Chemosensitization of non-small cell lung cancer to sorafenib via non-hydroxamate s-triazinedione-based MMP-9/10 inhibitors

Bioorg Chem. 2024 Mar:144:107155. doi: 10.1016/j.bioorg.2024.107155.

Hosam H Khalil ¹, Mohamed M El-Sheshtawy ¹, Sherine N Khattab ², Marwa M Abu-Serie ³, Michael G Shehat ⁴, Mohamed Teleb ⁵, Nesreen S Haiba ⁶

Affiliations

1 Chemistry Department, Faculty of Science, Alexandria University, Alexandria 21321, Egypt.
2 Chemistry Department, Faculty of Science, Alexandria University, Alexandria 21321, Egypt. Electronic address: sherinekhattab@alexu.edu.eg.
3 Medical Biotechnology Department, Genetic Engineering and Biotechnology Research Institute, City of Scientific Research and Technological Applications (SRTA-City), Egypt.
4 Department of Microbiology and Immunology, Faculty of Pharmacy, Alexandria University, 21521 Alexandria, Egypt.
5 Department of Pharmaceutical Chemistry, Faculty of Pharmacy, Alexandria University, 21521 Alexandria, Egypt; Cancer Nanotechnology Research Laboratory (CNRL), Faculty of Pharmacy, Alexandria University, 21521 Alexandria, Egypt.
6 Department of Physics and Chemistry, Faculty of Education, Alexandria University, Egypt.

PMID: 38306827 DOI: 10.1016/j.bioorg.2024.107155

Abstract

Non-small cell lung Cancer (NSCLC) continues to be a leading cause of Cancer death. Its fatality is associated with angiogenesis and metastasis. While VEGFR inhibitors are expected to be the central pillar for halting lung Cancer, several clinical reports declared their subpar activities as monotherapy. These results directed combination studies of VEGFR inhibitors, especially sorafenib (Nexavar®), with various chemotherapeutic agents. Matrix metalloproteinase (MMP) inhibitors are seldom utilized in such combinations despite the expected complementary therapeutic outcome. This could be attributed to the clinical unsuitability of MMP inhibitors from the hydroxamate family. Herein, we report new non-hydroxamate s-triazinedione-based inhibitors of MMP-9 (6b; IC₅₀ = 0.112 μM), and MMP-10 (6e; IC₅₀ = 0.076 μM) surpassing the hydroxamate inhibitor NNGH for chemosensitization of NSCLC to sorafenib. MMPs inhibition profiling of the hits revealed MMP-9 over -2 and MMP-10 over -13 selectivity. 6b and 6e were potent (IC₅₀ = 0.139 and 0.136 µM), safe (SI up to 6.77) and superior to sorafenib (IC₅₀ = 0.506 µM, SI = 6.27) against A549 cells. When combined with sorafenib, the studied MMP inhibitors enhanced its cytotoxic efficacy up to 26 folds as confirmed by CI and DRI values for 6b (CI = 0.160 and DRI = 22.175) and 6e (CI = 0.096 and DRI = 29.060). 6b and 6e exerted anti-invasive activities in A549 cells as single agents (22.66 and 39.67 %) and in sorafenib combinations (29.96 and 91.83 %) compared to untreated control. Both compounds downregulated VEGF in A549 cells by approximately 70 % when combined with sorafenib, highlighting enhanced anti-angiogenic activities. Collectively, combinations of 6b and 6e with sorafenib demonstrated synergistic NSCLC cytotoxicity with pronounced anti-invasive and anti-angiogenic activities introducing a promising start point for preclinical studies.

Keywords

Chemosensitization; Matrix metalloproteinases inhibitors; NSCLC; S-Triazine; Sorafenib.

Products

Cat. No.

Product Name

Description

Target

Research Area
HY-161285

MMP-9/10-IN-2

MMP9/10抑制剂

MMP

Cancer
HY-161284

MMP-9/10-IN-1

MMP-9/10抑制剂

MMP

Cancer

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MedChemExpress (MCE) 只为有资质的科研机构、医药企业基于科学研究或药证申报的用途提供医药研发服务，不为任何个人或者非科研性质的、非用于药证申报使用等其他用途提供服务。沪(浦)应急管危经许[2021]201709(QFYS)

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Chemosensitization of non-small cell lung cancer to sorafenib via non-hydroxamate s-triazinedione-based MMP-9/10 inhibitors

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