Human Apolipoprotein B: Structure of Carboxyl-Terminal Domains, Sites of Gene Expression, and Chromosomal Localization

Timothy J. Knott, Stanley C. Rall(Gladstone Institutes), Thomas L. Innerarity(Gladstone Institutes), Shellie F. Jacobson(Gladstone Institutes), Mickey S. Urdea, Beatriz Levy-Wilson(Gladstone Institutes), Lyn M. Powell, Richard J. Pease, Roger Eddy(Roswell Park Comprehensive Cancer Center), Hiroshi Nakai(Roswell Park Comprehensive Cancer Center), Mary Shannon Byers(Roswell Park Comprehensive Cancer Center), L. Priestley, E. Graeme Robertson, Leslie B. Rall, Christer Betsholtz(Uppsala University Hospital), Thomas B. Shows(Roswell Park Comprehensive Cancer Center), Robert W. Mahley(Gladstone Institutes), J. E. Scott
Science
October 4, 1985
10.1126/science.2994225
Cited by 279

Abstract

Apolipoprotein (apo-) B is the ligand responsible for the receptor-mediated catabolism of low density lipoproteins, the principal cholesterol-transporting lipoproteins in plasma. The primary structure of the carboxyl-terminal 30 percent (1455 amino acids) of human apo-B (apo-B100) has been deduced from the nucleotide sequence of complementary DNA. Portions of the protein structure that may relate to its receptor binding function and lipid binding properties have been identified. The apo-B100 messenger RNA is about 19 kilobases in length. The apo-B100 gene is expressed primarily in liver and, to a lesser extent, in small intestine, but in no other tissues. The gene for apo-B100 is located in the p24 region (near the tip of the short arm) of chromosome 2.

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