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Protective Role of Human Intravenous Immunoglobulin from Influenza AVirus Infection in Mice

机译:人类甲型流感病毒感染的人体免疫球蛋白的保护作用

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Intravenous immunoglobulin (IVIG) has been manufactured from pooled plasma of 10,000 or more units fromhealthy donors. Recently, we reported that the IVIG manufactured even before the 2009 influenza pandemic containedantibodies reactive to seasonal H1N1 and pandemic H1N1 2009 (H1N1 pdm) viruses. In this study, we used an animalmodel to evaluate the efficacy of IVIG against influenza infections. A seasonal influenza H1N1 strain (New Caledonia,A/NC/20/99) and an H1N1 pdm strain (A/Osaka/168/2009) were used. The BALB/c and severe combined immunodeficiencymice (SCID; C.B-17/lcr-scid/scid) were also used. Mice inoculated with A/NC/20/99 or A/Osaka/168/2009were administrated IVIG and monitored for 3 weeks. The administration of IVIG 48 h before and after inoculation with amouse-adapted seasonal H1N1 virus, resulted in survival rates of 80 and 88%, respectively. The rate among control micewas 30%. In addition, infectivity in lungs from IVIG-treated mice also decreased significantly. Similar effects of IVIG onthe survival rate were obtained with H1N1 pdm. Thus, IVIG was shown to be effective against both viruses in mice.
机译:静脉免疫球蛋白(IVIG)是由来自健康供体的10,000或更多单位的合并血浆制成的。最近,我们报告说,甚至在2009年流感大流行之前生产的IVIG都含有对季节性H1N1和2009年H1N1大流行(H1N1 pdm)病毒具有反应性的抗体。在这项研究中,我们使用了动物模型来评估IVIG对抗流感感染的功效。使用季节性H1N1流感毒株(New Caledonia,A / NC / 20/99)和H1N1 pdm毒株(A / Osaka / 168/2009)。还使用了BALB / c和严重的联合免疫缺陷小鼠(SCID; C.B-17 / lcr-scid / scid)。对接种了A / NC / 20/99或A / Osaka / 168/2009的小鼠进行IVIG监测,并监测3周。接种适应鼠适应性的季节性H1N1病毒前后48小时给予IVIG,存活率分别为80%和88%。对照小鼠中的比率为30%。此外,IVIG治疗小鼠的肺部感染性也显着降低。用H1N1 pdm获得了IVIG对存活率的类似影响。因此,IVIG被证明对小鼠的两种病毒均有效。

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