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首页> 外文期刊>The journal of immunology >Recognition and Prevention of Tumor Metastasis by the NK Receptor NKp46/NCR1
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Recognition and Prevention of Tumor Metastasis by the NK Receptor NKp46/NCR1

机译:NK受体NKp46 / NCR1识别和预防肿瘤转移

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NK cells employ a variety of activating receptors to kill virally infected and tumor cells. Prominent among these receptors are the natural cytotoxicity receptors (NCRs) (NKp30, NKp44, and NKp46), of which only NKp46 has a mouse ortholog (NCR1). The tumor ligand(s) of NKp46/NCR1 is still unknown, but it was shown that the human NKp46 and the mouse NCR1 are involved in tumor eradication both in vitro and in vivo. Whether any of the NK activating receptors is involved in the prevention of tumor metastasis is unknown. To address this question, we studied the activity of the NK cell receptor NKp46/NCR1 in two spontaneous metastasis models, the B16F10.9 melanoma (B16) and the Lewis lung carcinoma (D122) in the NCR1 knockout mouse that was generated by our group, in various in vitro and in vivo assays. We demonstrated that all B16 and D122 tumors, including those generated in vivo, express an unknown ligand(s) for NKp46/NCR1. We have characterized the properties of the NKp46/NCR1 ligand(s) and demonstrated that NKp46/NCR1 is directly involved in the killing of B16 and D122 cells. Importantly, we showed in vivo that NKp46/NCR1 plays an important role in controlling B16 and D122 metastasis. Thus, to our knowledge, in this study we provide the first evidence for the direct involvement of a specific NK killer receptor in preventing tumor metastasis.
机译:NK细胞利用多种激活受体杀死病毒感染的肿瘤细胞。这些受体中最突出的是天然细胞毒性受体(NCR)(NKp30,NKp44和NKp46),其中只有NKp46具有小鼠直系同源物(NCR1)。 NKp46 / NCR1的肿瘤配体仍是未知的,但已证明人NKp46和小鼠NCR1在体内和体外均参与了肿瘤的根除。 NK激活受体是否参与肿瘤转移的预防尚不清楚。为了解决这个问题,我们研究了由我们小组产生的两种自发转移模型,即B16F10.9黑色素瘤(B16)和Lewis肺癌(D122)在NCR1基因敲除小鼠中NK细胞受体NKp46 / NCR1的活性,在各种体外和体内测定中。我们证明,所有B16和D122肿瘤,包括体内产生的肿瘤,均表达未知的NKp46 / NCR1配体。我们已经表征了NKp46 / NCR1配体的性质,并证明了NKp46 / NCR1直接参与B16和D122细胞的杀伤。重要的是,我们在体内表明NKp46 / NCR1在控制B16和D122转移中起着重要作用。因此,据我们所知,在这项研究中,我们为特定的NK杀伤受体直接参与预防肿瘤转移提供了第一个证据。

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