VISTA drives macrophages towards a pro-tumoral phenotype that promotes cancer cell phagocytosis yet down-regulates T cell responses

IF 9.4 1区 医学 Q1 HEMATOLOGY Experimental Hematology & Oncology Pub Date : 2024-03-29 DOI:10.1186/s40164-024-00501-x
Yusheng Lin, Ghizlane Choukrani, Lena Dubbel, Lena Rockstein, Jimena Alvarez Freile, Yuzhu Qi, Valerie Wiersma, Hao Zhang, Karl-Wilhelm Koch, Emanuele Ammatuna, Jan Jacob Schuringa, Tom van Meerten, Gerwin Huls, Edwin Bremer
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Abstract

VISTA is a well-known immune checkpoint in T cell biology, but its role in innate immunity is less established. Here, we investigated the role of VISTA on anticancer macrophage immunity, with a focus on phagocytosis, macrophage polarization and concomitant T cell activation. Macrophages, differentiated from VISTA overexpressed THP-1 cells and cord blood CD34+ cell-derived monocytes, were used in phagocytosis assay using B lymphoma target cells opsonized with Rituximab. PBMC-derived macrophages were used to assess the correlation between phagocytosis and VISTA expression. qRT-PCR, flow cytometry, and enzyme-linked immunosorbent assay were performed to analyze the impact of VISTA on other checkpoints and M1/M2-like macrophage biology. Additionally, flow cytometry was used to assess the frequency of CD14+ monocytes expressing VISTA in PBMCs from 65 lymphoma patients and 37 healthy donors. Ectopic expression of VISTA in the monocytic model cell line THP-1 or in primary monocytes triggered differentiation towards the macrophage lineage, with a marked increase in M2-like macrophage-related gene expression and decrease in M1-like macrophage-related gene expression. VISTA expression in THP-1 and monocyte-derived macrophages strongly downregulated expression of SIRPα, a prominent ‘don’t eat me’ signal, and augmented phagocytic activity of macrophages against cancer cells. Intriguingly, expression of VISTA’s extracellular domain alone sufficed to trigger phagocytosis in ∼ 50% of cell lines, with those cell lines also directly binding to recombinant human VISTA, indicating ligand-dependent and -independent mechanisms. Endogenous VISTA expression was predominantly higher in M2-like macrophages compared to M0- or M1-like macrophages, with a positive correlation observed between VISTA expression in M2c macrophages and their phagocytic activity. VISTA-expressing macrophages demonstrated a unique cytokine profile, characterized by reduced IL-1β and elevated IL-10 secretion. Furthermore, VISTA interacted with MHC-I and downregulated its surface expression, leading to diminished T cell activation. Notably, VISTA surface expression was identified in monocytes from all lymphoma patients but was less prevalent in healthy donors. Collectively, VISTA expression associates with and drives M2-like activation of macrophages with a high phagocytic capacity yet a decrease in antigen presentation capability to T cells. Therefore, VISTA is a negative immune checkpoint regulator in macrophage-mediated immune suppression.
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VISTA 促使巨噬细胞向有利于肿瘤的表型发展,从而促进癌细胞的吞噬作用,同时下调 T 细胞反应
VISTA 是 T 细胞生物学中一个众所周知的免疫检查点,但它在先天免疫中的作用却鲜为人知。在这里,我们研究了 VISTA 对抗癌巨噬细胞免疫的作用,重点是吞噬、巨噬细胞极化和伴随的 T 细胞活化。由 VISTA 过表达的 THP-1 细胞和脐带血 CD34+ 细胞衍生的单核细胞分化出的巨噬细胞被用于利妥昔单抗鸦片化的 B 淋巴瘤靶细胞的吞噬试验。采用 qRT-PCR、流式细胞术和酶联免疫吸附试验分析 VISTA 对其他检查点和 M1/M2 样巨噬细胞生物学的影响。此外,还使用流式细胞术评估了 65 名淋巴瘤患者和 37 名健康供体的 PBMC 中表达 VISTA 的 CD14+ 单核细胞的频率。在单核细胞模型细胞系 THP-1 或原代单核细胞中异位表达 VISTA 会引发向巨噬细胞系的分化,M2 样巨噬细胞相关基因表达明显增加,M1 样巨噬细胞相关基因表达减少。VISTA 在 THP-1 和单核细胞衍生巨噬细胞中的表达强烈下调了 SIRPα 的表达,这是一个显著的 "别吃我 "信号,并增强了巨噬细胞对癌细胞的吞噬活性。耐人寻味的是,仅表达VISTA的胞外结构域就足以触发50%细胞系的吞噬作用,这些细胞系还能直接与重组人VISTA结合,这表明了配体依赖性和非依赖性机制。与 M0 或 M1 样巨噬细胞相比,M2 样巨噬细胞中内源性 VISTA 的表达主要较高,在 M2c 巨噬细胞中观察到 VISTA 的表达与其吞噬活性呈正相关。表达 VISTA 的巨噬细胞表现出独特的细胞因子谱,其特点是 IL-1β 分泌减少,IL-10 分泌增加。此外,VISTA 与 MHC-I 相互作用并下调其表面表达,从而导致 T 细胞活化减弱。值得注意的是,在所有淋巴瘤患者的单核细胞中都发现了 VISTA 的表面表达,但在健康供体中却不常见。总之,VISTA 的表达与巨噬细胞的 M2 类活化有关,并驱动巨噬细胞的 M2 类活化,巨噬细胞的吞噬能力很强,但向 T 细胞呈递抗原的能力却下降了。因此,在巨噬细胞介导的免疫抑制中,VISTA 是一种负性免疫检查点调节因子。
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来源期刊
CiteScore
12.60
自引率
7.30%
发文量
97
审稿时长
6 weeks
期刊介绍: Experimental Hematology & Oncology is an open access journal that encompasses all aspects of hematology and oncology with an emphasis on preclinical, basic, patient-oriented and translational research. The journal acts as an international platform for sharing laboratory findings in these areas and makes a deliberate effort to publish clinical trials with 'negative' results and basic science studies with provocative findings. Experimental Hematology & Oncology publishes original work, hypothesis, commentaries and timely reviews. With open access and rapid turnaround time from submission to publication, the journal strives to be a hub for disseminating new knowledge and discussing controversial topics for both basic scientists and busy clinicians in the closely related fields of hematology and oncology.
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