摘要
将3个苏拉灭敏感的伊氏锥虫原种的克隆连续培养于改良Baltz无细胞培养系统中,通过逐步提高培养基中苏拉灭的含量,培育了3个抗苏拉灭的伊氏锥虫克隆─JGc1-160、JX-1c1-160和ZJc1-140。它们体外药敏试验的IC50依次为358.5、412.3和246.4μg/mL,是各自亲本克隆的1292.5、1874.1和1760.o倍;小鼠治疗试验的CD100,对免疫功能正常小鼠依次为80、120和30mg/kg,为各自亲本克隆的5.3、8.0和3.0倍,对免疫抑制小鼠为250、300和100mg/kg,分别是相应免疫正常小鼠的3.1、2.5和3.3倍。试验结果表明,抗锥虫药治疗剂量不足和宿主免疫功能不全是导致产生抗药虫株的重要因素,各自既可单独发挥作用,又可相互协同。本文报道了体外培育伊氏锥虫抗药虫株的方法,这一方法对研究锥虫抗药性具有重要作用。
By exposure to gradually increasing concentrations of suramin in modi- fied Baltz's
cell-free culture system,3 suramin-resistant clones(JGc1-160, JX-1c1-160and ZJc1-l4o)were
derived from 3 suramin-sensitive strains of Trypanosoma evansi(JGc1,JX-lc1 and ZJc1 )over a
period of 550 days. The IC50 of in vitro drug susceptibility test in JGc1-160 was 358.5 μg/mL,
and 1292.5 times as much as that of its parent strain; in JX- lc1-160 , 412.3μg/mL and 1874.1
times; in ZJc1-140 , 246.μg/mL and 1760.0 times.The CD100 for intact mice and
immunosuppressed mice infected with JGc1-160 were 80 and 250 mg/kg respectively, the
doses for both groups of mice infected with JX-1c1-160 were 120 and 300 mg/kg; and for those
infected with ZJc1-140 were 30 and 100 mg/kg;The ra-tios of CD10O for immmunosuppressed
mice to those for intact mice were 3.13,2.5 and 3.33 in JGc1-160,JX -1c1-160 and
ZJc1-140,respectively. These results suggested that besides the inadequacy of curative
dosage of trypanosomicide, the deficiency of host immune de- fence appeared to be an
important factor resulting in the development of drug resistance. Both these factors play the
role alone or together.
出处
《中国兽医学报》
CAS
CSCD
1994年第1期26-30,共5页
Chinese Journal of Veterinary Science
关键词
伊氏锥虫
体外培养
抗药性
苏拉灭
Trypanosoma evansi
cloning
in vitro cultivation
drug
resistance
Suramin
immunosuppresion
