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2007年03月27日

【期刊论文】Cellulose Acetate/Chitosan Multimicrospheres Preparation and Ranitidine Hydrochloride Release In Vitro

陈西广, Hui Yun Zhou, Xi Guang Chen, Cheng Sheng Liu, Xiang Hong Meng, Chen Guang Liu, Jun He, Le Jun Yu

Drug Delivery, 13: 261-267, 2006,-0001,():

-1年11月30日

摘要

A noval cellulose acetate/chitosan multimicrospheres (CACM) was prepared by the method of w/o/w emulsion. The concentration of cellulose acetate (CA) and the ratio of CA/chitosan (CS) had influence on the CACM size, and appearance. Ranitidine hydrochloride loading, and releasing efficiency in vitro were investigated. The optimal condition for preparation of the microspheres was CA concentration at 2% and the ratio of CA/CS at 3/1. The microspheres size was 200-350 μm. The appearance of microspheres was spherical, porous, and nonaggregated. The highest loading efficiency was 21%. The ranitidine release from the CACM was 40% during 48 hr in buffers.

Cellulose Acetate,, Chitosan,, Controlled Release,, Multimicrosphere,, Ranitidine Hydrochloride

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2007年03月27日

【期刊论文】The effect of carboxymethyl-chitosan on proliferation and collagen secretion of normal and keloid skin fibroblasts

陈西广, Xi-Guang Chen, , Zhen Wang, Wan-Shun Liu, Hyun-Jin Park

X. -G. Chen et al. Biomaterials 23 (2002) 4609-4614,-0001,():

-1年11月30日

摘要

In this study, different molecular weight CM-chitosans were prepared and the effects on the growth and collagen secretion of normal skin fibroblasts and keloid fibroblasts were investigated in vitro. CM-chitosan promoted the proliferation of the normal skin fibroblast significantly but inhibited the proliferation of keloid fibroblast. The higher CM-chitosan concentration had a higher initial effect and the lower CM-chitosan concentration had a longer affecting time to the normal skin fibroblast. The lower molecular weight CM-chitosan had significant twofold activities. The CM-chitosan could reduce the ratio of type I/III collagen in keloid fibroblast by inhibiting the secretion of collagen type I; and had no effect on the secretion of types I and III collagen in the normal skin fibroblast. r 2002 Elsevier Science Ltd. All rights reserved.

CM-chitosan, Fibroblast, Keloid, Proliferation, Collagen, Biomaterial

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2007年03月27日

【期刊论文】Effect of MW and concentration of chitosan on antibacterial activity of Escherichia coli

陈西广, Nan Liu , , Xi-Guang Chen , Hyun-Jin Park, Chen-Guang Liu, Cheng-Sheng Liu, Xiang-Hong Meng, Le-Jun Yu

N. Liu et al. Carbohydrate Polymers 64 (2006) 60-65,-0001,():

-1年11月30日

摘要

Different molecular weight (MW) chitosans (5.5

Chitosan, Antibacterial activity, Molecular weight, Concentration, Time sensitivity, Mechanism

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2007年03月27日

【期刊论文】Chitosan and Chitosan/β-Cyclodextrin Microspheres as Sustained-Release Drug Carriers

陈西广, Wei Fen Zhang, Xi Guang Chen, Pi Wu Li, , Qiang Zhi He, Hui Yun Zhou

Journal of Applied Polymer Science, Vol. 103, 1183-1190 (2007),-0001,():

-1年11月30日

摘要

The main aim of this study was to compare two microspheres, chitosan (CTS) and CTS/β-cyclodextrin (β-CD), made by spray-drying, as pulmonary sustained drug-delivery carriers. Theophylline (TH) was used as a model drug. The characteristics of the microspheres and in vitro release were studied. The yield of CTS/β-CD microspheres was 46.1%, which was higher than that of the CTS microspheres (36.5%). The drug loads of the CTS and CTS/β-CD microspheres were 22.7 and 21.1%, respectively, whereas the encapsulation efficiencies were 90.7 and 91.4%, respectively. The distribution of 50% [(diameter) d (0.5)] of the CTS microspheres was below 6.49 mm and that of the CTS/β-CD microspheres was below 4.90 mm. Scanning electron microscopy showed that both microspheres yielded a spherical shape with smooth or wrinkled surfaces. Fourier transform infrared spectroscopy demonstrated that the carbonyl group of TH formed hydrogen bonds with the amide group of CTS and the hydroxyl group of b-CD. The swelling ability of the two microspheres was more than three times their weight, and their humidity rates attained equilibrium within 24 h. The ciliary beat movement times of CTS and CTS/β-CD microspheres were 493.00 and 512.33 min, respectively, which indicated that the two microspheres effectively reduced the ciliotoxicity and possessed better adaptability. In vitro release of TH from CTS/β-CD microspheres was slower than that from CTS microspheres at pH 6.8 and provided a sustained release of 72.0% within 12 h. The results suggest that CTS/β-CD microspheres are a promising carrier for sustained release for pulmonary delivery. 2006 Wiley Periodicals, Inc. J Appl Polym Sci 103: 1183-1190, 2007

drug delivery systems, particle size distribution, chitosan

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2007年03月27日

【期刊论文】羧甲基壳聚糖膜对皮肤成纤维细胞相容性研究

陈西广, 郑立, , 刘万顺, 韩笑天, 严小军

生物化学与生物物理进展(Prog. Biochem. Biophys.) 2003; 30 (2),-0001,():

-1年11月30日

摘要

通过玻璃流延法制备不同分子质量的壳聚糖及羧甲基壳聚糖膜,以体外培养的人皮肤成纤维细胞作为对象,利用膜的浸渍液培养及膜表面直接培养法研究比较了两种多糖膜的细胞相容性。实验发现两种多糖膜的浸渍液对细胞均无毒性效应,生物安全性是小分子质量膜好于大分子质量膜,羧甲基壳聚糖膜好于壳聚糖膜。皮肤成纤维细胞在壳聚糖膜上的生长受到抑制,生长一段时间后细胞有聚集和脱落现象,而羧甲基壳聚糖膜上细胞能很好地贴附、生长,没有聚集和脱落现象。结果表明羧甲基壳聚糖膜具有比壳聚糖膜更优越的细胞相容性。

壳聚糖, 羧甲基壳聚糖, 膜, 皮肤成纤维细胞, 细胞相容性

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    中国海洋大学,山东

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