新生儿药物乙酰化表型。

I Szórády, A Sánta, I Veress
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引用次数: 0

摘要

对100例健康新生儿药物乙酰化表型分布进行了研究,并与不同年龄组药物乙酰化表型频率进行了比较。在单次口服试验剂量/ 100mg后,通过测定尿液中的总和游离磺胺来进行表型分析。与老年受试者一样,慢乙酰化表型在健康新生儿中也占主导地位(83%),这是观察到的所有年龄组中频率最高的。新生儿乙酰化酶表型可能受到遗传、环境(如营养)以及发育因素(如出生后酶缺乏、器官功能年龄特异性变化等)的影响。在这种情况下,新生儿缓慢的乙酰化表型也可能与泛酸负平衡导致辅酶a合成不足有关。慢乙酰化表型的优势导致较高的药物敏感性,在临床上可视为人类新生儿的特殊危险因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Drug acetylator phenotypes in newborn infants.

The distribution of drug acetylator phenotypes in 100 healthy newborn infants was studied and compared with the acetylator phenotypes frequency in different age groups. Phenotyping was performed by assaying total and free sulphadimidine in the urine after single oral test dose of the drug/100 mg. As in elderly subjects, slow acetylator phenotype was predominant also in healthy newborns (83%), which was the highest frequency of all age groups observed. Acetylator phenotype in the newborn infants may be influenced by genetic, environmental (e.g., nutritive), as well as by developmental factors (e.g., postnatal enzyme deficiency, age-specific changes in organ functions, etc.). In this connection, slow acetylator phenotype of the neonate may be related to a negative pantothenic acid balance causing insufficient Coenzyme-A synthesis, too. The predominance of the slow acetylator phenotype resulting in higher drug sensitivity can be regarded clinically as a special risk factor in human neonates.

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