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肯尼亚拉姆韦山谷布氏锥虫的群体遗传学与人类昏睡病流行病学

Population genetics of Trypanosoma brucei and the epidemiology of human sleeping sickness in the Lambwe Valley, Kenya.

作者信息

Mihok S, Otieno L H, Darji N

机构信息

International Centre of Insect Physiology and Ecology, Nairobi, Kenya.

出版信息

Parasitology. 1990 Apr;100 Pt 2:219-33. doi: 10.1017/s0031182000061229.

Abstract

Numerical taxonomy was used to review isoenzyme variation in isolates of Trypanosoma brucei obtained from cattle, tsetse, humans and wildlife from the Lambwe Valley, Kenya. From isoenzyme information alone, it was possible to classify isolates as to source through the use of linear discriminant functions analysis, with an error rate of only 2% in humans, and 14% over all groups. Differentiation was mostly dependent on patterns in the enzymes ASAT, PEP1, and ICD. Parasites from non-human sources, especially tsetse, were characterized by high isoenzyme diversity, and many unique zymodemes. Observed frequencies of genotypes for ICD, ALAT, and ASAT did not agree with expected frequencies based on random mating of a diploid organism. Deviations were particularly large for tsetse isolates, and were mostly due to a deficiency of one homozygote. Cluster analysis revealed complex relationships among isolates, with patterns evolving through time. Major human zymodemes from the 1970s clustered together with most wildlife isolates from East Africa. This chronic human-wildlife transmission cycle was characterized by ASAT pattern I. Other, minor human zymodemes were associated with a human-cattle transmission cycle characterized by ASAT pattern VII. These original chronic transmission cycles appeared to change in 1980 with the appearance of two new zymodemes in humans. These zymodemes involved changes in ALAT and/or PGM to patterns typical of tsetse and cattle isolates. A resultant epidemic was halted with repeated aerial spraying of endosulfan in 1981. Since then, a variety of new zymodemes of unknown human infectivity have appeared. The origins of these changes are discussed in terms of genetic exchange in tsetse, adaptation to human and cattle transmission cycles, and selection resulting from chronic use of insecticides.

摘要

数值分类法被用于研究从肯尼亚拉姆韦山谷的牛、采采蝇、人类和野生动物体内分离出的布氏锥虫分离株的同工酶变异情况。仅根据同工酶信息,通过线性判别函数分析就有可能将分离株按来源进行分类,在人类中的错误率仅为2%,在所有组中的错误率为14%。区分主要取决于天冬氨酸转氨酶(ASAT)、磷酸烯醇式丙酮酸羧激酶1(PEP1)和异柠檬酸脱氢酶(ICD)的酶谱模式。来自非人类宿主的寄生虫,尤其是采采蝇体内的寄生虫,其同工酶多样性高,且有许多独特的酶型。观察到的ICD、丙氨酸转氨酶(ALAT)和ASAT基因型频率与基于二倍体生物随机交配的预期频率不一致。采采蝇分离株的偏差尤为显著,主要是由于一种纯合子的缺乏。聚类分析揭示了分离株之间复杂的关系,其模式随时间演变。20世纪70年代的主要人类酶型与东非的大多数野生动物分离株聚集在一起。这种慢性的人类-野生动物传播循环以ASAT模式I为特征。其他次要的人类酶型与以ASAT模式VII为特征的人类-牛传播循环相关。这些最初的慢性传播循环在1980年似乎发生了变化,当时人类中出现了两种新的酶型。这些酶型涉及ALAT和/或磷酸葡萄糖变位酶(PGM)变为采采蝇和牛分离株典型的模式。1981年通过反复空中喷洒硫丹制止了由此引发的疫情。从那时起,出现了多种人类感染性未知的新酶型。从采采蝇的基因交换、对人类和牛传播循环的适应以及长期使用杀虫剂导致的选择等方面讨论了这些变化的起源。

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