SEMISYNTHETIC CHEMICAL MODIFICATION OF THE ANTIFUNGAL LIPOPEPTIDE ECHINOCANDIN-B (ECB) - STRUCTURE-ACTIVITY STUDIES OF THE LIPOPHILIC AND GEOMETRIC PARAMETERS OF POLYARYLATED ACYL ANALOGS OF ECB

被引：94

作者：

DEBONO, M ^{[1
]}

TURNER, WW ^{[1
]}

LAGRANDEUR, L ^{[1
]}

BURKHARDT, FJ ^{[1
]}

NISSEN, JS ^{[1
]}

NICHOLS, KK ^{[1
]}

RODRIGUEZ, MJ ^{[1
]}

ZWEIFEL, MJ ^{[1
]}

ZECKNER, DJ ^{[1
]}

GORDEE, RS ^{[1
]}

TANG, J ^{[1
]}

PARR, TR ^{[1
]}

机构：

[1] ELI LILLY & CO,LILLY RES LAB,DIV INFECT DIS RES,INDIANAPOLIS,IN 46285

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 1995年 / 38卷 / 17期

关键词：

D O I：

10.1021/jm00017a012

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Echinocandin B (ECB) is a lipopeptide composed of a complex cyclic peptide acylated at the N-terminus by linoleic acid. Enzymatic deacylation of ECB provided the peptide ''nucleus'' as a biologically inactive substrate from which novel ECB analogs were generated by chemical, reacylation at the N-terminus. Varying the acyl group revealed that the structure and physical properties of the side chain, particularly its geometry and lipophilicity, played a pivotal role in determining the antifungal potency properties of the analog. Using CLOGP values to describe and compare the lipophilicities of the side chain fragments, it was shown that values of >3.5 were required for expression of antifungal activity. Secondly, a linearly rigid geometry of the side chain was the most effective shape in enhancing the antifungal potency. Using these parameters as a guide, a variety of novel ECB analogs were synthesized which included arylacyl groups that incorporated biphenyl, terphenyl, tetraphenyl, and arylethynyl groups. Generally the glucan synthase inhibition by these analogs correlated well with in vitro and in, vivo activities and was likewise influenced by the structure of the side chain. These structural variations resulted in enhancement of antifungal activity in both in vitro and in vivo assays. Some of these analogs, including LY303366 (14a), were effective by the oral route of administration.

引用

页码：3271 / 3281

页数：11

共 43 条

[1] OPPORTUNISTIC MYCOSES IN THE IMMUNOCOMPROMISED HOST - EXPERIENCE AT A CANCER CENTER AND REVIEW
ANAISSIE, E
[J]. CLINICAL INFECTIOUS DISEASES, 1992, 14 : S43 - S53
[2] ARMSTRONG D, 1990, HDB EXPT PHARM, V96, P439
[3] SYNTHESIS, STABILITY, AND BIOLOGICAL EVALUATION OF WATER-SOLUBLE PRODRUGS OF A NEW ECHINOCANDIN LIPOPEPTIDE - DISCOVERY OF A POTENTIAL CLINICAL AGENT FOR THE TREATMENT OF SYSTEMIC CANDIDIASIS AND PNEUMOCYSTIS-CARINII PNEUMONIA (PCP)
BALKOVEC, JM
BLACK, RM
HAMMOND, ML
HECK, JV
ZAMBIAS, RA
ABRUZZO, G
BARTIZAL, K
KROPP, H
TRAINOR, C
SCHWARTZ, RE
MCFADDEN, DC
NOLLSTADT, KH
PITTARELLI, LA
POWLES, MA
SCHMATZ, DM
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1992, 35 (01) : 194 - 198
[4] BALKOVEC JM, 1994, EXPERT OPIN INV DRUG, V3, P65, DOI DOI 10.1517/13543784.3.2.65
[5] METABOLIC PRODUCTS OF MICROORGANISM .143. ECHINOCANDIN B, A NEW POLYPEPTIDE ANTIBIOTIC FROM ASPERGILLUS NIDULANS VAR ECHINULATUS - ISOLATION AND BUILDING UNITS
BENZ, F
KNUSEL, F
NUESCH, J
TREICHLER, HJ
VOSER, W
[J]. HELVETICA CHIMICA ACTA, 1974, 57 (08) : 2459 - 2477
[6] DEACYLATION OF ECHINOCANDIN-B BY ACTINOPLANES-UTAHENSIS
BOECK, LD
FUKUDA, DS
ABBOTT, BJ
DEBONO, M
[J]. JOURNAL OF ANTIBIOTICS, 1989, 42 (03) : 382 - 388
[7] BOYD DB, 1984, UNPUB
[8] CASSONE A, 1986, DRUG EXP CLIN RES, V12, P635
[9] CURRENT WL, 1990, 30TH INT C ANT AG CH
[10] Debono M, 1988, Ann N Y Acad Sci, V544, P152, DOI 10.1111/j.1749-6632.1988.tb40398.x

← 1 2 3 4 5 →