The Tryptophan-Rich Region of HIV gp41 and the Promotion of Cholesterol-Rich Domains

Raquel F. Epand, Brian G. Sayer,§ and Richard M. Epand*
Department of Biochemistry, McMaster University, Hamilton, Ontario L8N 3Z5, Canada, and Department of Chemistry, McMaster University, Hamilton, Ontario L8S 4M1, Canada
Biochemistry, 2005, 44 (14), pp 5525–5531
DOI: 10.1021/bi0500224
Publication Date (Web): March 17, 2005
Copyright © 2005 American Chemical Society

 This work was supported by a grant from the Canadian Institutes of Health Research, Grant MT-7654.

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 Department of Biochemistry.

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 Department of Chemistry.

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 To whom correspondence should be addressed. E-mail: epand@mcmaster.ca. Tel:  (905) 525-9140, ext. 22073. Fax:  (905) 521-1397.

Abstract

Abstract Image

The peptide N-acetyl-KWASLWNWFNITNWLWYIK-amide has a sequence that corresponds to the juxtamembrane region of the HIV-1 gp41 fusion protein. We have studied how cholesterol modulates the interaction of this peptide with membranes containing cholesterol using differential scanning calorimetry, circular dichroism, fluorescence spectroscopy, and nuclear magnetic resonance. We find that this peptide is less able to sequester cholesterol into domains than is N-acetyl-LWYIK-amide. On the other hand, the peptide N-acetyl-LASWIK-amide, which corresponds to a segment of HIV-2 and SIV gp41 fusion proteins, has intermediate potency between N-acetyl-KWASLWNWFNITNWLWYIK-amide and N-acetyl-LWYIK-amide in forming areas enriched in cholesterol, even though it does not have a cholesterol recognition/interaction amino acid consensus sequence (CRAC). We suggest that the difference between HIV-1 and HIV-2 in their requirements for glycosphingolipids in determining their tropism is related to their difference in partitioning to cholesterol-rich domains in biological membranes.

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History

  • Published In Issue April 12, 2005
  • Received January 5, 2005
    Revised Manuscript Received February 10, 2005

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