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3. Parallel mechanisms of high molecular weight kininogen action as a cofactor inkallikrein inactivation and prekallikrein activation reactions

Author

Olson, Steven T., Francis, Ann Marie, Sheffer, Roberta, and Choay, Jean

Subjects
Kinins -- Research, Kallikrein -- Analysis, Antithrombins -- Usage, Biological control systems -- Research, Biological sciences, Chemistry
Abstract

An examination of the reactions of kallikrein and heparin, that cause the high molecular weight kininogen's (H-Kininogen's) stimulating influence on the reactions of antithrombin and kallikrein, reveals H-Kininogen as a cofactor in the inactivation of kallikrein through a pathway in a manner similar to its behavior as a cofactor in the stimulation of prekallikrein.

Published
1993

4. Chemical synthesis of glycosaminoglycans: new approaches to antithrombotic drugs

Author

Petitou, Maurice, Lormeau, Jean-Claude, and Choay, Jean

Subjects
Sanofi S.A. -- Research, Elf Aquitaine S.A. -- Research, Glycosaminoglycans -- Health aspects, Thrombolytic drugs -- Research, Pharmaceutical industry -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation
Published
1991

10. Selectively O-acylated glycosaminoglycan derivatives

Author

Petitou, Maurice, primary, Coudert, Catherine, additional, Level, Michel, additional, Lormeau, Jean-Claude, additional, Zuber, Martin, additional, Simenel, Catherine, additional, Fournier, Jean-Paul, additional, and Choay, Jean, additional

Published
1992
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18. In Vivo and in Vitro Stimulation of Nonspecific Immunity by the β-d-p-Aminophenyl Glycoside of N-Acetylmuramyl-l-Alanyl-d-Isoglutamine and an Oligomer Prepared by Cross-Linking with Glutaraldehyde.

Author

Parant, Monique, Damais, Chantal, Audibert, Francoise, Parant, Francine, Chedid, Louis, Sathe, Edgar, Lefrancier, Pierre, Choay, Jean, and Lederer, Edgar

Abstract

Several biological activities of N-acetylmuramyl-l-alanyl-d-isoglutamine (MDP for muramyl dipeptide), a synthetic immunoadjuvant, are inhibited after glycosidation with p-aminophenol. Thus, this glycoside does not induce an increased humoral antibody response in mice when injected in saline, although it retains its stimulatory effect on circulating antibodies and delayed hypersensitivity after administration in a water-in-oil emulsion. The capacity of MDP to stimulate mouse spleen cells is lost, and, moreover, the analogue is unable to increase nonspecific resistance to infection under conditions where MDP is active. After cross-linking of the β-d-p-aminophenyl glycoside of MDP with glutaraldehyde, several biological activities of MDP are recovered. Moreover, the cross-linked oligomer (molecular weight, ∼6,000 daltons) is able to stimulate the uptake of thymidine by spleen cells from a strain of mice weakly responsive to MDP and is more active than MDP in protecting mice against bacterial challenge. [ABSTRACT FROM PUBLISHER]

Published
1978

20. Interaction of heparin and antithrombin III. The role of <em>O</em>-sulfate groups.

Author

Petitou, Maurice, Lormeau, Jean-Claude, and Choay, Jean

Subjects
POLYSACCHARIDES, GLUCOSAMINE, HEPARIN, ANTICOAGULANTS, BLOOD coagulation, ANTITHROMBINS
Abstract

A synthetic pentasaccharide corresponding to the sequence involved in heparin for binding and activation of antithrombin III contains eight sulfate groups. The role of some of them in the interaction with the protein has been demonstrated through the study of fragments obtained from heparin. An approach based on the total chemical synthesis of heparin fragments allows us to provide new information on the O-sulfate groups borne by the iduronic acid and the glucosamine units that constitute the reducing-end disaccharide of the above pentasaccharide sequence. Although not strictly necessary for a weak interaction to take place, these two sulfates co-operate to express maximal activity. This suggests that they belong to a secondary sub-region of interaction with antithrombin III, the primary one being accounted for by other critical parts of the structure and particularly the trisaccharide sequence placed at the non-reducing end of the pentasaccharide. [ABSTRACT FROM AUTHOR]

Published
1988
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38. Synthesis of heparin fragments. A chemical synthesis of the pentasaccharide O-(2-deoxy-2-sulfamido-6-O-sulfo-α-d-glucopyranosyl)-(1→4)-O-(β-d-glucopyranosyluronic acid)-(1→4)-O-(2-deoxy-2-sulfamido-3,6-di-O-sulfo-α-d-glucopyranosyl)-(1→4)-O-(2-O-sulfo-α-l-idopyranosyluronic acid)-(1→4)-2-deoxy-2-sulfamido-6-O-sulfo-d-glucopyranose decasodium salt, a heparin fragment having high affinity for antithrombin III

Author

Petitou, Maurice, primary, Duchaussoy, Philippe, additional, Lederman, Isidore, additional, Choay, Jean, additional, Sinaÿ, Pierre, additional, Jacquinet, Jean-Claude, additional, and Torri, Giangiacomo, additional

Published
1986
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48. Synthesis of heparin fragments. A chemical synthesis of the trisaccharide O-(2-deoxy-2-sulfamido-3,6-di-O-sulfo-α-d-glucopyranosyl)-(1→4)-O-(2-O-sulfo-α-l-idopyranosyluronic acid)-(1→4)-2-deoxy-2-sulfamido-6-O-sulfo-d-glucopyranose heptasodium salt

Author

Jacquinet, Jean-Claude, primary, Petitou, Maurice, additional, Duchaussoy, Philippe, additional, Lederman, Isidore, additional, Choay, Jean, additional, Torri, Giangiacomo, additional, and Sinaÿ, Pierre, additional

Published
1984
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50. Apyrogenic, adjuvant-active N-acetylmuramyl-dipeptides

Author

Lefrancier, Pierre, primary, Derrien, Marcel, additional, Jamet, Xavier, additional, Choay, Jean, additional, Lederer, Edgar, additional, Audibert, Francoise, additional, Parant, Monique, additional, Parant, Francine, additional, and Chedid, Louis, additional

Published
1982
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