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通过免疫接种预防蓖麻毒素和相思子毒素的吸入毒性。

Protection against inhalation toxicity of ricin and abrin by immunisation.

作者信息

Griffiths G D, Lindsay C D, Allenby A C, Bailey S C, Scawin J W, Rice P, Upshall D G

机构信息

Biology Division, Chemical & Biological Defence Establishment, Porton Down, Wiltshire, UK.

出版信息

Hum Exp Toxicol. 1995 Feb;14(2):155-64. doi: 10.1177/096032719501400201.

DOI:10.1177/096032719501400201
PMID:7779439
Abstract
  1. Abrin and ricin are highly toxic plant proteins which are very similar in structure and function and inhibit protein synthesis in eukaryotes. 2. Rats have been immunised against either toxin using formaldehyde-toxoids by three subcutaneous injections at intervals of 3 weeks. For abrin, serum titres in 14 out of 15 rats were raised to between 1:12800 and 1:51200 after two injections, 6 weeks from the start of the experiment. Titres of between 1:256 and 1:1024 were also measured in lung washes after challenge with active abrin toxin. 3. The three major antibody classes, IgG, IgM and IgA were present in the immune sera but IgG and IgA only were detected in lung washes. The proportion of IgA to IgG was higher in the lung fluid than in sera. Rats immunised by abrin toxoid were protected against 5 LCt50's of abrin by inhalation but others exposed to ricin were not. 4. For ricin, serum titres ranged from 1:800 to 1:25600 after two injections and after a third injection the titre range was the same but population samples were weighted towards the higher titres. All rats immunised with ricin toxoid survived the challenge of 5 LCt50's of ricin toxin by inhalation over the observation period of 28 days post-challenge. 5. Representative immunised rats (abrin toxoid) were taken at various times post-exposure, humanely killed and tissues were examined for pathological changes. It was concluded that an apparently severe lung lesion occurred at a later time than in non-immunised, toxin challenged rats. This damage was not lethal over the experimental observation periods. 6. Immunisation by the sub-cutaneous route therefore protects against lethality from challenge by inhalation of ricin or abrin toxins but does not prevent significant lung damage.
摘要
  1. 相思子毒素和蓖麻毒素是剧毒植物蛋白,它们在结构和功能上非常相似,可抑制真核生物中的蛋白质合成。2. 用甲醛类毒素通过每隔3周进行3次皮下注射的方式对大鼠进行两种毒素的免疫。对于相思子毒素,在实验开始6周后进行两次注射后,15只大鼠中有14只的血清效价提高到了1:12800至1:51200之间。在用活性相思子毒素攻击后,肺灌洗液中的效价也测得在1:256至1:1024之间。3. 免疫血清中存在三种主要抗体类别,即IgG、IgM和IgA,但肺灌洗液中仅检测到IgG和IgA。肺液中IgA与IgG的比例高于血清。用相思子类毒素免疫的大鼠通过吸入可抵御5个半数致死浓度(LCt50)的相思子毒素,但暴露于蓖麻毒素的其他大鼠则不能。4. 对于蓖麻毒素,两次注射后的血清效价范围为1:800至1:25600,第三次注射后的效价范围相同,但群体样本的效价更倾向于较高水平。在28天的观察期内,所有用蓖麻类毒素免疫的大鼠在吸入5个半数致死浓度(LCt50)的蓖麻毒素攻击后均存活。5. 在暴露后的不同时间点选取代表性的免疫大鼠(相思子类毒素),进行人道处死,并检查组织的病理变化。得出的结论是,与未免疫且受到毒素攻击的大鼠相比,明显严重的肺部病变出现的时间较晚。在实验观察期内,这种损伤并不致命。6. 因此,通过皮下途径免疫可抵御吸入蓖麻毒素或相思子毒素攻击导致的致死性,但不能防止明显的肺部损伤。

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