A Novel HER2 Targeting Nanoagent Self-assembled from Affibody-epothilone B Conjugate for Cancer Therapy

Overview

Journal J Nanobiotechnology

Publisher Biomed Central

Specialty Biotechnology

Date 2024 Aug 21

PMID 39169343

Authors

Xuelin Xia

Xiaoyuan Yang

Wenhui Gao

Wei Huang

Xiaoxia Xia

Deyue Yan

Affiliations

Soon will be listed here.

Abstract

Epothilone B (Epo B), a promising antitumor compound effective against various types of cancer cells in vitro. However, its poor selectivity for tumor cells and inadequate therapeutic windows significantly limit its potential clinical application. Affibody is a class of non-immunoglobulin affinity proteins with precise targeting capability to overexpressed molecular receptors on cancer cells, has been intensively investigated due to its exceptional affinity properties. In this study, we present a targeted nanoagent self-assembled from the precursor of an affibody conjugated with Epo B via a linker containing the thioketal (tk) group that is sensitive to reactive oxygen species (ROS). The core-shell structure of the Z-Epo B Affibody-Drug Conjugate Nanoagent (Z-E ADCN), with the cytotoxin Epo B encapsulated within the Z affibody corona, leads to significantly reduced side effects on normal organs. Moreover, the abundant presence of Z on the surface effectively enhances the targeting capacity and tumor accumulation of the drug. Z-E ADCN can be internalized by cancer cells via HER2 receptor-mediated endocytosis followed by Epo B release in response to high levels of ROS, resulting in excellent anticancer efficacy in HER2-positive tumor models.

Citing Articles

Covalent Affibody-Molecular Glue Drug Conjugate Nanoagent for Proximity-Enabled Reactive Therapeutics.

Gao W, Yang X, Li Q, Liu Y, Huang W, Xia X Adv Sci (Weinh). 2025; 12(10):e2412273.

PMID: 39821590 PMC: 11905048. DOI: 10.1002/advs.202412273.

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