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动物核酸疫苗的研究现状及发展前景 总被引:2,自引:2,他引:0
核酸疫苗是近年来备受人们关注的一种新型疫苗。核酸疫苗以其特有的可诱导机体产生全面的免疫应答,对不同亚型的病原体具有交叉防御作用,以及安全、可靠、生产方便等优点被称之为“疫苗的第三次革命”。核酸疫苗由编码能引起保护性免疫反应的病原体抗原的基因片段和载体构建而成,包括DNA疫苗和RNA疫苗,目前研究较多的是DNA疫苗。DNA疫苗是指含有编码抗原基因的真核表达质粒DNA,经直接接种体内后,可被体细胞摄取,并转录、翻译、表达出相应的抗原,然后通过不同途径刺激机体产生针对此种抗原的应答。作者简单介绍了动物核酸疫苗的特点、免疫机制、免疫影响因素及在畜禽传染病中的应用,此外还分析了核酸疫苗的发展前景等问题,从而为核酸疫苗的发展提供了新思路和新途径。 相似文献
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Vandenberg GW 《Animal health research reviews / Conference of Research Workers in Animal Diseases》2004,5(2):301-304
Aquaculture is the fastest growing food-producing sector, providing an acceptable supplement to and substitute for wild fish and plants. Increased production intensification, particularly in high-value species, involves substantial stress, which, as in other captive livestock species, has resulted in outbreaks of major diseases and related mortalities. Widespread use of antibiotics has led to the development of antibiotic-resistant bacteria and the accumulation of antibiotics in the environment and the flesh of fish. Thus, recently effort has been dedicated to vaccine development. Vaccination in fish is complicated by their aquatic environment. Individual injections are labor-intensive and stressful, since fish have to be removed from the water and anaesthetized. Some vaccines offer a limited duration of protection, and thus booster applications are required. In salmonid species, many commercial vaccines use oil-based adjuvants, resulting in a greatly improved duration of protection. However, oil-based adjuvants have been related to significant growth depression, internal adhesions and injection site melanization, resulting in carcass downgrading. Oral administration to aquatic species is by far the most appealing method of vaccine delivery: there is no handling of the fish, which reduces stress; and administration is easy and suitable for mass immunization. However, few oral vaccines have been commercialized, due in part to the increased quantity of antigen required to provoke an immune response, and the lack of an adequate duration of protection. For effective oral delivery, protective antigens must avoid digestive hydrolysis and be taken up in the hindgut in order to induce an effective protective immune response. Antigen encapsulation technologies have been used to protect antigen; however, such strategies can be expensive and are not always effective. Alternative approaches, currently under development, are discussed. 相似文献
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DNA vaccination against influenza viruses: a review with emphasis on equine and swine influenza 总被引:2,自引:0,他引:2
Olsen CW 《Veterinary microbiology》2000,74(1-2):149-164
The influenza virus vaccines that are commercially-available for humans, horses and pigs in the United States are inactivated, whole-virus or subunit vaccines. While these vaccines may decrease the incidence and severity of clinical disease, they do not consistently provide complete protection from virus infection. DNA vaccines are a novel alternative to conventional vaccination strategies, and offer many of the potential benefits of live virus vaccines without their risks. In particular, because immunogens are synthesized de novo within DNA transfected cells, antigen can be presented by MHC class I and II molecules, resulting in stimulation of both humoral and cellular immune responses. Influenza virus has been used extensively as a model pathogen in DNA vaccine studies in mice, chickens, ferrets, pigs, horses and non-human primates, and clinical trials of DNA-based influenza virus vaccines are underway in humans. Our studies have focused on gene gun delivery of DNA vaccines against equine and swine influenza viruses in mice, ponies and pigs, including studies employing co-administration of interleukin-6 DNA as an approach for modulating and adjuvanting influenza virus hemagglutinin-specific immune responses. The results indicate that gene gun administration of plasmids encoding hemagglutinin genes from influenza viruses is an effective method for priming and/or inducing virus-specific immune responses, and for providing partial to complete protection from challenge infection in mice, horses and pigs. In addition, studies of interleukin-6 DNA co-administration in mice clearly demonstrate the potential for this approach to enhance vaccine efficacy and protection. 相似文献
