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自闭症中阿片类药物与免疫的相互作用:纳曲酮双盲治疗期间的行为和免疫学评估

Opioid-immune interactions in autism: behavioural and immunological assessment during a double-blind treatment with naltrexone.

作者信息

Scifo R, Cioni M, Nicolosi A, Batticane N, Tirolo C, Testa N, Quattropani M C, Morale M C, Gallo F, Marchetti B

机构信息

Servizio di Psichiatria, Istituto OASI per lo Studio del Ritardo Mentale e l'Involuzione Cerebrale, Troina (Enna), Italy.

出版信息

Ann Ist Super Sanita. 1996;32(3):351-9.

PMID:9028057
Abstract

The emerging concept of opioid peptides as a new class of chemical messengers of the neuroimmune axis and the presence of a number of immunological abnormalities in infantile autism prompted us to correlate biological (hormonal and immunological) determinations and behavioural performances during treatment with the potent opiate antagonist, naltrexone (NAL). Twelve autistic patients ranging from 7 to 15 years, diagnosed according to DSM-III-R, entered a double-blind crossover study with NAL at the doses of 0.5, 1.0 and 1.5 mg/kg every 48 hours. The behavioural evaluation was conducted using the specific BSE and CARS rating scales NAL treatment produced a significant reduction of the autistic symptomatology in seven ("responders") out of 12 children. The behavioural improvement was accompanied by alterations in the distribution of the major lymphocyte subsets, with a significant increase of the T-helper-inducers (CD4+CD8-) and a significant reduction of the T-cytotoxic-suppressor (CD4-CD8+) resulting in a normalization of the CD4/CD8 ratio. Changes in natural killer cells and activity were inversely related to plasma beta-endorphin levels. It is suggested that the mechanisms underlying opioid-immune interactions are altered in this population of autistic children and that an immunological screening may have prognostic value for the pharmacological therapy with opiate antagonists.

摘要

阿片肽作为神经免疫轴一类新型化学信使的新兴概念,以及婴儿自闭症中存在的一些免疫异常情况,促使我们将强效阿片拮抗剂纳曲酮(NAL)治疗期间的生物学(激素和免疫)测定结果与行为表现相关联。根据《精神疾病诊断与统计手册》第三版修订本(DSM-III-R)诊断的12名7至15岁自闭症患者,进入了一项双盲交叉研究,每48小时接受0.5、1.0和1.5 mg/kg剂量的NAL治疗。使用特定的BSE和CARS评定量表进行行为评估。NAL治疗使12名儿童中的7名(“反应者”)自闭症症状显著减轻。行为改善伴随着主要淋巴细胞亚群分布的改变,辅助诱导性T细胞(CD4+CD8-)显著增加,细胞毒性抑制性T细胞(CD4-CD8+)显著减少,导致CD4/CD8比值正常化。自然杀伤细胞及其活性的变化与血浆β-内啡肽水平呈负相关。提示在这群自闭症儿童中,阿片-免疫相互作用的潜在机制发生了改变,免疫筛查可能对阿片拮抗剂的药物治疗具有预后价值。

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