Abstract
Simple SummaryRenal cell carcinoma (RCC) is the most common kidney malignancy. Due to development of therapy resistance, efficacy of conventional drugs such as sunitinib is limited. Artesunate (ART), a drug originating from Traditional Chinese Medicine, has exhibited anti-tumor effects in several non-urologic tumors. ART inhibited growth, reduced metastatic properties, and curtailed metabolism in sunitinib-sensitive and sunitinib–resistant RCC cells. In three of four tested cell lines, ART’s growth inhibitory effects were accompanied by cell cycle arrest and modulation of cell cycle regulating proteins. In a fourth cell line, KTCTL-26, ART evoked ferroptosis, an iron-dependent cell death, and exhibited stronger anti-tumor effects than in the other cell lines. The regulatory protein, p53, was only detectable in the KTCTL-26 cells, possibly making p53 a predictive marker of cancer that may respond better to ART. ART, therefore, may hold promise as an additive therapy option for selected patients with advanced or therapy-resistant RCC.Although innovative therapeutic concepts have led to better treatment of advanced renal cell carcinoma (RCC), efficacy is still limited due to the tumor developing resistance to applied drugs. Artesunate (ART) has demonstrated anti-tumor effects in different tumor entities. This study was designed to investigate the impact of ART (1–100 µM) on the sunitinib-resistant RCC cell lines, Caki-1, 786-O, KTCTL26, and A-498. Therapy-sensitive (parental) and untreated cells served as controls. ART’s impact on tumor cell growth, proliferation, clonogenic growth, apoptosis, necrosis, ferroptosis, and metabolic activity was evaluated. Cell cycle distribution, the expression of cell cycle regulating proteins, p53, and the occurrence of reactive oxygen species (ROS) were investigated. ART significantly increased cytotoxicity and inhibited proliferation and clonogenic growth in both parental and sunitinib-resistant RCC cells. In Caki-1, 786-O, and A-498 cell lines growth inhibition was associated with G0/G1 phase arrest and distinct modulation of cell cycle regulating proteins. KTCTL-26 cells were mainly affected by ART through ROS generation, ferroptosis, and decreased metabolism. p53 exclusively appeared in the KTCTL-26 cells, indicating that p53 might be predictive for ART-dependent ferroptosis. Thus, ART may hold promise for treating selected patients with advanced and even therapy-resistant RCC.
Highlights
Accounting for ~85% of cases, renal cell carcinoma (RCC) is the most common kidney cancer and one of the most aggressive urologic cancers [1]
The anti-angiogenic activity of the tyrosine kinase inhibitor (TKI) sunitinib extends the progression-free survival of patients [3], but resistance occurs during treatment [4]
Sunitinib-sensitive and sunitinib-resistant RCC cell lines, Caki-1, 786-O, KTCTL-26, and A-498, were employed with the sunitinib-sensitive RCC sub-lines serving as controls
Summary
Accounting for ~85% of cases, renal cell carcinoma (RCC) is the most common kidney cancer and one of the most aggressive urologic cancers [1]. RCC patients often present at an advanced stage with an poor prognosis [2]. Better understanding of the molecular modes of action underlying RCC led to the development of targeted therapies affecting angiogenic activity and immune checkpoint inhibitors. The anti-angiogenic activity of the tyrosine kinase inhibitor (TKI) sunitinib extends the progression-free survival of patients [3], but resistance occurs during treatment [4]. Therapy resistance is one, if not the main, problem, in treating advanced RCC. Novel treatment strategies combining targeted therapy and immunotherapy have been introduced [5,6,7]. Even with combined drug application resistance occurs and adverse side effects are common [5,8,9]
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