AbstractWe contribute with the design and synthesis of novel 2,3‐diphenyl‐2H‐indazole hybrids series (1–14). Compounds 4 and 6 had the highest antiproliferative activity against the cancer cell lines, HeLa, SK‐LU‐1, K‐562, PC‐3, SW620 and MCF‐7 (CC50 values from 3 to 5.4 μM). Their activity was also evaluated against a normal human cell line, showing their higher Selectivity Index against the cancer cell lines than the reference drug CA‐4. The inhibition of tubulin assembly by compounds 4 and 6 was determined using in vitro tubulin polymerization assay and Western Blotting. The induction of mitotic catastrophe was observed with immunofluorescence assays. Besides, it was demonstrated by flow cytometry that compounds 4 and 6 arrest HeLa cell cycle at G2/M and promote apoptotic cell death. The mitotic arrest was also associated with elevated levels of cyclin B1 protein. We have identified two hybrids that behave as microtubule‐destabilizing agents on different cancer cell lines.