In Vivo Synthetic Anticancer Approach by Resourcing Mouse Blood Albumin as a Biocompatible Artificial Metalloenzyme

Author:

Imai Kyosuke1ORCID,Muguruma Kyohei23ORCID,Nakamura Akiko2,Kusakari Yuriko2,Chang Tsung‐Che1ORCID,Pradipta Ambara R.1ORCID,Tanaka Katsunori12ORCID

Affiliation:

1. Department of Chemical Science and Engineering, School of Materials and Chemical Technology Tokyo Institute of Technology 2-12-1 Ookayama, Meguro Tokyo 152-8552 Japan

2. Biofunctional Synthetic Chemistry Laboratory Cluster for Pioneering Research RIKEN 2-1 Hirosawa Wako Saitama 351-0198 Japan

3. Laboratory for Chemistry and Life Science Tokyo Institute of Technology R1-11, 4259 Nagatsuta-cho, Midori-ku Yokohama Kanagawa 226-8503 Japan

Abstract

AbstractMethods for producing drugs directly at the cancer site, particularly using bioorthogonal metal catalysts, are being explored to mitigate the side effects of therapy. Albumin‐based artificial metalloenzymes (ArMs) catalyze reactions in living mice while protecting the catalyst in the hydrophobic pocket. Here, we describe the in situ preparation and application of biocompatible tumor‐targeting ArMs using circulating albumin, which is abundant in the bloodstream. The ArM was formed using blood albumin through the intravenous injection of ruthenium conjugated with an albumin‐binding ligand; the tumor‐targeting unit was conjugated to the ArM using its catalytic activity, and the ArM was transported to the cancer site. The delivered ArM catalyzed a second tagging reaction of the proapoptotic peptide on the cancer surface, successfully suppressing cancer proliferation. This approach, which efficiently leveraged the persisting reactivity twice in vivo, holds promise for future in vivo metal‐catalyzed drug synthesis utilizing endogenous albumin.

Funder

Japan Agency for Medical Research and Development

Astellas Foundation for Research on Metabolic Disorders

Mizutani Foundation for Glycoscience

Publisher

Wiley

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