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In Vivo Administration of a JAK3 Inhibitor during Acute SIV Infection Leads to Significant Increases in Viral Load during Chronic Infection

机译：急性SIV感染期间的JAK3抑制剂体内给药导致慢性感染期间病毒载量的显着增加

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The studies reported herein are the first to document the effect of the in vivo administration of a JAK3 inhibitor for defining the potential role of NK cells during acute SIV infection of a group of 15 rhesus macaques (RM). An additional group of 16 MHC/KIR typed RM was included as controls. The previously optimized in vivo dose regimen (20 mg/kg daily for 35 days) led to a marked depletion of each of the major NK cell subsets both in the blood and gastro-intestinal tissues (GIT) during acute infection. While such depletion had no detectable effects on plasma viral loads during acute infection, there was a significant sustained increase in plasma viral loads during chronic infection. While the potential mechanisms that lead to such increased plasma viral loads during chronic infection remain unclear, several correlates were documented. Thus, during acute infection, the administration of the JAK3 inhibitor besides depleting all NK cell subsets also decreased some CD8⁺ T cells and inhibited the mobilization of the plasmacytoid dendritic cells in the blood and their localization to the GIT. Of interest is the finding that the administration of the JAK3 inhibitor during acute infection also resulted in the sustained maintenance during chronic infection of a high number of naïve and central memory CD4⁺ T cells, increases in B cells in the blood, but decreases in the frequencies and function of NKG2a⁺ NK cells within the GIT and blood, respectively. These data identify a unique role for JAK3 inhibitor sensitive cells, that includes NK cells during acute infection that in concert lead to high viral loads in SIV infected RM during chronic infection without affecting detectable changes in antiviral humoral/cellular responses. Identifying the precise mechanisms by which JAK3 sensitive cells exert their influence is critical with important implications for vaccine design against lentiviruses.

机译：本文报道的研究首次记载了JAK3抑制剂在体内给药对定义15只恒河猴（RM）在急性SIV感染期间NK细胞潜在作用的影响。另包括16组MHC / KIR型RM作为对照。先前优化的体内剂量方案（每天20 mg / kg，连续35天）导致急性感染期间血液和胃肠道组织（GIT）中主要NK细胞亚群的显着消耗。尽管这种消耗对急性感染期间的血浆病毒载量没有可检测的影响，但在慢性感染期间血浆病毒载量显着持续增加。虽然尚不清楚导致慢性感染期间血浆病毒载量增加的潜在机制，但已记录了一些相关性。因此，在急性感染期间，除了耗尽所有NK细胞亚群外，施用JAK3抑制剂还减少了一些CD8 ^{+ T细胞并抑制了血液中浆细胞样树突状细胞的动员及其在GIT中的定位。有趣的是，发现在急性感染期间施用JAK3抑制剂还导致慢性感染过程中持续维持大量幼稚和中枢记忆CD4 ^{+ T细胞，而B细胞的B细胞增加。血液中的NKG2a ^{+ NK细胞的频率和功能分别降低。这些数据确定了JAK3抑制剂敏感性细胞的独特作用，其中包括急性感染过程中的NK细胞，它们共同导致慢性感染过程中SIV感染的RM中病毒载量高，而不会影响抗病毒体液/细胞反应的可检测变化。鉴定JAK3敏感细胞发挥作用的精确机制至关重要，这对针对慢病毒的疫苗设计具有重要意义。}}}

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期刊名称 PLoS Pathogens
作者
Yoshiaki Takahashi; Siddappa N. Byrareddy; Christina Albrecht; Markus Brameier; Lutz Walter; Ann E. Mayne; Paul Dunbar; Robert Russo; Dawn M. Little; Tara Villinger; Ladawan Khowawisetsut; Kovit Pattanapanyasat; Francois Villinger; Aftab A. Ansari;
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年(卷),期 2014(10),3
年度 2014
页码 e1003929
总页数 20
原文格式 PDF
正文语种
中图分类微生物学;寄生动物、寄生虫学;医学寄生虫学;人体病毒学（致病病毒）;病毒（滤过性病毒）;
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1. In Vivo Administration of a JAK3 Inhibitor during Acute SIV Infection Leads to Significant Increases in Viral Load during Chronic Infection [J] . Yoshiaki Takahashi, Siddappa N. Byrareddy, Christina Albrecht, PLoS Pathogens . 2014,第3期

机译：急性SIV感染期间JAK3抑制剂的体内给药导致慢性感染期间病毒载量的显着增加
2. Increased killer B cells in chronic HCV infection may lead to autoimmunity and increased viral load [J] . Eiza N., Zuckerman E., Carlebach M., Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology . 2018,第2期

机译：慢性HCV感染中增加的杀手B细胞可能导致自身免疫和病毒载荷增加
3. Viral gene expression and provirus load of Orf-A defective FIV in lymphoid tissues and lymphocyte subpopulations of neonatal cats during acute and chronic infections. [J] . Novak JM, Crawford PC, Kolenda-Roberts HM, Virus Research: An International Journal of Molecular and Cellular Virology . 2007,第1a2期

机译：在急性和慢性感染期间，新生猫的淋巴组织和淋巴细胞亚群中Orf-A缺陷FIV的病毒基因表达和前病毒载量。
4. Cluster analysis in assessing the interdependencies of clinical and morphological parameters of patients with mixed infections (pulmonary tuberculosis, chronic viral hepatitis, HIV infection) and heroin addiction [C] . Pigul Evgeniia Yu, Filimonova Galina F., Tokin Ivan B., 2015 International Conference "Stability and Control Processes" in Memory of V.I. Zubov . 2015

机译：聚类分析评估混合感染（肺结核，慢性病毒性肝炎，HIV感染）和海洛因成瘾患者临床和形态学参数之间的相互依赖性
5. Dynamics of type I interferon and interleukin-6 production during acute and chronic viral infections. [D] . Mack, Lauren A. 2009

机译：急性和慢性病毒感染期间I型干扰素和白介素6产生的动力学。
6. In Vivo Administration of a JAK3 Inhibitor to Chronically SIV Infected Rhesus Macaques Leads to NK Cell Depletion Associated with Transient Modest Increase in Viral Loads [O] . Yoshiaki Takahashi, Ann E. Mayne, Ladawan Khowawisetsut, -1

机译：对慢性SIV感染的恒河猴的JAK3抑制剂的体内给药会导致NK细胞消耗与病毒载量的短暂适度增加相关
7. In vivo administration of a JAK3 inhibitor during acute SIV infection leads to significant increases in viral load during chronic infection. [O] . Yoshiaki Takahashi, Siddappa N Byrareddy, Christina Albrecht, 2014

机译：在急性sIV感染期间体内施用JaK3抑制剂导致慢性感染期间病毒载量的显着增加。
8. BACTERIOLOGICAL, IMMUNOLOGICAL AND VIRAL STUDIES ON RECTAL MUCUS ENTERIC INFECTIONS SHIGELLOSIS, SALMONELLOSIS, PATHOGENIC COLI INFECTIONS AND VIRAL ENTERIC INFECTIONS INCLUSIVE DATES 1 October 1961 TO 31 December 1961 [R] . 1961

机译：直肠粘膜肠炎感染的细菌学，免疫学和病毒学研究1961年10月1日至1961年12月31日，寄生虫，沙门氏菌，病原性感染和病毒感染包括感染

In Vivo Administration of a JAK3 Inhibitor during Acute SIV Infection Leads to Significant Increases in Viral Load during Chronic Infection

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