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对前列腺肿瘤细胞表面以及透明质酸/壳聚糖多层膜进行工程改造,以调节细胞与基质的粘附特性。

Engineering the surface of prostate tumor cells and hyaluronan/chitosan multilayer films to modulate cell-substrate adhesion properties.

作者信息

Rocha Neto J B M, Gomes Neto R J, Bataglioli R A, Taketa T B, Pimentel S B, Baratti M O, Costa C A R, Carvalho H F, Beppu M M

机构信息

School of Chemical Engineering, Department of Materials and Bioprocess Engineering, University of Campinas, Campinas 13083-852, São Paulo, Brazil.

School of Chemical Engineering, Department of Materials and Bioprocess Engineering, University of Campinas, Campinas 13083-852, São Paulo, Brazil.

出版信息

Int J Biol Macromol. 2020 Apr 30;158:197-207. doi: 10.1016/j.ijbiomac.2020.04.136.

Abstract

This paper explores different film assembly conditions of the polyelectrolyte solutions of hyaluronan (HA) and chitosan (CHI), as well as both substrate and cell surface modifications, to investigate PC3 cells adhesion properties. UV-Visible, AFM-IR and Zeta potential techniques indicate that the solution ionic strength is a relevant parameter to modulate the free carboxylic groups of HA on the film surface. In addition, capacitive coupling measurements suggest that assembly conditions that favor surface charge mobility inhibit cell adhesion due to polymer rearrangements that support non-specific electrostatic interactions of positively charged CHI residues and the negatively charged cell moieties, rather than specific CD44-hyaluronan interactions. Moreover, the PC3 cells treatment with hyaluronidase and anti-CD44 antibody also highlighted the importance of CD44 binding site availability on the tumor cell adhesion properties. Finally, the conjugation of wheat germ agglutinin on the film surface proved to be a suitable strategy to boost the PC3 cell adhesion properties. Our results reveal the remarkable capacity of HA/CHI films to modulate cell-substrate properties, which pave the road for the development of surfaces suitable for several applications based on biosensing.

摘要

本文探讨了透明质酸(HA)和壳聚糖(CHI)聚电解质溶液的不同成膜条件,以及底物和细胞表面修饰,以研究PC3细胞的粘附特性。紫外可见光谱、原子力显微镜红外光谱和zeta电位技术表明,溶液离子强度是调节膜表面HA游离羧基的一个相关参数。此外,电容耦合测量表明,有利于表面电荷迁移的组装条件会抑制细胞粘附,这是由于聚合物重排支持带正电的CHI残基与带负电的细胞部分之间的非特异性静电相互作用,而不是特异性的CD44-透明质酸相互作用。此外,用透明质酸酶和抗CD44抗体处理PC3细胞也突出了CD44结合位点可用性对肿瘤细胞粘附特性的重要性。最后,在膜表面偶联麦胚凝集素被证明是提高PC3细胞粘附特性的合适策略。我们的结果揭示了HA/CHI膜调节细胞-底物特性的显著能力,这为基于生物传感的多种应用开发合适的表面铺平了道路。

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