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类二十烷酸介导寄生黄蜂梨形肿腿蜂幼虫对病毒感染的黑化结节反应。

Eicosanoids mediate melanotic nodulation reactions to viral infection in larvae of the parasitic wasp, Pimpla turionellae.

作者信息

Durmuş Yonca, Büyükgüzel Ender, Terzi Burcin, Tunaz Hasan, Stanley David, Büyükgüzel Kemal

机构信息

Department of Biology, Faculty of Arts and Science, Karaelmas University, Zonguldak, Turkey.

出版信息

J Insect Physiol. 2008 Jan;54(1):17-24. doi: 10.1016/j.jinsphys.2007.03.019. Epub 2007 Jul 29.

Abstract

Nodulation is the quantitatively predominant insect cellular immune function activated in response to bacterial, fungal and some viral infections. We posed the hypothesis that parasitoid insects express melanotic nodulation reactions to viral challenge and that eicosanoids mediate these reactions. Treating fifth-instar larvae of the ichneumonid endoparasitoid Pimpla turionellae with Bovine Herpes Simplex Virus-1 (BHSV-1) induced nodulation reactions in a challenge dose-dependent manner. Experimental larvae treated with the cyclooxygenase inhibitor, indomethacin, the lipoxygenase inhibitor, esculetin, and the phospholipase A2 inhibitor, dexamethasone, resulted in severely impaired nodulation reactions to our standard BHSV-1 challenge dose. The immunoinhibitory influence of dexamethasone was reversed in larvae reared on culture medium amended with arachidonic acid, the fatty acid precursor of eicosanoid biosynthesis. Larvae that had been reared on media amended with indomethacin, esculetin, or dexamethasone were also compromised in their nodulation reactions to viral challenge. The influence of the orally administered pharmaceutical was expressed in a dose-dependent manner. Finally, wasp larvae reared in the presence of indomethacin and dexamethasone expressed significantly decreased levels of phenoloxidase activity in response to viral challenge. These findings draw attention to the idea that endoparasitoid insects express cellular immune reactions to viral challenge; they also support our hypothesis that eicosanoids mediate nodulation reactions to viral challenge in these highly specialized insects.

摘要

结瘤是昆虫在应对细菌、真菌和一些病毒感染时被激活的数量上占主导的细胞免疫功能。我们提出了这样一个假设:寄生性昆虫对病毒攻击会表现出黑化结瘤反应,并且类花生酸介导这些反应。用牛单纯疱疹病毒1型(BHSV - 1)处理膜翅目内寄生蜂梨形肿腿蜂的五龄幼虫,会以攻击剂量依赖的方式诱导结瘤反应。用环氧化酶抑制剂吲哚美辛、脂氧化酶抑制剂七叶亭和磷脂酶A2抑制剂地塞米松处理实验幼虫,会导致对我们标准的BHSV - 1攻击剂量的结瘤反应严重受损。在用花生四烯酸(类花生酸生物合成的脂肪酸前体)改良的培养基上饲养的幼虫中,地塞米松的免疫抑制作用被逆转。在用吲哚美辛、七叶亭或地塞米松改良的培养基上饲养的幼虫对病毒攻击的结瘤反应也受到损害。口服药物的影响呈剂量依赖性。最后,在吲哚美辛和地塞米松存在的情况下饲养的黄蜂幼虫对病毒攻击的酚氧化酶活性水平显著降低。这些发现引起了人们对以下观点的关注:内寄生性昆虫对病毒攻击会表现出细胞免疫反应;它们也支持了我们的假设,即类花生酸在这些高度特化的昆虫中介导对病毒攻击的结瘤反应。

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