Crystal structures of HINT demonstrate that histidine triad proteins are GalT-related nucleotide-binding proteins

被引：133

作者：

Brenner, C

Garrison, P

Gilmour, J

Peisach, D

Ringe, D

Petsko, GA

Lowenstein, JM

机构：

[1] BRANDEIS UNIV, DEPT CHEM, WALTHAM, MA 02254 USA

[2] BRANDEIS UNIV, ROSENSTIEL BASIC MED SCI RES CTR, WALTHAM, MA 02254 USA

[3] BRANDEIS UNIV, DEPT BIOCHEM, WALTHAM, MA 02254 USA

[4] UNIV TEXAS, HLTH SCI CTR, DEPT BIOCHEM, SAN ANTONIO, TX 78284 USA

来源：

NATURE STRUCTURAL BIOLOGY | 1997年 / 4卷 / 03期

关键词：

D O I：

10.1038/nsb0397-231

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：

Histidine triad nucleotide-binding protein (HINT), a dimeric purine nucleotide-binding protein from rabbit heart, is a member of the HIT (histidine triad) superfamily which includes HINT homologues and FHIT (HIT protein encoded at the chromosome 3 fragile site) homologues. Crystal structures of HINT-nucleotide complexes demonstrate that the most conserved residues in the superfamily mediate nucleotide binding and that the HIT motif forms part of the phosphate binding loop. Galactose-1-phosphate uridylyltransferase, whose deficiency causes galactosemia, contains tandem HINT domains with the same fold and mode of nucleotide binding as HINT despite having no overall sequence similarity, Features of FHIT, a diadenosine polyphosphate hydrolase and candidate tumour suppressor, are predicted from HINT-nucleotide structures.

引用

页码：231 / 238

页数：8

共 54 条

[1] Fhit, a putative tumor suppressor in humans, is a dinucleoside 5',5'''-P-1,P-3-triphosphate hydrolase [J].

Barnes, LD ;

Garrison, PN ;

Siprashvili, Z ;

Guranowski, A ;

Robinson, AK ;

Ingram, SW ;

Croce, CM ;

Ohta, M ;

Huebner, F .

BIOCHEMISTRY, 1996, 35 (36) :11529-11535

[2] ALSCRIPT - A TOOL TO FORMAT MULTIPLE SEQUENCE ALIGNMENTS [J].

BARTON, GJ .

PROTEIN ENGINEERING, 1993, 6 (01) :37-40

[3] AN ALLEGED YEAST POLYPHOSPHATE KINASE IS ACTUALLY DIADENOSINE-5',5'''-P-1,P-4-TETRAPHOSPHATE ALPHA,BETA-PHOSPHORYLASE [J].

BOOTH, JW ;

GUIDOTTI, G .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (33) :19377-19382

[4]

BRUNGER AT, 1997, IN PRESS METHODS ENZ, V277

[5]

BRUNGER AT, 1993, XPLOR VERSION 3 1 MA

[6] Cloning, mapping, and in vivo localization of a human member of the PKCI-1 protein family (PRKCNH1) [J].

Brzoska, PM ;

Chen, HY ;

Levin, NA ;

Kuo, WL ;

Collins, C ;

Fu, KK ;

Gray, JW ;

Christman, MF .

GENOMICS, 1996, 36 (01) :151-156

[7] THE PRODUCT OF THE ATAXIA-TELANGIECTASIA GROUP-D COMPLEMENTING GENE, ATDC INTERACTS WITH A PROTEIN-KINASE-C SUBSTRATE AND INHIBITOR [J].

BRZOSKA, PM ;

CHEN, HY ;

ZHU, YF ;

LEVIN, NA ;

DISATNIK, MH ;

MOCHLYROSEN, D ;

MURNANE, JP ;

CHRISTMAN, MF .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (17) :7824-7828

[8] Complete genome sequence of the methanogenic archaeon, Methanococcus jannaschii [J].

Bult, CJ ;

White, O ;

Olsen, GJ ;

Zhou, LX ;

Fleischmann, RD ;

Sutton, GG ;

Blake, JA ;

FitzGerald, LM ;

Clayton, RA ;

Gocayne, JD ;

Kerlavage, AR ;

Dougherty, BA ;

Tomb, JF ;

Adams, MD ;

Reich, CI ;

Overbeek, R ;

Kirkness, EF ;

Weinstock, KG ;

Merrick, JM ;

Glodek, A ;

Scott, JL ;

Geoghagen, NSM ;

Weidman, JF ;

Fuhrmann, JL ;

Nguyen, D ;

Utterback, TR ;

Kelley, JM ;

Peterson, JD ;

Sadow, PW ;

Hanna, MC ;

Cotton, MD ;

Roberts, KM ;

Hurst, MA ;

Kaine, BP ;

Borodovsky, M ;

Klenk, HP ;

Fraser, CM ;

Smith, HO ;

Woese, CR ;

Venter, JC .

SCIENCE, 1996, 273 (5278) :1058-1073

[9] DIFFERENT AND RAPID RESPONSES OF 4 CYANOBACTERIAL PSBA TRANSCRIPTS TO CHANGES IN LIGHT-INTENSITY [J].

BUSTOS, SA ;

SCHAEFER, MR ;

GOLDEN, SS .

JOURNAL OF BACTERIOLOGY, 1990, 172 (04) :1998-2004

[10] THE CHEMISTRY OF SIGNAL-TRANSDUCTION [J].

CLARDY, J .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (01) :56-61

← 1 2 3 4 5 6 →