Richard M. Lawn scite author profile

Lipoprotein(a) is an LDL-like lipoprotein whose concentration in plasma is correlated with atherosclerosis. The characteristic protein component of lipoprotein(a) is apolipoprotein(a) which is disulphide-linked to apolipoprotein B-100. Sequencing of cloned human apolipoprotein(a) complementary DNA shows that it is very similar to human plasminogen. It contains a serine protease domain and two types of plasminogen-like kringle domains, one of which is present in 37 copies.

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Structure of human factor VIII

Vehar¹,

Keyt²,

Eaton³

et al. 1984

Nature

875

602

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The deduced amino acid sequence of human factor VIII, obtained from the DNA sequence, predicts a mature polypeptide of 2,332 amino acids containing a triplicated domain structure. The polypeptide has 35% sequence homology with the copper-binding plasma protein, ceruloplasmin. Determination of the thrombin cleavage sites in plasma-derived factor VIII polypeptides allows prediction of the domains involved in the associated activation and inactivation of the protein.

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The Tangier disease gene product ABC1 controls the cellular apolipoprotein-mediated lipid removal pathway

Lawn¹,

Wade²,

Garvin³

et al. 1999

J. Clin. Invest.

695

486

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Characterization of the human factor VIII gene

Gitschier¹,

Wood²,

Goralka³

et al. 1984

Nature

919

432

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ABCA1 Is the cAMP-inducible Apolipoprotein Receptor That Mediates Cholesterol Secretion from Macrophages

Oram¹,

Lawn²,

Garvin³

et al. 2000

Journal of Biological Chemistry

506

426

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Lipid-poor high density lipoprotein apolipoproteins remove cholesterol and phospholipids from cells by an active secretory pathway controlled by an ABC transporter called ABCA1. This pathway is induced by cholesterol and cAMP analogs in a cell-specific manner. Here we provide evidence that increased plasma membrane ABCA1 accounts for the enhanced apolipoprotein-mediated lipid secretion from macrophages induced by cAMP analogs. Treatment of RAW264 macrophages with 8-bromo-cAMP caused parallel increases in apoA-I-mediated cholesterol efflux, ABCA1 mRNA and protein levels, incorporation of ABCA1 into the plasma membrane, and binding of apoA-I to cellsurface ABCA1. All of these parameters declined to near base-line values within 6 h after removal of 8-bromocAMP, indicating that ABCA1 is highly unstable and is degraded rapidly in the absence of inducer. Thus, ABCA1 is likely to be the cAMP-inducible apolipoprotein receptor that promotes removal of cholesterol and phospholipids from macrophages.

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Richard M. Lawn

cDNA sequence of human apolipoprotein(a) is homologous to plasminogen

Structure of human factor VIII

The Tangier disease gene product ABC1 controls the cellular apolipoprotein-mediated lipid removal pathway

Characterization of the human factor VIII gene

ABCA1 Is the cAMP-inducible Apolipoprotein Receptor That Mediates Cholesterol Secretion from Macrophages

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