Bacterial Cellulose-Chitosan Composite for Prolonged-Action L-Asparaginase in Treatment of Melanoma Cells.

IF 2.3 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Biochemistry (Moscow) Pub Date : 2024-10-01 DOI:10.1134/S0006297924100067
Anastasia N Shishparenok, Egor R Petryaev, Svetlana A Koroleva, Natalya V Dobryakova, Igor D Zlotnikov, Elena N Komedchikova, Olga A Kolesnikova, Elena V Kudryashova, Dmitry D Zhdanov
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Abstract

A significant challenge associated with the therapeutic use of L-ASP for treatment of tumors is its rapid clearance from plasma. Effectiveness of L-ASP is limited by the dose-dependent toxicity. Therefore, new approaches are being developed for L-ASP to improve its therapeutic properties. One of the approaches to improve properties of the enzymes, including L-ASP, is immobilization on various types of biocompatible polymers. Immobilization of enzymes on a carrier could improve stability of the enzyme and change duration of its enzymatic activity. Bacterial cellulose (BC) is a promising carrier for various drugs due to its biocompatibility, non-toxicity, high porosity, and high drug loading capacity. Therefore, this material has high potential for application in biomedicine. Native BC is known to have a number of disadvantages related to structural stability, which has led to consideration of the modified BC as a potential carrier for immobilization of various proteins, including L-ASP. In our study, a BC-chitosan composite in which chitosan is cross-linked with glutaraldehyde was proposed for immobilization of L-ASP. Physicochemical characteristics of the BC-chitosan films were found to be superior to those of native BC films, resulting in increase in the release time of L-ASP in vitro from 8 to 24 h. These films exhibited prolonged toxicity (up to 10 h) against the melanoma cell line. The suggested strategy for A-ASP immobilization on the BC-chitosan films could be potentially used for developing therapeutics for treatment of surface types of cancers including melanomas.

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细菌纤维素-壳聚糖复合材料用于治疗黑色素瘤细胞的长效天冬酰胺酶
使用 L-ASP 治疗肿瘤的一个重大挑战是,它能迅速从血浆中清除。L-ASP 的疗效受到剂量依赖性毒性的限制。因此,人们正在为 L-ASP 开发新的方法,以改善其治疗特性。改善酶(包括 L-ASP)特性的方法之一是将其固定在各种类型的生物相容性聚合物上。将酶固定在载体上可以提高酶的稳定性,改变酶活性的持续时间。细菌纤维素(BC)具有生物相容性、无毒性、高孔隙率和高药物负载能力,是一种很有前景的各种药物载体。因此,这种材料在生物医学中具有很大的应用潜力。众所周知,原生 BC 在结构稳定性方面存在一些缺点,因此人们开始考虑将改性 BC 作为固定包括 L-ASP 在内的各种蛋白质的潜在载体。在我们的研究中,提出了一种用于固定 L-ASP 的 BC-壳聚糖复合材料,其中壳聚糖与戊二醛交联。研究发现,BC-壳聚糖薄膜的理化特性优于原生BC薄膜,从而使L-ASP在体外的释放时间从8小时延长到24小时。所建议的在BC-壳聚糖薄膜上固定A-ASP的策略可用于开发治疗表面类型癌症(包括黑色素瘤)的疗法。
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来源期刊
Biochemistry (Moscow)
Biochemistry (Moscow) 生物-生化与分子生物学
CiteScore
4.70
自引率
3.60%
发文量
139
审稿时长
2 months
期刊介绍: Biochemistry (Moscow) is the journal that includes research papers in all fields of biochemistry as well as biochemical aspects of molecular biology, bioorganic chemistry, microbiology, immunology, physiology, and biomedical sciences. Coverage also extends to new experimental methods in biochemistry, theoretical contributions of biochemical importance, reviews of contemporary biochemical topics, and mini-reviews (News in Biochemistry).
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