AZD4547: An Orally Bioavailable, Potent, and Selective Inhibitor of the Fibroblast Growth Factor Receptor Tyrosine Kinase Family

Gavine, Paul R.; Mooney, Lorraine; Kilgour, Elaine; Thomas, Andrew P.; Al-Kadhimi, Katherine; Beck, Sarah; Rooney, Claire; Coleman, Tanya; Baker, Dawn; Mellor, Martine J.; Brooks, A. Nigel; Klinowska, Teresa

doi:10.1158/0008-5472.can-11-3034

Cited by 454 publications

(402 citation statements)

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“…Table 3). These results suggest FGFR1-gene amplification is important to predict sensitivity against FGFR inhibitors, and the apparent discrepancy may be a result of drug promiscuity; in contrast to NVP-BGJ398 and AZD4547 which are relatively selective pan-FGFR inhibitors 33,34 , Ponatinib inhibits a number of non-FGFR kinases with IC50 concentrations less than 10nM, including VEGFR, PDGFR, EPH receptors, SRC, KIT, and RET 35 .…”

Section: Resultsmentioning

confidence: 99%

Co-active receptor tyrosine kinases mitigate the effect of FGFR inhibitors in FGFR1-amplified lung cancers with low FGFR1 protein expression

et al. 2015

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Targeted therapies are effective in subsets of lung cancers with EGFR mutations and ALK translocations. Large-scale genomics have recently expanded the lung cancer landscape with FGFR1 amplification found in roughly 20% of squamous cell carcinomas (SCCs). However, the response rates have been low for biomarkerdirected FGFR inhibitor therapy in SCC, which contrasts to the relatively high rates of response seen in EGFR mutant and ALK translocated lung cancers treated with EGFR inhibitors and ALK inhibitors, respectively. In order to better understand the low response rates of FGFR1-amplified lung cancers to FGFR inhibitors, relationships between gene copy number, mRNA expression, and protein expression of FGFR1 were assessed in cell lines, tumor specimens, and data from The Cancer Genome Atlas (TCGA). The importance of these factors for the sensitivity to FGFR inhibitors was determined by analyzing drug screen data and conducting in vitro and in vivo experiments. We report that there was a discrepancy between FGFR1 amplification level and FGFR1 protein expression in a number of these cell lines, and the cancers with unexpectedly low FGFR1 expression were uniformly resistant to the different FGFR inhibitors.

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Section: Resultsmentioning

confidence: 99%

Co-active receptor tyrosine kinases mitigate the effect of FGFR inhibitors in FGFR1-amplified lung cancers with low FGFR1 protein expression

et al. 2015

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“…AZD4547 suppresses FGFR signaling and growth in tumor cell lines owing to deregulated FGFR expression. In a representative FGFR3-driven human tumor xenograft model, the oral administration of AZD4547 was well tolerated and resulted in potent antitumor activity ( 72 ). AZD4547 is currently being evaluated in a phase I clinical trial.…”

Section: Selective Anti-fgfr Tkismentioning

confidence: 99%

Fibroblast Growth Factor Receptor Inhibitors as a Cancer Treatment: From a Biologic Rationale to Medical Perspectives

et al. 2013

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The fi broblast growth factor/fi broblast growth factor receptor (FGF/FGFR) signaling pathway plays a fundamental role in many physiologic processes, including embryogenesis, adult tissue homeostasis, and wound healing, by orchestrating angiogenesis. Ligand-independent and ligand-dependent activation have been implicated in a broad range of human malignancies and promote cancer progression in tumors driven by FGF/FGFR oncogenic mutations or amplifi cations, tumor neoangiogenesis, and targeted treatment resistance, thereby supporting a strong rationale for anti-FGF/FGFR agent development. Efforts are being pursued to develop selective approaches for use against this pathway by optimizing the management of emerging, classspecifi c toxicity profi les and correctly designing clinical trials to address these different issues.Signifi cance: FGF/FGFR pathway deregulations are increasingly recognized across different human cancers. Understanding the mechanisms at the basis of these alterations and their multiple roles in cancer promotion and drug resistance is a fundamental step for further implementation of targeted therapies and research strategies. Cancer Discov;3(3);

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“…12,13 Thus, discovery of highly selective FGFR inhibitors is an unmet medical need. Currently, several selective FGFR inhibitors have progressed robustly into clinical trials, such as NVP-BGJ398, 14 AZD4547, 15 and CH5183284 16 (Figure 1). PD173074 (Figure 1), the first reported selective FGFR inhibitor, inhibits FGFR1 with an IC 50 value of 21.5 nM at the molecular level, while inhibiting PDGFR, c-Src and EGFR, as well as several serine/threonine kinases with 1000-fold or greater IC 50 values.…”

