重组结核杆菌融合蛋白(EC)的免疫特性和临床前安全性研究

doi:10.3969/j.issn.1000-6621.2020.08.006

摘要/Abstract

摘要：

目的通过对重组结核杆菌融合蛋白(EC)[该制品名称是国家药典委员会确定的药品中文通用名称,“EC”为重组融合蛋白“结核分枝杆菌早期分泌性抗原靶6(ESAT-6)和培养滤液蛋白10(CFP-10)”](简称“EC”)的免疫特性和临床前安全性研究,探讨其临床应用前景。方法 (1)免疫特性研究: 取6只雌性豚鼠,使用结核分枝杆菌H37Ra活菌菌液致敏,5周后,皮内注射2.5μg/ml EC原液0.2ml;取4只雌性豚鼠,使用卡介菌活菌菌液致敏,5周后,皮内注射20μg/ml EC原液0.2ml;观察注射部位平均硬结或红晕反应直径[(纵径+横径)/2],≥5mm判为阳性,<5mm判为阴性。(2)急性毒性试验:取80只ICR[(美国)Institute of Cancer Research]小鼠,分为单次肌内和皮内注射组,每组40只,雌雄各半;每组再分为4组,每组10只,雌雄各半。高剂量组(注射EC 53.61μg/0.1ml)、低剂量组(注射EC 0.2μg/0.1ml)、溶剂对照组(注射EC稀释液0.1ml)、空白对照组(不给予任何受试物),观察小鼠的外观、运动功能、体质量、各脏器和药物注射部位皮肤等是否有异常。(3)豚鼠全身主动过敏试验:取豚鼠24只,分为4组,每组6只,雌雄各半,各组豚鼠分别隔日腹腔注射高剂量(5μg/kg)EC、低剂量(0.5μg/kg)EC、牛血清白蛋白(60mg)和0.9%NaCl(质量分数为0.9%的NaCl溶液)注射液(2ml),连续3次。致敏结束,末次致敏后第12天静脉快速注射2倍致敏剂量对以上相应的各组致敏豚鼠进行激发。致敏期间,每天观察豚鼠的症状,并于初次和最后一次致敏及激发当日测定每只豚鼠的体质量。(4)皮内刺激试验:取6只新西兰兔,单次皮内注射EC 10μg(0.2ml)/点,每侧5个点,观察皮内注射后的刺激反应情况。结果 (1)免疫特性研究结果:EC原液对卡介菌活菌菌液致敏的4只豚鼠的皮肤试验,阳性为0只;EC原液对结核分枝杆菌H37Ra活菌菌液致敏的6只豚鼠的皮肤试验,阳性为6只。(2)急性毒性试验结果:所有小鼠未出现明显的急性中毒反应和显示急性中毒靶器官。小鼠皮内注射EC前、注射EC后1d、3d、5d、7d、8d、10d、12d、14d高剂量组、低剂量组小鼠平均体质量分别为(20.6±1.3)g~(24.9±2.1) g、(20.5±1.6) g~(26.0±3.1) g;注射后不同观察时间各组平均体质量与空白对照组[(21.0±1.1)g~(25.3±2.3)g]比较差异均无统计学意义(t值分别为0.571~0.392,0.695~0.615;P值分别为0.575~0.700,0.496~0.546);小鼠肌内注射EC前、注射EC后1d、3d、5d、7d、8d、10d、12d、14d高剂量组、低剂量组小鼠平均体质量分别为(21.0±1.5) g~(26.2±1.9) g、(20.5±2.1) g~(25.8±3.8) g;注射后不同观察时间各组平均体质量与空白对照组[(21.2±1.7)g~(25.8±3.1)g]比较差异均无统计学意义(t值分别为0.360~0.318,0.900~0.006;P值分别为0.723~0.754,0.380~0.995)。(3)豚鼠全身主动过敏试验结果:豚鼠无过敏反应。高剂量组、低剂量组豚鼠首次致敏、末次致敏、激发的平均体质量分别为(327.5±24.3) g、(347.2±32.7) g、(402.2±34.9) g;(331.3±26.7) g、(346.2±32.0) g、(411.3±38.9) g,与相应观察时间注射0.9%NaCl的阴性对照组[(329.5±27.4) g、(348.3±27.0) g、(399.4±25.4) g]比较,差异均无统计学意义(t值分别为0.328、0.181、0.284,0.474、0.366、0.875;P值分别为0.757、0.864、0.788,0.656、0.730、0.422)。(4)兔皮内刺激试验结果:单次皮内注射10μg(0.2ml)/点EC,无明显刺激反应。结论 EC能够鉴别结核感染与卡介苗免疫,临床前动物试验安全性好,有望应用于人群结核感染的诊断与鉴别诊断。

关键词: 重组结核杆菌融合蛋白(EC), 分枝杆菌, 结核, 动物实验, 免疫学试验, 免疫活性, 药物评价, 临床前

Abstract:

