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Targeting the Hepatocyte Growth Factor and c-Met Signaling Axis in Bone Metastases

机译:靶向骨转移中的肝细胞生长因子和C-MET信号轴

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Bone metastasis is the terminal stage disease of prostate, breast, renal, and lung cancers, and currently no therapeutic approach effectively cures or prevents its progression to bone metastasis. One of the hurdles to the development of new drugs for bone metastasis is the complexity and heterogeneity of the cellular components in the metastatic bone microenvironment. For example, bone cells, including osteoblasts, osteoclasts, and osteocytes, and the bone marrow cells of diverse hematopoietic lineages interact with each other via numerous cytokines and receptors. c-Met tyrosine kinase receptor and its sole ligand hepatocyte growth factor (HGF) are enriched in the bone microenvironment, and their expression correlates with the progression of bone metastasis. However, no drugs or antibodies targeting the c-Met/HGF signaling axis are currently available in bone metastatic patients. This significant discrepancy should be overcome by further investigation of the roles and regulation of c-Met and HGF in the metastatic bone microenvironment. This review paper summarizes the key findings of c-Met and HGF in the development of novel therapeutic approaches for bone metastasis.
机译:骨转移是前列腺,乳腺癌,肾癌和肺癌的末期疾病,目前没有治疗方法有效地治愈或防止其进程对骨转移。新用于骨转移的新药物的障碍是转移性骨微环境中细胞组分的复杂性和异质性。例如,骨细胞,包括成骨细胞,破骨细胞和骨细胞,各种造血谱系的骨髓细胞通过许多细胞因子和受体相互作用。 C-Met酪氨酸激酶受体及其唯一的配体肝细胞生长因子(HGF)富集在骨微环境中,其表达与骨转移的进展相关。然而,骨转移患者目前没有靶向C-Met / HGF信号轴的药物或抗体。通过进一步调查转移性骨微环境中C-Met和HGF的作用和调节,应克服这种显着的差异。本综述论文总结了C-SET和HGF在开发骨转移方面的关键结果。

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