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Mucosal immunization is advantageous over other routes of antigen delivery because it can induce both mucosal and systemic immune responses. In this study, we have developed fimbriae protein of enterotoxigenic Escherichia coli (ETEC) F41 was stably expressed on the surface Lactobacillus casei 525. The method of expressing vaccine antigens in L. casei induces both systemic and mucosal immunity after oral or intranasal administration. We demonstrate that an oral or intranasal vaccine based on live recombinant L. casei 525 protects infant mice from ETEC F41 infection. This platform technology can be applied to design oral or intranasal vaccine delivery vehicles against several microbial pathogens. 相似文献
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寄生虫病严重影响全球人类、动物的健康安全,所带来的经济损失巨大。因此,有必要研制针对寄生虫病的疫苗,以阻断寄生虫病在动物与动物、动物与人类之间的传播。寄生虫存在多种免疫逃避机制,已开发的亚单位疫苗、减毒活疫苗、灭活疫苗均未达到理想的预防效果,且商品化疫苗多为针剂疫苗,普通针剂疫苗操作繁琐、运输储藏要求高且易使动物发生应激,直接影响经济成本,因此在实际生产当中需更多操作简单、便于储存、免疫成本更低的新型疫苗,以有效防控寄生虫病。诸多研究表明口服疫苗操作方便,只需通过口服方式投喂且宿主获得的抗体效价水平较高,有望成为预防寄生虫病的有效手段。口服疫苗是一种新型疫苗,依靠宿主的黏膜免疫系统来产生作用,即通过机体黏膜表面接种便可同时诱导机体产生持久的黏膜免疫、体液免疫和细胞免疫,为宿主提供高效的免疫保护。与传统疫苗相比,口服疫苗最显著的优点就是便于接种且应激小,还能形成强大的黏膜免疫屏障。但胃肠道的环境及易形成免疫耐受等因素也为口服疫苗的开发带来很大的挑战。笔者就黏膜免疫系统与口服疫苗作用机理、近几年寄生虫口服疫苗的研究进展及优点与挑战进行综述,以期为寄生虫口服疫苗的开发提供理论依据。 相似文献
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New approaches in vaccine development 总被引:4,自引:0,他引:4
Leclerc C 《Comparative immunology, microbiology and infectious diseases》2003,26(5-6):329-341
In the last century, vaccines have been one of the most powerful tools for preventing infectious diseases. Smallpox has been eradicated and other diseases such as poliomyelitis or measles have been reduced to very low levels in many regions of the world. However, infectious diseases remain the leading cause of death worldwide. Thus, the development of vaccines to prevent diseases for which no vaccine currently exists such as AIDS or malaria as well as the improvement of efficacy and safety of existing vaccines remains a high priority. Achieving such ambitious goals in a near future will certainly require a strong modification of the methods that have been used so far to identify vaccine candidates. In particular, modern vaccinology could strongly benefit of the latest developments of molecular biology and immunology. Here, we will discuss some potential applications of the increasing knowledge of pathogen genomes as well as the immune system for the discovery of new antigenic targets and the development of new strategies of vaccination. 相似文献
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禽类DNA疫苗研究进展 总被引:2,自引:0,他引:2
新型疫苗的研究对于禽类传染病的防制意义重大。传统疫苗是基于抗原刺激机体产生特异性抗体的原理,它们大多数激发机体的体液免疫,很难启动细胞免疫。脱氧核糖核酸(DNA)疫苗作为第3代疫苗,具备传统疫苗和其它基因工程苗不可比拟的优点,能够诱导全方位的免疫反应且使用更安全更方便,DNA疫苗是将外源基因与真核质粒重组后直接导入细胞内,使外源基因在宿主细胞内表达合成保护性抗原蛋白。这是模拟病毒自然感染提呈过程,既能产生细胞免疫,又能产生体液免疫。文章对DNA疫苗在禽类应用的可行性和应用研究新进展作了综述。 相似文献
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In ovo vaccination is an alternative approach to post-hatch vaccination of chickens, particularly in broilers. Vaccination at embryonation day 18 helps to 'close the window' of susceptibility i.e. the time between vaccination and early exposure to infectious agents compared with post-hatch vaccination. Attempts on embryonal vaccination as a mode of vaccine delivery were approached from the observation that chickens already develop certain immunologic functions before hatching. The immune system in birds begins to develop early during embryogenesis and various immune reactions have been induced in the late stage chicken embryos. Compared with post-hatch vaccination, in ovo vaccination stimulates both the innate and adaptive immune responses with the advantage that because of the prenatal immunization, in ovo vaccinated chicks have developed an appreciable degree of protection by the time of hatch. Effects of maternal antibodies on vaccines to be used for in ovo vaccination can be prevented by developing vaccines that are insensitive to maternal antibodies. It has been described that vaccination of chicken embryos at embryonation day 18 did not significantly affect the immune competence of hatched chickens. The apparent absence of tolerance in chicks hatched from embryos exposed to an antigen at the late stage of embryonation implies the feasibility of in ovo vaccination. Investigations on in ovo vaccination to produce safe and efficient vaccines are still in progress. Currently a large number of vaccines are under investigation for viral, bacterial and protozoal diseases. 相似文献
