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Drosophila innate immunity: regional and functional specialization of prophenoloxidases

机译:果蝇先天免疫:原酚氧化酶的区域和功能专长

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Background The diversification of immune systems during evolution involves the expansion of particular gene families in given phyla. A better understanding of the metazoan immune system requires an analysis of the logic underlying such immune gene amplification. This analysis is now within reach due to the ease with which we can generate multiple mutations in an organism. In this paper, we analyze the contribution of the three Drosophila prophenoloxidases (PPOs) to host defense by generating single, double and triple mutants. PPOs are enzymes that catalyze the production of melanin at the site of infection and around parasites. They are the rate-limiting enzymes that contribute to the melanization reaction, a major immune mechanism of arthropods. The number of PPO-encoding genes is variable among insects, ranging from one in the bee to ten in the mosquito. Results By analyzing mutations alone and in combination, we ascribe a specific function to each of the three PPOs of Drosophila. Our study confirms that two PPOs produced by crystal cells, PPO1 and PPO2, contribute to the bulk of melanization in the hemolymph, upon septic or clean injury. In contrast, PPO3, a PPO restricted to the D. melanogaster group, is expressed in lamellocytes and contributes to melanization during the encapsulation process. Interestingly, another overlapping set of PPOs, PPO2 and PPO3, achieve melanization of the capsule upon parasitoid wasp infection. Conclusions The use of single or combined mutations allowed us to show that each PPO mutant has a specific phenotype, and that knocking out two of three genes is required to abolish fully a particular function. Thus, Drosophila PPOs have partially overlapping functions to optimize melanization in at least two conditions: following injury or during encapsulation. Since PPO3 is restricted to the D. melanogaster group, this suggests that production of PPO by lamellocytes emerged as a recent defense mechanism against parasitoid wasps. We conclude that differences in spatial localization, immediate or late availability, and mode of activation underlie the functional diversification of the three Drosophila PPOs, with each of them having non-redundant but overlapping functions.
机译:背景技术进化过程中免疫系统的多样化涉及给定门中特定基因家族的扩展。对后生动物免疫系统的更好理解需要对这种免疫基因扩增背后的逻辑进行分析。由于我们可以轻松地在生物体中产生多个突变,因此现在可以进行此分析。在本文中,我们通过生成单,双和三突变体来分析三种果蝇前酚氧化酶(PPO)对宿主防御的贡献。 PPO是在感染部位和寄生虫周围催化黑色素生成的酶。它们是导致节肢动物主要免疫机制黑化反应的限速酶。昆虫中PPO编码基因的数量是可变的,范围从蜜蜂中的一个到蚊子中的十个。结果通过单独或组合分析突变,我们将果蝇的三个PPO中的每个赋予特定功能。我们的研究证实,由结晶细胞产生的两种PPO(PPO1和PPO2)在败血性或干净性损伤后,可促进血淋巴中黑色素的大量表达。相比之下,PPO3(一种局限于黑腹果蝇(D. melanogaster)基团的PPO)在滑膜细胞中表达,并在封装过程中有助于黑色素化。有趣的是,另一组重叠的PPO,PPO2和PPO3在寄生类黄蜂感染后实现了胶囊的黑色素化。结论使用单一或组合突变使我们能够证明每个PPO突变体都具有特定的表型,并且需要敲除三个基因中的两个才能完全取消特定功能。因此,果蝇PPO具有部分重叠的功能,可在至少两种情况下优化黑化作用:受伤后或封装过程中。由于PPO3限于黑腹果蝇(D. melanogaster)组,这表明由弹状细胞产生PPO作为对抗寄生虫黄蜂的最新防御机制而出现。我们得出的结论是,空间定位,即时或后期可用性以及激活方式的差异是三个果蝇PPO功能多样化的基础,每个果蝇都具有非冗余但重叠的功能。

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