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犬心丝虫的发育对甾醇高度敏感,甾醇激活核受体 DAF-12 的同源物。

The development of the dog heartworm is highly sensitive to sterols which activate the orthologue of the nuclear receptor DAF-12.

机构信息

INTHERES, Université de Toulouse, INRAE, ENVT, 31027, Toulouse Cedex 3, France.

Institute of Parasitology, McGill University, Sainte-Anne-De-Bellevue, H9X3V9, QC, Canada.

出版信息

Sci Rep. 2020 Jul 8;10(1):11207. doi: 10.1038/s41598-020-67466-9.

Abstract

Prevention therapy against Dirofilaria immitis in companion animals is currently threatened by the emergence of isolates resistant to macrocyclic lactone anthelmintics. Understanding the control over developmental processes in D. immitis is important for elucidating new approaches to heartworm control. The nuclear receptor DAF-12 plays a role in the entry and exit of dauer stage in Caenorhabditis elegans and in the development of free-living infective third-stage larvae (iL3) of some Clade IV and V parasitic nematodes. We identified a DAF-12 ortholog in the clade III nematode D. immitis and found that it exhibited a much higher affinity for dafachronic acids than described with other nematode DAF-12 investigated so far. We also modelled the DimDAF-12 structure and characterized the residues involved with DA binding. Moreover, we showed that cholesterol derivatives impacted the molting process from the iL3 to the fourth-stage larvae. Since D. immitis is unable to synthesize cholesterol and only completes its development upon host infection, we hypothesize that host environment contributes to its further molting inside the host vertebrate. Our discovery contributes to a better understanding of the developmental checkpoints of D. immitis and offers new perspectives for the development of novel therapies against filarial infections.

摘要

目前,犬类预防心丝虫病的治疗方法受到大环内酯类驱虫药抗药性分离株的威胁。了解心丝虫发育过程的控制对于阐明新的心丝虫病控制方法非常重要。核受体 DAF-12 在秀丽隐杆线虫的 dauer 阶段的进入和退出以及一些 IV 类和 V 类寄生线虫的自由生活感染性第三期幼虫 (iL3) 的发育中发挥作用。我们在 III 类线虫犬恶丝虫中鉴定出了一个 DAF-12 同源物,并发现它对 dafachronic 酸的亲和力比迄今为止研究的其他线虫 DAF-12 高得多。我们还构建了 DimDAF-12 的结构并对与 DA 结合的残基进行了表征。此外,我们表明胆固醇衍生物会影响从 iL3 到第四期幼虫的蜕皮过程。由于犬恶丝虫不能合成胆固醇,并且只有在感染宿主后才能完成发育,我们假设宿主环境有助于其在宿主脊椎动物体内进一步蜕皮。我们的发现有助于更好地理解犬恶丝虫的发育检查点,并为开发针对丝虫感染的新型治疗方法提供了新的视角。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/66db/7343802/c8a01d78b33b/41598_2020_67466_Fig1_HTML.jpg

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