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Methyl 3-amino-6-chloro-5-(phenethylamino)pyrazine-2-carboxylate is a complex organic compound with the molecular formula C15H16ClN5O2. It is characterized by the presence of a pyrazine ring, which is a six-membered aromatic ring containing two nitrogen atoms. The compound features a chloro substituent at the 6-position, an amino group at the 3-position, and a phenethylamino group at the 5-position. The phenethylamino group is derived from phenethylamine, which is an ethylamine with a phenyl group attached. The carboxylate group is located at the 2-position of the pyrazine ring, and the entire molecule is esterified with a methyl group. methyl 3-amino-6-chloro-5-(phenethylamino)pyrazine-2-carboxylate is of interest in the field of medicinal chemistry and may have potential applications in the development of pharmaceuticals due to its unique structure and functional groups.

2032-81-7

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2032-81-7 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 2032-81-7 includes 7 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 4 digits, 2,0,3 and 2 respectively; the second part has 2 digits, 8 and 1 respectively.
Calculate Digit Verification of CAS Registry Number 2032-81:
(6*2)+(5*0)+(4*3)+(3*2)+(2*8)+(1*1)=47
47 % 10 = 7
So 2032-81-7 is a valid CAS Registry Number.

2032-81-7Relevant academic research and scientific papers

Amiloride as a new RNA-binding scaffold with activity against HIV-1 TAR

Patwardhan, Neeraj N.,Ganser, Laura R.,Kapral, Gary J.,Eubanks, Christopher S.,Lee, Janghyun,Sathyamoorthy, Bharathwaj,Al-Hashimi, Hashim M.,Hargrove, Amanda E.

supporting information, p. 1022 - 1036 (2017/07/12)

Diversification of RNA-targeted scaffolds offers great promise in the search for selective ligands of therapeutically relevant RNA such as HIV-1 TAR. We herein report the establishment of amiloride as a novel RNA-binding scaffold along with synthetic routes for combinatorial C(5)- and C(6)-diversification. Iterative modifications at the C(5)- and C(6)-positions yielded derivative 24, which demonstrated a 100-fold increase in activity over the parent dimethylamiloride in peptide displacement assays. NMR chemical shift mapping was performed using the 2D SOFAST-[1H-13C] HMQC NMR method, which allowed for facile and rapid evaluation of binding modes for all library members. Cheminformatic analysis revealed distinct differences between selective and non-selective ligands. In this study, we evolved dimethylamiloride from a weak TAR ligand to one of the tightest binding selective TAR ligands reported to date through a novel combination of synthetic methods and analytical techniques. We expect these methods to allow for rapid library expansion and tuning of the amiloride scaffold for a range of RNA targets and for SOFAST NMR to allow unprecedented evaluation of small molecule:RNA interactions.

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