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首页> 美国卫生研究院文献>Journal of Virology >Immunization with a live attenuated simian immunodeficiency virus (SIV) prevents early disease but not infection in rhesus macaques challenged with pathogenic SIV.
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Immunization with a live attenuated simian immunodeficiency virus (SIV) prevents early disease but not infection in rhesus macaques challenged with pathogenic SIV.

机译:用减毒的猿猴免疫缺陷病毒活疫苗进行免疫可以预防早期疾病但不能预防由致病性SIV感染的猕猴的感染。

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An infectious, virulence-attenuated molecular clone of simian immunodeficiency virus (SIV), SIVMAC-1A11, was derived from an SIV isolate that causes fatal immunodeficiency in rhesus macaques. When inoculated intravenously in rhesus macaques, SIVMAC-1A11 induced transient viremia (1 to 6 weeks) without clinical disease and a persistent humoral antibody response. The antibodies were directed mainly against the viral envelope glycoproteins, as determined by immunoblots and virus neutralization. The potential of this virulence-attenuated virus to protect against intravenous challenge with a pathogenic SIVMAC strain was assessed. Five rhesus macaques were each given two intravenous inoculations with SIVMAC-1A11 7 months apart. Three of the five immunized monkeys and four naive control animals were then challenged with 100 to 1,000 100% animal infectious doses of pathogenic SIVMAC. All seven animals became persistently viremic following the challenge. Four of four unimmunized animals developed severe clinical signs of simian acquired immunodeficiency syndrome by 38 to 227 days after challenge and were euthanatized 91 to 260 days postchallenge. However, no signs of illness were seen in immunized monkeys until 267 to 304 days postchallenge, when two of three immunized animals developed mild thrombocytopenia and lymphopenia; one of these animals died with clinical signs of simian immunodeficiency disease at 445 days after challenge. The two SIVMAC-1A11-immunized monkeys that were not challenged were healthy and antibody positive 22 months after the initial immunization. Thus, although live SIVMAC-1A11 was immunogenic and did not induce any disease, it failed to protect rhesus macaques against infection with a moderately high dose of pathogenic virus. However, immunization prevented severe, early disease and prolonged the lives of monkeys subsequently infected with pathogenic SIV.
机译:猿猴免疫缺陷病毒(SIV)的感染性,减毒力减弱的分子克隆SIVMAC-1A11源自引起恒河猴猕猴致命的免疫缺陷的SIV分离株。当在恒河猴中静脉注射时,SIVMAC-1A11诱导短暂病毒血症(1至6周),而没有临床疾病和持续的体液抗体反应。如通过免疫印迹和病毒中和所确定的,抗体主要针对病毒包膜糖蛋白。评估了这种减毒力减弱的病毒在抵抗病原性SIVMAC菌株静脉内攻击方面的潜力。五只恒河猴分别接受两次静脉注射,分别间隔7个月接种SIVMAC-1A11。然后用100到1,000 100%动物感染剂量的病原性SIVMAC攻击五只经免疫的猴子中的三只和四只幼稚对照动物。挑战后,所有七只动物都持续出现病毒血症。攻击后38至227天,四只未免疫的动物中有四只出现了猿猴获得性免疫缺陷综合症的严重临床体征,并在攻击后91至260天被安乐死。但是,在攻击后267至304天之前,在免疫猴子中没有发现任何疾病迹象,当时三只免疫动物中有两只出现轻度血小板减少和淋巴细胞减少。这些动物中的一只在攻击后445天以猿猴免疫缺陷疾病的临床体征死亡。两只未接受SIVMAC-1A11免疫接种的猴子是健康的,初次免疫后22个月抗体阳性。因此,尽管活的SIVMAC-1A11具有免疫原性并且没有引起任何疾病,但是它不能保护恒河猴免受中等剂量的病原性病毒的感染。但是,免疫预防了严重的早期疾病,并延长了后来感染病原性SIV的猴子的寿命。

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