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腺病毒载体疫苗。

Adenovirus vectored vaccines.

作者信息

Natuk R J, Davis A R, Chanda P K, Lubeck M D, Chengalvala M, Murthy S C, Wade M S, Dheer S K, Bhat B M, Murthy K K

机构信息

Wyeth-Ayerst Research, Biotechnology & Microbiology Division, Philadelphia, PA.

出版信息

Dev Biol Stand. 1994;82:71-7.

PMID:7958485
Abstract

Human recombinant adenoviruses (Ad) have been employed to develop experimental vaccines against a number of infectious agents. Ad-vectored vaccines express recombinant proteins, including any post-translational modifications, into functioning replicas of the native proteins capable of eliciting neutralizing antibodies in both abortive and permissive animal models. Human Ad types 4, 5, and 7 were used to construct recombinant viruses that express the respiratory syncytial virus F or G glycoproteins, the hepatitis B surface antigen, and the HIV env or gag genes. The recombinant Ad-HIV viruses are of particular interest and have been examined for their immunogenicity in dogs and chimpanzees. Dogs were immunized intratracheally with Ad-env recombinants (10(9) pfu/dog). Excellent humoral anti-HIV responses, including neutralizing antibodies, were detected in the sera following booster immunization (12-18 weeks after primary immunization) with a second Ad-env recombinant made in a different Ad serotype (heterotypic booster). Chimpanzees were immunized in two ways, orally with lyophilized virus (10(9) to 10(10) pfu/virus) in enteric-coated capsules or intranasally (10(7) pfu/virus). Intranasal immunization was superior to oral immunization with respect to replication of recombinant viruses as well as induction of anti-Ad and anti-HIV antibodies. Administration by both routes resulted in stimulation of cellular immune responses, as measured by antigen proliferation assays. Anti-HIV antibodies were detected in chimpanzee secretions (salivary, nasal, rectal, vaginal) taken from animals following intranasal immunization with a heterotypic recombinant. Intranasal administration effectively primed chimpanzees to produce high-titred (320-640) serum neutralizing antibodies to HIV following boosting with a baculovirus-derived env (gp160) subunit vaccine.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

人重组腺病毒(Ad)已被用于研发针对多种感染因子的实验性疫苗。腺病毒载体疫苗可表达重组蛋白,包括任何翻译后修饰,形成天然蛋白的功能性复制品,能够在流产型和允许型动物模型中引发中和抗体。人4型、5型和7型腺病毒被用于构建表达呼吸道合胞病毒F或G糖蛋白、乙肝表面抗原以及HIV env或gag基因的重组病毒。重组腺病毒-HIV病毒尤其令人关注,并已在犬类和黑猩猩中检测其免疫原性。犬经气管内接种腺病毒-env重组体(10⁹ 空斑形成单位/犬)。在初次免疫后12 - 18周用另一种腺病毒血清型制备的第二种腺病毒-env重组体(异型加强免疫)进行加强免疫后,在血清中检测到了良好的体液抗HIV反应,包括中和抗体。黑猩猩通过两种方式进行免疫,口服肠溶胶囊中的冻干病毒(10⁹ 至10¹⁰ 空斑形成单位/病毒)或经鼻接种(10⁷ 空斑形成单位/病毒)。就重组病毒的复制以及抗腺病毒和抗HIV抗体的诱导而言,经鼻免疫优于口服免疫。两种途径给药均导致细胞免疫反应受到刺激,通过抗原增殖试验进行检测。在用异型重组体经鼻免疫后的动物的黑猩猩分泌物(唾液、鼻腔、直肠、阴道)中检测到了抗HIV抗体。经鼻给药有效地使黑猩猩在使用杆状病毒衍生的env(gp160)亚单位疫苗加强免疫后产生高滴度(320 - 640)的血清HIV中和抗体。(摘要截短于250字)

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