Lung cancer is holding the position as the leading cause of cancer-related mortality worldwide, recorded approximately 2.5 million new cases and 1.8 million deaths in 2022. Non-small cell lung cancer, accounting for the majority of cases, faces significant treatment challenges due to its high invasiveness and rapid drug resistance development, necessitating novel strategies beyond conventional chemotherapy. Evodiamine, a natural alkaloid derived from Tetradium ruticarpum, has demonstrated anticancer potential through mechanisms involving apoptosis activation, reduction of Bcl-2 and phospho-AKT expression, as well as inhibition of phospho-NF-κB. The anti-apoptotic protein Bcl-2 (6GL8) prevents the release of mitochondrial factors, emerging as a critical target in cancer therapy. This study explored the molecular mechanism of Evodiamine against Bcl-2 (6GL8) in human non-small cell lung cancer using in silico methods. Molecular docking revealed that Evodiamine exhibited superior stability and stronger binding affinity within the protein pocket compared to navitoclax. In silico evaluation disclosed favorable pharmacokinetic properties of Evodiamine, including efficient absorption and stable metabolism, despite indications of toxicity. These findings affirm Evodiamine as a leading candidate for non-small cell lung cancer therapy through inhibition of Bcl-2-mediated apoptosis, providing a foundation for developing safer compounds with enhanced activity targeting apoptosis pathways in lung cancer treatment.

6GL8; Alkaloid; Apoptosis; Molecular docking; Drug-likeness; Evodiamine

[1] F. Bray, M. Laversanne, H. Sung, J. Ferlay, R. L. Siegel, I. Soerjomataram, and A. Jemal, “Global cancer statistics 2022: GLOBOCAN estimates of incidence and mortality worldwide for 36 cancers in 185 countries,” CA: A Cancer Journal for Clinicians, vol. 74, no. 3, pp. 229–263, 2024.

[2] F. H. Tang, H. Y. T. Wong, P. S. W. Tsang, M. Yau, S. Y. Tam, L. Law, K. Yau, J. Wong, F. H. M. Farah, and J. Wong, “Recent advancements in lung cancer research: a narrative review,” Translational Lung Cancer Research, vol. 14, no. 3, 2025, Art. no. 975.

[3] P. Garg, S. Singhal, P. Kulkarni, D. Horne, J. Malhotra, R. Salgia, and S. S. Singhal, “Advances in non-small cell lung cancer: current insights and future directions,” Journal of Clinical Medicine, vol. 13, no. 14, 2024, Art. no. 4189.

[4] Shivika, M. Sharma, A. Bajpai, Z. A. Dar, R. Singh, and R. Bansal, “Therapeutic dominance of tyrosine kinase inhibitors in non-small cell lung cancer (NSCLC),” Bioorganic Chemistry, vol. 163, 2025, Art. no. 108660.

[5] S. Hashem, T. A. Ali, S. Akhtar, S. Nisar, G. Sageena, S. Ali, S. Al-Mannai, L. Therachiyil, R. Mir, I. Elfaki, M. M. Mir, F. Jamal, T. Masoodi, S. Uddin, M. Singh, M. Haris, M. Macha, and A. A. Bhat, “Targeting cancer signaling pathways by natural products: Exploring promising anti-cancer agents,” Biomedicine & Pharmacotherapy, vol. 150, 2022, Art. no. 113054.

[6] A. S. Choudhari, P. C. Mandave, M. Deshpande, P. Ranjekar, and O. Prakash, “Phytochemicals in Cancer Treatment: From Preclinical Studies to Clinical Practice,” Frontiers in Pharmacology, vol. 10, 2020, Art. no. 1614.

[7] J. Sharifi-Rad, S. Rajabi, M. Martorell, M. D. López, M. T. Toro, S. Barollo, D. Armanini, P. V. T. Fokou, G. Zagotto, G. Ribaudo, and R. Pezzani, “Plant natural products with anti-thyroid cancer activity,” Fitoterapia, vol. 146, 2020, Art. no. 104640.

[8] V. Mohan, R. Agarwal, and R. P. Singh, “A novel alkaloid, evodiamine causes nuclear localization of cytochrome-c and induces apoptosis independent of p53 in human lung cancer cells,” Biochemical and Biophysical Research Communications, vol. 477, no. 4, pp. 1065–1071, 2016.

[9] S. H. Kim, J. G. Kang, C. S. Kim, S. H. Ihm, M. G. Choi, and S. J. Lee, “Evodiamine Suppresses Survival, Proliferation, Migration and Epithelial–Mesenchymal Transition of Thyroid Carcinoma Cells,” Anticancer Research, vol. 38, no. 11, pp. 6339–6352, 2018.

[10] G. Sliwoski, S. Kothiwale, J. Meiler, and E. W. Lowe, “Computational methods in drug discovery,” Pharmacological Reviews, vol. 66, no. 1, pp. 334–395, 2014.

[11] S. K. Niazi and Z. Mariam, “Computer-aided drug design and drug discovery: A prospective analysis,” Pharmaceuticals, vol. 17, no. 1, 2024, Art. no. 22.

