STRUCTURAL-ENGINEERING OF THE HIV-1 PROTEASE MOLECULE WITH A BETA-TURN MIMIC OF FIXED GEOMETRY

被引：39

作者：

BACA, M

ALEWOOD, PF

KENT, SBH

机构：

[1] SCRIPPS RES INST, LA JOLLA, CA 92037 USA

[2] UNIV QUEENSLAND, CTR DRUG DESIGN & DEV, BRISBANE, QLD 4072, AUSTRALIA

来源：

PROTEIN SCIENCE | 1993年 / 2卷 / 07期

关键词：

BETA-TURN MIMIC; CHEMICAL SYNTHESIS; HIV-1; PROTEASE; PROTEIN DESIGN; THERMAL STABILITY;

D O I：

10.1002/pro.5560020702

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：

An important goal in the de novo design of enzymes is the control of molecular geometry. To this end, an analog of the protease from human immunodeficiency virus 1 (HIV-1 protease) was prepared by total chemical synthesis, containing a constrained, nonpeptidic type II' beta-turn mimic of predetermined three-dimensional structure. The mimic beta-turn replaced residues Gly16,17 in each subunit of the homodimeric molecule. These residues constitute the central amino acids of two symmetry-related type I' beta-turns in the native, unliganded enzyme. The beta-turn mimic-containing enzyme analog was fully active, possessed the same substrate specificity as the Gly16,17-containing enzyme, and showed enhanced resistance to thermal inactivation. These results indicate that the precise geometry of the beta-turn at residues 15-18 in each subunit is not critical for activity, and that replacement of the native sequence with a rigid beta-turn mimic can lead to enhanced protein stability. Finally, the successful incorporation of a fixed element of secondary structure illustrates the potential of a ''molecular kit set'' approach to protein design and synthesis.

引用

页码：1085 / 1091

页数：7

共 27 条

[1] SOLID-PHASE SYNTHESIS OF HYDROXYETHYLAMINE PEPTIDE-BOND ISOSTERES - SYNTHESIS OF THE POTENT-HIV-1 PROTEASE INHIBITOR JG365
ALEWOOD, PF
BRINKWORTH, RI
DANCER, RJ
GARNHAM, B
JONES, A
KENT, SBH
[J]. TETRAHEDRON LETTERS, 1992, 33 (07) : 977 - 980
[2] Ball J B, 1990, J Mol Recognit, V3, P55, DOI 10.1002/jmr.300030202
[3] X-RAY CRYSTAL-STRUCTURE OF THE HIV PROTEASE COMPLEX WITH L-700,417, AN INHIBITOR WITH PSEUDO C2 SYMMETRY
BONE, R
VACCA, JP
ANDERSON, PS
HOLLOWAY, MK
[J]. JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1991, 113 (24) : 9382 - 9384
[4] CASTRO B, 1975, TETRAHEDRON LETT, V14, P1219
[5] HUMAN IMMUNODEFICIENCY VIRUS PROTEASE EXPRESSED IN ESCHERICHIA-COLI EXHIBITS AUTOPROCESSING AND SPECIFIC MATURATION OF THE GAG PRECURSOR
DEBOUCK, C
GORNIAK, JG
STRICKLER, JE
MEEK, TD
METCALF, BW
ROSENBERG, M
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (24) : 8903 - 8906
[6] FOLDING OF IMMUNOGENIC PEPTIDE-FRAGMENTS OF PROTEINS IN WATER SOLUTION .1. SEQUENCE REQUIREMENTS FOR THE FORMATION OF A REVERSE TURN
DYSON, HJ
RANCE, M
HOUGHTEN, RA
LERNER, RA
WRIGHT, PE
[J]. JOURNAL OF MOLECULAR BIOLOGY, 1988, 201 (01) : 161 - 200
[7] DESIGN, ACTIVITY, AND 2.8 A CRYSTAL-STRUCTURE OF A C2 SYMMETRICAL INHIBITOR COMPLEXED TO HIV-1 PROTEASE
ERICKSON, J
NEIDHART, DJ
VANDRIE, J
KEMPF, DJ
WANG, XC
NORBECK, DW
PLATTNER, JJ
RITTENHOUSE, JW
TURON, M
WIDEBURG, N
KOHLBRENNER, WE
SIMMER, R
HELFRICH, R
PAUL, DA
KNIGGE, M
[J]. SCIENCE, 1990, 249 (4968) : 527 - 533
[8] GILBERT DG, 1989, ENZYME KINETICS PROG
[9] DOMAIN COMMUNICATION IN THE DYNAMIC STRUCTURE OF HUMAN IMMUNODEFICIENCY VIRUS-1 PROTEASE
HARTE, WE
SWAMINATHAN, S
MANSURI, MM
MARTIN, JC
ROSENBERG, IE
BEVERIDGE, DL
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1990, 87 (22) : 8864 - 8868
[10] HIV PROTEASE - A NOVEL CHEMOTHERAPEUTIC TARGET FOR AIDS
HUFF, JR
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1991, 34 (08) : 2305 - 2314

← 1 2 3 →