Conformational changes in serpins: II. The mechanism of activation of antithrombin by heparin

James C. Whisstock; Robert N. Pike; Lei Jin; Richard Skinner; Xue Y. Pei; Robin W. Carrell; Arthur M. Lesk

doi:10.1006/jmbi.2000.3982

Conformational changes in serpins: II. The mechanism of activation of antithrombin by heparin

James C. Whisstock, Robert N. Pike, Lei Jin, Richard Skinner, Xue Y. Pei, Robin W. Carrell, Arthur M. Lesk

Biochemistry & Molecular Biology

Research output: Contribution to journal › Article › peer-review

83 Scopus citations

Abstract

Antithrombin, uniquely among plasma serpins acting as proteinase inhibitors in the control of the blood coagulation cascade, circulates in a relatively inactive form. Its activation by heparin, and specifically by a pentasaccharide core of heparin, has been shown to involve release of the peptide loop containing the reactive centre from partial insertion in the A sheet of the molecule. Here we compare the structures of the circulating inactive form of antithrombin with the activated structure in complex with heparin pentasaccharide. We show that the rearrangement of the reactive centre loop that occurs upon activation is part of a widespread conformational change involving a realignment of the two major domains of the molecule. We also examine natural mutants that possess high affinity for heparin pentasaccharide, and relate the kinetics of their interaction with heparin pentasaccharide to the structural transitions occuring in the activation process. (C) 2000 Academic Press.

Original language	English (US)
Pages (from-to)	1287-1305
Number of pages	19
Journal	Journal of Molecular Biology
Volume	301
Issue number	5
DOIs	https://doi.org/10.1006/jmbi.2000.3982
State	Published - Sep 1 2000

All Science Journal Classification (ASJC) codes

Structural Biology
Molecular Biology

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10.1006/jmbi.2000.3982

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title = "Conformational changes in serpins: II. The mechanism of activation of antithrombin by heparin",

abstract = "Antithrombin, uniquely among plasma serpins acting as proteinase inhibitors in the control of the blood coagulation cascade, circulates in a relatively inactive form. Its activation by heparin, and specifically by a pentasaccharide core of heparin, has been shown to involve release of the peptide loop containing the reactive centre from partial insertion in the A sheet of the molecule. Here we compare the structures of the circulating inactive form of antithrombin with the activated structure in complex with heparin pentasaccharide. We show that the rearrangement of the reactive centre loop that occurs upon activation is part of a widespread conformational change involving a realignment of the two major domains of the molecule. We also examine natural mutants that possess high affinity for heparin pentasaccharide, and relate the kinetics of their interaction with heparin pentasaccharide to the structural transitions occuring in the activation process. (C) 2000 Academic Press.",

author = "Whisstock, {James C.} and Pike, {Robert N.} and Lei Jin and Richard Skinner and Pei, {Xue Y.} and Carrell, {Robin W.} and Lesk, {Arthur M.}",

note = "Funding Information: We thank Dr M. Petitou for giving us the pentasaccharide used in the kinetic studies; and the Wellcome Trust, the Australian Research Council (A09702079), the National Heart Foundation of Australia (G98M0118) and the National Health and Medical Research Council (997144, 124301) for support.",

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doi = "10.1006/jmbi.2000.3982",

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T2 - II. The mechanism of activation of antithrombin by heparin

AU - Whisstock, James C.

AU - Pike, Robert N.

AU - Jin, Lei

AU - Skinner, Richard

AU - Pei, Xue Y.

AU - Carrell, Robin W.

AU - Lesk, Arthur M.

N1 - Funding Information: We thank Dr M. Petitou for giving us the pentasaccharide used in the kinetic studies; and the Wellcome Trust, the Australian Research Council (A09702079), the National Heart Foundation of Australia (G98M0118) and the National Health and Medical Research Council (997144, 124301) for support.

PY - 2000/9/1

Y1 - 2000/9/1

N2 - Antithrombin, uniquely among plasma serpins acting as proteinase inhibitors in the control of the blood coagulation cascade, circulates in a relatively inactive form. Its activation by heparin, and specifically by a pentasaccharide core of heparin, has been shown to involve release of the peptide loop containing the reactive centre from partial insertion in the A sheet of the molecule. Here we compare the structures of the circulating inactive form of antithrombin with the activated structure in complex with heparin pentasaccharide. We show that the rearrangement of the reactive centre loop that occurs upon activation is part of a widespread conformational change involving a realignment of the two major domains of the molecule. We also examine natural mutants that possess high affinity for heparin pentasaccharide, and relate the kinetics of their interaction with heparin pentasaccharide to the structural transitions occuring in the activation process. (C) 2000 Academic Press.

AB - Antithrombin, uniquely among plasma serpins acting as proteinase inhibitors in the control of the blood coagulation cascade, circulates in a relatively inactive form. Its activation by heparin, and specifically by a pentasaccharide core of heparin, has been shown to involve release of the peptide loop containing the reactive centre from partial insertion in the A sheet of the molecule. Here we compare the structures of the circulating inactive form of antithrombin with the activated structure in complex with heparin pentasaccharide. We show that the rearrangement of the reactive centre loop that occurs upon activation is part of a widespread conformational change involving a realignment of the two major domains of the molecule. We also examine natural mutants that possess high affinity for heparin pentasaccharide, and relate the kinetics of their interaction with heparin pentasaccharide to the structural transitions occuring in the activation process. (C) 2000 Academic Press.

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Conformational changes in serpins: II. The mechanism of activation of antithrombin by heparin

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