Isopentyl-Deoxynboquinone Induces Mitochondrial Dysfunction and G2/M Phase Cell Cycle Arrest to Selectively Kill NQO1-Positive Pancreatic Cancer Cells.

IF 5.9 2区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Antioxidants & redox signaling Pub Date : 2024-07-01 Epub Date: 2024-01-08 DOI:10.1089/ars.2022.0224

Lingxiang Jiang, Yingchun Liu, Soumya Tumbath, Matthew W Boudreau, Lindsay E Chatkewitz, Jiangwei Wang, Xiaolin Su, Kashif Rafiq Zahid, Katherine Li, Yaomin Chen, Kai Yang, Paul J Hergenrother, Xiumei Huang

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引用次数: 0

Abstract

Aims: Pancreatic cancer is among the top five leading causes of cancer-related deaths worldwide, with poor overall survival rates. Current therapies for pancreatic cancer lack tumor specificity, resulting in harmful effects on normal tissues. Therefore, developing tumor-specific agents for the treatment of pancreatic cancer is critical. NAD(P)H:quinone oxidoreductase 1 (NQO1), highly expressed in pancreatic cancers but not in associated normal tissues, makes NQO1 bioactivatable drugs a potential therapy for selectively killing NQO1-positive cancer cells. Our previous studies have revealed that the novel NQO1 bioactivatable drug deoxynyboquinone (DNQ) is 10-fold more potent than the prototypic NQO1 bioactivatable drug β-lapachone in killing of NQO1-positive cancer cells. However, DNQ treatment results in high-grade methemoglobinemia, a significant side effect that limits clinical development. Results: Here, we report for the first time on a DNQ derivative, isopentyl-deoxynboquinone (IP-DNQ), which selectively kills pancreatic ductal adenocarcinoma (PDAC) cells in an NQO1-dependent manner with equal potency to the parent DNQ. IP-DNQ evokes massive reactive oxygen species (ROS) production and oxidative DNA lesions that result in poly(ADP-ribose)polymerase-1 (PARP1) hyperactivation, mitochondrial catastrophe, and G2/M phase cell cycle arrest, leading to apoptotic and necrotic programmed cell death. Importantly, IP-DNQ treatment causes only mild methemoglobinemia in vivo, with a threefold improvement in the maximum tolerated dose (MTD) compared with DNQ, while it significantly suppresses tumor growth and extends the life span of mice in subcutaneous and orthotopic pancreatic cancer xenograft models. Innovation and Conclusion: Our study demonstrates that IP-DNQ is a promising therapy for NQO1-positive pancreatic cancers and may enhance the efficacy of other anticancer drugs. IP-DNQ represents a novel approach to treating pancreatic cancer with the potential to improve patient outcomes.

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IP-DNQ诱导线粒体功能障碍和G2/M期细胞周期阻滞，选择性杀伤nq01阳性胰腺癌细胞。

胰腺癌是全球癌症相关死亡的五大主要原因之一，生存率很低。目前的胰腺癌治疗方法缺乏肿瘤特异性，导致对正常组织的有害影响。因此，开发肿瘤特异性药物治疗胰腺癌至关重要。NAD(P)H:醌氧化还原酶1 (NQO1)在胰腺癌中高表达，而在正常组织中不表达，这使得NQO1生物活化药物成为选择性杀死NQO1阳性癌细胞的潜在治疗方法。我们的前期研究发现，新型NQO1生物活化药物脱氧氨基醌(deoxynyboquinone, DNQ)对NQO1阳性癌细胞的杀伤能力是NQO1生物活化药物β-lapachone的10倍。然而，DNQ治疗导致高级别高铁血红蛋白血症，这是一个限制临床发展的显著副作用。在这里，我们首次报道了DNQ衍生物异戊基-脱氧波醌(IP-DNQ)，它以依赖于nq01的方式选择性杀死胰腺导管腺癌细胞，其效力与亲本DNQ相同。IP-DNQ引起大量ROS产生和DNA氧化损伤，导致PARP1过度激活、线粒体突变和G2/ m期阻滞，导致细胞凋亡和坏死性程序性死亡。重要的是，IP-DNQ治疗在体内引起轻度高铁血红蛋白血症，与DNQ相比，最大耐受剂量提高了三倍，同时在皮下和原位胰腺癌异种移植模型中显著抑制肿瘤生长并延长小鼠寿命。我们的研究表明，IP-DNQ是一种很有前景的治疗nqo1阳性胰腺癌的方法，并可能增强其他抗癌药物的疗效。IP-DNQ代表了一种治疗胰腺癌的新方法，有可能改善患者的预后。

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来源期刊

Antioxidants & redox signaling 生物-内分泌学与代谢

CiteScore

14.10

自引率

1.50%

发文量

170

审稿时长

3-6 weeks

期刊介绍： Antioxidants & Redox Signaling (ARS) is the leading peer-reviewed journal dedicated to understanding the vital impact of oxygen and oxidation-reduction (redox) processes on human health and disease. The Journal explores key issues in genetic, pharmaceutical, and nutritional redox-based therapeutics. Cutting-edge research focuses on structural biology, stem cells, regenerative medicine, epigenetics, imaging, clinical outcomes, and preventive and therapeutic nutrition, among other areas. ARS has expanded to create two unique foci within one journal: ARS Discoveries and ARS Therapeutics. ARS Discoveries (24 issues) publishes the highest-caliber breakthroughs in basic and applied research. ARS Therapeutics (12 issues) is the first publication of its kind that will help enhance the entire field of redox biology by showcasing the potential of redox sciences to change health outcomes. ARS coverage includes: -ROS/RNS as messengers -Gaseous signal transducers -Hypoxia and tissue oxygenation -microRNA -Prokaryotic systems -Lessons from plant biology