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构建 SLC16A1/3 靶向没食子酸铁埃博霉素纳米粒子调节宫颈癌糖酵解和氧化还原通路。

Construction of SLC16A1/3 Targeted Gallic Acid-Iron-Embelin Nanoparticles for Regulating Glycolysis and Redox Pathways in Cervical Cancer.

机构信息

Key Laboratory of Xinjiang Phytomedicine Resource and Utilization, Ministry of Education, Shihezi University College of Pharmacy, Shihezi 832003, Xinjiang, China.

School of Medicine, Xinjiang University of Science & Technology, Korla, 841000, China.

出版信息

Mol Pharm. 2023 Sep 4;20(9):4574-4586. doi: 10.1021/acs.molpharmaceut.3c00294. Epub 2023 Jun 12.

Abstract

SLC16A1 and SLC16A3 (SLC16A1/3) are highly expressed in cervical cancers and associated with the malignant biological behavior of cancer. SLC16A1/3 is the critical hub for regulating the internal and external environment, glycolysis, and redox homeostasis in cervical cancer cells. Inhibiting SLC16A1/3 provides a new thought to eliminate cervical cancer effectively. There are few reports on effective treatment strategies to eliminate cervical cancer by simultaneously targeting SLC16A1/3. GEO database analysis and quantitative reverse transcription polymerase chain reaction experiment were used to confirm the high expression of SLC16A1/3. The potential inhibitor of SLC16A1/3 was screened from Siwu Decoction by using network pharmacology and molecular docking technology. The mRNA levels and protein levels of SLC16A1/3 in SiHa and HeLa cells treated by Embelin (EMB) were clarified, respectively. Furthermore, the Gallic acid-iron (GA-Fe) drug delivery system was used to improve its anti-cancer performance. Compared with normal cervical cells, SLC16A1/3 mRNA was over-expressed in SiHa and HeLa cells. Through the analysis of Siwu Decoction, a simultaneously targeted SLC16A1/3 inhibitor EMB was discovered. It was found for the first time that EMB promoted lactic acid accumulation and further induced redox dyshomeostasis and glycolysis disorder by simultaneously inhibiting SLC16A1/3. The gallic acid-iron-Embelin (GA-Fe@EMB) drug delivery system delivered EMB, which had a synergistic anti-cervical cancer effect. Under the irradiation of a near-infrared laser, the GA-Fe@EMB could elevate the temperature of the tumor area effectively. Subsequently, EMB was released and mediated the lactic acid accumulation and the GA-Fe nanoparticle synergistic Fenton reaction to promote ROS accumulation, thereby increasing the lethality of the nanoparticles on cervical cancer cells. GA-Fe@EMB can target cervical cancer marker SLC16A1/3 to regulate glycolysis and redox pathways, synergistically with photothermal therapy, which provides a new avenue for the synergistic treatment of malignant cervical cancer.

摘要

SLC16A1 和 SLC16A3(SLC16A1/3)在宫颈癌中高度表达,与癌症的恶性生物学行为相关。SLC16A1/3 是调节宫颈癌细胞内外环境、糖酵解和氧化还原平衡的关键枢纽。抑制 SLC16A1/3 为有效消除宫颈癌提供了新的思路。目前很少有报道称同时针对 SLC16A1/3 可有效治疗宫颈癌。本研究通过 GEO 数据库分析和定量逆转录聚合酶链反应实验,证实 SLC16A1/3 高表达。采用网络药理学和分子对接技术筛选四物汤中 SLC16A1/3 的潜在抑制剂。明确 Embelin(EMB)处理 SiHa 和 HeLa 细胞后 SLC16A1/3 的 mRNA 水平和蛋白水平。此外,采用没食子酸铁(GA-Fe)药物传递系统提高其抗癌性能。与正常宫颈细胞相比,SLC16A1/3 mRNA 在 SiHa 和 HeLa 细胞中过表达。通过对四物汤的分析,发现了一种同时靶向 SLC16A1/3 的抑制剂 EMB。首次发现 EMB 同时抑制 SLC16A1/3 可促进乳酸积累,进而诱导氧化还原失衡和糖酵解紊乱。没食子酸铁-Embelin(GA-Fe@EMB)药物传递系统输送 EMB,具有协同抗宫颈癌作用。在近红外激光照射下,GA-Fe@EMB 可有效升高肿瘤区域温度。随后,EMB 被释放并介导乳酸积累和 GA-Fe 纳米颗粒协同 Fenton 反应促进 ROS 积累,从而提高纳米颗粒对宫颈癌的杀伤力。GA-Fe@EMB 可以靶向宫颈癌标志物 SLC16A1/3 调节糖酵解和氧化还原途径,与光热疗法协同作用,为恶性宫颈癌的协同治疗提供了新途径。

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