Department of Pharmaceutical Sciences, College of Pharmacy, University of Nebraska Medical Center, Omaha, NE 68106, USA.
Department of Pharmaceutical Sciences, School of Pharmacy, Texas Tech University Health Sciences Center, Amarillo, TX 79106, USA.
ChemMedChem. 2021 Apr 8;16(7):1143-1162. doi: 10.1002/cmdc.202000729. Epub 2021 Jan 26.
Mitochondrial respiratory complex II (CII), also known as succinate dehydrogenase, plays a critical role in mitochondrial metabolism. Known but low potency CII inhibitors are selectively cytotoxic to cancer cells including the benzothiadiazine-based anti-hypoglycemic diazoxide. Herein, we study the structure-activity relationship of benzothiadiazine derivatives for CII inhibition and their effect on cancer cells for the first time. A 15-fold increase in CII inhibition was achieved over diazoxide, albeit with micromolar IC values. Cytotoxicity evaluation of the novel derivatives resulted in the identification of compounds with much greater antineoplastic effect than diazoxide, the most potent of which possesses an IC of 2.93±0.07 μM in a cellular model of triple-negative breast cancer, with high selectivity over nonmalignant cells and more than double the potency of the clinical agent 5-fluorouracil. No correlation between cytotoxicity and CII inhibition was found, thus indicating an as-yet-undefined mechanism of action of this scaffold. The derivatives described herein represent valuable hit compounds for therapeutic discovery in triple-negative breast cancer.
线粒体呼吸复合物 II(CII),也称为琥珀酸脱氢酶,在线粒体代谢中起着关键作用。已知但效力较低的 CII 抑制剂对癌细胞具有选择性细胞毒性,包括基于苯并噻二嗪的抗低血糖剂二氮嗪。本文首次研究了苯并噻二嗪衍生物的结构-活性关系及其对癌细胞的影响。与二氮嗪相比,CII 抑制活性提高了 15 倍,尽管 IC 值仍为微摩尔级。新型衍生物的细胞毒性评估结果表明,与二氮嗪相比,这些化合物具有更强的抗肿瘤作用,其中最有效的化合物在三阴性乳腺癌的细胞模型中 IC 值为 2.93±0.07 μM,对非恶性细胞具有高选择性,其效力是临床药物 5-氟尿嘧啶的两倍多。未发现细胞毒性与 CII 抑制之间存在相关性,因此表明该支架的作用机制尚不清楚。本文所述的衍生物代表了三阴性乳腺癌治疗发现的有价值的起始化合物。
