plasma residence time of 8 +/- 6 h and was converted entirely to large alpha-HDL having residence times of 13-14 h. Small alpha-HDL was converted entirely to large alpha-HDL. These findings suggest that selective HDL delipidation activates reverse cholesterol transport, in vivo and in vitro. Treatment with delipidated plasma tended to reduce diet-induced aortic atherosclerosis in monkeys measured by intravascular ultrasound. These findings link the conversion of small to large HDL, in vivo, to improvement in atherosclerosis.

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عنوان ژورنال:
  • Journal of lipid research

دوره 50 5  شماره 

صفحات  -

تاریخ انتشار 2009