Finerty S, Stokes C R, Gruffydd-Jones T J, Hillman T J, Reeves N A, Whiting C V, Schaaper W M, Dalsgaard K, Harbour D A
Department of Clinical Veterinary Science, University of Bristol, Langford, BS40 5DU, Bristol, UK.
Vaccine. 2000 Aug 1;18(28):3254-65. doi: 10.1016/s0264-410x(00)00131-6.
Feline immunodeficiency virus (FIV) is a natural lentiviral pathogen of cats which can be experimentally transmitted via rectal and vaginal routes--the major routes of human immunodeficiency virus type 1 transmission in man. An important objective for lentiviral research is the development of vaccine strategies which generate good mucosal immune responses capable of giving protection from a mucosal virus challenge. The experimental vaccines employed in this study were based on (a) a peptide from the third variable region of the FIV envelope glycoprotein and (b) fixed whole FIV, Glasgow-8 strain. Adjuvants used were Quil A and cholera toxin for mucosal administration and incomplete Freund's adjuvant and immune stimulating complexes for subcutaneous injection. Mucosal immunization was given by rectal and intranasal routes. Both antibody and proliferative responses were elicited by mucosal immunization and cholera toxin was found to be a good mucosal adjuvant. The addition of a lipo thioester to the FIV peptide improved IgG and IgA responses upon parenteral administration. However, no protection from a rectal FIV challenge was achieved.
猫免疫缺陷病毒(FIV)是猫的一种天然慢病毒病原体,可通过直肠和阴道途径进行实验性传播,这是人类1型免疫缺陷病毒在人类中的主要传播途径。慢病毒研究的一个重要目标是开发能够产生良好黏膜免疫反应、从而抵御黏膜病毒攻击的疫苗策略。本研究中使用的实验性疫苗基于:(a)FIV包膜糖蛋白第三可变区的一种肽,以及(b)固定化全FIV格拉斯哥-8株。使用的佐剂中,用于黏膜给药的是Quil A和霍乱毒素,用于皮下注射的是不完全弗氏佐剂和免疫刺激复合物。通过直肠和鼻内途径进行黏膜免疫。黏膜免疫引发了抗体和增殖反应,并且发现霍乱毒素是一种良好的黏膜佐剂。在FIV肽中添加硫酯脂质可改善肠胃外给药后的IgG和IgA反应。然而,未能实现抵御直肠FIV攻击的保护作用。
