Rational steering of insulin binding specificity by intra-chain chemical crosslinking

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作者
Jitka Viková
Michaela Collinsová
Emília Kletvíková
Miloš Buděšínský
Vojtěch Kaplan
Lenka Žáková
Václav Veverka
Rozálie Hexnerová
Roberto J. Tarazona Aviñó
Jana Straková
Irena Selicharová
Václav Vaněk
Daniel W. Wright
Christopher J. Watson
Johan P. Turkenburg
Andrzej M. Brzozowski
Jiří Jiráček
机构
[1] Institute of Organic Chemistry and Biochemistry,Department of Chemistry
[2] the Czech Academy of Sciences,undefined
[3] v.v.i.,undefined
[4] York Structural Biology Laboratory,undefined
[5] University of York,undefined
来源
Scientific Reports | / 6卷
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摘要
Insulin is a key hormone of human metabolism with major therapeutic importance for both types of diabetes. New insulin analogues with more physiological profiles and better glycemic control are needed, especially analogues that preferentially bind to the metabolic B-isoform of insulin receptor (IR-B). Here, we aimed to stabilize and modulate the receptor-compatible conformation of insulin by covalent intra-chain crosslinking within its B22–B30 segment, using the CuI-catalyzed Huisgen 1,3-dipolar cycloaddition reaction of azides and alkynes. This approach resulted in 14 new, systematically crosslinked insulin analogues whose structures and functions were extensively characterized and correlated. One of the analogues, containing a B26–B29 triazole bridge, was highly active in binding to both IR isoforms, with a significant preference for IR-B. Our results demonstrate the potential of chemistry-driven modulation of insulin function, also shedding new light on the functional importance of hormone’s B-chain C-terminus for its IR-B specificity.
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