Curbing Exosome Communications via Introducing Artificial Membrane Receptors for Metastatic Pancreatic Cancer Therapy

Author:

Deng Miao1,Guo Rong1,Wang Yang2,Li Jia‐Xin1,He Jiao1,Li Man1,He Qin1ORCID

Affiliation:

1. Key Laboratory of Drug‐Targeting and Drug Delivery System of the Education Ministry and Sichuan Province Sichuan Engineering Laboratory for Plant‐Sourced Drug and Sichuan Research Center for Drug Precision Industrial Technology West China School of Pharmacy Sichuan University Chengdu 610041 P. R. China

2. Department of Medical Biochemistry and Biophysics Karolinska Institutet Stockholm SE‐17177 Sweden

Abstract

AbstractTumor‐derived exosomes (TDEs) carry various biomolecular cargos and play crucial roles in metastasis. TDEs migrate to distal organs for intercellular communication and induce the formation of pre‐metastatic niches (PMNs) to support tumor implantation and proliferation. Precise interference in the bioprocess of TDEs is expected to be efficacious for suppressing tumor metastasis. However, targeting both TDEs and the primary tumor is challenging. Here, based on metabolic glycoengineering and bio‐orthogonal click chemistry, a two‐step delivery strategy is designed to overcome this. During the first step, the tetraacetylated N‐azidoacetyl‐d‐mannosamine‐loaded nanoparticle responds to the metabolic activity of tumor cells in the primary tumor, tagging both tumor cells and TDEs with azide groups; dibenzyl‐cyclootyne‐modified nanoparticles then can, as the second step, specifically react with tumor cells and TDEs through a bio‐orthogonal click reaction. This strategy not only inhibits tumor growth in pancreatic cancer models but also curbs the communicative role of TDEs in inducing liver PMNs and metastasis by tracking and downregulating the exosomal macrophage migration inhibitory factor.

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials,General Materials Science

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