多种 UDP 糖基转移酶以相加的方式调节线虫秀丽隐杆线虫对苯并咪唑类药物的敏感性

IF 3.7 2区 医学 Q1 PARASITOLOGY International journal for parasitology Pub Date : 2024-09-01 DOI:10.1016/j.ijpara.2024.05.003
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引用次数: 0

摘要

异生物的生物转化是抗蠕虫药药效的重要调节因素,也是产生抗蠕虫药耐药性的潜在机制。自由生活的线虫秀丽隐杆线虫(Caenorhabditis elegans)和反刍动物寄生虫柯氏血吸虫(Haemonchus contortus)都通过葡萄糖共轭作用对苯并咪唑类药物进行生物转化,这种作用可能是由 UDP-糖基转移酶(UGT)催化的。为了确定参与苯并咪唑类药物解毒的秀丽隐杆线虫基因,我们首先对来自人类、秀丽隐杆线虫和H. contortus的UGT进行了系统发育比较分析,并结合现有的RNAseq数据集,确定了63个秀丽隐杆线虫ugt基因中哪些基因最有可能参与苯并咪唑类药物的生物转化。通过 RNA 干扰敲除 15 个优先考虑的秀丽隐杆线虫基因,确定了那些能使动物对苯并咪唑衍生物阿苯达唑(ABZ)过敏的基因。随后的基因突变显示,ugt-9 和 ugt-11 基因的缺失影响最大。ugt-9基因簇 "包括这些基因以及其他六个密切相关的ugts基因。通过 CRISPR-Cas-9 基因缺失,去除了 8 个 ugt-9 簇基因中的 7 个,其对 ABZ 的敏感性要高于单一的最大效应突变。此外,ugt-22(不属于 ugt-9 基因簇)与 ugt-9 基因簇缺失的双突变体进一步提高了 ABZ 的敏感性。ugt突变对不同的苯并咪唑衍生物有不同的影响,这表明具有不同特异性的酶可以共同更有效地解毒。ugt-9、ugt-11 和 ugt-22 gfp 报告基因的表达模式不同,因此可能作用于不同的组织,这至少可以部分解释它们对药物效力的叠加效应。单独过表达 ugt-9 就足以产生部分 ABZ 抗性,这表明保护动物的总 UGT 活性在增加。总之,我们的研究结果表明,多种 UGT 酶在苯并咪唑类药物解毒过程中具有重叠但非完全冗余的功能,可能是提高苯并咪唑类药物药效的 "可药物 "靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Multiple UDP glycosyltransferases modulate benzimidazole drug sensitivity in the nematode Caenorhabditis elegans in an additive manner

Xenobiotic biotransformation is an important modulator of anthelmintic drug potency and a potential mechanism of anthelmintic resistance. Both the free-living nematode Caenorhabditis elegans and the ruminant parasite Haemonchus contortus biotransform benzimidazole drugs by glucose conjugation, likely catalysed by UDP-glycosyltransferase (UGT) enzymes. To identify C. elegans genes involved in benzimidazole drug detoxification, we first used a comparative phylogenetic analysis of UGTs from humans, C. elegans and H. contortus, combined with available RNAseq datasets to identify which of the 63 C. elegans ugt genes are most likely to be involved in benzimidazole drug biotransformation. RNA interference knockdown of 15 prioritized C. elegans genes identified those that sensitized animals to the benzimidazole derivative albendazole (ABZ). Genetic mutations subsequently revealed that loss of ugt-9 and ugt-11 had the strongest effects. The “ugt-9 cluster” includes these genes, together with six other closely related ugts. A CRISPR-Cas-9 deletion that removed seven of the eight ugt-9 cluster genes had greater ABZ sensitivity than the single largest-effect mutation. Furthermore, a double mutant of ugt-22 (which is not a member of the ugt-9 cluster) with the ugt-9 cluster deletion further increased ABZ sensitivity. This additivity of mutant phenotypes suggest that ugt genes act in parallel, which could have several, not mutually exclusive, explanations. ugt mutations have different effects with different benzimidazole derivatives, suggesting that enzymes with different specificities could together more efficiently detoxify drugs. Expression patterns of ugt-9, ugt-11 and ugt-22 gfp reporters differ and so likely act in different tissues which may, at least in part, explain their additive effects on drug potency. Overexpression of ugt-9 alone was sufficient to confer partial ABZ resistance, indicating increasing total UGT activity protects animals. In summary, our results suggest that the multiple UGT enzymes have overlapping but not completely redundant functions in benzimidazole drug detoxification and may represent “druggable” targets to improve benzimidazole drug potency.

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来源期刊
CiteScore
8.40
自引率
2.50%
发文量
76
审稿时长
23 days
期刊介绍: International Journal for Parasitology offers authors the option to sponsor nonsubscriber access to their articles on Elsevier electronic publishing platforms. For more information please view our Sponsored Articles page. The International Journal for Parasitology publishes the results of original research in all aspects of basic and applied parasitology, including all the fields covered by its Specialist Editors, and ranging from parasites and host-parasite relationships of intrinsic biological interest to those of social and economic importance in human and veterinary medicine and agriculture.
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