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275371-94-3 | Taspoglutide

Taspoglutide NLT 98%

Product Number : MC545905

CAS Number : 275371-94-3

Molecular Formula : C152H232N40O45 | Molecular Weight : 3339.71

Synonyms : ITM077;R1583;BIM51077

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Purity NLT 98%
Storage at 20ºC 2 years
MolCore specializes in manufacturing high-purity CAS No.275371-94-3, Taspoglutide with the molecular formula C152H232N40O45 and molecular weight 3339.71 delivering critical API intermediates for global pharmaceutical and research industries, certified under ISO quality systems.

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Chemical Name Taspoglutide
CAS Number 275371-94-3
MDL Number MFCD13195564
Molecular Formula C152H232N40O45
Molecular Weight 3339.71
Synonyms ITM077;R1583;BIM51077
Introduction of 275371-94-3 :

Taspoglutide is a long-acting glucagon-like peptide 1 (GLP-1) receptor agonist developed for treatment of type 2 diabetes, with an EC50 value of 0.06 nM. IC50 & Target: EC50: 0.06 nM (GLP-1)[1] In Vitro: Taspoglutide (R1583/BIM51077) is a long acting 10% formulation of (Aib8-35) human GLP-1 (7-36 amides) with 93% homology with the native polypeptide. It activates the GLP-1 receptor. Taspoglutide has comparable affinity (affinity constant 1.1±0.2 nM) to the natural ligand (affinity constant 1.5±0.3 nM) for the hGLP-1 receptor and exhibits comparable potency in stimulating cAMP production[2]. In Vivo: Taspoglutide has been shown to enhance the rate of glucose-induced insulin secretion from isolated, cultured rat islets and the perfused ZDF rat pancreas. Taspoglutide in Sprague-Dawley rats and diabetic db/db mice have shown a dose-related enhancement of glucose-dependent insulin release, which lower blood glucose in the db/db mouse model of type 2 diabetes[3]. Acute treatment with taspoglutide reduces glucose excursion and increased insulin response during oGTT. In chronically treated rats, glucose excursion and levels of GIP, PYY and triglycerides during oGTT on day 21 are significantly reduced[4]. Hepatic triglyceride levels are significantly reduced in livers from taspoglutide-treated. Taspoglutide does not reduce plaque area or lipid content in the aortic arch or abdominal aorta, and no significant change in aortic macrophage accumulation is detected after taspoglutide or metformin mice[5].