Dynamic Co-evolution of Host and Pathogen: HCMV Downregulates the Prevalent Allele MICA*008 to Escape Elimination by NK Cells

Einat Seidel; Vu?Thuy?Khanh Le; Yotam Bar-On; Pinchas Tsukerman; Jonatan Enk; Rachel Yamin; Natan Stein; Dominik Schmiedel; Esther Oiknine?Djian; Yiska Weisblum; Boaz Tirosh; Peter Stastny; Dana?G. Wolf; Hartmut Hengel; Ofer Mandelboim

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Dynamic Co-evolution of Host and Pathogen: HCMV Downregulates the Prevalent Allele MICA*008 to Escape Elimination by NK Cells

机译：宿主和病原体的动态共同进化：HCMV下调流行的等位基因MICA * 008，以逃避NK细胞的清除

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Natural killer (NK) cells mediate innate immune responses against hazardous cells and are particularly important for the control of human cytomegalovirus (HCMV). NKG2D is a key NK activating receptor that recognizes a family of stress-induced ligands, including MICA, MICB, and ULBP1-6. Notably, most of these ligands are targeted by HCMV proteins and a miRNA to prevent the killing of infected cells by NK cells. A particular highly prevalent MICA allele, MICA^*008, is considered to be an HCMV-resistant ''escape variant'' that confers advantage to human NK cells in recognizing infected cells. However, here we show that HCMV uses its viral glycoprotein US9 to specifically target MICA^*008 and thus escapes NKG2D attack. The finding that HCMV evolved a protein dedicated to countering a single host allele illustrates the dynamic co-evolution of host and pathogen.

机译：天然杀伤细胞（NK）介导针对有害细胞的先天免疫应答，对于控制人类巨细胞病毒（HCMV）尤其重要。 NKG2D是关键的NK激活受体，可识别应力诱导的配体家族，包括MICA，MICB和ULBP1-6。值得注意的是，这些配体中的大多数都被HCMV蛋白和miRNA靶向，以防止被NK细胞杀死感染的细胞。特定的高度流行的MICA等位基因MICA ^ * 008被认为是HCMV抗性的“逃脱变体”，在识别受感染的细胞方面赋予了人类NK细胞以优势。但是，这里我们显示HCMV使用其病毒糖蛋白US9特异性靶向MICA ^ * 008，从而逃脱了NKG2D攻击。 HCMV进化出一种专门用于对抗单个宿主等位基因的蛋白质的发现说明了宿主和病原体的动态共同进化。

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《Cell Reports》 |2015年第6期|共15页
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Einat Seidel; Vu?Thuy?Khanh Le; Yotam Bar-On; Pinchas Tsukerman; Jonatan Enk; Rachel Yamin; Natan Stein; Dominik Schmiedel; Esther Oiknine?Djian; Yiska Weisblum; Boaz Tirosh; Peter Stastny; Dana?G. Wolf; Hartmut Hengel; Ofer Mandelboim;
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1. Dynamic Co-evolution of Host and Pathogen: HCMV Downregulates the Prevalent Allele MICA*008 to Escape Elimination by NK Cells [J] . Einat Seidel, Vu?Thuy?Khanh Le, Yotam Bar-On, Cell Reports . 2015,第6期

机译：宿主和病原体的动态共同进化：HCMV下调流行的等位基因MICA * 008，以逃避NK细胞的清除
2. Frequencies of Gag-restricted T-cell escape "footprints" differ across HIV-1 clades A1 and D chronically infected Ugandans irrespective of host HLA B alleles [J] . Serwanga Jennifer, Nakiboneka Ritah, Mugaba Susan, Vaccine . 2015,第14期

机译：长期受HIV-1感染的乌干达人中，受gag限制的T细胞逃逸“足迹”的频率各不相同，而与宿主HLA B等位基因无关
3. Co-evolution and exploitation of host cell signaling pathways by bacterial pathogens. [J] . Shames SR, Auweter SD, Finlay BB The international journal of biochemistry and cell biology . 2009,第2期

机译：细菌病原体共同进化和利用宿主细胞信号通路。
4. System-Wide Elimination of Unreferenced Code and Data in Dynamically Linked Programs [C] . Vladislav Ivanishin, Evgeny Kudryashov, Alexander Monakov, Ivannikov ISPRAS Open Conference . 2017

机译：系统范围内消除动态链接程序中未引用的代码和数据
5. NK cells dynamically regulate CCL22-mediated regulatory T-cell recruitment [D] . Mailloux, Adam William 2009

机译：NK细胞动态调节CCL22介导的调节性T细胞募集
6. Dynamic Co-evolution of Host and Pathogen: HCMV Downregulates the Prevalent Allele MICA*008 to Escape Elimination by NK Cells [O] . Einat Seidel, Vu Thuy Khanh Le, Yotam Bar-On, -1

机译：宿主和病原体的动态共同进化：HCMV下调流行的等位基因MICA * 008以逃避NK细胞的清除
7. Dynamic Co-evolution of Host and Pathogen: HCMV Downregulates the Prevalent Allele MICA∗008 to Escape Elimination by NK Cells [O] . Einat Seidel, Vu Thuy Khanh Le, Yotam Bar-On, 2015

机译：宿主和病原体的动态共同进化：HCmV下调普遍存在的等位基因mICa * 008以逃避NK细胞的消除

Dynamic Co-evolution of Host and Pathogen: HCMV Downregulates the Prevalent Allele MICA*008 to Escape Elimination by NK Cells

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