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寄生虫病带来了相当大的社会经济影响,人畜共患寄生虫给人们带来巨大的疾病负担,并给养殖业造成严重的经济损失。因此,寄生虫病的防治是人们迫切需要研究的课题。寄生虫存在很多形式的免疫逃避机制,灭活疫苗、减毒活疫苗、亚单位疫苗等未达到理想的预防寄生虫病的效果,很多研究表明DNA疫苗有望成为预防和治疗寄生虫病的有效方法。DNA疫苗是一种新型疫苗,可同时诱导机体产生持久的体液免疫和细胞免疫,通过在宿主内表达外源蛋白来提供保护性免疫。DNA疫苗与其他亚单位疫苗不同的是,免疫原由摄取抗原编码DNA的细胞在宿主内合成。体内蛋白质的合成也能进行抗原加工、修饰并递呈到宿主的免疫系统中,类似于自然感染的方式。笔者就DNA疫苗免疫机制、设计原则、免疫途径、优缺点及近几年寄生虫DNA疫苗的研究进展进行综述,以期为寄生虫DNA疫苗的开发提供理论参考。 相似文献
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Combadière B Mahé B 《Comparative immunology, microbiology and infectious diseases》2008,31(2-3):293-315
Immunization concepts evolve with increasing knowledge of how the immune system works and the development of new vaccination methods. Traditional vaccines are made of live, attenuated, killed or fragmented pathogens. New vaccine strategies can take advantage of particulate compounds—microspheres or nanoparticles—to target antigen-presenting cells better, which must subsequently reach the secondary lymphoid organs, which are the sites of the immune response. The use of the skin as a target organ for vaccine delivery stems from the fact that immature dendritic cells (DCs), which are professional antigen-presenting cells can be found at high density in the epidermis and dermis of human or animal skin. This has led to design various methods of dermal or transcutaneous vaccination. The quality and duration of the humoral and cellular responses to vaccination depend on the appropriate targeting of antigen-presenting cells, of the vaccine dose, route of administration and use of adjuvant. In this review, we will focus on the use of micro- and nano-particles to target the skin antigen-presenting cells and will discuss recent advances in the field of transcutaneous vaccination in animal models and humans. 相似文献
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非洲猪瘟(ASF)自2018年8月在我国暴发,对养猪业构成巨大威胁.该病是由非洲猪瘟病毒(ASFV)引起的家养猪高热、急性和高死亡率的出血症和淋巴组织坏死症;认识和了解病原ASFV与宿主的相互作用是理解致病机制的基础和疫病防控的前提.本文对ASFV与宿主细胞受体和内体系统的互作、基因转录和蛋白合成系统的互作、细胞凋亡和内质网应激系统的互作、天然免疫干扰素应答系统的互作、抗原递呈细胞的互作五个方面现有研究进展进行综述;并试图在此基础上理解ASFV的免疫保护和免疫逃逸作用,思考ASFV与宿主互作中需要回答的问题,为研制保护性疫苗和深入认识ASF致病机制提供线索. 相似文献
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Mucosal vaccination is proving to be one of the greatest challenges in modern vaccine development. Although highly beneficial for achieving protective immunity, the induction of mucosal immunity, especially in the gastro-intestinal tract, still remains a difficult task. As a result, only very few mucosal vaccines are commercially available for domestic animals. Here, we critically review various strategies for mucosal delivery of vaccines in domestic animals. This includes live bacterial and viral vectors, particulate delivery-systems such as polymers, alginate, polyphosphazenes, immune stimulating complex and liposomes, and receptor mediated-targeting strategies to the mucosal tissues. The most commonly used routes of immunization, strategies for delivering the antigen to the mucosal surfaces, and future prospects in the development of mucosal vaccines are discussed. 相似文献
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Torché AM Le Dimna M Le Corre P Mesplède A Le Gal S Cariolet R Le Potier MF 《Veterinary immunology and immunopathology》2006,109(3-4):209-217
Oral vaccination of large animals using PLGA MS (poly(D,L-lactide-co-glycolide)microspheres) appeared to be more challenging than immunization of mice. The purpose of this study was to deliver to GALT an immunogenic model protein (IgY), free or encapsulated by spray-drying in PLGA MS, and to evaluate systemic immune response in SPF Large White pigs. Pigs were surgically processed for local administration of IgY in three sets of experiments. In two sets of experiments, administration was locally performed in temporary ligatured intestinal segments, in jejunal Peyer's patches and in mesenteric lymph nodes. In the third experiment, pigs received IgY via an intestinal cannula. Total IgY-specific antibodies were detected in the sera of pigs after a single local immunization, but not in the sera of cannulated pigs. The study of IgG1 and IgG2 isotypes indicated that PLGA MS are able to elicit a combined serum IgG2/G1 response with a predominance of IgG1 response when locally administered. PLGA MS can be a potential oral delivery system for antigen but our results underlined the difficulty to immunize large animals like pigs. Transposition of data between small and large animals appears to be complex and suggests that physiological features need to be considered to increase intestinal availability of oral encapsulated vaccines. 相似文献
