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Author:

Zeng Cheng-Chu (Zeng Cheng-Chu.) (Scholars:曾程初) | Li Xue-Mei (Li Xue-Mei.) | Yan Hong (Yan Hong.) | Zhong Ru-Gang (Zhong Ru-Gang.) (Scholars:钟儒刚)

Indexed by:

Scopus SCIE

Abstract:

Diketo acid derivatives are potent and selective HIV-1 integrase inhibitors. To investigate the detailed synthesis of those derivatives, a series of p/m-[p-(un)substituted phenylsulfonamidolphenyl beta-diketo acid derivatives have been designed and synthesized. The quinoxalone derivatives as the potential bioisosteres of the biologically labile beta-diketoacid pharmacophores have also been synthesized from reactions of the corresponding diketo acids with o-phenylenediamine. The structures of all diketo acid (ester) and quinoxalone derivatives were confirmed by H-1 NMR, C-13 NMR, IR, HRMS and/or MS (ESI). X-ray crystallographic analysis of 11b demonstrates a similar arrangement of the side chain of quinoxalone derivatives with the parent diketoacids due to the intramolecular hydrogen bond (O center dot center dot center dot H-N) and the sp(2) hybridization configuration of the two nitrogen atoms of the quinoxalone ring.

Keyword:

quinoxalone derivative HIV-1 integrase inhibitor beta-diketo acid X-ray crystal structure

Author Community:

  • [ 1 ] Beijing Univ Technol, Coll Life Sci & Bioengn, Beijing 100022, Peoples R China

Reprint Author's Address:

  • 曾程初

    [Zeng Cheng-Chu]Beijing Univ Technol, Coll Life Sci & Bioengn, Beijing 100022, Peoples R China

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Source :

CHINESE JOURNAL OF CHEMISTRY

ISSN: 1001-604X

Year: 2007

Issue: 8

Volume: 25

Page: 1174-1182

5 . 4 0 0

JCR@2022

ESI Discipline: CHEMISTRY;

JCR Journal Grade:3

Cited Count:

WoS CC Cited Count: 4

SCOPUS Cited Count: 7

ESI Highly Cited Papers on the List: 0 Unfold All

WanFang Cited Count:

Chinese Cited Count:

30 Days PV: 6

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