Objective By perform the immunological characteristics and preclinical animal safety study of recombinant Mycobacterium tuberculosis fusion protein ESAT-6-CFP-10 (Which is the Chinese generic name of the drug determined by the National Pharmacopoeia Committee, EC stands for recombinant fusion protein 6 kDa early secretory antigenic target (ESAT-6) and 10 kDa culture filtrate protein (CFP-10))(EC), to discuss its clinical application prospect. Methods (1) Immunological characteristics study: 6 female guinea pigs were sensitized with Mycobacterium tuberculosis live bacteria solution (H37Ra), 5 weeks later, intradermally injected 0.2ml EC (2.5μg/ml); and 4 female guinea pigs were sensitized with live BCG bacteria solution, 5 weeks later, intradermally injected 0.2ml EC (20μg/ml). Observed the mean diameter of the induration or redness reaction ((longitudinal diameter + transverse diameter)/2, ≥5 mm is considered positive, <5 mm is considered negative). (2) Acute toxicity test: 80 ICR mice (Institute of Cancer Research (USA)) were divided into single intramuscular injection group and intradermal injection group, each group with 40, half male and half female. And then, each group was divided into 4 subgroups, each subgroup with 10, half male and half female. High dose subgroup was injected with EC of 53.61μg/0.1ml, while low does subgroup was 0.2μg/0.1ml, solvent control subgroup was injected with diluent (0.1ml) of EC, and the blank control subgroup would receive no injection. These mice were observed for abnormality in appearance, motor function, body weight, various organs and skin of injection site. (3) Guinea pig systemic active allergy test: 24 guinea pigs were divided into 4 subgroups, each subgroup with 6, half male and half female. Subgroups were injected intraperitoneally every other day with EC of 5μg/kg (high dose), 0.5μg/kg (low dose), bovine Serum Albumin, and 0.9%NaCl (2 ml) respectively, after 3 successive times, the sensitization finished. On the 12th day after the last sensitization, the sensitized guinea pigs were irritated by rapid intravenous injection with 2 times doses or more sensitizer. During sensitization, each animal’s symptom was observed daily and the body mass of each animal was measured on the first and last sensitization and irritation days. (4) Intradermal irritation experiment: 6 New Zealand rabbit was injected intradermally with EC of 10μg(0.2 ml)/spot, 5 spots on each side, observed the intradermal irritation reaction on the injection site. Results (1) Immunological characteristics study: In 4 BCG live bacteria solution sensitized guinea pigs, the skin tests with EC showed 0 positivity, and in 6 live MTB (H37Ra) sensitized guinea pigs, skin tests showed 6 with positivity. (2) Acute toxicity test: No significant acute toxic reactions or acute target organ poisoning were observed in all mice. The mean body masses of EC intradermally injected mice group at the time of: before injection, 1 d,3 d,5 d,7 d,8 d,10 d,12 d,14 d post injection, respectively in high dose subgroup and low dose subgroup were (20.6±1.3) g-(24.9±2.1) g,(20.5±1.6) g-(26.0±3.1) g;and compare to blank control group ((21.0±1.1) g-(25.3±2.3) g) in the corresponding time, the t values were 0.571-0.392;0.695-0.615;while P values were 0.575-0.700;0.496-0.546, respectively; the differences were not statistically significant. The mean body masses of EC intramuscularly injected mice group at the time of: before injection, 1 d,3 d,5 d,7 d,8 d,10 d,12 d,14 d post injection, respectively in high dose subgroup and low dose subgroup were (21.0±1.5) g-(26.2±1.9) g,(20.5±2.1) g-(25.8±3.8) g;and compare to blank control group ((21.2±1.7) g-(25.8±3.1) g) in the corresponding time, the t values were 0.360-0.318;0.900-0.006;while P values were 0.723-0.754;0.380-0.995;the differences were not statistically significant. (3) Guinea pig systemic active allergy test: no allergic reactions in guinea pigs. The average body mass of guinea pigs in the high,the low dose group of EC and 0.9%NaCl injected negative control group at the time of the first sensitization, the last sensitization, irritation and post irritation were (327.5±24.3) g,(347.2±32.7) g,(402.2±34.9) g;(331.3±26.7) g,(346.2±32.0) g,(411.3±38.9) g;(329.5±27.4) g,(348.3±27.0) g,(399.4±25.4) g, respectively. Compare to 0.9%NaCl injected negative control group, the t values were 0.328,0.181,0.284;0.474,0.366,0.875;while P values were 0.757,0.864,0.788;0.656,0.730,0.422, respectively, the differences were not statistically significant. (4) Intradermal irritation experiments in rabbits: for rabbits with single intradermal injection with 10μg(0.2 ml)/spot EC, no significant irritation reaction were observed. Conclusion EC is able to differentiate tuberculosis infection from BCG immunization. With good preclinical safety, it is expected to be applied in the in vivo diagnosis for Mycobacterium tuberculosis infection.

