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Differential Scanning Fluorimetry provides high throughput data on silk protein transitions.

机译:差示扫描荧光法可提供有关丝蛋白转变的高通量数据。

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摘要

Here we present a set of measurements using Differential Scanning Fluorimetry (DSF) as an inexpensive, high throughput screening method to investigate the folding of silk protein molecules as they abandon their first native melt conformation, dehydrate and denature into their final solid filament conformation. Our first data and analyses comparing silks from spiders, mulberry and wild silkworms as well as reconstituted ‘silk' fibroin show that DSF can provide valuable insights into details of silk denaturation processes that might be active during spinning. We conclude that this technique and technology offers a powerful and novel tool to analyse silk protein transitions in detail by allowing many changes to the silk solutions to be tested rapidly with microliter scale sample sizes. Such transition mechanisms will lead to important generic insights into the folding patterns not only of silks but also of other fibrous protein (bio)polymers.
机译:在这里,我们介绍了使用差示扫描荧光法(DSF)作为廉价,高通量的筛选方法进行的一系列测量,以研究丝绸蛋白分子在放弃其最初的天然熔体构象,脱水和变性为最终固体长丝构象时的折叠。我们的第一个数据和分析比较了蜘蛛,桑蚕和野生蚕的蚕丝以及重组的“蚕丝”丝蛋白,结果表明DSF可以提供有价值的见解,以了解纺丝过程中可能活跃的蚕丝变性过程的细节。我们得出的结论是,该技术为通过微升规模的样本量快速测试丝绸溶液的许多变化提供了强大而新颖的工具来详细分析丝绸蛋白质的转变。这样的过渡机制将导致重要的一般性见识,不仅是丝绸的折叠模式,还有其他纤维状蛋白质(生物)聚合物的折叠模式。

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