首页> 外文期刊>Cell biochemistry and biophysics >A serendipitous discovery of antifreeze protein-specific activity in C-linked antifreeze glycoprotein analogs.
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A serendipitous discovery of antifreeze protein-specific activity in C-linked antifreeze glycoprotein analogs.

机译:偶然发现了C联抗冻糖蛋白类似物中的抗冻蛋白特异性活性。

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摘要

Structurally diverse carbon-linked (C-linked) analogs of antifreeze glycoprotein (AFGP) have been prepared via linear or convergent solid phase synthesis. These analogs range in molecular weight from approx 1.5-4.1 KDa and do not possess the beta-D-galactose-1,3-alpha-D-N-acetylgalactosamine carbohydrate moiety or the L-threonine-L-alanine-L-alanine polypeptide backbone native to the AFGP wild-type. Despite these dramatic structural modifications, the 2.7-KDa and 4.1-KDa analogs possess antifreeze protein-specific activity as determined by recrystallization-inhibition (RI) and thermal hysteresis (TH) assays. These analogs are weaker than the wild-type in their activity, but nanoliter osmometry indicates that these compounds are binding to ice and affecting a localized freezing point depression. This is the first example of a C-linked AFGP analog that possesses TH and RI activity and suggests that the rational design and synthesis of chemically and biologically stable AFGP analogs is a feasible and worthwhile endeavor. Given the low degree of TH activity, these compounds may prove useful for the protection of cells during freezing and thawing cycles.
机译:已经通过线性或聚合固相合成制备了结构多样的抗冻糖蛋白(AFGP)的碳连接(C联)类似物。这些类似物的分子量范围约为1.5-4.1 KDa,并且不具有天然的β-D-半乳糖-1,3-α-DN-乙酰半乳糖胺碳水化合物部分或L-苏氨酸-L-丙氨酸-L-丙氨酸多肽骨架AFGP野生型。尽管进行了这些显着的结构修饰,但2.7-KDa和4.1-KDa类似物仍具有抗冻蛋白特异活性,这是通过重结晶抑制(RI)和热滞后(TH)分析确定的。这些类似物的活性比野生型弱,但是纳升渗透压法表明这些化合物与冰结合并影响局部冰点降低。这是具有TH和RI活性的C链AFGP类似物的第一个例子,表明化学和生物稳定AFGP类似物的合理设计和合成是可行且值得的。由于TH活性较低,因此这些化合物可能在冷冻和解冻循环中对保护细胞有用。

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