Chiral adaptive recognition with sequence specificity of aromatic dipeptides in aqueous solution by an achiral cage

Lin Cheng; Ping Tian; Honghong Duan; Qingfang Li; Xiaowen Song; Anyang Li; Liping Cao

doi:10.1039/d2sc05854e

Chiral adaptive recognition with sequence specificity of aromatic dipeptides in aqueous solution by an achiral cage

Chem Sci. 2022 Dec 17;14(4):833-842. doi: 10.1039/d2sc05854e. eCollection 2023 Jan 25.

Authors

Lin Cheng¹, Ping Tian¹, Honghong Duan¹, Qingfang Li¹, Xiaowen Song¹, Anyang Li¹, Liping Cao¹

Affiliation

¹ Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of the Ministry of Education, Xi'an Key Laboratory of Functional Supramolecular Structure and Materials, College of Chemistry and Materials Science, Northwest University Xi'an 710069 China chcaoliping@nwu.edu.cn.

Abstract

Sequence-specific recognition of peptides and proteins by synthetic compounds or systems remains a huge challenge in biocompatible media. Here, we report the chiral adaptive recognition (CAR) with sequence specificity of aromatic dipeptides in a purely aqueous solution using an achiral tetraphenylethene-based octacationic cage (1) as both a molecular receptor and chiroptical sensor. 1 can selectively bind and dimerize aromatic dipeptides to form 1 : 2 host-guest complexes with high binding affinity (>10¹⁰ M^-2), especially up to ∼10¹⁴ M^-2 for TrpTrp. Given the dynamic rotational conformation of TPE units, achiral 1 can exhibit chiral adaptive responses with mirror-symmetrical circular dichroism (CD) and circularly polarized luminescence (CPL) spectra to enantiomeric dipeptides via supramolecular chirality transfer in the host-guest complexes. Furthermore, this CAR with sequence specificity of 1 can be applied for molecular recognition of TrpTrp- or PhePhe-containing tetrapeptides, polypeptides (e.g., amyloid β-peptide_1-20 and somatostatin), and proteins (e.g., human insulin) with characteristic CD responses.