PD‐L2<sup>+</sup> wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses

Tavukçuoğlu, Ece; Horzum, Utku; Yılmaz, Kerim Bora; Esendağlı, Güneş

doi:10.1111/imcb.12310

Cited by 8 publications

(4 citation statements)

References 51 publications

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“…When macrophages are stimulated with IL4 (with or without IL13, which also signals through the IL4Rα; hereafter we used a combination of IL4+IL13 to harmonize the results with previous studies [ Kratochvill et al, 2015b ]), a characteristic gene expression program is activated, which was first described as “alternative activation” ( Gordon & Martinez, 2010 ) and often referred to as “M2.” The physiology of only a handful of M2-associated targets, such as Arg1 and PD-L2, are understood in terms of their relationship to M2 functions in type 2 immunity and metabolic maintenance of OXPHOS, which is essential for the M2 phenotype ( Pesce et al, 2009 ; Huber et al, 2010 ; Gundra et al, 2017 ; Van de Velde et al, 2017 ; Baardman et al, 2018 ; Wang et al, 2018 ; Tavukcuoglu et al, 2020 ). To begin to dissect the influence of TNF on M2 gene expression in molecular terms, we chose one M2 target, Retnla (encoding RELMα), as a paradigmatic gene induced by IL4+IL13 and negatively regulated by TNF ( Kratochvill et al, 2015b ).…”

Section: Resultsmentioning

confidence: 99%

Gene-selective transcription promotes the inhibition of tissue reparative macrophages by TNF

et al. 2022

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Anti-TNF therapies are a core anti-inflammatory approach for chronic diseases such as rheumatoid arthritis and Crohn’s Disease. Previously, we and others found that TNF blocks the emergence and function of alternative-activated or M2 macrophages involved in wound healing and tissue-reparative functions. Conceivably, anti-TNF drugs could mediate their protective effects in part by an altered balance of macrophage activity. To understand the mechanistic basis of how TNF regulates tissue-reparative macrophages, we used RNAseq, scRNAseq, ATACseq, time-resolved phospho-proteomics, gene-specific approaches, metabolic analysis, and signaling pathway deconvolution. We found that TNF controls tissue-reparative macrophage gene expression in a highly gene-specific way, dependent on JNK signaling via the type 1 TNF receptor on specific populations of alternative-activated macrophages. We further determined that JNK signaling has a profound and broad effect on activated macrophage gene expression. Our findings suggest that TNF’s anti-M2 effects evolved to specifically modulate components of tissue and reparative M2 macrophages and TNF is therefore a context-specific modulator of M2 macrophages rather than a pan-M2 inhibitor.

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Section: Resultsmentioning

confidence: 99%

Gene-selective transcription promotes the inhibition of tissue reparative macrophages by TNF

et al. 2022

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“…(2) TAMs secret the immunosuppression cytokines regulate the T cell-induced ant-tumor immunity, including IL-10, IL-6, PGE2, and TGF-beta1 [ 97 ]. (3) TAMs express PD-L1 and PD-L2 and participate exhaustion of CD8 + T cell by cell–cell interaction[ 98 , 99 ].…”

Section: Tumor-associated Macrophagementioning

confidence: 99%

Estrogen/ER in anti-tumor immunity regulation to tumor cell and tumor microenvironment

