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在具有不同抗菌活性的拟穴青蟹中,SpCrus3和SpCrus4具有高度相似性。

SpCrus3 and SpCrus4 share high similarity in mud crab (Scylla paramamosain) exhibiting different antibacterial activities.

作者信息

Wang Yue, Zhang Xiao-Wen, Wang Hui, Fang Wen-Hong, Ma Hongyu, Zhang Fengxia, Wang Yuan, Li Xin-Cang

机构信息

East China Sea Fisheries Research Institute, Chinese Academy of Fishery Sciences, Key Laboratory of East China Sea Fishery Resources Exploitation, Ministry of Agriculture, Shanghai, 200090, China; College of Life Science, Henan Normal University, Xinxiang, Henan, 453007, China.

College of Life Science, Henan Normal University, Xinxiang, Henan, 453007, China.

出版信息

Dev Comp Immunol. 2018 May;82:139-151. doi: 10.1016/j.dci.2018.01.006. Epub 2018 Jan 17.

Abstract

Type I crustins are crucial effectors of crustacean immune system. Various type I crustins with high sequence diversity possess different antimicrobial activities. To date, the mechanism on how the sequence diversity of type I crustins affects their antimicrobial activities is largely unclear, and how different crustins function together against bacterial invasion still remains unknown. In this study, we identified two novel type I crustins, namely, SpCrus3 and SpCrus4, from an economically important crab, Scylla paramamosain. Either SpCrus3 or SpCrus4 was highly expressed in gill. After challenges with Vibrio parahemolyticus or Staphylococcus aureus, SpCrus4 was up-regulated, whereas SpCrus3 was down-regulated. No significant expression change of SpCrus3 and SpCrus4 was observed after white spot syndrome virus injection, suggesting that these two genes may not participate in the antiviral immune responses. SpCrus3 and SpCrus4 had the common 5' terminus and high similarity of 66.06%, but SpCrus4 exhibited stronger antimicrobial activity than that of SpCrus3. Microorganism-binding assay results revealed that both SpCrus3 and SpCrus4 exhibited binding ability to all tested microorganisms. Furthermore, the polysaccharide-binding assay showed that these two proteins exhibited strong binding activity to bacterial polysaccharides, such as lipopolysaccharide (LPS), lipoteichoic acid (LTA), and peptidoglycan (PGN). SpCrus3 and SpCrus4 exhibited stronger binding activity to LPS or LTA than to PGN. Moreover, SpCrus4 showed stronger binding activity to LTA than that of SpCrus3, which may be responsible for the significantly distinct antimicrobial activity between these two proteins. In addition, SpCrus4 displayed stronger agglutination activity against several kinds of microorganisms than that of SpCrus3. This increased agglutination activity may also contribute to the strong antibacterial activity of SpCrus4. On the basis of all these results, a possible antibacterial mode exerted by SpCrus3 and SpCrus4 was proposed as follows. SpCrus3 was highly expressed in normal crabs to maintain low-level antibacterial activity without bacterial challenges. When crabs were challenged with bacteria, large amount of SpCrus4 was generated to exhibit strong antibacterial activity against bacterial invasion. This study provides new insights to understand the antibacterial functions and mechanisms of type I crustins.

摘要

I型抗真菌肽是甲壳类动物免疫系统的关键效应分子。各种具有高度序列多样性的I型抗真菌肽具有不同的抗菌活性。迄今为止,I型抗真菌肽的序列多样性如何影响其抗菌活性的机制尚不清楚,不同的抗真菌肽如何协同作用抵抗细菌入侵也仍然未知。在本研究中,我们从一种经济上重要的螃蟹——拟穴青蟹中鉴定出两种新型I型抗真菌肽,即SpCrus3和SpCrus4。SpCrus3和SpCrus4在鳃中均高表达。在用副溶血性弧菌或金黄色葡萄球菌攻毒后,SpCrus4表达上调,而SpCrus3表达下调。注射白斑综合征病毒后,未观察到SpCrus3和SpCrus4的表达有显著变化,表明这两个基因可能不参与抗病毒免疫反应。SpCrus3和SpCrus4具有共同的5'末端,相似度高达66.06%,但SpCrus4表现出比SpCrus3更强的抗菌活性。微生物结合试验结果表明,SpCrus3和SpCrus4对所有测试微生物均表现出结合能力。此外,多糖结合试验表明,这两种蛋白质对细菌多糖,如脂多糖(LPS)、脂磷壁酸(LTA)和肽聚糖(PGN)表现出很强的结合活性。SpCrus3和SpCrus4对LPS或LTA的结合活性比对PGN更强。此外,SpCrus4对LTA的结合活性比SpCrus3更强,这可能是这两种蛋白质抗菌活性显著不同的原因。此外,SpCrus4对几种微生物的凝集活性比SpCrus3更强。这种增强的凝集活性也可能有助于SpCrus4的强抗菌活性。基于所有这些结果,提出了SpCrus3和SpCrus4可能的抗菌模式如下。SpCrus3在正常螃蟹中高表达,以维持在无细菌攻毒情况下的低水平抗菌活性。当螃蟹受到细菌攻毒时,会产生大量的SpCrus4以表现出对细菌入侵的强抗菌活性。本研究为理解I型抗真菌肽的抗菌功能和机制提供了新的见解。

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