A Novel Pyrazole Exhibits Potent Anticancer Cytotoxicity via Apoptosis, Cell Cycle Arrest, and the Inhibition of Tubulin Polymerization in Triple-Negative Breast Cancer Cells

Author:

Borrego Edgar A.12,Guerena Cristina D.12,Schiaffino Bustamante Austre Y.12ORCID,Gutierrez Denisse A.12,Valenzuela Carlos A.12,Betancourt Ana P.12,Varela-Ramirez Armando12ORCID,Aguilera Renato J.12ORCID

Affiliation:

1. The Border Biomedical Research Center, The University of Texas El Paso, El Paso, TX 79968, USA

2. Department of Biological Sciences, The University of Texas El Paso, El Paso, TX 79968, USA

Abstract

In this study, we screened a chemical library to find potent anticancer compounds that are less cytotoxic to non-cancerous cells. This study revealed that pyrazole PTA-1 is a potent anticancer compound. Additionally, we sought to elucidate its mechanism of action (MOA) in triple-negative breast cancer cells. Cytotoxicity was analyzed with the differential nuclear staining assay (DNS). Additional secondary assays were performed to determine the MOA of the compound. The potential MOA of PTA-1 was assessed using whole RNA sequencing, Connectivity Map (CMap) analysis, in silico docking, confocal microscopy, and biochemical assays. PTA-1 is cytotoxic at a low micromolar range in 17 human cancer cell lines, demonstrating less cytotoxicity to non-cancerous human cells, indicating a favorable selective cytotoxicity index (SCI) for the killing of cancer cells. PTA-1 induced phosphatidylserine externalization, caspase-3/7 activation, and DNA fragmentation in triple-negative breast MDA-MB-231 cells, indicating that it induces apoptosis. Additionally, PTA-1 arrests cells in the S and G2/M phases. Furthermore, gene expression analysis revealed that PTA-1 altered the expression of 730 genes at 24 h (198 upregulated and 532 downregulated). A comparison of these gene signatures with those within CMap indicated a profile similar to that of tubulin inhibitors. Subsequent studies revealed that PTA-1 disrupts microtubule organization and inhibits tubulin polymerization. Our results suggest that PTA-1 is a potent drug with cytotoxicity to various cancer cells, induces apoptosis and cell cycle arrest, and inhibits tubulin polymerization, indicating that PTA-1 is an attractive drug for future clinical cancer treatment.

Funder

NIH

core facilities of the Border Biomedical Research Center

Research Centers at Minority Institutions

NIGMS

Publisher

MDPI AG

Reference59 articles.

1. (2022, March 31). What Is Cancer?—National Cancer Institute, Available online: https://www.cancer.gov/about-cancer/understanding/what-is-cancer.

2. (2022, March 31). Cancer—Symptoms and Causes—Mayo Clinic. Available online: https://www.mayoclinic.org/diseases-conditions/cancer/symptoms-causes/syc-20370588.

3. Hallmarks of Cancer: The next Generation;Hanahan;Cell,2011

4. Wang, B., He, F., Hu, Y., Wang, Q., Wang, D., Sha, Y., and Wu, J. (2022). Cancer Incidence and Mortality and Risk Factors in Member Countries of the “ Belt and Road “ Initiative. BMC Cancer, 22.

5. Cancer Statistics, 2023;Siegel;CA Cancer J. Clin.,2023

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