Wang¹,

Jin

Qian

et al. 2021

Cancer Cell Int

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As the essential sexual hormone, estrogen and its receptor has been proved to participate in the regulation of autoimmunity diseases and anti-tumor immunity. The adjustment of tumor immunity is related to the interaction between cancer cells, immune cells and tumor microenvironment, all of which is considered as the potential target in estrogen-induced immune system regulation. However, the specific mechanism of estrogen-induced immunity is poorly understood. Typically, estrogen causes the nuclear localization of estrogen/estrogen receptor complex and alternates the transcription pattern of target genes, leading to the reprogramming of tumor cells and differentiation of immune cells. However, the estrogen-induced non-canonical signal pathway activation is also crucial to the rapid function of estrogen, such as NF-κB, MAPK-ERK, and β-catenin pathway activation, which has not been totally illuminated. So, the investigation of estrogen modulatory mechanisms in these two manners is vital for the tumor immunity and can provide the potential for endocrine hormone targeted cancer immunotherapy. Here, this review summarized the estrogen-induced canonical and non-canonical signal transduction pathway and aimed to focus on the relationship among estrogen and cancer immunity as well as immune-related tumor microenvironment regulation. Results from these preclinical researches elucidated that the estrogen-target therapy has the application prospect of cancer immunotherapy, which requires the further translational research of these treatment strategies.

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“…Interestingly, IRF1 is the key factor of PD-L1 promoter function, while PD-L2 is mainly regulated by STAT1/3 [ 33 ], which also explain our results that only PD-L2 is upregulated in LXN −/− macrophages. It has been reported that PD-1 ligands (PD-Ls) contribute to the M2 polarization and immunosuppressive effects of macrophages [ 48 ], and PD-L2 expression correlated with other established markers for alternatively activated macrophages [ 49 ]. As early as ten years ago, Huber et al reported that PD-L2 appears to be a more specific and distinctive marker for M2, and IL-4 induced the expression of PD-L2 on classically activated macrophages, however, LPS increased the expression of PD-L1 on M2 [ 50 ].…”

Section: Discussionmentioning

confidence: 99%

Loss of LXN promotes macrophage M2 polarization and PD-L2 expression contributing cancer immune-escape in mice

Tan²,

Li³

et al. 2022

Cell Death Discov.

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Latexin (LXN) plays an important role in tumorigenesis and inflammatory response and as a tumor suppressor in many tumors. However, whether LXN regulates tumorigenesis through immune regulation remains uncertain. Here, we demonstrate that LXN deficiency increases hematopoietic stem cells, as well as affects the proportion of immune cells in the peripheral system. Animal studies show that mice loss of LXN promotes tumor growth in subcutaneous tumor model and AOM/DSS-induced colorectal cancer model. We found that loss of LXN promotes macrophage M2 polarization and PD-L2 expression in macrophage, thus, inhibits the function of T cells. Adoptive transfer of wild-type macrophage rescues the function of T cells in LXN-deficient mice. LXN deficiency in hematopoietic lineage exacerbates colorectal carcinogenesis, and targeted inhibition of PD-L2 ameliorates cancer growth in LXN-deficient mice. Mechanistically, we demonstrate that LXN inhibits STAT3 transcriptional activity by targeting inhibition of JAK1 in macrophages. LXN deficiency enhances PD-L2 expression rather than PD-L1 in macrophages, which lead to inhibition of T cells in tumor microenvironment. Collectively, we define a critical role of LXN/JAK1/STAT3 signal in macrophage and highlights the potential role of LXN in tumor immune-escape by regulating macrophage polarization, as well as the expression of immune checkpoint PD-L2.

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PD‐L2⁺ wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses

Cited by 8 publications

References 51 publications

Gene-selective transcription promotes the inhibition of tissue reparative macrophages by TNF

Gene-selective transcription promotes the inhibition of tissue reparative macrophages by TNF

Estrogen/ER in anti-tumor immunity regulation to tumor cell and tumor microenvironment

Loss of LXN promotes macrophage M2 polarization and PD-L2 expression contributing cancer immune-escape in mice

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PD‐L2+ wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses

Cited by 8 publications

References 51 publications

Gene-selective transcription promotes the inhibition of tissue reparative macrophages by TNF

Gene-selective transcription promotes the inhibition of tissue reparative macrophages by TNF

Estrogen/ER in anti-tumor immunity regulation to tumor cell and tumor microenvironment

Loss of LXN promotes macrophage M2 polarization and PD-L2 expression contributing cancer immune-escape in mice

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PD‐L2⁺ wound zone macrophage‐like cells display M1/M2‐mixed activation and restrain the effector Th1 responses