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Dunham SP 《Research in veterinary science》2002,73(1):9-16
Nucleic acid immunisation entails the delivery of DNA (or RNA) encoding a vaccine antigen to the recipient. The DNA is taken up by host cells and transcribed to mRNA, from which the vaccine proteins are then translated. The expressed proteins are recognised as foreign by the host immune system and elicit an immune response, which may have both cell-mediated and humoral components. DNA vaccines offer a number of advantages over conventional vaccines, including ease of production, stability and cost. They also allow the production of vaccines against organisms which are difficult or dangerous to culture in the laboratory. This review describes the principles of DNA vaccination and the application of DNA vaccines to veterinary species. Although a great deal of developmental work is required before the technology can give rise to commercial vaccines in domestic animals, there is ongoing research in many fields and it is expected that a number of exciting developments will arise in the next decade. 相似文献
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ABSTRACT: Staphylococcus aureus is an important cause of nosocomial and community-acquired infections in humans and animals, as well as the cause of mastitis in dairy cattle. Vaccines aimed at preventing S. aureus infection in bovine mastitis have been studied for many years, but have so far been unsuccessful due to the complexity of the bacteria, and the lack of suitable vaccine delivery vehicles. The current study developed an Escherichia coli protein expression system that produced a recombinant staphylococcal enterotoxin A (rSEA) encapsulated into biodegradable microparticles generated by polylactic-co-glycolic acid (PLGA) dissolved in methylene chloride and stabilized with polyvinyl acetate. Antigen loading and surface properties of the microparticles were investigated to optimize particle preparation protocols. The prepared PLGA-rSEA microspheres had a diameter of approximately 5 μm with a smooth and regular surface. The immunogenicity of the PLGA-rSEA vaccine was assessed using mice as an animal model and showed that the vaccine induced a strong humoral immune response and increased the percent survival of challenged mice and bacterial clearance. Histological analysis showed moderate impairment caused by the pathogen upon challenge afforded by immunization with PLGA-rSEA microspheres. Antibody titer in the sera of mice immunized with PLGA-rSEA microparticles was higher than in vaccinated mice with rSEA. In conclusion, the PLGA-rSEA microparticle vaccine developed here could potentially be used as a vaccine against enterotoxigenic S. aureus. 相似文献
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Brucellosis causes serious economic losses to goat farmers by way of reproductive losses in the form of abortions and stillbirths. Nucleic acid vaccines provide an exciting approach for antigen presentation to the immune system. In this study, we evaluated the ability of DNA vaccine encoding the omp31 protein of Brucella melitensis 16M to induce cellular and humoral immune responses in mice. We constructed eukaryotic expression vectors called pTargeTomp31, encoding outer membrane protein (omp31) of B. melitensis 16M. pTargeTomp31 was injected intramuscularly three times, at 3-week intervals in groups of mice 6 weeks of age. pTargeTomp31 induced good antibody response in ELISA . pTargeTomp31 elicited a T-cell-proliferative response and also induced a strong gamma interferon production upon restimulation with either the omp31 antigen or B. melitensis 16M extract. We also demonstrate that animals immunized with this plasmid elicited a strong and long-lived memory immune response. Furthermore, pTargeTomp31 elicited a typical T-helper 1-dominated immune response in mice, as determined by immunoglobulin G isotype analysis. This vaccine also provided the moderate degree of protection to the mice. This study for the first time focuses on DNA immunization of a gene from B. melitensis. These results may lead to the development of a DNA-based vaccine for the control of brucellosis in goats. 相似文献