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综述丝中化合物稳定化的物理化学方面。

Review physical and chemical aspects of stabilization of compounds in silk.

机构信息

Department for Biomedical Engineering, Tufts University, Medford, MA 02155, USA.

出版信息

Biopolymers. 2012 Jun;97(6):479-98. doi: 10.1002/bip.22026. Epub 2012 Jan 23.

Abstract

The challenge of stabilization of small molecules and proteins has received considerable interest. The biological activity of small molecules can be lost as a consequence of chemical modifications, while protein activity may be lost due to chemical or structural degradation, such as a change in macromolecular conformation or aggregation. In these cases, stabilization is required to preserve therapeutic and bioactivity efficacy and safety. In addition to use in therapeutic applications, strategies to stabilize small molecules and proteins also have applications in industrial processes, diagnostics, and consumer products like food and cosmetics. Traditionally, therapeutic drug formulation efforts have focused on maintaining stability during product preparation and storage. However, with growing interest in the fields of encapsulation, tissue engineering, and controlled release drug delivery systems, new stabilization challenges are being addressed; the compounds or protein of interest must be stabilized during: (1) fabrication of the protein or small molecule-loaded carrier, (2) device storage, and (3) for the duration of intended release needs in vitro or in vivo. We review common mechanisms of compound degradation for small molecules and proteins during biomaterial preparation (including tissue engineering scaffolds and drug delivery systems), storage, and in vivo implantation. We also review the physical and chemical aspects of polymer-based stabilization approaches, with a particular focus on the stabilizing properties of silk fibroin biomaterials.

摘要

小分子和蛋白质的稳定性问题一直受到广泛关注。小分子的生物活性可能会由于化学修饰而丧失,而蛋白质的活性可能会由于化学或结构降解而丧失,例如大分子构象或聚集的改变。在这些情况下,需要进行稳定化处理以保持治疗和生物活性的功效和安全性。除了在治疗应用中使用外,稳定小分子和蛋白质的策略在工业过程、诊断以及食品和化妆品等消费品中也有应用。传统上,治疗药物制剂的努力重点是在产品制备和储存过程中保持稳定性。然而,随着对封装、组织工程和控制释放药物输送系统等领域的兴趣日益浓厚,新的稳定化挑战正在得到解决;在:(1) 载有蛋白质或小分子的载体的制造,(2) 设备储存,以及 (3) 在体外或体内进行预期释放需求的期间,必须稳定感兴趣的化合物或蛋白质。我们回顾了小分子和蛋白质在生物材料制备(包括组织工程支架和药物输送系统)、储存和体内植入过程中的常见化合物降解机制。我们还回顾了基于聚合物的稳定化方法的物理和化学方面,特别关注丝素蛋白生物材料的稳定化特性。

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