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含糖壳聚糖衍生物的合成与表征:水溶性和生物降解性

Synthesis and characterization of sugar-bearing chitosan derivatives: aqueous solubility and biodegradability.

作者信息

Park Jae Hyung, Cho Yong Woo, Chung Hesson, Kwon Ick Chan, Jeong Seo Young

机构信息

Biomedical Research Center, Korea Institute of Science and Technology, 39-1 Haweolgog-dong, Sungbook-gu, Seoul 136-791, Korea.

出版信息

Biomacromolecules. 2003 Jul-Aug;4(4):1087-91. doi: 10.1021/bm034094r.

DOI:10.1021/bm034094r
PMID:12857096
Abstract

The extended use of chitosan in biomedical fields has been limited by its insoluble nature in a biological solution. To endow the water solubility in a broad range of pH, chitosan derivatives were prepared by the covalent attachment of a hydrophilic sugar moiety, gluconic acid, through the formation of an amide bond. These sugar-bearing chitosans (SBCs) were further modified by the N-acetylation in an alcoholic aqueous solution. Thereafter, the effect of the gluconyl group and the degree of N-acetylation (DA) on the water solubility at different pHs and on the biodegradability of chitosan were investigated. The SBCs showed the water solubility in a broader range of pH than chitosan, whereas they were still insoluble at neutral and alkali pH. The N-acetylation of SBCs significantly affected the water solubility, for example, the SBCs with the DA, ranging from 29% to 63%, were soluble in the whole range of pH. This might result from the improved hydrophilicity by the gluconyl group, accompanied by the role of the N-acetyl group that disturbed the hydrogen bonding between amino groups of chitosan. From the biodegradation tests, determined by the decrease in the viscosity of a polymer solution exposed to lysozyme, it was evident that the gluconyl group attached to chitosan improved the biodegradability. Thus, it was possible to control the biodegradability of chitosan by adjusting the amounts of gluconyl and N-acetyl groups in the chitosan backbone. The N-acetylated SBCs, soluble in the broad range of pH, might be useful for various biomedical applications.

摘要

壳聚糖在生物医学领域的广泛应用受到其在生物溶液中不溶性的限制。为了使其在广泛的pH范围内具有水溶性,通过形成酰胺键将亲水性糖部分葡萄糖酸共价连接制备壳聚糖衍生物。这些含糖壳聚糖(SBCs)在醇水溶液中通过N - 乙酰化进一步改性。此后,研究了葡萄糖酰基和N - 乙酰化程度(DA)对不同pH下的水溶性以及壳聚糖生物降解性的影响。SBCs在比壳聚糖更宽的pH范围内表现出水溶性,而在中性和碱性pH下仍不溶。SBCs的N - 乙酰化显著影响水溶性,例如,DA范围为29%至63%的SBCs在整个pH范围内均可溶。这可能是由于葡萄糖酰基提高了亲水性,同时N - 乙酰基扰乱了壳聚糖氨基之间的氢键作用。从通过暴露于溶菌酶的聚合物溶液粘度降低来测定的生物降解试验中可以明显看出,连接到壳聚糖上的葡萄糖酰基提高了生物降解性。因此,通过调节壳聚糖主链中葡萄糖酰基和N - 乙酰基的量来控制壳聚糖的生物降解性是可能的。在广泛pH范围内可溶的N - 乙酰化SBCs可能对各种生物医学应用有用。

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