Non-nucleoside HIV-1 reverse transcriptase inhibitors: synthesis and biological evaluation of novel quinoxalinylethylpyridylthioureas as potent antiviral agents

被引：15

作者：

Campiani, G

Fabbrini, M

Morelli, E

Nacci, V

Greco, G

Novellino, E

Maga, G

Spadari, S

Bergamini, A

Faggioli, E

Uccella, I

Bolacchi, F

Marini, S

Coletta, M

Fracasso, C

Caccia, S

机构：

[1] Univ Salerno, Fac Farm, Dipartimento Sci Farmaceut, I-84084 Salerno, Italy

[2] Univ Siena, Dipartimento Farmaco Chim Tecnol, I-53100 Siena, Italy

[3] Univ Naples Federico II, Dipartimento Chim Farmaceut & Tossicol, I-80131 Naples, Italy

[4] CNR, Ist Genet Biochim & Evoluzionist, I-27100 Pavia, Italy

[5] Univ Roma Tor Vergata, Dipartimento Sanita Pubbl & Biol Cellulare, I-00133 Rome, Italy

[6] Univ Roma Tor Vergata, Dipartimento Med Sperimentale & Sci Biochim, I-00133 Rome, Italy

[7] Ist Ric Farmacol Mario Negri, I-20157 Milan, Italy

来源：

ANTIVIRAL CHEMISTRY & CHEMOTHERAPY | 2000年 / 11卷 / 02期

关键词：

HIV; non-nucleoside HIV-1 RT inhibitors; thioureas; QXPTs;

D O I：

10.1177/095632020001100206

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：

New heterocyclic derivatives of ethylpyridylthiourea, quinoxalinylethylpyridylthiourea (QXPT) and analogues, inhibited human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) activity and prevented HIV-1 cytopathogenicity in T4 lymphocytes. Several of these novel non-nucleoside RT inhibitors, with a substituted pyrroloquinoxalinone heteroaromatic skeleton, showed inhibitory activity against wild-type RT as well as against mutant RTs containing the single amino acid substitutions L100I, K103N, V106A, Y181I and Y188L that was much greater than other non-nucleoside inhibitors such as nevirapine. Maximum potency in enzymatic assays was achieved with a fluoropyrroloquinoxaline skeleton linked to the ethylpyridylthiourea moiety (FQXPT). In cell-based assays on different cell lines and on human monocyte-macrophages, 6-FQXPT exhibited EC50 values in the nanomolar range, with a promising selectivity index. Moreover, 6-FQXPT showed synergistic antiviral activity with zidovudine.

引用

页码：141 / 155

页数：15

共 43 条

[1] THE PETT SERIES, A NEW CLASS OF POTENT NONNUCLEOSIDE INHIBITORS OF HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 REVERSE-TRANSCRIPTASE [J].

AHGREN, C ;

BACKRO, K ;

BELL, FW ;

CANTRELL, AS ;

CLEMENS, M ;

COLACINO, JM ;

DEETER, JB ;

ENGELHARDT, JA ;

HOGBERG, M ;

JASKUNAS, SR ;

JOHANSSON, NG ;

JORDAN, CL ;

KASHER, JS ;

KINNICK, MD ;

LIND, P ;

LOPEZ, C ;

MORIN, JM ;

MUESING, MA ;

NOREEN, R ;

OBERG, B ;

PAGET, CJ ;

PALKOWITZ, JA ;

PARRISH, CA ;

PRANC, P ;

RIPPY, MK ;

RYDERGARD, C ;

SAHLBERG, C ;

SWANSON, S ;

TERNANSKY, RJ ;

UNGE, T ;

VASILEFF, RT ;

VRANG, L ;

WEST, SJ ;

ZHANG, H ;

XHOU, XX .

ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1995, 39 (06) :1329-1335

[2]

AKIRA M, 1974, Patent No. 129461

[3]

AKIRA M, 1975, Patent No. 27877

[4] ISOLATION OF A T-LYMPHOTROPIC RETROVIRUS FROM A PATIENT AT RISK FOR ACQUIRED IMMUNE-DEFICIENCY SYNDROME (AIDS) [J].

