Lydon N B, Mett H, Mueller M, Becker M, Cozens R M, Stover D, Daniels D, Traxler P, Buchdunger E
Novartis Pharma AG, Oncology Research, Basel, Switzerland.
Int J Cancer. 1998 Mar 30;76(1):154-63. doi: 10.1002/(sici)1097-0215(19980330)76:1<154::aid-ijc24>3.0.co;2-b.
A calculated 3-D model of the kinase domain of the epidermal growth factor receptor (EGF-R) protein-tyrosine kinase (PTK) was used to develop a pharmacophore model for ATP-competitive inhibitors and, subsequently, a new class of selective EGF-R kinase inhibitors. CGP 59326A, a highly selective and potent inhibitor of the EGF-R in vitro, inhibited the proliferation of EGF-R-expressing epithelial lines, while having little anti-proliferative activity against EGF-R-negative lines. In contrast to previously described inhibitors, CGP 59326A had potent and selective in vivo anti-tumor activity at well-tolerated doses against EGF-R-expressing tumors (e.g., ED50 of 0.78 to 1.5 mg/kg for inhibition of A431 tumor growth). CGP 59326A inhibited growth of human tumor xenografts expressing the EGF-R but showed little activity against EGF-R-negative xenografts. Combination of CGP 59326A with cytotoxic agents resulted in tumor regression and cures. The high selectivity and attractive biological profile of CGP 59326A suggest that it could have therapeutic value in the treatment of proliferative diseases which involve mitogenic signaling from the EGF-R.
利用表皮生长因子受体(EGF-R)蛋白酪氨酸激酶(PTK)激酶结构域的计算三维模型,开发了一种用于ATP竞争性抑制剂的药效团模型,并随后开发了一类新型的选择性EGF-R激酶抑制剂。CGP 59326A是一种在体外对EGF-R具有高度选择性和强效的抑制剂,它能抑制表达EGF-R的上皮细胞系的增殖,而对EGF-R阴性细胞系几乎没有抗增殖活性。与先前描述的抑制剂不同,CGP 59326A在耐受性良好的剂量下,对表达EGF-R的肿瘤具有强效且选择性的体内抗肿瘤活性(例如,抑制A431肿瘤生长的ED50为0.78至1.5 mg/kg)。CGP 59326A抑制表达EGF-R的人肿瘤异种移植瘤的生长,但对EGF-R阴性异种移植瘤几乎没有活性。CGP 59326A与细胞毒性药物联合使用可导致肿瘤消退和治愈。CGP 59326A的高选择性和诱人的生物学特性表明,它在治疗涉及来自EGF-R的促有丝分裂信号传导的增殖性疾病方面可能具有治疗价值。
