Chemical Genetics in C. elegans Identifies Anticancer Mycotoxins Chaetocin and Chetomin as Potent Inducers of a Nuclear Metal Homeostasis Response

IF 3.5 2区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY ACS Chemical Biology Pub Date : 2024-04-23 DOI:10.1021/acschembio.4c00131

Elijah Abraham, A. M. Gihan K. Athapaththu, Kalina R. Atanasova, Qi-Yin Chen, Taylor J. Corcoran, Juan Piloto, Cheng-Wei Wu, Ranjala Ratnayake, Hendrik Luesch and Keith P. Choe*,

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Abstract

C. elegans numr-1/2 (nuclear-localized metal-responsive) is an identical gene pair encoding a nuclear protein previously shown to be activated by cadmium and disruption of the integrator RNA metabolism complex. We took a chemical genetic approach to further characterize regulation of this novel metal response by screening 41,716 compounds and extracts for numr-1p::GFP activation. The most potent activator was chaetocin, a fungal 3,6-epidithiodiketopiperazine (ETP) with promising anticancer activity. Chaetocin activates numr-1/2 strongly in the alimentary canal but is distinct from metal exposure, because it represses canonical cadmium-responsive metallothionine genes. Chaetocin has diverse targets in cancer cells including thioredoxin reductase, histone lysine methyltransferase, and acetyltransferase p300/CBP; further work is needed to identify the mechanism in C. elegans as genetic disruption and RNAi screening of homologues did not induce numr-1/2 in the alimentary canal and chaetocin did not affect markers of integrator dysfunction. We demonstrate that disulfides in chaetocin and chetomin, a dimeric ETP analog, are required to induce numr-1/2. ETP monomer gliotoxin, despite possessing a disulfide linkage, had almost no effect on numr-1/2, suggesting a dimer requirement. Chetomin inhibits C. elegans growth at low micromolar levels, and loss of numr-1/2 increases sensitivity; C. elegans and Chaetomiaceae fungi inhabit similar environments raising the possibility that numr-1/2 functions as a defense mechanism. There is no direct orthologue of numr-1/2 in humans, but RNaseq suggests that chaetocin affects expression of cellular processes linked to stress response and metal homeostasis in colorectal cancer cells. Our results reveal interactions between metal response gene regulation and ETPs and identify a potential mechanism of resistance to this versatile class of preclinical compounds.

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elegans 的化学遗传学发现抗癌霉菌毒素茶托菌素（Chaetocin）和车托菌素（Chetomin）是核金属平衡反应的强力诱导剂

秀丽隐杆线虫numr-1/2（核定位金属响应）是一对相同的基因，编码一种核蛋白，以前曾被证明可被镉和整合器RNA代谢复合物破坏激活。我们采用化学遗传学方法，通过筛选 41,716 种化合物和提取物对 numr-1p::GFP的激活作用，进一步确定了这种新型金属响应的调控特征。最有效的激活剂是chaetocin，它是一种真菌3,6-表二硫基二酮哌嗪（ETP），具有良好的抗癌活性。Chaetocin能强烈激活消化管中的numr-1/2，但与金属暴露不同，因为它能抑制典型的镉响应金属硫氨酸基因。Chaetocin在癌细胞中有多种靶标，包括硫氧还蛋白还原酶、组蛋白赖氨酸甲基转移酶和乙酰转移酶p300/CBP；由于同源物的基因干扰和RNAi筛选不能诱导消化道中的numr-1/2，而且Chaetocin也不影响整合器功能障碍的标志物，因此还需要进一步的工作来确定其在C.elegans中的机制。我们证明，chaetocin 和二聚 ETP 类似物 chetomin 中的二硫化物是诱导 numr-1/2 所必需的。ETP单体gliotoxin尽管具有二硫连接，但对numr-1/2几乎没有影响，这表明需要二聚体。Chetomin能在低微摩尔水平上抑制秀丽隐杆线虫的生长，而numr-1/2的缺失会增加其敏感性；秀丽隐杆线虫和链格孢属真菌栖息在相似的环境中，这提高了numr-1/2作为一种防御机制发挥作用的可能性。人类中没有numr-1/2的直系同源物，但RNaseq表明，chaetocin会影响结直肠癌细胞中与应激反应和金属平衡相关的细胞过程的表达。我们的研究结果揭示了金属反应基因调控与 ETPs 之间的相互作用，并确定了对这一类多用途临床前化合物产生耐药性的潜在机制。

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来源期刊

ACS Chemical Biology 生物-生化与分子生物学

CiteScore

7.50

自引率

5.00%

发文量

353

审稿时长

3.3 months

期刊介绍： ACS Chemical Biology provides an international forum for the rapid communication of research that broadly embraces the interface between chemistry and biology. The journal also serves as a forum to facilitate the communication between biologists and chemists that will translate into new research opportunities and discoveries. Results will be published in which molecular reasoning has been used to probe questions through in vitro investigations, cell biological methods, or organismic studies. We welcome mechanistic studies on proteins, nucleic acids, sugars, lipids, and nonbiological polymers. The journal serves a large scientific community, exploring cellular function from both chemical and biological perspectives. It is understood that submitted work is based upon original results and has not been published previously.