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Titlebook: Antimalarial Drug II; Current Antimalarial Wallace Peters (Professor of Medical Protozoology) Book 1984 Springer-Verlag Berlin Heidelberg 1

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期刊全称Antimalarial Drug II
期刊简称Current Antimalarial
影响因子2023Wallace Peters (Professor of Medical Protozoology)
视频videohttp://file.papertrans.cn/159/158588/158588.mp4
学科分类Handbook of Experimental Pharmacology
图书封面Titlebook: Antimalarial Drug II; Current Antimalarial Wallace Peters (Professor of Medical Protozoology) Book 1984 Springer-Verlag Berlin Heidelberg 1
影响因子The construction of this volume has been guided by two personal convictions. Experience in the field of experimental chemotherapy, both in the pharmaceutical industry and academia, has convinced us that recent quantum technological advances in biochemistry, molecular biology, and immunology will permit and, indeed, necessitate an increasingly greater use of rational drug development in the future than has been the custom up to now. In Part l, therefore, we asked our contributors to provide detailed reviews covering the biology of the malaria parasites and their relation with their hosts, the experimental procedures including culture techniques that are necessary to take a drug from primary screening to clinical trial, and an account of antimalarial drug resistance. Our second conviction is that many research workers are all too loath to learn from the lessons of the past. For this reason we asked the contributors to Part 2 of this volume to review very thoroughly the widely scattered but voluminous literature on those few chemical groups that have provided the antimalarial drugs in clinical use at the present time. Much can be learned from the history of their development and the p
Pindex Book 1984
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Dihydrofolate Reductase Inhibitorsowerful, selective inhibition of the activity of malarial dihydrofolate reductase (. et al. 1969). Thus, one compound which was inadvertently synthesised as a prodrug and another which derived from a programme of synthesis of untargeted antimetabolites, together stand as prime examples of chemothera
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Lapinone, Menoctone, Hydroxyquinolinequinones and Similar Structures3-(9-hydroxy-9-pentyltetradecyl)1,4-naphthoquinone (II) (lapinone) was synthesised (. et al. 1948a) and shown to be effective in curing patients infected with . (. and . 1951). However, parenteral administration of the drug at fairly high doses was required and this, coupled with the emergence of su
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Antibioticsecies, chlortetracycline appeared to be somewhat more active than the other two compounds. The three drugs also exerted a causal prophylactic activity against sporozoite-induced infections of avian malaria. The two tetracyclines and chloramphenicol were the only antibiotics of those tested which wer
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Book 1984 we asked the contributors to Part 2 of this volume to review very thoroughly the widely scattered but voluminous literature on those few chemical groups that have provided the antimalarial drugs in clinical use at the present time. Much can be learned from the history of their development and the p
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Luis Baringo,Miguel Carrión,Ruth Domínguez abandoned (in favour of sontoquine) as being “too toxic for human use.” The magnitude of this error of judgement became apparent when, in the course of the American wartime antimalarial survey (. 1946), CQ proved to be the best of the many compounds which were tested for prophylactic-suppressive ac
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Maedeh Yazdandoust,Masoud Aliakbar Golkarizontocide is more effective or less toxic than primaquine there is a recognised need for investigations to differentiate the efficacy and the toxicity of prima-quine as well as to discover new, less toxic, tissue schizontocides. Thus the Third Meeting of the Scientific Working Group on the Chemothe
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