Lymphatic vessels regulate immune microenvironments in human and murine melanoma
Amanda W. Lund, … , Helge Wiig, Melody A. Swartz
Amanda W. Lund, … , Helge Wiig, Melody A. Swartz
Published August 15, 2016
Citation Information: J Clin Invest. 2016;126(9):3389-3402. https://doi.org/10.1172/JCI79434.
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Research Article Angiogenesis

Lymphatic vessels regulate immune microenvironments in human and murine melanoma

Abstract

Lymphatic remodeling in tumor microenvironments correlates with progression and metastasis, and local lymphatic vessels play complex and poorly understood roles in tumor immunity. Tumor lymphangiogenesis is associated with increased immune suppression, yet lymphatic vessels are required for fluid drainage and immune cell trafficking to lymph nodes, where adaptive immune responses are mounted. Here, we examined the contribution of lymphatic drainage to tumor inflammation and immunity using a mouse model that lacks dermal lymphatic vessels (K14-VEGFR3-Ig mice). Melanomas implanted in these mice grew robustly, but exhibited drastically reduced cytokine expression and leukocyte infiltration compared with those implanted in control animals. In the absence of local immune suppression, transferred cytotoxic T cells more effectively controlled tumors in K14-VEGFR3-Ig mice than in control mice. Furthermore, gene expression analysis of human melanoma samples revealed that patient immune parameters are markedly stratified by levels of lymphatic markers. This work suggests that the establishment of tumor-associated inflammation and immunity critically depends on lymphatic vessel remodeling and drainage. Moreover, these results have implications for immunotherapies, the efficacies of which are regulated by the tumor immune microenvironment.

Authors

Amanda W. Lund, Marek Wagner, Manuel Fankhauser, Eli S. Steinskog, Maria A. Broggi, Stefani Spranger, Thomas F. Gajewski, Kari Alitalo, Hans P. Eikesdal, Helge Wiig, Melody A. Swartz

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Figure 3

B16F10 melanomas implanted in K14-VEGFR3-Ig mice lack a local inflammatory infiltrate.

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B16F10 melanomas implanted in K14-VEGFR3-Ig mice lack a local inflammato...
The inflammatory infiltrate was determined on day 9 in B16F10 tumors grown in WT and K14-VEGFR3-Ig (Tg) mice. (A) Immunohistochemical analysis of tumor immune infiltrates in WT and Tg mice. Scale bars: 50 μm (CD11b, F4/80, and CD3ε) and 100 μm (MHCII). (BG) Analysis of immune cell populations in the tumor (BD) and spleen (EG) by flow cytometry. (B and E) Total leukocytes (CD45+), (C and F) Treg cells (CD3ε+CD4+CD25+FoxP3+), and (D and G) inflammatory monocytes (CD11cCD11b+F4/80Ly6chiLy6g, n ≥ 4). Statistical analysis with Man-Whitney U test. *P < 0.05, **P < 0.01.