A serendipitous discovery of antifreeze protein-specific activity in C-linked antifreeze glycoprotein analogs

被引:0
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作者
Adewale Eniade
Madhusudhan Purushotham
Robert N. Ben
J. B. Wang
Kathleen Horwath
机构
[1] State University of New York at Binghamton,Department of Chemistry
[2] State University of New York at Binghamton,Department of Biological Sciences
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关键词
Antifreeze glycoproteins; glycoconjugate; thermal hysteresis; recrystallization-inhibition; carbon-linked;
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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 β-d-galactose-1,3-α-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.
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页码:115 / 124
页数:9
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