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Study of the Antimicrobial Activity of Tilapia Piscidin 3 (TP3) and TP4 and Their Effects on Immune Functions in Hybrid Tilapia (Oreochromis spp.)

机译:罗非鱼罗非鱼3(TP3)和TP4的抗菌活性及其对杂交罗非鱼(Oreochromis spp。)免疫功能的影响的研究

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摘要

To address the growing concern over antibiotic-resistant microbial infections in aquatic animals, we tested several promising alternative agents that have emerged as new drug candidates. Specifically, the tilapia piscidins are a group of peptides that possess antimicrobial, wound-healing, and antitumor functions. In this study, we focused on tilapia piscidin 3 (TP3) and TP4, which are peptides derived from Oreochromis niloticus, and investigated their inhibition of acute bacterial infections by infecting hybrid tilapia (Oreochromis spp.) with Vibrio vulnificus and evaluating the protective effects of pre-treating, co-treating, and post-treating fish with TP3 and TP4. In vivo experiments showed that co-treatment with V. vulnificus and TP3 (20 μg/fish) or TP4 (20 μg/fish) achieved 95.3% and 88.9% survival rates, respectively, after seven days. When we co-injected TP3 or TP4 and V. vulnificus into tilapia and then re-challenged the fish with V. vulnificus after 28 days, the tilapia exhibited survival rates of 35.6% and 42.2%, respectively. Pre-treatment with TP3 (30 μg/fish) or TP4 (20 μg/fish) for 30 minutes prior to V. vulnificus infection resulted in high survival rates of 28.9% and 37.8%, respectively, while post-treatment with TP3 (20 μg/fish or 30 μg/fish) or TP4 (20 μg/fish) 30 minutes after V. vulnificus infection yielded high survival rates of 33.3% and 48.9%. In summary, pre-treating, co-treating, and post-treating fish with TP3 or TP4 all effectively decreased the number of V. vulnificus bacteria and promoted significantly lower mortality rates in tilapia. The minimum inhibitory concentrations (MICs) of TP3 and TP4 that were effective for treating fish infected with V. vulnificus were 7.8 and 62.5 μg/ml, respectively, whereas the MICs of kanamycin and ampicillin were 31.2 and 3.91 μg/ml. The antimicrobial activity of these peptides was confirmed by transmission electron microscopy (TEM) and scanning electron microscopy (SEM), both of which showed that V. vulnificus disrupted the outer membranes of cells, resulting in the loss of cell shape and integrity. We examined whether TP3 and TP4 increased the membrane permeability of V. vulnificus by measuring the fluorescence resulting from the uptake of 1-N-phenyl-naphthylamine (NPN). Treating fish with TP3 and TP4 under different pH and temperature conditions did not significantly increase MIC values, suggesting that temperature and the acid-base environment do not affect AMP function. In addition, the qPCR results showed that TP3 and TP4 influence the expression of immune-responsive genes, including interleukin (IL)-1β, IL-6, and IL-8. In this study, we demonstrate that TP3 and TP4 show potential for development as drugs to combat fish bacterial infections in aquaculture.
机译:为了解决对水生动物中抗生素抗药性微生物感染的日益关注的问题,我们测试了几种有前途的替代药物,这些替代药物已成为新的候选药物。具体地说,罗非鱼piscidins是一组具有抗菌,伤口愈合和抗肿瘤功能的肽。在这项研究中,我们集中于罗非鱼piscidin 3(TP3)和TP4,它们是尼罗罗非鱼(Oreochromis niloticus)衍生的肽,并研究了通过用创伤弧菌感染杂交罗非鱼(Oreochromis spp。)并评估其对罗非鱼的急性细菌感染抑制作用。用TP3和TP4对鱼进行前处理,共处理和后处理。体内实验表明,在7天后,与创伤弧菌和TP3(20μg/鱼)或TP4(20μg/鱼)共同治疗分别达到95.3%和88.9%的存活率。当我们将TP3或TP4和V. vulnificus共同注入罗非鱼中,然后在28天后用V. vulnificus对鱼进行再攻击时,罗非鱼的存活率分别为35.6%和42.2%。在创伤弧菌感染前用TP3(30μg/鱼)或TP4(20μg/鱼)预处理30分钟,分别导致高存活率,分别为28.9%和37.8%,而用TP3(20 V. vulnificus感染后30分钟,每公斤鱼或30 µg /鱼)或TP4(20 µg /鱼)产生了33.3%和48.9%的高存活率。总之,用TP3或TP4对鱼进行前处理,共处理和后处理均能有效减少V. vulnificus细菌的数量,并显着降低罗非鱼的死亡率。 TP3和TP4的最小抑菌浓度(MICs)对治疗受 V 感染的鱼有效。 vulnificus 分别为7.8和62.5μg/ ml,而卡那霉素和氨苄青霉素的MIC分别为31.2和3.91μg/ ml。通过透射电子显微镜(TEM)和扫描电子显微镜(SEM)证实了这些肽的抗菌活性,两者均显示 V vulnificus 破坏了细胞的外膜,导致细胞形状和完整性的丧失。我们检查了TP3和TP4是否增加了 V 的膜通透性。通过测量摄取1-N-苯基-萘胺(NPN)产生的荧光来检测 vulnificus 。在不同的pH和温度条件下用TP3和TP4处理鱼并没有显着增加MIC值,这表明温度和酸碱环境不会影响AMP功能。此外,qPCR结果显示TP3和TP4影响免疫应答基因的表达,包括白介素(IL)-1β,IL-6和IL-8。在这项研究中,我们证明了TP3和TP4具有发展潜力,可作为对抗水产养殖中鱼类细菌感染的药物。

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