ASPH inhibitors, as identified in this context, represent a group of chemicals that target various signaling pathways potentially linked to the function of ASPH. These inhibitors primarily focus on disrupting kinase activity, which indirectly affects the processes and pathways in which ASPH is involved. The primary mechanism of action of these inhibitors is through the modulation of cell signaling pathways, particularly those related to cell adhesion, migration, and growth factor signaling. Kinase inhibitors form the major component of this class. Compounds like Sorafenib, Sunitinib, and Pazopanib target multiple kinases including VEGF receptors, which play a role in angiogenesis and cell migration. By inhibiting these kinases, these chemicals can indirectly influence the cellular processes associated with ASPH. Similarly, EGFR inhibitors like Erlotinib and Gefitinib target the epidermal growth factor receptor, a key player in cell growth and migration, pathways where ASPH is thought to be involved.
Other inhibitors in this class, such as Dasatinib, Lapatinib, and Vandetanib, have a broader spectrum of targets, including Src family kinases, HER2, and RET kinases. These broad-spectrum inhibitors provide an insight into the complex network of signaling pathways that intersect with ASPH's function. Multi-targeted inhibitors like Regorafenib and Cabozantinib, which inhibit a range of kinases including MET, VEGFR2, and RET, highlight the interconnected nature of signaling pathways that can indirectly influence ASPH activity.
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