[12] V. T. Sabe, T. Ntombela, L. A. Jhamba, G. E. M. Maguire, T. Govender, T. Naicker, and H. G. Kruger, “Current trends in computer aided drug design and a highlight of drugs discovered via computational techniques: A review,” European Journal of Medicinal Chemistry, vol. 224, 2021, Art. no. 113705.

[13] Y. Wang, H. Ma, A. Narula, L. Liu, and K. S. Ahn, “Molecular targets and anticancer potential of evodiamine,” Phytochemistry Letters, vol. 52, pp. 92–103, 2022.

[14] J. J. Lu, J. L. Bao, X. P. Chen, M. Huang, and Y. T. Wang, “Alkaloids isolated from natural herbs as the anticancer agents,” Evidence‐Based Complementary and Alternative Medicine, vol. 2012, no. 1, 2012, Art. no. 485042.

[15] J. Y. Hong, S. H. Park, H. Y. Min, H. J. Park, and S. K. Lee, “Anti-proliferative effects of evodiamine in human lung cancer cells,” Journal of Cancer Prevention, vol. 19, no. 1, pp. 7–13, 2014.

[16] N. S. N. Hisam, A. Ugusman, N. F. Rajab, M. F. Ahmad, M. Fenech, S. L. Liew, and N. N. M. Anuar, “Combination therapy of navitoclax with chemotherapeutic agents in solid tumors and blood cancer: a review of current evidence,” Pharmaceutics, vol. 13, no. 9, 2021, Art. no. 1353.

[17] C. V. Hoang, T. Q. Tu, H. D. Nguyen, and M. H. Chu, “In silico studies of saponins from Hoya verticillata var. verticillate with important apoptosis potency,” Letters in Organic Chemistry, vol.22, pp. 1-9, 2025.

[18] P. Casara, J. Davidson, A. Claperon, G. Le Toumelin-Braizat, M. Vogler, A. Bruno, M. Chanrion, G. Lysiak-Auvity, T. Le Diguarher, J. B. Starck, and I. Chen, “S55746 is a novel orally active Bcl-2 selective and potent inhibitor that impairs hematological tumor growth,” Oncotarget, vol. 9, no. 28, 2018, Art. no. 20075.

[19] P. Chihomvu, A. Ganesan, S. Gibbons, K. Woollard, and M. A. Hayes, “Phytochemicals in drug discovery-A confluence of tradition and innovation,” International journal of molecular sciences, vol. 25, no. 16, 2024, Art. no. 8792.

[20] D. E. V Pires, T. L. Blundell, and D. B. Ascher, “pkCSM: Predicting Small-Molecule Pharmacokinetic and Toxicity Properties Using Graph-Based Signatures,” Journal of Medicinal Chemistry, vol. 58, no. 9, pp. 4066–4072, 2015.

[21] E. Sun and F. E. Cohen, “Computer-assisted drug discovery - a review,” Gene, vol. 137, no. 1, pp. 127–132, 1993.

[22] G. G. Ferenczy and M. Kellermayer, “Contribution of hydrophobic interactions to protein mechanical stability,” Computational and Structural Biotechnology Journal, vol. 20, pp. 1946–1956, 2022.

[23] B. Yang, P. Ren, L. Xing, S. Wang, and C. Sun, “Roles of hydrogen bonding interactions and hydrophobic effects on enhanced water structure in aqueous solutions of amphiphilic organic molecules,” Spectrochimica Acta Part A: Molecular and Biomolecular Spectroscopy, vol. 296, 2023, Art. no. 122605.

[24] S. M. Vinod, S. M. Sreedevi, A. Krishnan, K. Ravichandran, P. Karthikeyan, B. Kotteswaran, and K. Rajendran, “Complexity of the role of various site-specific and selective sudlow binding site drugs in the energetics and stability of the acridinedione dye–bovine serum albumin complex: A molecular docking approach,” ACS Omega, vol. 8, no. 6, pp. 5634–5654, 2023.

[25] M. Y. Alsedfy, A. A. Ebnalwaled, M. Moustafa, and A. H. Said, “Investigating the binding affinity, molecular dynamics, and ADMET properties of curcumin-IONPs as a mucoadhesive bioavailable oral treatment for iron deficiency anemia,” Scientific Reports, vol. 14, no. 1, 2024, Art. no. 22027.

[26] F. Cheng, W. Li, G. Liu, and Y. Tang, “In silico ADMET prediction: recent advances, current challenges and future trends,” Current topics in medicinal chemistry, vol. 13, no. 11, pp. 1273-1289, 2013.

[27] Z. Hong, Z. Wang, B. Zhou, J. Wang, H. Tong, Y. Liao, P. Zheng, M. N. Jamshed, Q. Zhang, and H. Chen, “Effects of evodiamine on PI3K/Akt and MAPK/ERK signaling pathways in pancreatic cancer cells,” International Journal of Oncology, vol. 56, no. 3, pp. 783-793, 2020.