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伯氏疟原虫约氏疟原虫因果预防活性的评估及其在新型抗疟药物开发中的价值。

Assessment of causal prophylactic activity in Plasmodium berghei yoelii and its value for the development of new antimalarial drugs.

作者信息

Fink E

出版信息

Bull World Health Organ. 1974;50(3-4):213-22.

Abstract

The causal prophylactic activity of several reference and experimental antimalarial compounds was assessed in sporozoite-induced infections of NMRI mice with Plasmodium berghei yoelii (strain 17X). The animals were inoculated with 10 000 sporozoites per mouse and treated once 2-4 hours later. The test system has proved to be very suitable in experiments involving more than 3 000 mice. The infection rate in 448 untreated controls was 97.3%. Lowering the sporozoite content of the inoculum to 1 000 or 100 sporozoites markedly reduced the rate (65.1% and 32.7%). In experiments with primaquine the causal prophylactic activity was also influenced by the time of drug administration before or after sporozoite inoculation. No causal prophylactic effect was demonstrable with quinine, chloroquine, amodiaquine, amopyroquine, RC-12, or B 505. Primaquine was active, but pamaquine and pentaquine were only sporadically active. The pre-erythrocytic stages of P. b. yoelii were only slightly sensitive to dapsone, sulfadiazine, and sulformethoxine; they were 10-100 times more susceptible to proguanil, cycloguanil, and pyrimethamine. The experimental 6-aminoquinolines NI 147/36, NI 187/82, and BA 138/111 and the 7-chlorolincomycin derivative U 24729 were also studied. Experiments in which curative activity against blood-induced infections of P. b. yoelii was evaluated showed that the causal prophylactics act more specifically against the pre-erythrocytic than against the erythrocytic forms. This specificity was most pronounced among the DHFR-inhibitors, whose outstanding activity may be explained by the fact that the rate of multiplication of the pre-erythrocytic forms of P. b. yoelii is greater than that of other plasmodia used hitherto; it is also greater than the rate shown by the malaria parasites of man and that of the erythrocytic forms of P. b. yoelii itself. We believe that this feature will render P. b. yoelii very useful for determination of the causal prophylactic activity of new compounds, but it may also overrate the potency of drugs that interfere with nucleic acid biosynthesis.

摘要

用伯氏疟原虫约氏株(17X 株)的子孢子感染 NMRI 小鼠,评估了几种标准抗疟化合物和实验性抗疟化合物的病因性预防活性。每只小鼠接种 10000 个子孢子,2 - 4 小时后进行一次治疗。该测试系统已被证明非常适合涉及 3000 多只小鼠的实验。448 只未治疗对照的感染率为 97.3%。将接种物中的子孢子含量降至 1000 个或 100 个子孢子,感染率显著降低(分别为 65.1%和 32.7%)。在用伯氨喹进行的实验中,病因性预防活性也受子孢子接种前后给药时间的影响。奎宁、氯喹、阿莫地喹、阿莫吡喹、RC - 12 或 B 505 未显示出病因性预防作用。伯氨喹有活性,但帕马喹和喷他喹只是偶尔有活性。约氏疟原虫的红细胞前期对氨苯砜、磺胺嘧啶和周效磺胺仅稍有敏感性;它们对氯胍、环氯胍和乙胺嘧啶的敏感性高 10 - 100 倍。还研究了实验性 6 - 氨基喹啉 NI 147/36、NI 187/82 和 BA 138/111 以及 7 - 氯林可霉素衍生物 U 24729。评估针对约氏疟原虫血液感染的治疗活性的实验表明,病因性预防剂对红细胞前期的作用比对红细胞期的作用更具特异性。这种特异性在二氢叶酸还原酶抑制剂中最为明显,其显著活性可能是由于约氏疟原虫红细胞前期的增殖速率高于迄今使用的其他疟原虫;它也高于人类疟原虫以及约氏疟原虫红细胞期本身的增殖速率。我们认为,这一特性将使约氏疟原虫对于测定新化合物的病因性预防活性非常有用,但它也可能高估干扰核酸生物合成的药物的效力。

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