Issue 86, 2022
From the journal:

Chemical Communications

Non-aqueous bonding of leuprorelin to ochratoxin A for peptide-based solid-phase extraction

Naoki Yamato,b   Noriaki Kumagai,b   Momoha Okahira,b   Satoru Kosaka,b   Shuji Kodama,d   Ryohei Yamamoto,b   Atsushi Yamamoto,b   Koichiro Takao ORCID logo c  and  Masanori Yamamoto ORCID logo *abc  

* Corresponding authors

a Institute of Multidisciplinary Research for Advanced Materials Tohoku University, 2-1-1 Katahira, Aoba, Sendai 980-8577, Japan
E-mail: yamamoto@mol-chem.com

b College of Bioscience and Biotechnology, Chubu University, Matsumoto 1200, Kasugai, Aichi 487-8501, Japan

c Laboratory for Zero-Carbon Energy, Institute of Innovative Research, Tokyo Institute of Technology, Ookayama 2-12-1, Meguro, Tokyo, Japan

d School of Science, Tokai University, 4-1-1 Kitakaname, Hiratsuka, Kanagawa 259-1292, Japan

Abstract

The anticancer therapeutic leuprorelin was found to have excellent affinity to the carcinogen ochratoxin A (OTA), with an equilibrium constant of 2.2 × 108 M−1 at 273 K (dissociation constant Kd = 4.5 nM) when functionalized into a mesoporous polymer. Binding between the surface-bound leuprorelin and mycotoxin was corroborated with DFT calculations, and it was extended to the extraction of OTA from the heavily fatty matrices of coffee, achieving 95% recovery with improved cyclability as compared with immunoaffinity. This work presents the potential of peptide–mycotoxin interactions for durable non-aqueous extraction.

Graphical abstract: Non-aqueous bonding of leuprorelin to ochratoxin A for peptide-based solid-phase extraction

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Article information

DOI
https://doi.org/10.1039/D2CC04430G
Article type
Communication
Submitted
08 Aug 2022
Accepted
23 Sep 2022
First published
26 Sep 2022

Chem. Commun., 2022,58, 12106-12109

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Non-aqueous bonding of leuprorelin to ochratoxin A for peptide-based solid-phase extraction

N. Yamato, N. Kumagai, M. Okahira, S. Kosaka, S. Kodama, R. Yamamoto, A. Yamamoto, K. Takao and M. Yamamoto, Chem. Commun., 2022, 58, 12106 DOI: 10.1039/D2CC04430G

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