Targeted Intervention in Nerve-cancer Crosstalk Enhances Pancreatic Cancer Chemotherapy

Overview

Journal Nat Nanotechnol

Specialty Biotechnology

Date 2024 Nov 4

PMID 39496914

Authors

Jiaqi Qin

Jingjie Liu

Zhaohan Wei

Xin Li

Zhaoxia Chen

Jianye Li

Wenxia Zheng

Haojie Liu

Shiyi Xu

Tuying Yong

Ben Zhao

Shanmiao Gou

Shenghong Ju

Gao-Jun Teng

Xiangliang Yang

Lu Gan

Affiliations

Soon will be listed here.

Abstract

Nerve-cancer crosstalk has gained substantial attention owing to its impact on tumour growth, metastasis and therapy resistance. Effective therapeutic strategies targeting tumour-associated nerves within the intricate tumour microenvironment remain a major challenge in pancreatic cancer. Here we develop Escherichia coli Nissle 1917-derived outer membrane vesicles conjugated with nerve-binding peptide NP41, loaded with the tropomyosin receptor kinase (Trk) inhibitor larotrectinib (Lar@NP-OMVs) for tumour-associated nerve targeting. Lar@NP-OMVs achieve efficient nerve intervention to diminish neurite growth by disrupting the neurotrophin/Trk signalling pathway. Moreover, OMV-mediated repolarization of M2-like tumour-associated macrophages to an M1-like phenotype results in nerve injury, further accentuating Lar@NP-OMV-induced nerve intervention to inhibit nerve-triggered proliferation and migration of pancreatic cancer cells and angiogenesis. Leveraging this strategy, Lar@NP-OMVs significantly reduce nerve infiltration and neurite growth promoted by gemcitabine within the tumour microenvironment, leading to augmented chemotherapy efficacy in pancreatic cancer. This study sheds light on a potential avenue for nerve-targeted therapeutic intervention for enhancing pancreatic cancer therapy.

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