Short Communication: Preferential Killing of HIV Latently Infected CD4+ T Cells by MALT1 Inhibitor

Li Hongmei; He Hui; Gong Leyi; Fu Mingui; Wang Tony T

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Short Communication: Preferential Killing of HIV Latently Infected CD4+ T Cells by MALT1 Inhibitor

机译：短期通信：MALT1抑制剂优先杀死艾滋病毒潜伏期的CD4 + T细胞

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We report that the addition of an host paracaspase MALT1 inhibitor, MI-2, to HIV latently infected ACH-2, Jurkat E4, and J-LAT cells accelerated cell death in the presence of cell stimuli or the protein kinase C agonist, bryostatin 1. MI-2-mediated cell death correlated with the induction of the cellular RNase MCPIP1 and requires the presence of viral component(s). Altogether, the combination of MI-2 and bryostatin 1 displays selective killing of HIV latently infected CD4+ T cells.

机译：我们认为，在细胞刺激或蛋白激酶C激动剂中，将宿主帕拉克酶Malt1抑制剂，MI-2，Jurkat E4和J-Lat细胞加速了细胞死亡的宿主潜伏期的ACH-2，Jurkat E4和J-Lat细胞加速了细胞死亡。MI-2介导的细胞死亡与细胞RNA酶MCPIP1的诱导相关，并且需要存在病毒组分。总共，MI-2和BRYOSTATIN 1的组合显示了艾滋病毒潜伏期的CD4 + T细胞的选择性杀死。

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《AIDS Research and Human Retroviruses》 |2016年第2期|共4页
作者
Li Hongmei; He Hui; Gong Leyi; Fu Mingui; Wang Tony T;
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Bioscience Division Center for Immunology and Infectious Diseases SRI International Harrisonburg;

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原文格式 PDF
正文语种 eng
中图分类传染病;
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1. Short Communication: Preferential Killing of HIV Latently Infected CD4+ T Cells by MALT1 Inhibitor [J] . Li Hongmei, He Hui, Gong Leyi, AIDS Research and Human Retroviruses . 2016,第2期

机译：短期通信：MALT1抑制剂优先杀死艾滋病毒潜伏期的CD4 + T细胞
2. Effect of Histone Deacetylase Inhibitors on HIV Production in Latently Infected, Resting CD4+ T Cells From Infected Individuals Receiving Effective Antiretroviral Therapy [J] . Jana Blazkova1a Tae-Wook Chun1a Bietel W. Belay1 Danielle Murray1 J. Shawn Justement1 Emily K. Funk1 Amy Nelson1 Claire W. Hallahan1 Susan Moir1 Paul A. Wender2 and Anthony S. Fauci1 Journal of Infectious Diseases . 2012,第5期

机译：组蛋白脱乙酰基酶抑制剂对受感染个体进行有效抗逆转录病毒治疗的潜伏感染，静息CD4 + T细胞中HIV产生的影响
3. Short communication: Factors influencing time to CD4+ T cell counts 200 cells/mm3 in HIV-infected individuals with CD4 + T Cell 50 Cells/mm3 at the time of starting combination antiretroviral therapy [J] . KuN.S., SongY.G., HanS.H., AIDS Research and Human Retroviruses . 2012,第12期

机译：简短的交流：开始联合抗逆转录病毒治疗时，CD4 + T细胞<50细胞/ mm3的HIV感染个体中影响CD4 + T细胞计数> 200细胞/ mm3的时间的因素
4. Effects of HIV-1 Proteins on the Fas-Mediated Apoptotic Signaling Cascade: A Computational Study of Latent CD4+ T Cell Activation [C] . John Jack, Andrei Paun, Alfonso Rodriguez-Paton International Workshop on Membrane Computing . 2009

机译：HIV-1蛋白对Fas介导的凋亡信号级联的影响：潜在CD4 + T细胞活化的计算研究
5. A model of HIV-1 disease progression and treatment: The subclass of latently infected CD4+ T cells becomes undetectable when both IL-2 and HAART are used. [D] . O'Hara, Karen Ann Bradford. 2002

机译：HIV-1疾病进展和治疗的模型：当同时使用IL-2和HAART时，无法检测到潜在感染的CD4 + T细胞的亚类。
6. Short Communication: Preferential Killing of HIV Latently Infected CD4+ T Cells by MALT1 Inhibitor [O] . Hongmei Li, Hui He, Leyi Gong, -1

机译：简短交流：通过MALT1抑制剂优先杀死HIV潜伏感染的CD4 + T细胞
7. Short Communication: Preferential Killing of HIV Latently Infected CD4+T Cells by MALT1 Inhibitor [O] . Hongmei Li, Hui He, Leyi Gong, 2016

机译：短期通信：MALT1抑制剂优先杀死艾滋病毒潜伏期的CD4 + T细胞

Short Communication: Preferential Killing of HIV Latently Infected CD4+ T Cells by MALT1 Inhibitor

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