目錄:MedChemExpress LLC>>生化試劑>> ADU-S100 | MCE
CAS | 1638241-89-0 | 純度 | 99.85% |
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分子量 | 690.54 | 分子式 | C??H??N??O??P?S? |
供貨周期 | 現貨 | 貨號 | HY-12885 |
應用領域 | 醫療衛生,化工,生物產業,制藥 |
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CAS No. : 1638241-89-0
產品活性:ADU-S100 (MIW815), an activator of stimulator of interferon genes (STING), leads to potent and systemic tumor regression and immunity.
研究領域:Immunology/Inflammation
作用靶點:STING
In Vitro: ADU-S100 is unstable in its free base form. ADU-S100 ammonium salt (HY-12885B) improves both stability and lipophilicity, promoting significantly increased STING signaling as compared to endogenous and pathogen-derived cyclic dinucleotides (CDNs).
ADU-S100 shows enhanced type I IFN production over CDA in THP-1 human monocytes. In contrast, the dithio, mixed-linkage CDN derivatives (ML RR-CDA, ML RR-S2 CDG, and ML RR-S2 cGAMP) potently activate all five hSTING alleles, including the refractory hSTINGREF and hSTINGQ alleles. ADU-S100 induces the highest expression of IFN-β and the pro-inflammatory cytokines TNF-α, IL-6, and MCP-1 on a molar equivalent basis, as compared to endogenous ML cGAMP and the TLR3 agonist poly I:C. ADU-S100 is also found to induce aggregation of STING and induce phosphorylation of TBK1 and IRF3 in mouse bone marrow macrophage (BMM). ADU-S100 induces significantly higher levels of IFN-α when compared to ML cGAMP.
In Vivo: ADU-S100 shows higher anti-tumor control than the endogenous ML cGAMP. A dose response of the ADU-S100 compound is performed in B16 tumor-bearing mice, which identifies an optimal antitumor dose level that also elicites maximum tumor antigen-specific CD8+ T cell responses, and improves long-term survival to 50%.
相關產品:Cyclic-di-GMP disodium | Dazostinag disodium | STING-IN-2 | CL845-PAB-Ala-Val-C5-MC | STING agonist-13 | STING agonist-26 | ADU-S100 ammonium salt | cGAMP | Ulevostinag | STING ligand-1 | STING agonist-28 | C-178 | C-176 | STING agonist-20 | 2',3'-cGAMP sodium | PROTAC STING Degrader-1 | CL656 | H-151 | STING agonist-12 | JAK-IN-23 | BSP16 | STING agonist-8 | STING modulator-5 | CCCP | IACS-8803 | STING agonist-11 | STING agonist-22 | STING agonist-24
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