'Flu' and structure-based drug design

被引：64

作者：

Wade, RC

机构：

[1] Structural Biology Programme, Europ. Molecular Biology Laboratory, 69012 Heidelberg

来源：

STRUCTURE | 1997年 / 5卷 / 09期

关键词：

D O I：

10.1016/S0969-2126(97)00265-7

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The threat of a catastrophic outbreak of influenza is ever present. Vaccines are only partially effective and the two compounds, amantidine and rimantidine, used clinically against influenza A cause side-effects and rapid viral resistance. Recent advances bring hope that specific and potent drugs against influenza may soon be available in the clinic. These compounds were designed to inhibit influenza neuraminidase (NA), one of the viral coat glycoproteins, using the crystal structure of NA which was first published in 1983. In this review, the application of structure-based drug design approaches to the design of anti-influenza agents targeted at NA and haemagglutinin (HA), the other viral surface glycoprotein, is discussed.

引用

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页码：1139 / 1145

页数：7

相关论文

共 38 条

[1] Neuraminidase inhibitors as potential anti-influenza drugs [J].

Bamford, MJ .

JOURNAL OF ENZYME INHIBITION, 1995, 10 (01) :1-16

[2] INHIBITION OF THE FUSION-INDUCING CONFORMATIONAL CHANGE OF INFLUENZA HEMAGGLUTININ BY BENZOQUINONES AND HYDROQUINONES [J].

BODIAN, DL ;

YAMASAKI, RB ;

BUSWELL, RL ;

STEARNS, JF ;

WHITE, JM ;

KUNTZ, ID .

BIOCHEMISTRY, 1993, 32 (12) :2967-2978

[3] THE 2.2-A RESOLUTION CRYSTAL-STRUCTURE OF INFLUENZA-B NEURAMINIDASE AND ITS COMPLEX WITH SIALIC-ACID [J].

BURMEISTER, WP ;

RUIGROK, RWH ;

CUSACK, S .

EMBO JOURNAL, 1992, 11 (01) :49-56

[4] STRUCTURE OF THE CATALYTIC AND ANTIGENIC SITES IN INFLUENZA-VIRUS NEURAMINIDASE [J].

COLMAN, PM ;

VARGHESE, JN ;

LAVER, WG .

NATURE, 1983, 303 (5912) :41-44

[5] INFLUENZA-VIRUS NEURAMINIDASE - STRUCTURE, ANTIBODIES, AND INHIBITORS [J].

COLMAN, PM .

PROTEIN SCIENCE, 1994, 3 (10) :1687-1696

[6] INHIBITION OF NEURAMINIDASE AND ANTIVIRAL ACTION [J].

EDMOND, JD ;

JOHNSTON, RG ;

KIDD, D ;

RYLANCE, HJ ;

SOMMERVILLE, RG .

BRITISH JOURNAL OF PHARMACOLOGY AND CHEMOTHERAPY, 1966, 27 (02) :415-+

[7] HOOK - A PROGRAM FOR FINDING NOVEL MOLECULAR ARCHITECTURES THAT SATISFY THE CHEMICAL AND STERIC REQUIREMENTS OF A MACROMOLECULE BINDING-SITE [J].

EISEN, MB ;

WILEY, DC ;

KARPLUS, M ;

HUBBARD, RE .

PROTEINS-STRUCTURE FUNCTION AND GENETICS, 1994, 19 (03) :199-221

[8] A COMPUTATIONAL-PROCEDURE FOR DETERMINING ENERGETICALLY FAVORABLE BINDING-SITES ON BIOLOGICALLY IMPORTANT MACROMOLECULES [J].

GOODFORD, PJ .

JOURNAL OF MEDICINAL CHEMISTRY, 1985, 28 (07) :849-857

[9] STRUCTURE OF INFLUENZA-VIRUS NEURAMINIDASE B/LEE/40 COMPLEXED WITH SIALIC-ACID AND A DEHYDRO ANALOG AT 1.8-ANGSTROM RESOLUTION - IMPLICATIONS FOR THE CATALYTIC MECHANISM [J].

JANAKIRAMAN, MN ;

WHITE, CL ;

LAVER, WG ;

AIR, GM ;

LUO, M .

BIOCHEMISTRY, 1994, 33 (27) :8172-8179

[10] STRUCTURES OF AROMATIC INHIBITORS OF INFLUENZA-VIRUS NEURAMINIDASE [J].

JEDRZEJAS, MJ ;

SINGH, S ;

BROUILLETTE, WJ ;

LAVER, WG ;

AIR, GM ;

LUO, M .

BIOCHEMISTRY, 1995, 34 (10) :3144-3151

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