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Alloimmunity does not protect from challenge with the feline immunodeficiency virus

机译:同种免疫不能抵抗猫免疫缺陷病毒的攻击

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Immune responses against polymorphic host molecules incorporated into lentiviral envelopes during cell budding have induced protection against primate immunodeficiency virus infection. Dendritic cells (DCs) express high levels of MHC molecules and are infectable by lentiviruses. Therefore, in this pilot study we addressed the hypothesis that immunization of cats with allogeneic DC would induce immune responses that protect against challenge with the feline immunodeficiency virus. Two groups of 3 cats each received 3 subcutaneous injections of allogeneic or autologous DC, and were then challenged with viruses propagated in the immunizing DC. Infection status and lymphocyte parameters of cats were assessed during 6 weeks after challenge. MHC II antigens were incorporated into viral particles as identified by Western blot; and antibodies reactive with MHC class II antigens were detected in the serum of cats immunized with allogeneic but not autologous DC. After challenge, all cats had proviral DNA in blood leukocytes from 2 weeks post-challenge onward and seroconverted. Cats immunized with allogeneic DC maintained higher total and CD21 lymphocyte concentrations, and higher CD4/CD8 lymphocyte ratios; however, these differences were not significantly different from cats that received autologous DC immunizations. Plasma viral load was not significantly different between groups of cats (p =0.204). These results suggest that immunization of cats with allogeneic DC does not induce protective immunity against FIV infection.
机译:在细胞出芽过程中,针对掺入慢病毒包膜的多态性宿主分子的免疫反应已诱导出针对灵长类免疫缺陷病毒感染的保护作用。树突状细胞(DC)表达高水平的MHC分子,可被慢病毒感染。因此,在这项前瞻性研究中,我们提出了以下假设:同种异体DC免疫猫会诱导免疫反应,从而抵御猫免疫缺陷病毒的攻击。两组3只猫各接受3次皮下注射同种异体或自体DC,然后用免疫DC中繁殖的病毒攻击。攻击后6周内评估猫的感染状况和淋巴细胞参数。如Western印迹所鉴定,将MHC II抗原掺入病毒颗粒中。在同种异体但非自体DC免疫的猫的血清中检测到了与MHC II类抗原具有反应性的抗体。攻击后,从攻击后2周开始,所有猫的血液白细胞中均含有原病毒DNA,并进行血清转化。用同种异体DC免疫的猫维持较高的总CD21和CD21淋巴细胞浓度,以及较高的CD4 / CD8淋巴细胞比例。但是,这些差异与接受自体DC免疫的猫没有显着差异。两组猫之间的血浆病毒载量无显着差异(p = 0.204)。这些结果表明,用同种异体DC免疫猫不会诱导针对FIV感染的保护性免疫。

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