Shetty Swathi R, Debnath Sudhan, Majumdar Khokan, Rajagopalan Muthukumaran, Ramaswamy Amutha, Das Amitava
Department of Applied Biology, Council of Scientific & Industrial Research-Indian Institute of Chemical Technology (CSIR-IICT), Uppal Road, Tarnaka, Hyderabad 500007 TS, India; Academy of Scientific and Innovative Research (AcSIR), Ghaziabad 201002, India.
Maharaja Bir Bikram College, Agartala, Tripura, India; Department of Chemistry, Netaji Subhash Mahavidyalaya, Udaipur, Tripura, India.
Bioorg Chem. 2024 Dec;153:107849. doi: 10.1016/j.bioorg.2024.107849. Epub 2024 Oct 1.
A high abundance of Epidermal Growth Factor Receptor (EGFR) in malignant cells makes them a prospective therapeutic target for basal breast tumors. Although EGFR inhibitors are in development as anticancer therapeutics, there exists limitations due to the dose-limiting cytotoxicity that limits their clinical utilization, thereby necessitating the advancement of effective inhibitors. In the present study, we have developed common pharmacophore hypotheses using 30 known EGFR inhibitors. The best pharmacophore hypothesis DHRRR_1 was utilized for virtual screening (VS) of the Phase database containing 4.3 × 10 fully prepared compounds. The top 1000 hits were further subjected to ADME filtration followed by structure-based VS and Molecular Dynamics (MD) simulation investigations. Based on pharmacophore hypothesis matching, XP glide score, interactions between ligands and active site residues, ADME properties, and MD simulations, the five best hits (SN-01 through SN-05) were preferred for in-vitro cytotoxicity studies. All the molecules except SN-02 exhibited cytotoxicity in Triple Negative Breast Cancer (TNBC) cells. These potential EGFR inhibitors effectively downregulated the EGF-induced proliferation, migration, in-vitro tumorigenic capability, and EGFR activation (pEGFR) in the TNBCs. Additionally, in combination with doxorubicin, the identified EGFR inhibitors significantly decreased the EGF-induced proliferation. SN-04, and SN-05 in the presence of a lower concentration of doxorubicin markedly increased the apoptotic markers expression in the TNBCs, an effect which was comparable to a higher concentration of doxorubicin treatment, alone. These observations suggest that both SN-04 and/or SN-05 can improve the efficacy of chemotherapeutic drug, doxorubicin at a lower concentration to avert the higher dose of chemotherapeutic-induced side effects during breast cancer treatment.
恶性细胞中高丰度的表皮生长因子受体(EGFR)使其成为基底型乳腺癌的一个潜在治疗靶点。尽管EGFR抑制剂正在作为抗癌治疗药物进行研发,但由于剂量限制性细胞毒性限制了它们的临床应用,因此需要开发有效的抑制剂。在本研究中,我们利用30种已知的EGFR抑制剂建立了共同药效团假说。最佳药效团假说DHRRR_1被用于对包含4.3×10个完全制备好的化合物的阶段数据库进行虚拟筛选(VS)。对前1000个命中结果进一步进行ADME过滤,然后进行基于结构的VS和分子动力学(MD)模拟研究。基于药效团假说匹配、XP glide评分、配体与活性位点残基之间的相互作用、ADME性质以及MD模拟,选择了五个最佳命中结果(SN-01至SN-05)进行体外细胞毒性研究。除SN-02外,所有分子在三阴性乳腺癌(TNBC)细胞中均表现出细胞毒性。这些潜在的EGFR抑制剂有效地下调了TNBC中表皮生长因子(EGF)诱导的增殖、迁移、体外致瘤能力以及EGFR激活(pEGFR)。此外,与阿霉素联合使用时,所鉴定的EGFR抑制剂显著降低了EGF诱导的增殖。在较低浓度阿霉素存在的情况下,SN-04和SN-05显著增加了TNBC中凋亡标志物的表达,这一效果与单独使用较高浓度阿霉素治疗相当。这些观察结果表明,SN-04和/或SN-05均可在较低浓度下提高化疗药物阿霉素的疗效,以避免乳腺癌治疗期间高剂量化疗引起的副作用。
