Targeting TREM1 augments antitumor T cell immunity by inhibiting myeloid-derived suppressor cells and restraining anti–PD-1 resistance
Ashwin Ajith, Kenza Mamouni, Daniel D. Horuzsko, Abu Musa, Amiran K. Dzutsev, Jennifer R. Fang, Ahmed Chadli, Xingguo Zhu, Iryna Lebedyeva, Giorgio Trinchieri, Anatolij Horuzsko
Ashwin Ajith, Kenza Mamouni, Daniel D. Horuzsko, Abu Musa, Amiran K. Dzutsev, Jennifer R. Fang, Ahmed Chadli, Xingguo Zhu, Iryna Lebedyeva, Giorgio Trinchieri, Anatolij Horuzsko
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Research Article Oncology

Targeting TREM1 augments antitumor T cell immunity by inhibiting myeloid-derived suppressor cells and restraining anti–PD-1 resistance

Abstract

The triggering receptor expressed on myeloid cell 1 (TREM1) plays a critical role in development of chronic inflammatory disorders and the inflamed tumor microenvironment (TME) associated with most solid tumors. We examined whether loss of TREM1 signaling can abrogate the immunosuppressive TME and enhance cancer immunity. To investigate the therapeutic potential of TREM1 in cancer, we used mice deficient in Trem1 and developed a novel small molecule TREM1 inhibitor, VJDT. We demonstrated that genetic or pharmacological TREM1 silencing significantly delayed tumor growth in murine melanoma (B16F10) and fibrosarcoma (MCA205) models. Single-cell RNA-Seq combined with functional assays during TREM1 deficiency revealed decreased immunosuppressive capacity of myeloid-derived suppressor cells (MDSCs) accompanied by expansion in cytotoxic CD8+ T cells and increased PD-1 expression. Furthermore, TREM1 inhibition enhanced the antitumorigenic effect of anti-PD-1 treatment, in part, by limiting MDSC frequency and abrogating T cell exhaustion. In patient-derived melanoma xenograft tumors, treatment with VJDT downregulated key oncogenic signaling pathways involved in cell proliferation, migration, and survival. Our work highlights the role of TREM1 in cancer progression, both intrinsically expressed in cancer cells and extrinsically in the TME. Thus, targeting TREM1 to modify an immunosuppressive TME and improve efficacy of immune checkpoint therapy represents what we believe to be a promising therapeutic approach to cancer.

Authors

Ashwin Ajith, Kenza Mamouni, Daniel D. Horuzsko, Abu Musa, Amiran K. Dzutsev, Jennifer R. Fang, Ahmed Chadli, Xingguo Zhu, Iryna Lebedyeva, Giorgio Trinchieri, Anatolij Horuzsko

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Figure 10

TREM1 inhibition by VJDT treatment restrains tumor growth in PDX models.

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TREM1 inhibition by VJDT treatment restrains tumor growth in PDX models....
(A) Tumor growth curve of PDX melanoma xenograft in NSG mice receiving vehicle (DMSO) or VJDT (20 mg/kg) treatment every alternate day from 30 to 48 days (n = 4 mice/group, mean ± SEM). (B) Heatmap depicts hierarchical clustering of differentially expressed genes in PDX tumors between VJDT-treated versus vehicle. (C) Wikipathway analysis identify signaling pathways in PDX tumors significantly affected by VJDT treatment. (D) GSEA analysis showing downregulated signaling pathways during VJDT treatment. Enrichment score (ES) are shown. (E) Scatter plot depicts expression profile of specific genes of interest in VJDT-treated versus vehicle control. (F) Custom RT-qPCR confirmation of expression profile for key genes altered by VJDT treatment. Data from 3 independent experiments performed in triplicate (mean ± SD shown). P value calculated by 2-way ANOVA with Tukey’s correction t test for multiple comparison of longitudinal tumor growth between various groups (A [tumor growth]) or using 2-sided Fisher’s exact t test in pathway analysis (C).