Recent developments and rationale towards new strategies for malarial chemotherapy

被引:28
作者
Vial, H
机构
[1] Dynamique Molec. des Intrac. M., CNRS URA 1856, Université Montpellier II, 34095 Montpellier Cedex 5, Place Eugène-Bataillon
来源
PARASITE | 1996年 / 3卷 / 01期
关键词
Antimalarials; Molecular structure of the target; New drug concepts; Phospholipid; Purine; Pyrimidine; Replication;
D O I
10.1051/parasite/1996031003
中图分类号
R38 [医学寄生虫学]; Q [生物科学];
学科分类号
07 ; 0710 ; 09 ; 100103 ;
摘要
The major problem facing world research for new antimalarials lies in encountered difficulties in the search for new promising paths. The past 20 years have witnessed a very impressive increase in our understanding of the biochemistry and molecular biology of malaria parasites, with attention focused on specific parasite molecules that are keys to the parasite life cycle or the induction of its pathogenesis. Directed pharmacology research has involved the identification and characterization of targets that can be specifically pharmacologically affected, including the replicating machinery of the parasites, various metabolisms such as the purine salvage pathway, and biosynthesis of pyrimidines or phospholipids. Protease inhibitors [e.g. those degrading haemoglobin), the use of iron chelators or inhibition of heme polymerization, induction of oxidative stress or inhibition of antioxidant enzymes are also investigated. Some pathways have already been validated with current antimalarials but, due to the development of resistance, complete characterization of the molecular structure of the target should allow attack oi these exceptional molecules at novel and distinct sites with new drug concepts. The problem in the quest to develop new antimalarials is the fact that the results are not being materialized, but there is no lack of pharmacological targets.
引用
收藏
页码:3 / 23
页数:21
相关论文
共 148 条
[1]   INHIBITORS OF CHOLINE TRANSPORT INTO PLASMODIUM-INFECTED ERYTHROCYTES ARE EFFECTIVE ANTIPLASMODIAL COMPOUNDS INVITRO [J].
ANCELIN, ML ;
VIAL, HJ ;
PHILIPPOT, JR .
BIOCHEMICAL PHARMACOLOGY, 1985, 34 (22) :4068-4071
[2]   REGULATION OF PHOSPHATIDYLCHOLINE BIOSYNTHESIS IN PLASMODIUM-INFECTED ERYTHROCYTES [J].
ANCELIN, ML ;
VIAL, HJ .
BIOCHIMICA ET BIOPHYSICA ACTA, 1989, 1001 (01) :82-89
[3]   QUATERNARY AMMONIUM-COMPOUNDS EFFICIENTLY INHIBIT PLASMODIUM-FALCIPAUM GROWTH-INVITRO BY IMPAIRMENT OF CHOLINE TRANSPORT [J].
ANCELIN, ML ;
VIAL, HJ .
ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1986, 29 (05) :814-820
[4]   INCREASED PERMEABILITY TO CHOLINE IN SIMIAN ERYTHROCYTES AFTER PLASMODIUM-KNOWLESI INFECTION [J].
ANCELIN, ML ;
PARANT, M ;
THUET, MJ ;
PHILIPPOT, JR ;
VIAL, HJ .
BIOCHEMICAL JOURNAL, 1991, 273 :701-709
[5]   FUNCTIONAL-GROUPS, DRUG RECEPTOR INTERACTIONS AND DRUG DESIGN [J].
ANDREWS, P .
TRENDS IN PHARMACOLOGICAL SCIENCES, 1986, 7 (04) :148-151
[6]   REACTION OF ANTIMALARIAL ENDOPEROXIDES WITH SPECIFIC PARASITE PROTEINS [J].
ASAWAMAHASAKDA, W ;
ITTARAT, I ;
PU, YM ;
ZIFFER, H ;
MESHNICK, SR .
ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1994, 38 (08) :1854-1858
[7]   HEXOSE-MONOPHOSPHATE SHUNT ACTIVITY IN INTACT PLASMODIUM-FALCIPARUM-INFECTED ERYTHROCYTES AND IN FREE PARASITES [J].
ATAMNA, H ;
PASCARMONA, G ;
GINSBURG, H .
MOLECULAR AND BIOCHEMICAL PARASITOLOGY, 1994, 67 (01) :79-89
[8]   ORIGIN OF REACTIVE OXYGEN SPECIES IN ERYTHROCYTES INFECTED WITH PLASMODIUM-FALCIPARUM [J].
ATAMNA, H ;
GINSBURG, H .
MOLECULAR AND BIOCHEMICAL PARASITOLOGY, 1993, 61 (02) :231-241
[9]   PLASMODIUM-FALCIPARUM - DIFFERENTIAL SENSITIVITY INVITRO TO E-64 (CYSTEINE PROTEASE INHIBITOR) AND PEPSTATIN-A (ASPARTYL PROTEASE INHIBITOR) [J].
BAILLY, E ;
JAMBOU, R ;
SAVEL, J ;
JAUREGUIBERRY, G .
JOURNAL OF PROTOZOOLOGY, 1992, 39 (05) :593-599
[10]   THE ROLE OF THE CYTOSKELETON IN PLASMODIUM-FALCIPARUM MEROZOITE BIOLOGY - AN ELECTRON-MICROSCOPIC VIEW [J].
BANNISTER, LH ;
MITCHELL, GH .
ANNALS OF TROPICAL MEDICINE AND PARASITOLOGY, 1995, 89 (02) :105-111
12345678910