الصفحة الرئيسية>>Signaling Pathways>> Immunology/Inflammation>> STING>>ADU-S100 disodium salt

ADU-S100 disodium salt (Synonyms: MIW815 disodium salt; ML RR-S2 CDA disodium salt)

رقم الكتالوجGC39161

ملح ثنائي الصوديوم ADU-S100 (ملح ثنائي الصوديوم MIW815) هو منشط لمحفز جينات الإنترفيرون (ستينج)

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ADU-S100 disodium salt التركيب الكيميائي

Cas No.: 1638750-95-4

الحجم السعر المخزون الكميّة
1mg
306٫00
متوفر
5mg
1112٫00
متوفر
10mg
1854٫00
متوفر

Tel:(909) 407-4943 Email: sales@glpbio.com

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Sample solution is provided at 25 µL, 10mM.

Description Protocol Chemical Properties Product Documents Related Products

ADU-S100 disodium salt (MIW815 disodium salt) is an activator of stimulatory interferon gene (STING) protein with a Kd of 4.61±0.42μM[1]. The mechanism of action of ADU-S100 disodium salt is to activate the STING pathway by simulating the effect of cyclic GMP-AMP (cGAMP), thereby inducing the production of inflammatory cytokines such as IFN-β[2]. ADU-S100 disodium salt shows higher anti-tumor ability than endogenous ML cGAMP [3].

In vitro, ADU-S100 disodium salt (0-100µM) treated glioblastoma (GBM) cells without toxicity, but in the presence of PBMC, ADU-S100 produced immune-mediated cytotoxicity against GBM cells at 12.5 and It is effective between 50µM and less effective at 100µM[4]. ADU-S100 disodium salt stimulated the THP-1 Dual cell line for 48 hours, and the EC50 values of activated cell IRF 3 and NF-κB pathways were 3.031 and 4.839µg/mL respectively [5].

In vivo, ADU-S100 disodium salt (50µg) was administered via intracranial injection to GL 261 and CT-2A tumor model mice 3 days after treatment, causing suppression of microglia and T cell populations, as well as NK and inflammatory responses. In the infiltration of immune cells, the proportion of T cells recovered 7 days after treatment and increased compared with the baseline level [4]. ADU-S100 disodium salt (20 or 40µg) was treated by subcutaneous injection in colon cancer model mice, which effectively inhibited the growth of CT-26 tumors, significantly increased the number of lymphocytes, and prevented tumor metastasis to liver and spleen tissues[6].

 

References:

[1]Jekle A, Thatikonda S, Stevens S, et al. Abstract 4520: Preclinical characterization of ALG-031048, a novel STING agonist with potent anti-tumor activity in mice[C]//Proceedings: AACR Annual Meeting 2020; April 27-28, 2020 and June 22-24.

[2]Jneid B, Bochnakian A, Hoffmann C, et al. Selective STING stimulation in dendritic cells primes antitumor T cell responses[J]. Science Immunology, 2023, 8(79): eabn6612.

[3]Corrales L, et al. Direct Activation of STING in the Tumor Microenvironment Leads to Potent and Systemic Tumor Regression and Immunity[J]. Cell Rep. 2015 May 19;11(7):1018-30. 

[4]Berger G, Knelson E H, Jimenez-Macias J L, et al. STING activation promotes robust immune response and NK cell–mediated tumor regression in glioblastoma models[J]. Proceedings of the National Academy of Sciences, 2022, 119(28): e2111003119.

[5]Ji N, Wang M, Tan C. Liposomal delivery of MIW815 (ADU-S100) for potentiated STING activation[J]. Pharmaceutics, 2023, 15(2): 638.

[6]Zaidi A H, Kelly R J, Gorbunova A, et al. Intratumoral immunotherapy with STING agonist, ADU-S100, induces CD8+ T-cell mediated anti-tumor immunity in an esophageal adenocarcinoma model[J]. Oncotarget, 2021, 12(4): 292.

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