Interfacial Self‐assembly of Chiral Selenide Nanomembrane for Enantiospecific Recognition

Author:

Meng Dan1,Li Chen1,Hao Changlong1,Shi Wenxiong2,Xu Jun3,Sun Maozhong1,Kuang Hua1,Xu Chuanlai1,Xu Liguang1ORCID

Affiliation:

1. International Joint Research Laboratory for Biointerface and Biodetection State Key Laboratory of Food Science and Resources Jiangnan University Wuxi Jiangsu 214122 P. R. China

2. Institute for New Energy Materials and Low Carbon Technologies School of Materials Science and Engineering Tianjin University of Technology Tianjin 300384 China

3. Department of Neurology Beijing Tiantan Hospital Capital Medical University China National Clinical Research 8 Center for Neurological Diseases No. 119 South 4th Ring West Road Beijing 100070 P. R. China

Abstract

AbstractHere, we report the synthesis of chiral selenium nanoparticles (NPs) using cysteine and the interfacial assembly strategy to generate a self‐assembled nanomembrane on a large‐scale with controllable morphology and handedness. The selenide (Se) NPs exhibited circular dichroism (CD) bands in the ultraviolet and visible region with a maximum intensity of 39.96 mdeg at 388 nm and optical anisotropy factors (g‐factors) of up to 0.0013 while a self‐assembled monolayer nanomembrane exhibited symmetrical CD approaching 72.8 mdeg at 391 nm and g‐factors up to 0.0034. Analysis showed that a photocurrent of 20.97±1.55 nA was generated by the D‐nanomembrane when irradiated under light while the L‐nanomembrane generated a photocurrent of 20.58±1.36 nA. Owing to the asymmetric intensity of the photocurrent with respect to the handedness of the nanomembrane, an ultrasensitive recognition of enantioselective kynurenine (Kyn) was achieved by the ten‐layer (10L) D‐nanomembrane exhibiting a photocurrent for L‐kynurenine (L‐Kyn) that was 8.64‐fold lower than that of D‐Kyn, with a limit of detection (LOD) of 0.0074 nM for the L‐Kyn, which was attributed to stronger affinity between L‐Kyn and D‐Se NPs. Noticeably, the chiral Se nanomembrane precisely distinguished L‐Kyn in serum and cerebrospinal fluid samples from Alzheimer's disease patients and healthy subjects.

Funder

National Key Research and Development Program of China

Publisher

Wiley

Subject

General Medicine

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