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首页> 外文期刊>Saudi Journal of Biological Sciences >Efficacy of bacteriophage Lysed Pasteurella marker vaccine in laboratory animal models with a novel DIVA for haemorrhagic septicaemia
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Efficacy of bacteriophage Lysed Pasteurella marker vaccine in laboratory animal models with a novel DIVA for haemorrhagic septicaemia

机译:新型DIVA噬菌体裂解巴氏杆菌标记疫苗在实验动物模型中对出血性败血病的功效

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Objective The present study aimed at evaluating the efficacy of an improved phage lysate marker vaccine for haemorrhagic septicaemia in mice and rabbit model and development of a DIVA ELISA based on iron restricted outer membrane protein (IROMP). Method The experimental vaccine was prepared by lysing P. multocida B:2 grown under iron restricted conditions with a Pasteurella b acteriophage and addition of an alum adjuvant to enhance the immunogenicity. The vaccine was administered in mice and rabbits divided into two group each. Phage lysate vaccine (PL-VacI) was administered to group I mice and rabbits whereas group II mice and rabbits received alum precipitated HS vaccine (HS-VacII). Antibody titres were monitored 0, 30, 60, 90, 210 and 240?dpv. An IROMP (130?kDa) based indirect ELISA was also developed to differentiate between infected and vaccinated animals. The Pasteurella phage isolated in present study was sequenced at Georgia Genomic Facilty, Georgia. Result The sequence of PMP-GAD-IND ( Pasteurella bacteriophage) was deposited in GenBank under no KY203335. The group I mice and rabbits vaccinated with Phage lysate vaccine (PL-VacI) group revealed significantly higher antibody titres than group II mice and rabbits receiving alum-precipitated bacterin (HS-VacII) by MAT, IHA and ELISA (P??0.05 and P??0.001). The peak log sub10/sub values (3.46) in case of group I mice by ELISA were attained at 90DPI whereas in group II mice the peak values at 90DPI were 2.82. Mean logsub10/sub titres by ELISA in group I and II rabbits were 2.43 and 2.35 respectively at 30DPI whereas at 120DPI the titres were 3.29 and 2.75, respectively. The DIVA ELISA detected presence of a novel 137?kDa IROMP/siderophore antibody in sera of group I mice and rabbits (PL-VacI) absent in sera of mice and rabbits given HS-VacII. Conclusion The bacteriophage based marker vaccine (PL-VacI) had a more effective and longer immune response against HS in mice and rabbit in comparison to the widely used alum precipitated HS vaccine (HS-VacII). Moreover, the development of a recombinant IROMP based indirect ELISA could serve as an excellent tool to differentiate between infected and vaccinated cattle and buffaloes for effective control of HS.
机译:目的本研究旨在评估改良的噬菌体裂解物标志物疫苗对小鼠和兔模型出血性败血病的功效,并开发基于铁限制外膜蛋白(IROMP)的DIVA ELISA。方法通过用巴斯德氏菌噬菌体裂解在铁限制条件下生长的多杀毕赤酵母B:2并添加明矾佐剂以增强免疫原性来制备实验疫苗。该疫苗分别在小鼠和兔子中分为两组。将噬菌体裂解物疫苗(PL-VacI)给予I组小鼠和兔子,而II组小鼠和兔则接受明矾沉淀的HS疫苗(HS-VacII)。监测抗体滴度0、30、60、90、210和240?dpv。还开发了基于IROMP(130?kDa)的间接ELISA来区分感染和接种的动物。在本研究中分离出的巴斯德氏菌噬菌体在佐治亚州佐治亚州基因组实验室进行了测序。结果PMP-GAD-IND(巴斯德氏杆菌噬菌体)的序列保藏在GenBank中,编号为KY203335。接种了噬菌体裂解物疫苗(PL-VacI)的I组小鼠和兔子的抗体效价显着高于通过MAT,IHA和ELISA接受明矾细菌素(HS-VacII)的II组小鼠和兔子(P <0.05并且P≤<0.001)。通过ELISA,I组小鼠在90DPI时达到log log 10 峰值(3.46),而II组小鼠在90DPI时达到2.82。用ELISA法测定的I和II组兔子在30DPI时的平均log 10 滴度分别为2.43和2.35,而在120DPI时的滴度分别为3.29和2.75。 DIVA ELISA检测到在给予HS-VacII的小鼠和兔子的血清中不存在I组小鼠和兔子的血清(PL-VacI)中存在新的137?kDa IROMP /铁载体抗体。结论与广泛使用的明矾沉淀HS疫苗(HS-VacII)相比,基于噬菌体的标记疫苗(PL-VacI)在小鼠和兔子中具有更有效,更长的针对HS的免疫反应。此外,基于重组IROMP的间接ELISA的开发可以作为区分感染和接种牛与水牛以有效控制HS的极佳工具。

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