Nonpeptidic inhibitors of human neutrophil elastase .7. Design, synthesis, and in vitro activity of a series of pyridopyrimidine trifluoromethyl ketones

被引：38

作者：

Edwards, PD ^{[1
]}

Andisik, DW ^{[1
]}

Strimpler, AM ^{[1
]}

Gomes, B ^{[1
]}

Tuthill, PA ^{[1
]}

机构：

[1] ZENECA PHARMACEUT,DEPT PULM PHARMACOL,WILMINGTON,DE 19850

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 1996年 / 39卷 / 05期

关键词：

D O I：

10.1021/jm950684z

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Using molecular modeling and the information derived from X-ray crystal structures of human neutrophil elastase (HNE) and porcine pancreatic elastase (PPE) complexed to peptidic ligands, we have developed a new series of nonpeptidic inhibitors of HNE, the pyridopyrimidine trifluoromethyl ketones (TFMKs). These bicyclic inhibitors were designed to extend the concept of the related pyridone trifluoromethyl ketones by incorporating a rigidly positioned carbonyl group to participate in a hydrogen bonding interaction with the backbone NH groups of Gly-218 and Gly-219 of the enzyme. In addition, the pyrimidine ring serves as a scaffold to vector substituents toward the S-5-S-4 subsites of the enzyme's extended binding pocket. Furthermore, the heteroatoms of the pyrimidine ring generally increase the aqueous solubility of the pyridopyrimidines relative to pyridone TFMKs. Pyridopyrimidine TFMKs containing a 6-phenyl substituent afforded potent inhibitors of elastase, and several inhibitors from this class of compounds possessed aqueous solubilities of > 0.1 mg/mL and K-i values of less than or equal to 10 nM.

引用

页码：1112 / 1124

页数：13

共 40 条

[1] INHIBITION OF HUMAN NEUTROPHIL ELASTASE WITH PEPTIDYL ELECTROPHILIC KETONES .2. ORALLY-ACTIVE P-G-VAL-PRO-VAL PENTAFLUOROETHYL KETONES
ANGELASTRO, MR
BAUGH, LE
BEY, P
BURKHART, JP
CHEN, TM
DURHAM, SL
HARE, CM
HUBER, EW
JANUSZ, MJ
KOEHL, JR
MARQUART, AL
MEHDI, S
PEET, NP
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1994, 37 (26) : 4538 - 4553
[2] BERGESON S, 1990, Patent No. 4910190
[3] BERGESON SH, 1987, 193 NAT M AM CHEM SO
[4] Bernstein P R, 1994, Prog Med Chem, V31, P59, DOI 10.1016/S0079-6468(08)70019-5
[5] NONPEPTIDIC INHIBITORS OF HUMAN-LEUKOCYTE ELASTASE .6. DESIGN OF A POTENT, INTRATRACHEALLY ACTIVE, PYRIDONE-BASED TRIFLUOROMETHYL KETONE
BERNSTEIN, PR
GOMES, BC
KOSMIDER, BJ
VACEK, EP
WILLIAMS, JC
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1995, 38 (01) : 212 - 215
[6] NONPEPTIDIC INHIBITORS OF HUMAN-LEUKOCYTE ELASTASE .3. DESIGN, SYNTHESIS, X-RAY CRYSTALLOGRAPHIC ANALYSIS, AND STRUCTURE-ACTIVITY-RELATIONSHIPS FOR A SERIES OF ORALLY-ACTIVE 3-AMINO-6-PHENYLPYRIDIN-2-ONE TRIFLUOROMETHYL KETONES
BERNSTEIN, PR
ANDISIK, D
BRADLEY, PK
BRYANT, CB
CECCARELLI, C
DAMEWOOD, JR
EARLEY, R
EDWARDS, PD
FEENEY, S
GOMES, BC
KOSMIDER, BJ
STEELMAN, GB
THOMAS, RM
VACEK, EP
VEALE, CA
WILLIAMS, JC
WOLANIN, DJ
WOOLSON, SA
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1994, 37 (20) : 3313 - 3326
[7] Bieth JG, 1986, REGULATION MATRIX AC, P217
[8] PHARMACOLOGICAL PROFILE OF THE SUBSTITUTED BETA-LACTAM L-659,286 - A MEMBER OF A NEW CLASS OF HUMAN-PMN ELASTASE INHIBITORS
BONNEY, RJ
ASHE, B
MAYCOCK, A
DELLEA, P
HAND, K
OSINGA, D
FLETCHER, D
MUMFORD, R
DAVIES, P
FRANKENFIELD, D
NOLAN, T
SCHAEFFER, L
HAGMANN, W
FINKE, P
SHAH, S
DORN, C
DOHERTY, J
[J]. JOURNAL OF CELLULAR BIOCHEMISTRY, 1989, 39 (01) : 47 - 53
[9] BORCH RF, 1972, J ORG CHEM, V27, P1141
[10] DESIGN OF ORALLY-ACTIVE, NONPEPTIDIC INHIBITORS OF HUMAN-LEUKOCYTE ELASTASE
BROWN, FJ
ANDISIK, DW
BERNSTEIN, PR
BRYANT, CB
CECCARELLI, C
DAMEWOOD, JR
WOOLSON, SA
EDWARDS, PD
EARLEY, RA
FEENEY, S
GREEN, RC
GOMES, B
KOSMIDER, BJ
KRELL, RD
SHAW, A
STEELMAN, GB
THOMAS, RN
VACEK, EP
VEALE, CA
TUTHILL, PA
WARNER, P
WILLIAMS, JC
WOLANIN, DJ
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1994, 37 (09) : 1259 - 1261

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