Abstract
Tubulin has been regarded as an attractive and successful molecular target in cancer therapy and drug discovery. Vicinal diaryl is a simple scaffold found in many colchicine site tubulin inhibitors, which is also an important pharmacophoric point of tubulin binding and anti-cancer activity. As the continuation of our research work on colchicine binding site tubulin inhibitors, we designed and synthesized a series of diarylamide N-containing heterocyclic derivatives by the combination of vicinal diaryl core and N-containing heterocyclic skeletons into one hybrid though proper linkers. Among of these compounds, compound 15b containing a 5-methoxyindole group exhibited the most potent inhibitory activity against the tested three human cancer cell lines (MGC-803, PC-3 and EC-109) with IC50 values of 1.56 μM, 3.56 μM and 14.5 μM, respectively. Besides, the SARs of these compounds were preliminarily studied and summarized. The most active compound 15b produced the inhibition of tubulin polymerization in a dose-dependent manner and caused microtubule network disruption in MGC-803 cells. Therefore, compound 15b was identified as a novel tubulin polymerization inhibitor targeting the colchicine binding site. In addition, the results of molecular docking also suggested compound 15b could tightly bind into the colchicine binding site of β-tubulin.
Highlights
Tubulin is an important component of the cytoskeleton and plays a vital role in the process of maintaining normal cell formation, cell mitosis, signal transduction and material transportation [1,2]
No colchicine site tubulin inhibitors have not been approved for clinical use; it is necessary to develop novel colchicine site tubulin inhibitors
Vicinal diaryl is a simple scaffold found in many colchicine site tubulin inhibitors, which is an important pharmacophoric of tubulin binding and anti-cancer acVicinal diaryl is a simple scaffold found point in many colchicine site tubulin inhibitors, tivity
Summary
Tubulin is an important component of the cytoskeleton and plays a vital role in the process of maintaining normal cell formation, cell mitosis, signal transduction and material transportation [1,2]. Analog, Natural which colchicine site tubulin inhibitor combretastatin is a 1,2including multidrug cancer potent cells and could effectively inhibit the polymerization diarylethylene analog,resistant which exhibits inhibitory potency against many cancer cells of tubulinmultidrug [14]. 5 as an anti-tubulin agent thebinding colchicine indole derivative 5 as an anti-tubulin agent targeting thetargeting colchicine sitebinding showed site showed effective inhibition effect against tested cancer cell lines with. Tetrahydroquinoline-pyrimidine [38] showed strong anti-proliferative activity (IC50 anti-proliferative activity (IC50 values ranging from 5.6 to 18.3 nM) via tubulin polymerization inhibition and potently inhibited tumor growth in an A375 melanoma xenograft model (Figure 2). Nbindingsite site tubulin tubulin inhibitors, we Nbinding we designed designed and andsynthesized synthesizeda aseries seriesofofdiarylamide diarylamide containing heterocyclic derivatives by the combination of vicinal diaryl core and.
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