Attempts to Stimulate Immunology Responses by Intramuscular and Intraperitoneal Delivery of EPS-Adjuvanted Mannheimiosis Vaccine

Q3 Veterinary

American Journal of Animal and Veterinary Sciences Pub Date : 2022-04-01 DOI:10.3844/ajavsp.2022.322.331

Ghaith Hussein Mansour, L. Razzak, H. Sheikh, Mohd Effendy ABD WAHID

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引用次数: 1

Abstract

: This study was conducted on 48 male Sprague Dawley rats to determine the immunological responses of experimental adjuvanted vaccines of Mannheimia haemolytica A2 ( M. haemolytica A2) injection and to observe their protection level upon live M. haemolytica A2 challenge. Forty-eight clinically healthy Sprague Dawley rats were divided into four groups; Groups 1 and 2 were vaccinated intramuscularly and intraperitoneally, respectively, with an Exo-Polysaccharide (EPS)-adjuvanted vaccine prepared from formalin-killed M. haemolytica serotypes A2, Group 3 with formalin killed M . haemolytica seed. At the same time, Group 4 received intraperitoneally Phosphate Buffer Saline (PBS) as a control. After the first vaccination dose, Groups 1,2, and 3 showed a gradual increase in IgM, IgG, and IgA levels significantly (p<0.05). However, their level started to decline six weeks post-vaccination, indicating that the booster dose was needed. Upon the delivery of the second booster dose, antibodies titer showed a persistent increase significantly (p<0.05), especially the serum IgG level. All groups were challenged with live virulent Mannheimia haemolytica A2 after the level of antibodies declined twice after the second booster was delivered. No rat deaths were found in the Combined EPS - M. haemolytica adjuvant vaccine after 14 days following the challenge (0%). In unvaccinated rats, higher mortality and morbidity were noted (100%) and less was reported in rats receiving M. haemolytica A2 Vaccine seed (8%). Histologically at two weeks, post-challenge revealed negligible lung lesions in groups 1 and 2 and mild lesions in group 3. Lung lesions were recorded in all unvaccinated control rats. Furthermore, M. haemolytica A2 re-isolated successfully from lung samples in groups 3 and 4. In conclusion, Rats receiving adjuvant- M. haemolytica vaccine confers reasonably high preventive efficacy compared to M. haemolytica A2 by itself. Further studies should be conducted on measuring the antibody titer in different vivo, such as goats or sheep.

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通过肌肉和腹腔注射eps佐剂男子汉贫血症疫苗刺激免疫反应的尝试

本研究对48只雄性Sprague Dawley大鼠进行了实验，以确定溶血曼海姆病A2 (M. haemolytica A2)佐剂实验性疫苗注射的免疫应答，并观察其对溶血曼海姆病A2活体攻击的保护水平。48只临床健康的Sprague Dawley大鼠分为4组;第1组和第2组分别接种由福尔马林灭活的溶血分枝杆菌血清型A2制备的外源性多糖(EPS)佐剂疫苗，肌肉和腹腔注射。haemolytica种子。同时，第4组腹腔注射磷酸缓冲盐水(PBS)作为对照。第一次接种后，1、2、3组IgM、IgG、IgA水平逐渐升高，差异均有统计学意义(p<0.05)。然而，它们的水平在接种疫苗六周后开始下降，表明需要加强剂量。在第二次加强剂量后，抗体滴度持续显著升高(p<0.05)，尤其是血清IgG水平。在第二次增强后抗体水平下降两次后，所有组都用活的毒力溶血曼海氏症A2进行攻击。接种EPS -溶血分枝杆菌联合佐剂疫苗14天后未发现大鼠死亡(0%)。在未接种疫苗的大鼠中，死亡率和发病率较高(100%)，而接受溶血支原体A2疫苗种子的大鼠报告的死亡率和发病率较低(8%)。两周后的组织学显示，1组和2组的肺部病变可以忽略不计，而3组的病变较轻。所有未接种疫苗的对照大鼠均记录肺病变。此外，从第3组和第4组的肺样本中成功分离出溶血分枝杆菌A2。综上所述，与单独接种溶血支原体A2相比，大鼠接种佐剂-溶血支原体疫苗具有较高的预防效果。在不同的体内，如山羊或绵羊，抗体效价的测定有待进一步的研究。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

American Journal of Animal and Veterinary Sciences Veterinary-Veterinary (all)

CiteScore

1.90

自引率

0.00%

发文量

期刊介绍： American Journal of Animal and Veterinary Sciences, a quarterly, peer reviewed publication and is dedicated for publication of research articles in the field of biology of animals and with the scientific understanding of how animals work: from the physiology and biochemistry of tissues and major organ systems down to the structure and function of bio molecules and cells; particular emphasis would given to the studies of growth, reproduction, nutrition and lactation of farm and companion animals and how these processes may be optimized to improve animal re- productivity, health and welfare. Articles in support areas, such as genetics, soils, agricultural economics and marketing, legal aspects and the environment also are encouraged. AJAVS is an important source of researcher to study articles on protection of animal production practices, herd health and monitoring the spread of disease and prevention in both domestic and wild animals.