Key words: Recombinant Mycobacterium tuberculosis fusion protein(EC), Mycobacterium tuberculosis, Animal experimentation, Immunologic tests, Immunocompetence, Drug evaluation, preclinical

张凯, 陶立峰, 韦芬, 都伟欣, 仇晶晶, 陈伟, 陈保文, 朱银猛, 程兴, 苏城, 钟再新, 卢锦标, 蒲江. 重组结核杆菌融合蛋白(EC)的免疫特性和临床前安全性研究[J]. 中国防痨杂志, 2020, 42(8): 807-813. doi: 10.3969/j.issn.1000-6621.2020.08.006

ZHANG Kai, TAO Li-feng, WEI Fen, DU Wei-xin, QIU Jing-jing, CHEN Wei, CHEN Bao-wen, ZHU Yin-meng, CHENG Xing, SU Cheng, ZHONG Zai-xin, LU Jin-biao, PU Jiang. Immune characteristics and preclinical animal safety studies of recombinant Mycobacterium tuberculosis fusion protein(EC)[J]. Chinese Journal of Antituberculosis, 2020, 42(8): 807-813. doi: 10.3969/j.issn.1000-6621.2020.08.006

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参考文献 12

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豚鼠编号	皮肤试验24h后观察硬结或红晕平均直径(mm)			反应结果
豚鼠编号	横径	纵径	平均直径	反应结果
1	16.0	17.5	16.75	阳性
2	15.6	14.7	15.15	阳性
3	16.4	17.0	16.70	阳性
4	14.3	15.6	14.95	阳性
5	17.6	19.2	18.40	阳性
6	16.3	17.2	16.75	阳性

观察时间	空白对照组 (g, $\bar{x}$±s)	高剂量组 (g, $\bar{x}$±s)	t值^a	P值	低剂量组 (g,$\bar{x}$±s)	t值^a	P值	溶剂对照组 (g, $\bar{x}$±s)	t值^a	P值
注射前	21.0±1.1	20.6±1.3	0.571	0.575	20.5±1.6	0.695	0.496	20.5±1.1	0.945	0.357
注射后1d	21.3±1.3	20.6±1.6	1.047	0.309	21.0±1.6	0.453	0.656	20.2±1.7	1.686	0.109
注射后3d	21.1±2.1	21.3±2.6	0.151	0.882	22.2±2.7	0.920	0.370	20.4±3.0	0.682	0.504
注射后5d	20.3±2.3	20.9±2.8	0.570	0.576	22.2±2.9	1.676	0.111	20.6±3.6	0.221	0.828
注射后7d	21.6±2.1	22.0±2.4	0.379	0.709	23.2±2.8	1.462	0.161	21.6±3.3	0.000	1.000
注射后8d	22.2±2.1	22.6±1.8	0.452	0.657	23.8±2.7	1.574	0.133	22.3±3.5	0.108	0.915
注射后10d	23.2±2.3	23.4±1.6	0.189	0.852	24.5±2.6	1.184	0.252	24.2±3.2	0.765	0.454
注射后12d	24.4±2.0	24.3±2.0	0.099	0.922	25.5±3.0	0.933	0.363	24.7±2.9	0.262	0.796
注射后14d	25.3±2.3	24.9±2.1	0.392	0.700	26.0±3.1	0.615	0.546	25.5±3.1	0.145	0.886

观察时间	空白对照组 (g, $\bar{x}$±s)	高剂量组 (g, $\bar{x}$±s)	t值^a	P值	低剂量组 (g, $\bar{x}$±s)	t值^a	P值	溶剂对照组 (g, $\bar{x}$±s)	t值^a	P值
注射前	21.2±1.7	21.0±1.5	0.360	0.723	20.5±2.1	0.900	0.380	20.8±1.8	0.552	0.588
注射后1d	21.7±2.5	21.2±2.0	0.549	0.590	20.7±2.4	0.870	0.396	20.9±2.4	0.767	0.453
注射后3d	22.3±3.3	21.6±3.1	0.543	0.594	21.6±3.1	0.509	0.617	21.3±2.7	0.786	0.442
注射后5d	22.2±3.7	21.5±3.0	0.489	0.631	22.2±3.2	0.006	0.995	21.5±2.6	0.480	0.637
注射后7d	22.5±3.5	22.2±2.1	0.251	0.805	23.0±3.5	0.312	0.759	22.8±2.5	0.214	0.833
注射后8d	23.2±3.1	22.9±1.9	0.305	0.764	23.3±3.3	0.070	0.945	23.8±2.9	0.421	0.679
注射后10d	24.3±2.9	24.0±2.2	0.277	0.785	23.6±3.9	0.433	0.670	25.2±3.0	0.716	0.483
注射后12d	25.0±3.0	25.0±1.8	0.018	0.986	24.9±3.7	0.093	0.927	25.8±3.4	0.531	0.602
注射后14d	25.8±3.1	26.2±1.9	0.318	0.754	25.8±3.8	0.006	0.995	26.7±3.4	0.565	0.579

组别	过敏反应的豚鼠数(只)	死亡豚鼠数(只)	反应级别	过敏反应结果
高剂量组	0	0	-	阴性
低剂量组	0	0	-	阴性
阳性对照组	6	3	++++	极强阳性
阴性对照组	0	0	-	阴性