Lymphatic-derived oxysterols promote anti-tumor immunity and response to immunotherapy in melanoma

淋巴来源的氧固醇可促进黑色素瘤的抗肿瘤免疫和免疫治疗反应。

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作者:Mengzhu Sun ,Laure Garnier ,Romane Chevalier ,Martin Roumain ,Chen Wang ,Julien Angelillo ,Julien Montorfani ,Robert Pick ,Dale Brighouse ,Nadine Fournier ,David Tarussio ,Stéphanie Tissot ,Jean-Marc Lobaccaro ,Tatiana V Petrova ,Camilla Jandus ,Daniel E Speiser ,Manfred Kopf ,Caroline Pot ,Christoph Scheiermann ,Krisztian Homicsko ,Giulio G Muccioli ,Abhishek D Garg ,Stéphanie Hugues
In melanoma, lymphangiogenesis correlates with metastasis and poor prognosis and promotes immunosuppression. However, it also potentiates immunotherapy by supporting immune cell trafficking. We show in a lymphangiogenic murine melanoma that lymphatic endothelial cells (LECs) upregulate the enzyme Ch25h, which catalyzes the formation of 25-hydroxycholesterol (25-HC) from cholesterol and plays important roles in lipid metabolism, gene regulation, and immune activation. We identify a role for LECs as a source of extracellular 25-HC in tumors inhibiting PPAR-γ in intra-tumoral macrophages and monocytes, preventing their immunosuppressive function and instead promoting their conversion into proinflammatory myeloid cells that support effector T cell functions. In human melanoma, LECs also upregulate Ch25h, and its expression correlates with the lymphatic vessel signature, infiltration of pro-inflammatory macrophages, better patient survival, and better response to immunotherapy. We identify here in mechanistic detail an important LEC function that supports anti-tumor immunity, which can be therapeutically exploited in combination with immunotherapy.

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