Blue Ridge Institute for Medical Research, 3754 Brevard Road, Suite 116, Box 19, Horse Shoe, NC, 28742-8814, United States.
Pharmacol Res. 2020 Jan;151:104567. doi: 10.1016/j.phrs.2019.104567. Epub 2019 Nov 23.
The human fibroblast growth factor family consists of 22 factors and five transmembrane receptors. Of the 22 factors, eighteen are secreted while four of them function exclusively within the cell. Four of the fibroblast growth factor receptors (FGFRs) possess intracellular protein-tyrosine kinase activity while the fifth (FGFRL1) has a short 105-residue intracellular non-enzymatic component. The FGFR protein kinase domain consists of a bi-lobed structure that is similar to that of all other protein kinases. FGFR gene alterations occur in a wide variety of cancers including those of the urinary bladder, breast, ovary, prostate, endometrium, lung, and stomach. The majority (66 %) of FGFR gene alterations involve gene amplifications, followed by mutations (26 %), and rearrangements that produce fusion proteins (8 %). Erdafitinib was the first orally effective FGFR antagonist approved by the FDA (2019) for the treatment of advanced cancer, that of the urinary bladder. FGF23 suppresses phosphate reabsorption in the proximal tubules of the kidney; FGF23 blockade allows phosphate reabsorption to occur and leads to elevated serum phosphate levels. Erdafitinib and several other, but not all, FGFR antagonists produce hyperphosphatemia. Erdafitinib binds to an inactive DGF-D conformation of FGFR1 and is classified as a type I½ inhibitor. Similarly, dovitinib, AZD4547, CH5183284, infigratinib, lenvatinib, LY2874455, and lucitanib are type I½ inhibitors. The inactive conformations contain an autoinhibitory brake that is made up of three main residues: an asparagine (N) within the αC-β4 back loop, a glutamate (E) corresponding to the second hinge residue, and a lysine (K) in the β8-strand (the NEK triad). PDGFRα/β, Kit, CSF1R, VEGFR1/2/3, Flt3, Tek, and Tie protein kinases are also regulated by a similar autoinhibitory brake mechanism. Ponatinib binds to FGFR4 in a DFG-D conformation and is classified as a type II inhibitor. Futibatinib, roblitinib, H3B-6527, fisogatinib, and PRN1371 bind covalently to their FGFR target and are classified as type VI inhibitors. Nintedanib, pazopanib, pemigatinib, rogaratinib, fisogatinib, and PRN1371 are FGFR inhibitors lacking drug-enzyme crystal structures. All of the aforementioned FGFR antagonists are orally effective. The development of FGFR inhibitors has lagged behind those of other receptor protein-tyrosine kinases. However, the FDA approval of erdafitinib for the treatment of urinary bladder cancers may stimulate additional work targeting the many other FGFR-driven neoplasms.
人类成纤维细胞生长因子家族由 22 个因子和 5 个跨膜受体组成。在这 22 个因子中,有 18 个是分泌型的,而其中 4 个仅在细胞内发挥作用。4 种成纤维细胞生长因子受体(FGFRs)具有细胞内蛋白酪氨酸激酶活性,而第 5 种(FGFRL1)具有 105 个残基的短细胞内非酶成分。FGFR 蛋白激酶结构域由一个双叶结构组成,与所有其他蛋白激酶相似。FGFR 基因改变发生在多种癌症中,包括膀胱癌、乳腺癌、卵巢癌、前列腺癌、子宫内膜癌、肺癌和胃癌。大多数(66%)FGFR 基因改变涉及基因扩增,其次是突变(26%)和产生融合蛋白的重排(8%)。厄达替尼是 FDA(2019 年)批准的第一种用于治疗晚期膀胱癌的口服有效 FGFR 拮抗剂。FGF23 抑制肾脏近端小管中的磷酸盐重吸收;FGF23 阻断允许磷酸盐重吸收发生,并导致血清磷酸盐水平升高。厄达替尼和其他几种(但不是全部)FGFR 拮抗剂会产生高磷血症。厄达替尼与 FGFR1 的无活性 DGF-D 构象结合,被归类为 I 型½抑制剂。同样,多韦替尼、AZD4547、CH5183284、英菲格拉替尼、仑伐替尼、LY2874455 和卢昔替尼也是 I 型½抑制剂。无活性构象包含由三个主要残基组成的自动抑制刹车:αC-β4 回环中的天冬酰胺(N)、对应于第二个铰链残基的谷氨酸(E)和β8-链中的赖氨酸(K)(NEK 三联体)。PDGFRα/β、Kit、CSF1R、VEGFR1/2/3、Flt3、Tek 和 Tie 蛋白激酶也受类似的自动抑制刹车机制调节。泊那替尼与 FGFR4 结合在 DFG-D 构象中,被归类为 II 型抑制剂。呋他替尼、罗格列替尼、H3B-6527、菲索替尼和 PRN1371 与 FGFR 靶标共价结合,被归类为 VI 型抑制剂。尼替西农、帕唑帕尼、培美替尼、罗加替尼、菲索替尼和 PRN1371 是缺乏药物酶晶体结构的 FGFR 抑制剂。上述所有 FGFR 拮抗剂均为口服有效。FGFR 抑制剂的开发落后于其他受体蛋白酪氨酸激酶。然而,FDA 批准厄达替尼治疗膀胱癌可能会刺激针对许多其他 FGFR 驱动的肿瘤的额外工作。
