4.7 Article

Metabolism of ApoA-I as lipid-free protein or as component of discoidal and spherical reconstituted HDLs studies in wild-type and hepatic lipase transgenic rabbits

Journal

ARTERIOSCLEROSIS THROMBOSIS AND VASCULAR BIOLOGY
Volume 22, Issue 11, Pages 1912-1917

Publisher

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1161/01.ATV.0000038485.94020.7F

Keywords

apolipoprotein A-I; hepatic lipase; high density lipoproteins; metabolism; rabbits

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Objective-Apolipoprotein (apo)A-I exists in 3 forms in plasma: as lipid-free apoA-I, as a component of pre-beta-migrating, discoidal high density lipoproteins (HDLs), and as a component of alpha-migrating sphcriclal HDLs. This study investigates (1) the in vivo metabolism of apoA-I in each of these forms, and (2) the effects of hepatic lipase (HL) on apoA-I metabolism. Methods and Results-Wild-type and HL transgenic rabbits were studied. When lipid-free I-125-apoA-I and I-125-apoA-I in pre-beta-migrating discoidal reconstituted HDLs (rHDLs) were injected into wild-type rabbits, the label rapidly appeared in a-migrating particles and decayed with the same fractional catabolic rate (FCR) as when they were injected Lis a component of spherical rHDLs. Spherical rHDLs did not change in size when they were injected into wild-type rabbits but were reduced in size in HL transgenic rabbits. The FCR of apoA-I in HL transgenic rabbits was double that in wild-type rabbits. Conclusions-In vivo, (1) lipid-ftee apoA-I rapidly incorporates into preexisting alpha-migrating particles, (2) pre-beta-migrating discoidal HDLs are rapidly converted into a-migrating HDLs, (3) the FCR of apoA-I is independent of the form in which it is introduced into plasma, and (4) HL reduces the size of alpha-migrating HDLs and increases the rate of catabolism of apoA-I.

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