apoB-100 has a pentapartite structure composed of three amphipathic alpha-helical domains alternating with two amphipathic beta-strand domains. Detection by the computer program LOCATE - PubMed (original) (raw)

apoB-100 has a pentapartite structure composed of three amphipathic alpha-helical domains alternating with two amphipathic beta-strand domains. Detection by the computer program LOCATE

J P Segrest et al. Arterioscler Thromb. 1994 Oct.

Abstract

Due to the great length of apolipoprotein (apo) B-100, the localization of lipid-associating domains in this protein has been difficult. To address this question, we developed a computer program called Locate that searches amino acid sequences to identify potential amphipathic alpha-helixes and beta-strands by using sets of rules for helix and strand termination. A series of model chimeric protein test datasets were created by tandem linking of amino acid sequences of multiple proteins containing four different secondary structural motifs: motif A (exchangeable plasma apolipoproteins); motif G (globular alpha-helical proteins); motif C (coiled-coil alpha-helical proteins); and motif B (beta pleated-sheet proteins). These four test datasets, as well as randomly scrambled sequences of each dataset, were analyzed by Locate using increasingly stringent parameters. Using intermediately stringent parameters under which significant numbers of amphipathic helixes were found only in the unscrambled motif A, two dense clusters of putative lipid-associating amphipathic helixes were located precisely in the middle and at the C-terminal end of apoB-100 (a sparse cluster of class G* helixes is located at the N-terminus). The dense clusters are located between residues 2103 through 2560 and 4061 through 4338 and have densities of 2.4 and 2.2 amphipathic helixes per 100 residues, respectively; under these conditions, motif A has a density of 1.4 amphipathic helixes per 100 residues. These two domains correspond closely to the two major apoB-100 lipid-associated domains at residues 2100 through 2700 and 4100 through 4500 using the principle of releasability of tryptic peptides from trypsin-treated intact low-density lipoprotein. The classes of amphipathic helixes identified within these two putative lipid-associating domains are considerably more diverse than those found in the exchangeable plasma apolipoproteins. Interestingly, apoB-48 terminates at the N-terminal edge of the middle cluster. By using a similar strategy for analysis of amphipathic beta-strands, we discovered that the two gap regions between the three amphipathic helix clusters are highly enriched in putative amphipathic beta-strands, while the three amphipathic helical domains are essentially devoid of this putative lipid-associating motif. We propose, therefore, that apoB-100 has a pentapartite structure, NH2-alpha 1-beta 1-alpha 2-beta 2-alpha 3-COOH, with alpha 1 representing a globular domain.

PubMed Disclaimer

Similar articles

• Apolipoprotein B-100: conservation of lipid-associating amphipathic secondary structural motifs in nine species of vertebrates.
  Segrest JP, Jones MK, Mishra VK, Pierotti V, Young SH, Borén J, Innerarity TL, Dashti N. Segrest JP, et al. J Lipid Res. 1998 Jan;39(1):85-102. J Lipid Res. 1998. PMID: 9469589
• Structure of apolipoprotein B-100 in low density lipoproteins.
  Segrest JP, Jones MK, De Loof H, Dashti N. Segrest JP, et al. J Lipid Res. 2001 Sep;42(9):1346-67. J Lipid Res. 2001. PMID: 11518754 Review.
• Computer programs to identify and classify amphipathic alpha helical domains.
  Jones MK, Anantharamaiah GM, Segrest JP. Jones MK, et al. J Lipid Res. 1992 Feb;33(2):287-96. J Lipid Res. 1992. PMID: 1569380
• The amphipathic helix in the exchangeable apolipoproteins: a review of secondary structure and function.
  Segrest JP, Jones MK, De Loof H, Brouillette CG, Venkatachalapathi YV, Anantharamaiah GM. Segrest JP, et al. J Lipid Res. 1992 Feb;33(2):141-66. J Lipid Res. 1992. PMID: 1569369 Review.

Cited by

• Identification and Functional Analysis of APOB Variants in a Cohort of Hypercholesterolemic Patients.
  Rodríguez-Jiménez C, de la Peña G, Sanguino J, Poyatos-Peláez S, Carazo A, Martínez-Hernández PL, Arrieta F, Mostaza JM, Gómez-Coronado D, Rodríguez-Nóvoa S. Rodríguez-Jiménez C, et al. Int J Mol Sci. 2023 Apr 21;24(8):7635. doi: 10.3390/ijms24087635. Int J Mol Sci. 2023. PMID: 37108800 Free PMC article.
• Structural analysis of APOB variants, p.(Arg3527Gln), p.(Arg1164Thr) and p.(Gln4494del), causing Familial Hypercholesterolaemia provides novel insights into variant pathogenicity.
  Fernández-Higuero JA, Etxebarria A, Benito-Vicente A, Alves AC, Arrondo JL, Ostolaza H, Bourbon M, Martin C. Fernández-Higuero JA, et al. Sci Rep. 2015 Dec 8;5:18184. doi: 10.1038/srep18184. Sci Rep. 2015. PMID: 26643808 Free PMC article.
• Defining lipid-interacting domains in the N-terminal region of apolipoprotein B.
  Jiang ZG, Gantz D, Bullitt E, McKnight CJ. Jiang ZG, et al. Biochemistry. 2006 Oct 3;45(39):11799-808. doi: 10.1021/bi060600w. Biochemistry. 2006. PMID: 17002280 Free PMC article.
• Increased very low density lipoprotein (VLDL) secretion, hepatic steatosis, and insulin resistance.
  Choi SH, Ginsberg HN. Choi SH, et al. Trends Endocrinol Metab. 2011 Sep;22(9):353-63. doi: 10.1016/j.tem.2011.04.007. Epub 2011 May 26. Trends Endocrinol Metab. 2011. PMID: 21616678 Free PMC article. Review.
• Surface study of apoB1694-1880, a sequence that can anchor apoB to lipoproteins and make it nonexchangeable.
  Wang L, Martin DD, Genter E, Wang J, McLeod RS, Small DM. Wang L, et al. J Lipid Res. 2009 Jul;50(7):1340-52. doi: 10.1194/jlr.M900040-JLR200. Epub 2009 Feb 26. J Lipid Res. 2009. PMID: 19251580 Free PMC article.

Publication types

MeSH terms

Substances

LinkOut - more resources

• Full Text Sources

  • Ovid Technologies, Inc.

• Other Literature Sources

  • The Lens - Patent Citations Database

• Miscellaneous

  • NCI CPTAC Assay Portal