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生长因子和基质分子可维持热响应性培养表面上细胞的功能。

Growth factor and matrix molecules preserve cell function on thermally responsive culture surfaces.

作者信息

von Recum H, Kikuchi A, Yamato M, Sakurai Y, Okano T, Kim S W

机构信息

Department of Bioengineering, University of Utah, Salt Lake City, UT, USA.

出版信息

Tissue Eng. 1999 Jun;5(3):251-65. doi: 10.1089/ten.1999.5.251.

DOI:10.1089/ten.1999.5.251
PMID:10434072
Abstract

Thermally-responsive culture surfaces were designed using copolymers of N-isopropylacrylamide, 4-(aminomethyl)styrene, and acrylic acid. These surfaces contained functional amine and carboxyl groups, which allowed biomolecules to be grafted by amide formation. Epidermal growth factor (EGF), and extracellular matrix (ECM) molecules (collagen type IV, and chondroitin sulfate) were investigated, as surface-grafted biomolecules, for their ability to stimulate cell attachment, proliferation, and function by signaling only from the basal side of cultured cells. Surface analysis of biomolecule-grafted porous inserts showed covalent binding of biomolecules to either amine or carboxyl groups. Multiple attachment to amine and/or carboxyl groups served as cross-linking points that made the polymer hydrogel permanently adherent to the culture surface. Immunofluorescence microscopy techniques gave positive identification of grafted biomolecules. Grafting of EGF improved cell proliferation versus that on nongrafted controls, or controls grafted only with ECM molecules. ECM grafting induced cell attachment on attachment-resistant surfaces. Analysis of trans-epithelial resistance, fluid transport, and polarized g-glutamyl transpeptidase activity indicated that simultaneous grafting of both EGF and ECM produced better polarized cell function than nongrafted controls, or controls grafted with only one type of biomolecule. Covalent grafting of biomolecules did not interfere with cells ability to detach from thermally responsive surfaces upon temperature decrease.

摘要

使用N-异丙基丙烯酰胺、4-(氨甲基)苯乙烯和丙烯酸的共聚物设计了热响应性培养表面。这些表面含有功能性胺基和羧基,这使得生物分子能够通过酰胺形成进行接枝。研究了表皮生长因子(EGF)和细胞外基质(ECM)分子(IV型胶原和硫酸软骨素)作为表面接枝生物分子,仅从培养细胞的基底侧发出信号来刺激细胞附着、增殖和功能的能力。对生物分子接枝的多孔插入物进行表面分析,结果表明生物分子与胺基或羧基发生了共价结合。与胺基和/或羧基的多重连接充当交联点,使聚合物水凝胶永久附着在培养表面。免疫荧光显微镜技术对接枝的生物分子进行了阳性鉴定。与未接枝的对照或仅接枝ECM分子的对照相比,EGF的接枝改善了细胞增殖。ECM接枝在抗附着表面上诱导细胞附着。对跨上皮电阻、液体转运和极化γ-谷氨酰转肽酶活性的分析表明,与未接枝的对照或仅接枝一种生物分子的对照相比,同时接枝EGF和ECM产生了更好的极化细胞功能。生物分子的共价接枝并不干扰细胞在温度降低时从热响应表面脱离的能力。

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