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Therapeutic implications of fibroblast growth factor receptor inhibitors in a combination regimen for solid tumors (Review)

Hong Luo, Tao� Zhang, Peng Cheng, Dong Li, Oleksandr Ogorodniitchouk, C. Lahmamssi, Ge Wang, Meiling Lan

2020Oncology Letters17 citationsDOIOpen Access PDF

Abstract

A number of novel drugs targeting the fibroblast growth factor receptor (FGFR) signaling pathway have been developed, including mostly tyrosine kinase inhibitors, selective inhibitors or monoclonal antibodies. Multiple preclinical and clinical studies have been conducted worldwide to ascertain their effects on diverse solid tumors. Drugs, such as lenvatinib, dovitinib and other non-specific FGFR inhibitors, widely used in clinical practice, have been approved by the Food and Drug Administration for cancer therapy, although the majority of drugs remain in preclinical tests or clinical research. The resistance to a single agent for FGFR inhibition with synthetic lethal action may be overcome by a combination of therapeutic approaches and FGFR inhibitors, which could also enhance the sensitivity to other therapeutics. Therefore, the aim of the present review is to describe the pharmacological characteristics of FGFR inhibitors that may be combined with other therapeutic agents and the preclinical data supporting their combination. Additionally, their clinical implications and the remaining challenges for FGFR inhibitor combination regimens are discussed.

Topics & Concepts

Fibroblast growth factor receptorMedicinePharmacologyTyrosine kinaseCancer researchCancerCombination therapyReceptor tyrosine kinaseFibroblast growth factorReceptorInternal medicineFibroblast Growth Factor ResearchKruppel-like factors researchMetastasis and carcinoma case studies
Therapeutic implications of fibroblast growth factor receptor inhibitors in a combination regimen for solid tumors (Review) | Litcius