Tubulysins, a family of natural products originally isolated from myxobacteria culture, inhibit tubulin polymerization, leading to apoptosis, thereby making them potential candidates for anticancer drug development. In this article, we report an advancement in the synthesis of third‐generation tubulin inhibitors developed in our laboratory by leveraging the first application of solid‐phase peptide synthesis (SPPS) to circumvent the limitations of conventional multistep solution‐phase synthesis. The tubulin inhibitors have been synthesized in high yields without incorporating tubuvaline and tubuphenylalanine fragments present in the natural tubulysins, which are known to be essential for their anticancer activity. The most active inhibitor contains 4 fragments, i.e., N ‐methyl‐ d ‐pipecolic acid ( N ‐Mep), l ‐isoleucine ( l ‐Ile), valine‐thiazole, and asparagine (Asn), arranged sequentially from the N‐terminus to the C‐terminus. The protocols enumerate an efficient synthesis of valine thiazole and N ‐methyl‐ d ‐pipecolic acid fragments, which are tethered using SPPS with a single purification step, resulting in high yields and enhancing their potential for scalable synthesis and therapeutic applications. The newly synthesized tubulin inhibitors exhibit anticancer activities with IC 50 values in the low nanomolar range. The incorporation of a simplified thiazole ring structure preserves the biological activity and chiral integrity of the molecules. The structure–activity relationship studies highlight that small changes at the N‐terminal fragment with various heterocyclic groups significantly reduce potency from nM to µM. In contrast, aliphatic C‐terminal changes have little effect, though aromatic C‐terminal modifications significantly impact the activity. This article describes an efficient method to synthesize simplified tubulin inhibitors, supporting further development of potent anticancer drugs. © 2025 Wiley Periodicals LLC. Basic Protocol 1 : Synthesis of Fmoc‐protected valine thiazole and N ‐methyl‐ d ‐pipecolic acid fragments Basic Protocol 2 : Synthesis and purification of tubulin inhibitors ( 11a to 11l ) using SPPS Basic Protocol 3 : In vitro cytotoxicity assay of tubulin inhibitors ( 11a to 11l ) against cancer cells derived from prostate, cervical, breast, lung, and skin using MTT assay

01 Sep 2025·BIOCHEMICAL PHARMACOLOGY

Synthetic homoisoflavane derivatives suppress the growth of colorectal cancer cells by disturbing microtubule dynamics

Article

Author: Choi, Jun-Kyu ; Kwon, Sangil ; Park, Insun ; Park, Sangkyu ; Shin, Ha-Eun ; Lee, Myeong-Heon ; Kwon, Hyung-Joo ; Lee, Younghee ; Eom, Won-Joon ; Seo, Seung-Yong ; Lee, Bit ; Kim, Dongbum ; Ji, Minkyu

Microtubules, composed of tubulin proteins, have a crucial role in various cellular processes, including cell cycle regulation. The dynamic instability of microtubules has been an attractive target for cancer therapy. This study investigated two potent anticancer drug candidates, homoisoflavane derivatives SH-19021 and SHA-035, and evaluated their potential as microtubule-targeting agents (MTAs) in human colorectal cancer cells. At early time points, both SH-19021 and SHA-035 induced G2/M phase arrest. They altered the expression of multiple cell cycle-related genes, notably downregulating tubulin mRNA levels, leading to reduced cell viability and apoptosis. To further explore their mechanism of action, we conducted in silico docking studies, which demonstrated the potential of SH-19021 and SHA-035 as tubulin inhibitors. Both compounds were shown to bind directly to tubulin proteins, inhibiting microtubule polymerization in vitro and disrupting microtubule structures in colorectal cancer cells. Additionally, SH-19021 exhibited antitumor activity in a mouse xenograft model implanted with HCT116 cells. These findings suggest that SH-19021 and SHA-035 are novel and potent microtubule destabilizers with promising potential for cancer treatment.

01 Aug 2025·BIOORGANIC CHEMISTRY

Discovery of novel flavonoid derivatives targeting VEGFR2 and tubulin with potent anticancer efficacy

Article

Author: Deng, Xiangping ; Liu, Renbo ; Wang, LiLi ; Tang, Guotao ; Yuan, Weixi ; Yang, Xiaoyan ; Lei, Xiaoyong ; Ye, Pengju ; Yang, Bo ; Xie, Zhizhong ; Peng, Yijiao ; He, Xiang ; Fu, Chengxiao ; Wang, Zhe

The clinical efficacy of VEGFR inhibitors and tubulin inhibitors as monotherapies is restricted by adverse reactions and resistance. We reported a classic pharmacophore hybridization strategy to develop dual VEGFR2/tubulin inhibitors that simultaneously inhibited tumor angiogenesis and tubulin assembly. A series of novel flavonoid derivatives containing N, N'-diethylurea group and trimethoxyphenyl were designed and synthesized. Among them, compound 6r demonstrated excellent antitumor activity in vitro and in vivo. Mechanistic studies revealed that 6r exerted antitumor activity by inhibiting VEGFR2 and tubulin in the micromolar range. Further studies showed that 6r inhibited angiogenesis in the CAM model. Additionally, 6r also demonstrated moderate PK profiles with broad tissue distribution characteristics and good safety. Notably, 6r inhibited tumor growth in the HGC-27 xenograft model. All the reported results suggested that 6r may be a potent anticancer candidate and merited further investigation.

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Indication	Highest Phase	Country/Location	Organization	Date
Neoplasms	Discovery	Czechia	Palacky University	22 Mar 2024

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