Wu Guikai, Qiu Xiao-Long, Zhou Longen, Zhu Jiewen, Chamberlin Richard, Lau Johnson, Chen Phang-Lang, Lee Wen-Hwa
Department of Biological Chemistry, School of Medicine, University of California, Irvine, California 92697, USA.
Cancer Res. 2008 Oct 15;68(20):8393-9. doi: 10.1158/0008-5472.CAN-08-1915.
Hec1 is a conserved mitotic regulator critical for spindle checkpoint control, kinetochore functionality, and cell survival. Overexpression of Hec1 has been detected in a variety of human cancers and is linked to poor prognosis of primary breast cancers. Through a chemical genetic screening, we have identified a small molecule, N-(4-[2,4-dimethyl-phenyl]-thiazol-2-yl)-benzamide (INH1), which specifically disrupts the Hec1/Nek2 interaction via direct Hec1 binding. Treating cells with INH1 triggered reduction of kinetochore-bound Hec1 as well as global Nek2 protein level, consequently leading to metaphase chromosome misalignment, spindle aberrancy, and eventual cell death. INH1 effectively inhibited the proliferation of multiple human breast cancer cell lines in culture (GI(50), 10-21 micromol/L). Furthermore, treatment with INH1 retarded tumor growth in a nude mouse model bearing xenografts derived from the human breast cancer line MDA-MB-468, with no apparent side effects. This study suggests that the Hec1/Nek2 pathway may serve as a novel mitotic target for cancer intervention by small compounds.
Hec1是一种保守的有丝分裂调节因子,对纺锤体检查点控制、动粒功能和细胞存活至关重要。在多种人类癌症中均检测到Hec1的过表达,且其与原发性乳腺癌的不良预后相关。通过化学遗传学筛选,我们鉴定出一种小分子N-(4-[2,4-二甲基苯基]-噻唑-2-基)-苯甲酰胺(INH1),它通过直接结合Hec1特异性破坏Hec1/Nek2相互作用。用INH1处理细胞会引发动粒结合的Hec1以及整体Nek2蛋白水平降低,进而导致中期染色体排列紊乱、纺锤体异常,最终导致细胞死亡。INH1有效抑制了多种人乳腺癌细胞系在培养中的增殖(半数生长抑制浓度,10 - 21微摩尔/升)。此外,在携带源自人乳腺癌细胞系MDA-MB-468异种移植瘤的裸鼠模型中,用INH1治疗可延缓肿瘤生长,且无明显副作用。这项研究表明,Hec1/Nek2通路可能作为小分子化合物干预癌症的新型有丝分裂靶点。
