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腔肠动物珊瑚先天免疫对弧菌病的反应。

Innate immune responses of a scleractinian coral to vibriosis.

机构信息

UMR 5244, CNRS UPVD EPHE, Université de Perpignan Via Domitia, 66000 Perpignan, France.

出版信息

J Biol Chem. 2011 Jun 24;286(25):22688-98. doi: 10.1074/jbc.M110.216358. Epub 2011 May 2.

Abstract

Scleractinian corals are the most basal eumetazoan taxon and provide the biological and physical framework for coral reefs, which are among the most diverse of all ecosystems. Over the past three decades and coincident with climate change, these phototrophic symbiotic organisms have been subject to increasingly frequent and severe diseases, which are now geographically widespread and a major threat to these ecosystems. Although coral immunity has been the subject of increasing study, the available information remains fragmentary, especially with respect to coral antimicrobial responses. In this study, we characterized damicornin from Pocillopora damicornis, the first scleractinian antimicrobial peptide (AMP) to be reported. We found that its precursor has a segmented organization comprising a signal peptide, an acidic proregion, and the C-terminal AMP. The 40-residue AMP is cationic, C-terminally amidated, and characterized by the presence of six cysteine molecules joined by three intramolecular disulfide bridges. Its cysteine array is common to another AMP and toxins from cnidarians; this suggests a common ancestor, as has been proposed for AMPs and toxins from arthropods. Damicornin was active in vitro against Gram-positive bacteria and the fungus Fusarium oxysporum. Damicornin expression was studied using a combination of immunohistochemistry, reverse phase HPLC, and quantitative RT-PCR. Our data show that damicornin is constitutively transcribed in ectodermal granular cells, where it is stored, and further released in response to nonpathogenic immune challenge. Damicornin gene expression was repressed by the coral pathogen Vibrio coralliilyticus. This is the first evidence of AMP gene repression in a host-Vibrio interaction.

摘要

石珊瑚是最原始的后生动物类群,为珊瑚礁提供了生物和物理框架,而珊瑚礁是所有生态系统中最多样化的生态系统之一。在过去的三十年中,与气候变化同时发生,这些光合共生生物经常受到越来越频繁和严重的疾病的影响,这些疾病现在在地理上广泛分布,是这些生态系统的主要威胁。尽管珊瑚的免疫功能一直是研究的主题,但现有的信息仍然很零散,尤其是关于珊瑚抗菌反应的信息。在这项研究中,我们从鹿角珊瑚(Pocillopora damicornis)中鉴定了鹿角珊瑚素,这是第一种被报道的石珊瑚抗菌肽(AMP)。我们发现,其前体具有分段组织,包括信号肽、酸性前区和 C 端 AMP。该 40 个残基的 AMP 带正电荷,C 端酰胺化,并具有六个半胱氨酸分子通过三个分子内二硫键连接的特征。其半胱氨酸排列与另一种 AMP 和来自刺胞动物的毒素相同;这表明存在共同的祖先,正如从节肢动物中分离出的 AMP 和毒素所提出的那样。鹿角珊瑚素在体外对革兰氏阳性菌和真菌镰刀菌(Fusarium oxysporum)具有活性。我们通过免疫组织化学、反相高效液相色谱和定量 RT-PCR 相结合的方法研究了鹿角珊瑚素的表达。我们的数据表明,鹿角珊瑚素在表皮颗粒细胞中持续转录,在这些细胞中储存,并在受到非致病性免疫挑战时进一步释放。珊瑚病原体珊瑚弧菌(Vibrio coralliilyticus)抑制了鹿角珊瑚素基因的表达。这是宿主-弧菌相互作用中 AMP 基因抑制的第一个证据。

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