Shc4 Inhibitors primarily functions by indirectly modulating the signaling pathways associated with Shc4, an adaptor protein. For example, Lapatinib and Gefitinib, which inhibit EGFR, and Dasatinib, targeting Src family kinases, can impede processes related to Shc4's involvement in cellular signaling. Imatinib, with its ability to target BCR-ABL and c-KIT, and Saracatinib, a Src kinase inhibitor, further exemplify the strategy of influencing Shc4's activity by modulating proximal signaling events.
Additionally, compounds like Sunitinib and Pazopanib, known for their action on receptor tyrosine kinases, offer another avenue to indirectly adjust Shc4's activity. This is especially relevant given Shc4's association with receptor tyrosine kinase-mediated pathways. Vandetanib, Bosutinib, and Linsitinib similarly extend this approach by targeting an array of kinases and receptors, demonstrating the intricate interplay and for indirect modulation of Shc4 activity within a cell.
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