BARRESINOUSSI, F ;

CHERMANN, JC ;

REY, F ;

NUGEYRE, MT ;

CHAMARET, S ;

GRUEST, J ;

DAUGUET, C ;

AXLERBLIN, C ;

VEZINETBRUN, F ;

ROUZIOUX, C ;

ROZENBAUM, W ;

MONTAGNIER, L .

SCIENCE, 1983, 220 (4599) :868-871

[5] PHENETHYLTHIAZOLETHIOUREA (PETT) COMPOUNDS, A NEW CLASS OF HIV-1 REVERSE-TRANSCRIPTASE INHIBITORS .1. SYNTHESIS AND BASIC STRUCTURE-ACTIVITY RELATIONSHIP STUDIES OF PETT ANALOGS [J].

BELL, FW ;

CANTRELL, AS ;

HOGBERG, M ;

JASKUNAS, SR ;

JOHANSSON, NG ;

JORDAN, CL ;

KINNICK, MD ;

LIND, P ;

MORIN, JM ;

NOREEN, R ;

OBERG, B ;

PALKOWITZ, JA ;

PARRISH, CA ;

PRANC, P ;

SAHLBERG, C ;

TERNANSKY, RJ ;

VASILEFF, RT ;

VRANG, L ;

WEST, SJ ;

ZHANG, H ;

ZHOU, XX .

JOURNAL OF MEDICINAL CHEMISTRY, 1995, 38 (25) :4929-4936

[6] A TETRAZOLIUM-BASED COLORIMETRIC ASSAY FOR QUANTIFICATION OF HIV-1-INDUCED CYTOPATHOGENICITY IN MONOCYTE-MACROPHAGES EXPOSED TO MACROPHAGE-COLONY-STIMULATING FACTOR [J].

BERGAMINI, A ;

PERNO, CF ;

CAPOZZI, M ;

MANNELLA, E ;

SALANITRO, A ;

CALIO, R ;

ROCCHI, G .

JOURNAL OF VIROLOGICAL METHODS, 1992, 40 (03) :275-286

[7] In memory of Thomas E. Tremain 1934-1995 [J].

Campbell, JP .

IEEE TRANSACTIONS ON SPEECH AND AUDIO PROCESSING, 1996, 4 (01) :1-1

[8] Pyrrolobenzoxazepinone derivatives as non-nucleoside HIV-1 RT inhibitors: Further structure-activity relationship studies and identification of more potent broad-spectrum HIV-1 RT inhibitors with antiviral activity [J].

Campiani, G ;

Morelli, E ;

Fabbrini, M ;

Nacci, V ;

Greco, G ;

Novellino, E ;

Ramunno, A ;

Maga, G ;

Spadari, S ;

Caliendo, G ;

Bergamini, A ;

Faggioli, E ;

Uccella, I ;

Bolacchi, F ;

Marini, S ;

Coletta, M ;

Nacca, A ;

Caccia, S .

JOURNAL OF MEDICINAL CHEMISTRY, 1999, 42 (21) :4462-4470

[9] A PALLADIUM-CATALYZED ROUTE TO HUPERZINE-A AND ITS ANALOGS AND THEIR ANTICHOLINESTERASE ACTIVITY [J].

CAMPIANI, G ;

SUN, LQ ;

KOZIKOWSKI, AP ;

AAGAARD, P ;

MCKINNEY, M .

JOURNAL OF ORGANIC CHEMISTRY, 1993, 58 (27) :7660-7669

[10] Pyrroloquinoxaline derivatives as high-affinity and selective 5-HT3 receptor agonists:: Synthesis, further structure-activity relationships, and biological studies [J].

Campiani, G ;

Morelli, E ;

Gemma, S ;

Nacci, V ;

Butini, S ;

Hamon, M ;

Novellino, E ;

Greco, G ;

Cagnotto, A ;

Goegan, M ;

Cervo, L ;

Dalla Valle, F ;

Fracasso, C ;

Caccia, S ;

Mennini, T .

JOURNAL OF MEDICINAL CHEMISTRY, 1999, 42 (21) :4362-4379

← 1 2 3 4 5 →