Laboratory of Catalysis and Organic Synthesis, Ecole Polytechnique Fédérale de Lausanne, EPFL SB ISIC LCSO, BCH 1402, 1015, Lausanne, Switzerland.
Laboratory of Therapeutic Proteins and Peptides, Ecole Polytechnique Fédérale de Lausanne, EPFL SB ISIC LPPT, BCH 5305, 1015, Lausanne, Switzerland.
Angew Chem Int Ed Engl. 2021 Apr 12;60(16):9022-9031. doi: 10.1002/anie.202014511. Epub 2021 Mar 8.
Easy access to a wide range of structurally diverse stapled peptides is crucial for the development of inhibitors of protein-protein interactions. Herein, we report bis-functional hypervalent iodine reagents for two-component cysteine-cysteine and cysteine-lysine stapling yielding structurally diverse thioalkyne linkers. This stapling method works with unprotected natural amino acid residues and does not require pre-functionalization or metal catalysis. The products are stable to purification and isolation. Post-stapling modification can be accessed via amidation of an activated ester, or via cycloaddition onto the formed thioalkyne group. Increased helicity and binding affinity to MDM2 was obtained for a i,i+7 stapled peptide.
方便获得结构多样的订书肽对于开发蛋白-蛋白相互作用抑制剂至关重要。在此,我们报告了双功能高价碘试剂,用于二组分半胱氨酸-半胱氨酸和半胱氨酸-赖氨酸订书,得到结构多样的硫代炔烃接头。这种订书方法适用于未保护的天然氨基酸残基,不需要预功能化或金属催化。产物在纯化和分离过程中稳定。通过活化酯的酰胺化或通过形成的硫代炔烃基团的环加成,可以进行后订书修饰。i,i+7 订书肽的螺旋度和与 MDM2 的结合亲和力增加。
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