JP1 normalizes tumor vasculature to suppress metastasis and facilitate drug delivery by inhibiting IL-8
Jiahua Cui, … , Jianwei Zhou, Yongqian Shu
Jiahua Cui, … , Jianwei Zhou, Yongqian Shu
Published May 16, 2023
Citation Information: JCI Insight. 2023;8(12):e161675. https://doi.org/10.1172/jci.insight.161675.
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Research Article Angiogenesis Oncology

JP1 normalizes tumor vasculature to suppress metastasis and facilitate drug delivery by inhibiting IL-8

Abstract

Tumor vascular normalization prevents tumor cells from breaking through the basement membrane and entering the vasculature, thereby inhibiting metastasis initiation. In this study, we report that the antitumor peptide JP1 regulated mitochondrial metabolic reprogramming through AMPK/FOXO3a/UQCRC2 signaling, which improved the tumor microenvironment hypoxia. The oxygen-rich tumor microenvironment inhibited the secretion of IL-8 by tumor cells, thereby promoting tumor vascular normalization. The normalized vasculature resulted in mature and regular blood vessels, which made the tumor microenvironment form a benign feedback loop consisting of vascular normalization, sufficient perfusion, and an oxygen-rich microenvironment, prevented tumor cells from entering the vasculature, and inhibited metastasis initiation. Moreover, the combined therapy of JP1 and paclitaxel maintained a certain vascular density in the tumor and promoted tumor vascular normalization, increasing the delivery of oxygen and drugs and enhancing the antitumor effect. Collectively, our work highlights the antitumor peptide JP1 as an inhibitor of metastasis initiation and its mechanism of action.

Authors

Jiahua Cui, Zhen Che, Lu Zou, Dongyin Chen, Zhan Xie, Kun Ding, Huning Jiang, Aiping Li, Jianwei Zhou, Yongqian Shu

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Figure 2

JP1 promotes tumor vascular normalization and reduces vascular permeability.

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JP1 promotes tumor vascular normalization and reduces vascular permeabil...
(A) Representative fluorescence images of α-SMA (green), claudin 5 (green), desmin (green), CD31 (red), and DAPI nuclear staining of B16F10 tumor nodules treated with Ctrl-R or JP1. (BE) The CD31 coverage (B), α-SMA coverage (C), claudin 5 coverage (D), and desmin coverage (E) in the interstitial microenvironment of B16F10 tumor nodules (n = 6). Scale bars: 100 μm. (F) Representative fluorescence images of α-SMA (green), claudin 5 (green), desmin (green), CD31 (red), and DAPI nuclear staining of LLC tumor nodules treated with Ctrl-R or JP1. (GJ) The CD31 coverage (G), α-SMA coverage (H), claudin 5 coverage (I), and desmin coverage (J) in the interstitial microenvironment of LLC tumor nodules (n = 6). Scale bars: 100 μm. (K and L) Schematic of vessel permeability assays (K) and quantitation of vascular permeability (L) after Ctrl-R or JP1 treatment (n = 6). *P < 0.05, **P < 0.01 by unpaired, 2-tailed Student’s t test (BD, E, GJ, and L).