Fexinidazole and Corallopyronin A target Wolbachia-infected sheath cells present in filarial nematodes.

IF 4.9 1区 医学 Q1 MICROBIOLOGY
PLoS Pathogens Pub Date : 2025-09-08 eCollection Date: 2025-09-01 DOI:10.1371/journal.ppat.1012929
Laura Chappell, Ricardo Peguero, William R Conner, Sommer Fowler, Brandon S Cooper, Kenneth Pfarr, Achim Hoerauf, Sara Lustigman, Judy Sakanari, William Sullivan
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引用次数: 0

Abstract

The discovery of the endosymbiotic bacteria Wolbachia as an obligate symbiont of. filarial nematodes has led to antibiotic-based treatments for filarial diseases. While lab. and clinical studies have yielded promising results, recent animal studies revealed that Wolbachia levels rebound following treatment with the antibiotic rifampicin. Previous work revealed that a potential source of the bacterial rebound in female worms were dense clusters of Wolbachia in ovarian tissue. The number, size, and density of these Wolbachia clusters were not diminished despite antibiotic treatment. Here we define the cellular characteristics of the Wolbachia clusters in Brugia pahangi (wBp) and identify drugs that target them. We show that the Wolbachia clusters originate from newly formed sheath cells adjacent to the distal tip cell. The dramatically enlarged volume of a Wolbachia-infected sheath cell is strikingly similar to endosymbiont-induced bacteriocytes found in many insect species. Ultrastructural analysis reveals that the clustered Wolbachia present within the sheath cells have a distinct morphology from those present within the oocytes, and that the sheath cell membrane appears to have interdigitations with the adjacent oocyte membrane. This includes membrane-based channels that provide a connection between Wolbachia-infected sheath cells and oocytes. We determined that the Wolbachia within the sheath cells are either quiescent or replicating at a very low rate. Screens of 11 known antibiotics and other drugs revealed that Fexinidazole, Corallopyronin A and Rapamycin reduced the number of Wolbachia clusters infecting sheath cells but only Fexinidazole and Corallopyronin A showed a highly significant difference (p < 0.0001) compared to the control group.

非昔硝唑和珊瑚蛋白靶沃尔巴克氏体感染鞘细胞存在于丝状线虫。
内共生细菌沃尔巴克氏体作为专性共生体的发现。丝虫病导致了基于抗生素的丝虫病治疗。虽然实验室。尽管临床研究已经取得了令人鼓舞的结果,但最近的动物研究显示,在使用抗生素利福平治疗后,沃尔巴克氏体水平会反弹。先前的研究表明,雌性蠕虫体内细菌反弹的一个潜在来源是卵巢组织中密集的沃尔巴克氏体。尽管抗生素治疗,这些沃尔巴克氏菌群的数量、大小和密度并没有减少。在这里,我们定义了布鲁贾帕汉吉沃尔巴克氏菌群(wBp)的细胞特征,并确定了针对它们的药物。我们发现沃尔巴克氏菌群起源于与远端尖端细胞相邻的新形成的鞘细胞。沃尔巴克氏体感染的鞘细胞体积急剧增大,与许多昆虫物种中发现的内共生诱导的细菌细胞惊人地相似。超微结构分析显示,鞘细胞内的沃尔巴克氏体与卵母细胞内的沃尔巴克氏体具有不同的形态,鞘细胞膜与相邻的卵母细胞膜有交叉。这包括在沃尔巴克氏体感染的鞘细胞和卵母细胞之间提供连接的基于膜的通道。我们确定鞘细胞内的沃尔巴克氏体要么是静止的,要么是以非常低的速度复制。对11种已知抗生素和其他药物的筛选显示,非昔硝唑、珊瑚pyronin A和雷帕霉素均能减少感染鞘细胞的沃尔巴克氏菌簇的数量,但只有非昔硝唑和珊瑚pyronin A表现出高度显著的差异(p
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来源期刊
PLoS Pathogens
PLoS Pathogens MICROBIOLOGY-PARASITOLOGY
自引率
3.00%
发文量
598
期刊介绍: Bacteria, fungi, parasites, prions and viruses cause a plethora of diseases that have important medical, agricultural, and economic consequences. Moreover, the study of microbes continues to provide novel insights into such fundamental processes as the molecular basis of cellular and organismal function.
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