Preparation and anticoagulant activity of carboxybutyrylated hydroxyethyl chitosan sulfates

A new method of introduction carboxyl groups to chitosan sulfate by the acylation reaction between hydroxyethyl chitosan sulfates and butane dioic anhydride in homogeneous solution was used to obtain carboxybutyrylated hydroxyethyl chitosan sulfates. The structures of the derivatives were characteri...

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Bibliographic Details
Published inCarbohydrate polymers Vol. 51; no. 4; pp. 431 - 438
Main Authors Ronghua, Huang, Yumin, Du, Jianhong, Yang
Format Journal Article
LanguageEnglish
Published Oxford Elsevier Ltd 01.03.2003
Elsevier Science
Subjects
Anticoagulant activity
Applied sciences
Carboxybutyrylation
Chitosan
Chitosan sulfate
Exact sciences and technology
Natural polymers
Physicochemistry of polymers
Starch and polysaccharides
Carboxybutyrylation
Chitosan
Anticoagulant activity
Chitosan sulfate
Carboxylate polymer
Chemoselectivity
Anticoagulant
Experimental study
Corn starch
Biological activity
Chemical modification
Chitosan derivatives
Structure activity relation
Preparation
Organic sulfate
Carboxylation
Oside polymer
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Summary:A new method of introduction carboxyl groups to chitosan sulfate by the acylation reaction between hydroxyethyl chitosan sulfates and butane dioic anhydride in homogeneous solution was used to obtain carboxybutyrylated hydroxyethyl chitosan sulfates. The structures of the derivatives were characterized by element analysis, FT-IR, 13C-NMR, and gel permeation chromatography. The content and position of the carboxyl groups could be controlled favorably. Their anticoagulant activity was determined for human plasma with respect to activated partial thromboplastin time (APTT), thrombin time (TT), and prothombin time (PT). The introducing of carboxyl groups to amino groups greatly prolonged the APTT and TT. The best result occurred when the degree of substitution of the carboxyl groups was about 0.4/unit that prolonged APTT and TT with about 5 and 1.5 times compared to that of the uncarboxylated hydroxyethyl chitosan sulfates; another conclusion is that introducing of carboxyl groups into N, O-position gave better results than that just into N-positions. Low S% chitosan sulfate and 6- O-desulfated chitosan sulfate showed little anticoagulant activity but their N, O-carboxybutyrylated derivatives (0.6/unit ds) showed increased APTT or TT, while their N-carboxybutyrylated derivatives (0.6/unit ds) gave no improvement. Generally, the introducing of carboxyl groups could not increase PT in spite of the position introduced.
ISSN:0144-8617
1879-1344
DOI:10.1016/S0144-8617(02)00208-4