DOI: 10.1042/bj3100497. Molecular organization of the interferon <i>γ</i>-binding domain in heparan sulphate

Molecular organization of the interferon γ-binding domain in heparan sulphate

10.1042/bj3100497

Crossref journal-article

Portland Press Ltd.

Biochemical Journal (288)

Abstract

Interferon (IFN)-gamma, in common with a number of cytokines or growth factors, strongly interacts with heparan sulphate (HS). It has been shown previously that one of the C-terminal basic clusters of amino acids (a regulatory element of IFN-gamma activity) is involved in this interaction. The structural organization of the HS domain that binds to human IFN-gamma has been investigated here. IFN-gamma-affinity chromatography of HS oligosaccharides released by either enzymic or chemical cleavage showed that the binding site is not found in a domain that is resistant to either heparinase or heparitinase or exclusively N-sulphated or N-acetylated. This led us to take a ‘footprinting’ approach in which HS was depolymerized in the presence of IFN-gamma and the cytokine-protected sequences were separated from the digested fragments. Using this strategy we consistently isolated an IFN-gamma-protected domain (IPD; approx. 10 kDa) which displayed the same affinity as full-length HS for the cytokine. Treatment of IPD with either heparinase or heparitinase strongly reduced its affinity, confirming that the high-affinity binding site encompassed a mixture of HS structural domains. Patterns of depolymerization with either enzymic or chemical agents were consistent with IPD being composed of an extended internal domain (approx. 7 kDa) which is predominantly N-acetylated and GlcA-rich, flanked by small N-sulphated oligosaccharides (mainly hexa- to octasaccharides). This is the first description of an HS protein-binding sequence with this type of molecular organization. Furthermore, using a cross-linking strategy, we demonstrated that one HS molecule bound to an IFN-gamma dimer. Together these results lead us to propose a novel model for the interaction of HS with a protein, in which two sulphated terminal sequences of the binding domain interact directly with the two IFN-gamma C-termini and bridge the two cytokine monomers through an internal N-acetyl-rich sequence.

Bibliography

Lortat-Jacob, H., Turnbull, J. E., & Grimaud, J. A. (1995). Molecular organization of the interferon Î³-binding domain in heparan sulphate. Biochemical Journal, 310(2), 497â505.

Authors 3

H Lortat-Jacob (first)
J E Turnbull (additional)
J A Grimaud (additional)

References 0 Referenced 115

None

Dates

Type	When
Created	10 years ago (Aug. 10, 2015, 5:44 p.m.)
Deposited	3 years, 9 months ago (Nov. 23, 2021, 6:56 p.m.)
Indexed	3 weeks, 5 days ago (Aug. 7, 2025, 5:02 a.m.)
Issued	30 years ago (Sept. 1, 1995)
Published	30 years ago (Sept. 1, 1995)
Published Print	30 years ago (Sept. 1, 1995)

Funders 0

None

BibTeX

@article{Lortat_Jacob_1995, title={Molecular organization of the interferon γ-binding domain in heparan sulphate}, volume={310}, ISSN={1470-8728}, url={http://dx.doi.org/10.1042/bj3100497}, DOI={10.1042/bj3100497}, number={2}, journal={Biochemical Journal}, publisher={Portland Press Ltd.}, author={Lortat-Jacob, H and Turnbull, J E and Grimaud, J A}, year={1995}, month=sep, pages={497–505} }

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