4.6 Article

Quantitative role of LAL, NPC2, and NPC1 in lysosomal cholesterol processing defined by genetic and pharmacological manipulations

期刊

JOURNAL OF LIPID RESEARCH
卷 52, 期 4, 页码 688-698

出版社

ELSEVIER
DOI: 10.1194/jlr.M013789

关键词

Niemann-Pick type C disease; Wolman disease; liver disease; neurodegeneration; macrophage; inflammation; cholesterol balance; lysosomal acid lipase

资金

  1. US Public Health Service [R01 HL009610]
  2. Moss Heart Fund
  3. Ara Parseghian Medical Research Foundation
  4. UT Southwestern, NIH [T32 GM007062-32]

向作者/读者索取更多资源

Lipoprotein cholesterol taken up by cells is processed in the endosomal/lysosomal (E/L) compartment by the sequential action of lysosomal acid lipase (LAL), Niemann-Pick C2 (NPC2), and Niemann-Pick C1 (NPC1). Inactivation of NPC2 in mouse caused sequestration of unesterified cholesterol (UC) and expanded the whole animal sterol pool from 2,305 to 4,337 mg/kg. However, this pool increased to 5,408 and 9,480 mg/kg, respectively, when NPC1 or LAL function was absent. The transport defect in mutants lacking NPC2 or NPC1, but not in those lacking LAL, was reversed by cyclodextrin (CD), and the ED50 values for this reversal varied from similar to 40 mg/kg in kidney to >20,000 mg/kg in brain in both groups. This reversal occurred only with a CD that could interact with UC. Further, a CD that could interact with, but not solubilize, UC still overcame the transport defect.jlr These studies showed that processing and export of sterol from the late E/L compartment was quantitatively different in mice lacking LAL, NPC2, or NPC1 function. In both npc2(-/-) and npc1(-/-) mice, the transport defect was reversed by a CD that interacted with UC, likely at the membrane/bulk-water interface, allowing sterol to move rapidly to the export site of the E/L compartment.-Ramirez, C. M., B. Liu, A. Aqul, A. M. Taylor, J. J. Repa, S. D. Turley, and J. M. Dietschy. Quantitative role of LAL, NPC2, and NPC1 in lysosomal cholesterol processing defined by genetic and pharmacological manipulations. J. Lipid Res. 2011. 52: 688-698.

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