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Design and synthesis of 6-arylpyridine-tethered sulfonamides as novel selective inhibitors of carbonic anhydrase IX with promising antitumor features toward the human colorectal cancer

化学 癌症研究 活力测定 结直肠癌 细胞生长 细胞凋亡 癌症 血管生成 细胞培养 碳酸酐酶 癌细胞 生物化学 内科学 生物 医学 遗传学
作者
Wagdy M. Eldehna,Eslam Essam Mohammed,Ghada H. Al-Ansary,Emanuela Berrino,Mostafa M. Elbadawi,Tamer M. Ibrahim,Maiy Y. Jaballah,Sara T. Al‐Rashood,Faizah A. Binjubair,M. Salih Celik,Alessio Nocentini,Fawzy Elbarbry,Fikrettin Şahi̇n,Hatem A. Abdel‐Aziz,Claudiu T. Supuran,Mohamed Farès
出处
期刊:European journal of medicinal chemistry [Elsevier BV]
卷期号:258: 115538-115538 被引量:23
标识
DOI:10.1016/j.ejmech.2023.115538
摘要

Hypoxia, a characteristic feature of solid tumors, develops as a result of excessive cell proliferation and rapid tumor growth exceeding the oxygen supply, and can result in angiogenesis activation, increased invasiveness, aggressiveness, and metastasis, leading to improved tumor survival and suppression of anticancer drug therapeutic impact. SLC-0111, a ureido benzenesulfonamide, is a selective human carbonic anhydrase (hCA) IX inhibitor in clinical trials for the treatment of hypoxic malignancies. Herein, we describe the design and synthesis of novel 6-arylpyridines 8a-l and 9a-d as structural analogues of SLC-0111, in the aim of exploring new selective inhibitors for the cancer-associated hCA IX isoform. The para-fluorophenyl tail in SLC-0111 was replaced by the privileged 6-arylpyridine motif. Moreover, both ortho- and meta-sulfonamide regioisomers, as well as an ethylene extended analogous were developed. All 6-arylpyridine-based SLC-0111 analogues were screened in vitro for their inhibitory potential against a panel of hCAs (hCA I, II, IV and IX isoforms) using stopped-flow CO2 hydrase assay. In addition, the anticancer activity was firstly explored against a panel of 57 cancer cell lines at the USA NCI-Developmental Therapeutic Program. Compound 8g emerged as the best anti-proliferative candidate with mean GI% value equals 44. Accordingly, a cell viability assay (MTS) for 8g was applied on colorectal HCT-116 and HT-29 cancer cell lines as well as on the healthy HUVEC cells. Thereafter, Annexin V-FITC apoptosis detection, cell cycle, TUNEL, and qRT-PCR, colony formation, and wound healing assays were applied to gain mechanistic insights and to understand the behavior of colorectal cancer cells upon the treatment of compound 8g. Also, a molecular docking analysis was conducted to provide in silico insights into the reported hCA IX inhibitory activity and selectivity.

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