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confidence: 99%

“…AZD4547 inhibits FGFR1−4 (IC 50 = 0.2, 2.5, 1.8, and 165 nM, respectively) with low nanomolar potency at the molecular level, while inhibiting VEGFR2 with an IC 50 value of 24 nM. 15 Based on these findings, we wished to explore new scaffolds based on the structure of AZD4547, which had higher potency and higher selectivity for FGFR over VEGFR2 than AZD4547. By utilizing the scaffold hopping strategy and incorporation of chlorines at the 2-and 6-positions of the phenyl ring, we designed novel 1H-pyrazolo [3,4-b]pyridine scaffold derivatives (Figure 2), which demonstrated excellent in vitro and in vivo antitumor activities and high selectivity for FGFR over VEGFR2.…”

mentioning

confidence: 99%

Discovery of Substituted 1H-Pyrazolo[3,4-b]pyridine Derivatives as Potent and Selective FGFR Kinase Inhibitors

Zhao

et al. 2016

ACS Med. Chem. Lett.

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Fibroblast growth factor receptors (FGFRs) are important targets for cancer therapy. Herein, we describe the design, synthesis, and biological evaluation of a novel series of 1H-pyrazolo [3,4-b]pyridine derivatives as potent and selective FGFR kinase inhibitors. On the basis of its excellent in vitro potency and favorable pharmacokinetic properties, compound 7n was selected for in vivo evaluation and showed significant antitumor activity in a FGFR1-driven H1581 xenograft model. These results indicated that 7n would be a promising candidate for further drug development. Cancer, FGFR, inhibitor, pyrazolo[3,pyridine F ibroblast growth factors (FGFs) and their receptors regulate a wide range of biological functions, including embryogenesis, tissue repair, wound healing, and angiogenesis. 1−3 The fibroblast growth factor receptor (FGFR) family comprises four highly conserved transmembrane tyrosine kinase receptors (FGFR1−4), which are differentially activated by binding to a subset of 18 FGF ligands. 3,4 Upon FGF binding, FGFR undergoes dimerization and autophosphorylation, resulting in activation of downstream signaling pathways, such as the MAPK and PLCγ pathways. 4,5 These FGFR cascades play crucial roles in key cell behaviors, such as proliferation, survival, differentiation, and migration, which makes FGFR signaling susceptible to subversion by cancer cells. 6 Dysregulation of FGFR signaling has been documented in clinical samples of bladder, lung, breast cancers, etc., 7 and aberrant FGFR activation is closely correlated with metastatic progression and poor prognosis. 8,9 Knockdown studies and pharmaceutical inhibition of FGFRs in preclinical models have further demonstrated that FGFRs are attractive targets for cancer therapy. 4,7,10 In recent years, many small molecules have been in clinical development, such as nintedanib, dovitinib, and cediranib, which are reported to target FGFR. 11 However, because of the high degree of homology of FGFRs with VEGFRs, most of these compounds have multitarget specificity, which leads to undesired side effects in their anticancer therapies. 12,13 Thus, discovery of highly selective FGFR inhibitors is an unmet medical need. Currently, several selective FGFR inhibitors have progressed robustly into clinical trials, such as NVP-BGJ398, 14 AZD4547, 15 and CH5183284 16 (Figure 1). PD173074 (Figure 1), the first reported selective FGFR inhibitor, inhibits FGFR1 with an IC 50 value of 21.5 nM at the molecular level, while inhibiting PDGFR, c-Src and EGFR, as well as several serine/threonine kinases with 1000-fold or greater IC 50 values. 17 Nevertheless, PD173074 exhibits submicromolar inhibitory activity at the cellular level against VEGFR2 (IC 50 = 100−200 nM). 17 The crystal structure of PD173074 in complex with the FGFR1 kinase domain elucidates that its high affinity and selectivity for FGFR1 stem from the presence of 3,5-dimethoxy phenyl ring that adopts an almost perpendicular orientation to the plane of the KEYWORDS:

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AZD4547: An Orally Bioavailable, Potent, and Selective Inhibitor of the Fibroblast Growth Factor Receptor Tyrosine Kinase Family

Cited by 454 publications

References 40 publications

Co-active receptor tyrosine kinases mitigate the effect of FGFR inhibitors in FGFR1-amplified lung cancers with low FGFR1 protein expression

Co-active receptor tyrosine kinases mitigate the effect of FGFR inhibitors in FGFR1-amplified lung cancers with low FGFR1 protein expression

Fibroblast Growth Factor Receptor Inhibitors as a Cancer Treatment: From a Biologic Rationale to Medical Perspectives

Discovery of Substituted 1H-Pyrazolo[3,4-b]pyridine Derivatives as Potent and Selective FGFR Kinase Inhibitors

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