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Rhodoquinone biosynthesis in C. elegans requires precursors generated by the kynurenine pathway

机译:C.秀丽隐杆线虫的rhodoquinone生物合成需要由kynurenine途径产生的前体

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摘要

Parasitic helminths infect over a billion humans. To survive in the low oxygen environment of their hosts, these parasites use unusual anaerobic metabolism — this requires rhodoquinone (RQ), an electron carrier that is made by very few animal species. Crucially RQ is not made or used by any parasitic hosts and RQ synthesis is thus an ideal target for anthelmintics. However, little is known about how RQ is made and no drugs are known to block RQ synthesis. C. elegans makes RQ and can use RQ-dependent metabolic pathways — here, we use C. elegans genetics to show that tryptophan degradation via the kynurenine pathway is required to generate the key amine-containing precursors for RQ synthesis. We show that C. elegans requires RQ for survival in hypoxic conditions and, finally, we establish a high throughput assay for drugs that block RQ-dependent metabolism. This may drive the development of a new class of anthelmintic drugs. This study is a key first step in understanding how RQ is made in parasitic helminths.
机译:寄生蠕虫感染了超过十亿人。为了在宿主的低氧环境中存活,这些寄生虫使用不寻常的厌氧代谢 - 这需要罗经醌(RQ),一种由极少数动物物种制成的电子载体。任何寄生宿主都没有制备或使用至关重要的RQ,并且RQ合成因此是Anthelmintics的理想目标。然而,关于RQ的制造方法很少,并且已知没有药物阻断RQ合成的任何药物。 C.秀丽隐杆线,可以使用RQ依赖性代谢途径 - 在这里,我们使用C. elegans遗传学来表明,需要通过kynurenine途径降解rq合成的含键胺的前体。我们展示了秀丽隐杆线虫需要RQ在缺氧条件下存活,最后,我们为阻断RQ依赖性新陈代谢的药物建立了高通量测定。这可能推动开发一类新类的血清药物。本研究是了解RQ如何在寄生蠕虫中进行的关键第一步。

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