从组合肽选择到药物原型(二):针对表皮生长因子受体途径。
From combinatorial peptide selection to drug prototype (II): targeting the epidermal growth factor receptor pathway.
机构信息
David H Koch Center, The University of Texas MD Anderson Cancer Center, Houston, TX 77030, USA.
出版信息
Proc Natl Acad Sci U S A. 2010 Mar 16;107(11):5118-23. doi: 10.1073/pnas.0915146107. Epub 2010 Feb 26.
Abstract
The epidermal growth factor receptor (EGFR), a tyrosine kinase, is central to human tumorigenesis. Typically, three classes of drugs inhibit tyrosine kinase pathways: blocking antibodies, small kinase inhibitors, and soluble ligand receptor traps/decoys. Only the first two types of EGFR-binding inhibitory drugs are clinically available; notably, no EGFR decoy has yet been developed. Here we identify small molecules mimicking EGFR and that functionally behave as soluble decoys for EGF and TGFalpha, ligands that would otherwise activate downstream signaling. After combinatorial library selection on EGFR ligands, a panel of binding peptides was narrowed by structure-function analysis. The most active motif was CVRAC (EGFR 283-287), which is necessary and sufficient for specific EGFR ligand binding. Finally, a synthetic retro-inverted derivative, (D)(CARVC), became our preclinical prototype of choice. This study reveals an EGFR-decoy drug candidate with translational potential.
摘要
表皮生长因子受体(EGFR)是一种酪氨酸激酶,在人类肿瘤发生中起着核心作用。通常,有三类药物可以抑制酪氨酸激酶途径:阻断抗体、小分子激酶抑制剂和可溶性配体受体陷阱/诱饵。只有前两种类型的 EGFR 结合抑制药物在临床上可用;值得注意的是,尚未开发出 EGFR 诱饵。在这里,我们鉴定了模拟 EGFR 的小分子,并且这些小分子在功能上表现为 EGF 和 TGFalpha 的可溶性诱饵,这些配体否则会激活下游信号。在对 EGFR 配体进行组合文库选择后,通过结构-功能分析对一组结合肽进行了筛选。最活跃的基序是 CVRAC(EGFR 283-287),它是特异性 EGFR 配体结合所必需和充分的。最后,合成的反向反转衍生物(D)(CARVC)成为我们选择的临床前原型。这项研究揭示了一种具有转化潜力的 EGFR 诱饵候选药物。
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