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3-[2-(4-chlorophenyl)-3-(methyloxy)-3-oxopropanoyl]-2-pyrazinecarboxylic acid is a chemical with a specific purpose. Lookchem provides you with multiple data and supplier information of this chemical.

1401246-69-2

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1401246-69-2 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 1401246-69-2 includes 10 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 7 digits, 1,4,0,1,2,4 and 6 respectively; the second part has 2 digits, 6 and 9 respectively.
Calculate Digit Verification of CAS Registry Number 1401246-69:
(9*1)+(8*4)+(7*0)+(6*1)+(5*2)+(4*4)+(3*6)+(2*6)+(1*9)=112
112 % 10 = 2
So 1401246-69-2 is a valid CAS Registry Number.

1401246-69-2Downstream Products

1401246-69-2Relevant academic research and scientific papers

Synthesis and pharmacological investigation of azaphthalazinone human histamine H1 receptor antagonists

Procopiou, Panayiotis A.,Browning, Christopher,Gore, Paul M.,Lynn, Sean M.,Richards, Stephen A.,Slack, Robert J.,Sollis, Steven L.

, p. 6097 - 6108 (2012/11/07)

5-Aza, 6-aza, 7-aza and 8-aza-phthalazinone, and 5,8-diazaphthalazinone templates were synthesised by stereoselective routes starting from the appropriate pyridine/pyrazine dicarboxylic acids by activation with CDI, reaction with 4-chlorophenyl acetate ester enolate to give a β-ketoester, which was hydrolysed, and decarboxylated. The resulting ketone was condensed with hydrazine to form the azaphthalazinone core. The azaphthalazinone cores were alkylated with N-Boc-D-prolinol at N-2 by Mitsunobu reaction, de-protected, and then alkylated at the pyrrolidine nitrogen to provide the target H 1 receptor antagonists. All four mono-azaphthalazinone series had higher affinity (pKi) for the human H1 receptor than azelastine, but were not as potent as the parent non-aza phthalazinone. The 5,8-diazaphthalazinone was equipotent with azelastine. The least potent series were the 7-azaphthalazinones, whereas the 5-azaphthalazinones were the most lipophilic. The more hydrophilic series were the 8-aza series. Replacement of the N-methyl substituent on the pyrrolidine with the n-butyl group caused an increase in potency (pA2) and a corresponding increase in lipophilicity. Introduction of a β-ether oxygen in the n-butyl analogues (2-methoxyethyl group) decreased the H1 pA2 slightly, and increased the selectivity against hERG. The duration of action in vitro was longer in the 6-azaphthalazinone series. The more potent and selective 6-azaphthalazinone core was used to append an H3 receptor antagonist fragment, and to convert the series into the long acting single-ligand, dual H1 H3 receptor antagonist 44. The pharmacological profile of 44 was very similar to our intranasal clinical candidate 1.

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