Immunoreceptor tyrosine-based inhibitory motif–dependent functions of an MHC class I-specific NK cell receptor

Bern, Michael D.; Beckman, Diana L.; Ebihara, Takashi; Taffner, Samantha M.; Poursine-Laurent, Jennifer; White, Janicé; Yokoyama, Wayne M.

doi:10.1073/pnas.1713064114

Cited by 19 publications

(23 citation statements)

References 49 publications

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“…Astonishingly, “memory-like” NK cells expressing the receptor Ly49H have been found to sustain their activation state and exhibit accelerated responses upon reengagement of this receptor ( 119 ). With recent observations describing the expression of PD1 on ILC3 subsets and additional inhibitory receptors being expressed by NK cells and ILC2 subsets (e.g., Ly49A, KLRG1, or CTLA4), a critical role of check point inhibitors and their ligands on myeloid cells requires future investigations ( 120 – 122 ). Noteworthy, two recent reports identified regulatory functions in ILC subsets suggest ILC-mediated negative regulations, particularly during inflammation ( 107 , 123 ).…”

Section: Type 1 Immune Responses and Myeloid Activation Of Ilc1 Nk Cmentioning

confidence: 99%

Cytokine Networks between Innate Lymphoid Cells and Myeloid Cells

Mortha

Burrows

2018

Front. Immunol.

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Innate lymphoid cells (ILCs) are an essential component of the innate immune system in vertebrates. They are developmentally rooted in the lymphoid lineage and can diverge into at least three transcriptionally distinct lineages. ILCs seed both lymphoid and non-lymphoid tissues and are locally self-maintained in tissue-resident pools. Tissue-resident ILCs execute important effector functions making them key regulator in tissue homeostasis, repair, remodeling, microbial defense, and anti-tumor immunity. Similar to T lymphocytes, ILCs possess only few sensory elements for the recognition of non-self and thus depend on extrinsic cellular sensory elements residing within the tissue. Myeloid cells, including mononuclear phagocytes (MNPs), are key sentinels of the tissue and are able to translate environmental cues into an effector profile that instructs lymphocyte responses. The adaptation of myeloid cells to the tissue state thus influences the effector program of ILCs and serves as an example of how environmental signals are integrated into the function of ILCs via a tissue-resident immune cell cross talks. This review summarizes our current knowledge on the role of myeloid cells in regulating ILC functions and discusses how feedback communication between ILCs and myeloid cells contribute to stabilize immune homeostasis in order to maintain the healthy state of an organ.

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Section: Type 1 Immune Responses and Myeloid Activation Of Ilc1 Nk Cmentioning

confidence: 99%

Cytokine Networks between Innate Lymphoid Cells and Myeloid Cells

Mortha

Burrows

2018

Front. Immunol.

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“…4e,f ). MHC-I molecules are known for their inhibitory activity against NK cell killing on tumour cells 23 . Thus, anisomycin-mediated downregulation of MHC-I may increase the susceptibility of HCC cells to NK cell killing.…”

Section: Resultsmentioning

confidence: 99%

Novel natural killer cell-mediated cancer immunotherapeutic activity of anisomycin against hepatocellular carcinoma cells

Kim

Lee

Shin

et al. 2018

Sci Rep

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Despite advances in the clinical management of hepatocellular carcinoma (HCC), this form of cancer remains the second leading cause of cancer-related death worldwide. Currently, there are few treatment options for advanced HCC. Therefore, novel treatment strategies for HCC are required. Here, we described the promising antitumour effects of anisomycin, which exerts both direct killing effects and natural killer cell (NK)-mediated immunotherapeutic effects in HCC. To better elucidate the mechanisms through which anisomycin mediates its antitumour effects, we performed a genome-scale transcriptional analysis. We found that anisomycin treatment of HCC differentially modulated a broad range of immune regulation-associated genes. Among these immune regulation-associated genes, we found that lymphocyte function-associated antigen-3 (LFA-3, also called CD58), whose expression was significantly increased in anisomycin-treated HCC cells, was a critical player in NK-mediated immunotherapeutic effects. Furthermore major histocompatibility complex molecules class I (MHC-I) on HCC cells were also significantly regulated by treatment of anisomycin. Those adhesion molecules like CD58, MHC-I, and ICAM4 should be important for immune synapse formation between NK cells and HCC cells to boost NK-mediated immunotherapeutic effects. Notably, this is the first report of NK-dependent immunomodulatory effects of anisomycin suggesting anisomycin as a novel therapeutic drug for treatment of HCC.

