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THI0019 Sale

目录号 : GC61332

THI0019是一种有效的整联蛋白α4β1(VLA-4)激动剂,EC50范围为1-2μM。THI0019诱导干/祖细胞粘附。THI0019还调节由α4β7,α5β1和αLβ2介导的粘附。

THI0019 Chemical Structure

Cas No.:1378532-99-0

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5mg
¥2,070.00
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10mg
¥3,510.00
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产品描述

THI0019 is a potent integrin α4β1 (VLA-4) agonist with an EC50 range of 1-2 μM. THI0019 induces stem/progenitor cells adhesion. THI0019 also regulates adhesion mediated by α4β7, α5β1 and αLβ2[1].

In cell adhesion assays in which Jurkat cells bound to CS1-conjugated BSA, THI0019 shows a dose-dependent enhancement in cell binding with an EC50 of 1.7 μM. When VCAM-1 is used as the ligand, THI0019 induces an even more pronounced 100-fold increase in Jurkat cell binding, with an EC50 of 1.2 μM. THI0019 induces a dose-dependent increase in EPC binding to VCAM-1 (EC50 of 3.7 μM). THI0019 facilitates the rolling and spreading of cells on VCAM-1 and the migration of cells toward SDF-1α[1].

[1]. Peter Vanderslice, et al. Small molecule agonist of very late antigen-4 (VLA-4) integrin induces progenitor cell adhesion. J Biol Chem. 2013 Jul 5;288(27):19414-28.

Chemical Properties

Cas No. 1378532-99-0 SDF
Canonical SMILES O=C(N[C@@H](CCCC)COC(N(CC1=CC=CS1)CC2=CC=CS2)=O)N[C@H](C3=CC=C4C(OCO4)=C3)CC(OC)=O
分子式 C29H35N3O7S2 分子量 601.73
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1 mM 1.6619 mL 8.3094 mL 16.6187 mL
5 mM 0.3324 mL 1.6619 mL 3.3237 mL
10 mM 0.1662 mL 0.8309 mL 1.6619 mL
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Research Update

Small molecule agonist of very late antigen-4 (VLA-4) integrin induces progenitor cell adhesion

J Biol Chem 2013 Jul 5;288(27):19414-28.PMID:23703610DOI:PMC3707645

Activation of the integrin family of cell adhesion receptors on progenitor cells may be a viable approach to enhance the effects of stem cell-based therapies by improving cell retention and engraftment. Here, we describe the synthesis and characterization of the first small molecule agonist identified for the integrin α4β1 (also known as very late antigen-4 or VLA-4). The agonist, THI0019, was generated via two structural modifications to a previously identified α4β1 antagonist. THI0019 greatly enhanced the adhesion of cultured cell lines and primary progenitor cells to α4β1 ligands VCAM-1 and CS1 under both static and flow conditions. Furthermore, THI0019 facilitated the rolling and spreading of cells on VCAM-1 and the migration of cells toward SDF-1α. Molecular modeling predicted that the compound binds at the α/β subunit interface overlapping the ligand-binding site thus indicating that the compound must be displaced upon ligand binding. In support of this model, an analog of THI0019 modified to contain a photoreactive group was used to demonstrate that when cross-linked to the integrin, the compound behaves as an antagonist instead of an agonist. In addition, THI0019 showed cross-reactivity with the related integrin α4β7 as well as α5β1 and αLβ2. When cross-linked to αLβ2, the photoreactive analog of THI0019 remained an agonist, consistent with it binding at the α/β subunit interface and not at the ligand-binding site in the inserted ("I") domain of the αL subunit. Co-administering progenitor cells with a compound such as THI0019 may provide a mechanism for enhancing stem cell therapy.