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Increased vessel perfusion predicts the efficacy of immune checkpoint blockade
Xichen Zheng, … , Qingyu Wu, Yuhui Huang
Xichen Zheng, … , Qingyu Wu, Yuhui Huang
Published April 16, 2018
Citation Information: J Clin Invest. 2018;128(5):2104-2115. https://doi.org/10.1172/JCI96582.
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Research Article Immunology Vascular biology Article has an altmetric score of 9

Increased vessel perfusion predicts the efficacy of immune checkpoint blockade

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Abstract

Immune checkpoint blockade (ICB) has demonstrated curative potential in several types of cancer, but only for a small number of patients. Thus, the identification of reliable and noninvasive biomarkers for predicting ICB responsiveness is an urgent unmet need. Here, we show that ICB increased tumor vessel perfusion in treatment-sensitive EO771 and MMTV-PyVT breast tumor as well as CT26 and MCA38 colon tumor models, but not in treatment-resistant MCaP0008 and 4T1 breast tumor models. In the sensitive tumor models, the ability of anti–cytotoxic T lymphocyte–associated protein 4 or anti–programmed cell death 1 therapy to increase vessel perfusion strongly correlated with its antitumor efficacy. Moreover, globally enhanced tumor vessel perfusion could be detected by Doppler ultrasonography before changes in tumor size, which predicted final therapeutic efficacy with more than 90% sensitivity and specificity. Mechanistically, CD8+ T cell depletion, IFN-γ neutralization, or implantation of tumors in IFN-γ receptor knockout mice abrogated the vessel perfusion enhancement and antitumor effects of ICB. These results demonstrated that ICB increased vessel perfusion by promoting CD8+ T cell accumulation and IFN-γ production, indicating that increased vessel perfusion reflects the successful activation of antitumor T cell immunity by ICB. Our findings suggest that vessel perfusion can be used as a novel noninvasive indicator for predicting ICB responsiveness.

Authors

Xichen Zheng, Zhaoxu Fang, Xiaomei Liu, Shengming Deng, Pei Zhou, Xuexiang Wang, Chenglin Zhang, Rongping Yin, Haitian Hu, Xiaolan Chen, Yijie Han, Yun Zhao, Steven H. Lin, Songbing Qin, Xiaohua Wang, Betty Y.S. Kim, Penghui Zhou, Wen Jiang, Qingyu Wu, Yuhui Huang

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Figure 2

IVP correlates with the antitumor effectiveness of CTLA4 blockade.

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IVP correlates with the antitumor effectiveness of CTLA4 blockade.
(A) E...
(A) EO771 tumors were stratified as responders or nonresponders according to whether 4 doses of anti–CTLA4 therapy stopped their progression or not. (B and C) Anti–CTLA4 therapy increased tumor vessel perfusion in responders, but not nonresponders, of EO771 tumors (n = 10–14 mice per group). Scale bars: 100 μM. (D) IVP was observed in 100% of responder tumors. Among the EO771 tumors treated with anti–CTLA4 therapy and assessed for vessel perfusion (122 mice total), 49 were responders and 60 had increased vessel perfusion. Significance was determined by 1-way ANOVA with Bonferroni’s adjusted post hoc t tests for multiple comparisons (A and C). Data are from 1 experiment representative of 3 independent experiments (A–C), or are pooled from multiple independent experiments (D). **P < 0.01, ***P < 0.001.

Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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