化学
螯合作用
钯
肽
金属
阿托品
镍
组合化学
立体化学
有机化学
生物化学
催化作用
作者
Maxwell O. Bowles,Evan L. Willis,Meric D. Trombley,Chun‐Hsing Chen,Caroline Proulx
摘要
We present the first approach to controlled metal chelation of peptide backbones, where the anchoring site is an aza-amino acid nitrogen and the directionality of chelation events is dictated by the acidity of neighboring NHs. Selective backbone chelation precludes the need for metal-binding side chains and/or free N- or C-termini in peptides. We show that the presence and location of an aza-amino acid impact complex formation and report the first X-ray crystal structures of azapeptides bound to palladium and nickel. Evidence of atropisomerism in metallo-azapeptides is also presented.
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