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“…have been previously described [31]. KLRA7 em1(IMPC)J (Ly49G KO) mice on the C57BL/6NJ background were 309 purchased from the Jackson Laboratory (027444); this allele was generated at the Jackson Laboratory by 310 CRISPR-Cas9 injection of Cas9 RNA and 3 gRNAs: TCTTGTACTTGTGCATAACC, CAGTCCTCACTAGTTTCTGC 311 and GACATGGACTGACCAAATT resulting in a 241 bp deletion beginning in 5-prime upstream sequence 312 and ending within exon 1.…”

Section: Methods 297mentioning

confidence: 99%

“…We next tested whether loss of inhibitory Ly49s would affect missing-self recognition in vivo as 185 suggested by in vitro studies [5,31] and anti-Ly49 antibody experiments in vivo [32]. Upon injection, 186 labelled KODO (MHC-I-deficient) splenocytes were effectively cleared in D8-KODO mice that were either 187 WT, or lacked only Ly49A or only Ly49G (Fig 4C, S4), in an NK cell-dependent manner as shown by NK 188 cell depletion (Fig S4A, B) We recently generated KI mice carrying Ly49A with a non-functional ITIM (termed Ly49AYF), 195 demonstrating that effector inhibition and licensing are both mediated by the Ly49A ITIM [31]. Ly49AYF 196 D8-KODO mice were resistant to Δm157-MCMV (Fig 4D) similar to D8-KODO mice but, in contrast to D8-197 KODO mice (Fig 3A, B), Ly49G depletion led to significantly elevated viral titers, similar to anti-NK1.1 198 depletion (Fig 4D).…”

mentioning

confidence: 99%

Major histocompatibility complex class I-restricted protection against murine cytomegalovirus requires missing-self recognition by the natural killer cell inhibitory Ly49 receptors

Parikh¹,

Bern²,

Piersma³

et al. 2019

Preprint

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16Viruses have evolved strategies that highlight critical, intertwined host immune mechanisms. As 17 postulated by the missing-self hypothesis, natural killer (NK) cells and major histocompatibility complex 18 class I (MHC-I)-restricted cytotoxic T lymphocytes (CTLs) have opposing requirements for ubiquitously 19 expressed MHC-I molecules. Since NK cell MHC-I-specific Ly49 inhibitory receptors prevent killing of cells 20 with normal MHC-I, viruses evading CTLs by down-regulating MHC-I should be vulnerable to NK cells. 21However, definitive integrated in vivo evidence for this interplay has been lacking, in part due to 22 receptor polymorphism and a proposed second function of Ly49 receptors in licensing NK cells via self-23 MHC-I. Here we generated mice lacking specific Ly49 inhibitory receptors to show their essential role in 24 licensing and controlling murine cytomegalovirus (MCMV) infection in vivo in an MHC-restricted 25 manner. When MCMV cannot down-regulate MHC-I, NK cells cannot control infection that instead is 26 mediated by CTLs, as predicted by the missing-self hypothesis.control of Δm157-MCMV requires cytotoxicity, implying direct target contact, but NKG2D was not 96 required. 97 98 NK cell resistance requires Ly49 receptor expression 99Since Ly49s recognize MHC-I, we assessed their candidacy for being responsible for the MHC-I-100 restricted, NK-dependent resistance to Δm157-MCMV by using CRISPR-Cas9 to target their deletion 101 directly in B6 zygotes. When we used a guide RNA (gRNA) intentionally chosen for its promiscuity for 102 several Ly49s, we generated ΔLy49-1 mice with two distinct deletions: 1) 149kb deletion between Ly49a 103and Ly49g with an out-of-frame fusion; and 2) 66Kb deletion between two pseudogenes, Ly49n (Klra14-104 ps) and Ly49k (Klra11-ps), such that Ly49h was deleted (Fig 2A). Flow cytometry confirmed the loss of 105Ly49A, Ly49C, Ly49G, and Ly49H expression. Ly49D expression was markedly decreased but its coding 106 sequence was intact, suggesting an as yet unidentified locus control region within one of the deleted 107 segments. We also generated single and compound Ly49 deleted mice, detailed below (Fig S1 and Fig 108 S2). Predicted potential off-target sites were absent by PCR amplification and sequencing (Table S1). To 109 further eliminate any off-target effects and genetic mosaicism, we backcrossed all CRISPR-Cas9 founder 110 mice to WT B6 for two generations followed by additional crosses to KODO mice, then D8 (H2D d ) 111 transgenic mice, to generate the indicated homozygous Ly49 knockout mice on the D8-KODO 112 background. 113 114 MHC-restricted, NK cell-dependent resistance to Δm157-MCMV in D8-KODO mice was absent in ΔLy49-1 115 D8-KODO mice (Fig 2B). Additionally, KODO mice with intact Ly49s complemented ΔLy49-1 D8-KODO 116 mice as their F1 hybrids showed fully restored Δm157-MCMV resistance (Fig 2B), indicating that 117 heterozygous expression of Ly49A, Ly49C, Ly49G, Ly49H (Fig S2), deleted in ΔLy49-1, was sufficient for

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Immunoreceptor tyrosine-based inhibitory motif–dependent functions of an MHC class I-specific NK cell receptor

Cited by 19 publications

References 49 publications

Cytokine Networks between Innate Lymphoid Cells and Myeloid Cells

Cytokine Networks between Innate Lymphoid Cells and Myeloid Cells

Novel natural killer cell-mediated cancer immunotherapeutic activity of anisomycin against hepatocellular carcinoma cells

Major histocompatibility complex class I-restricted protection against murine cytomegalovirus requires missing-self recognition by the natural killer cell inhibitory Ly49 receptors

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