哌啶类吩噻嗪抗精神病药物的代谢。III. 美索达嗪在犬、人和大鼠体内的代谢

The metabolism of piperidine-type phenothiazine antipsychotic agents. III. Mesoridazine in dog, human and rat.

作者信息

Lin G, Hawes E M, McKay G, Korchinski E D, Midha K K

机构信息

College of Pharmacy, University of Saskatchewan, Saskatoon, Canada.

出版信息

Xenobiotica. 1993 Jan;23(1):37-52. doi: 10.3109/00498259309059360.

DOI:10.3109/00498259309059360

PMID:8097900

Abstract

The metabolism of mesoridazine was studied in female rats (20 mg/kg, oral), female dogs (50 mg over 30 h, oral) and adult male volunteers (25 mg, oral). 2. Solvent extracts of urines from each species were directly analysed by h.p.l.c.-mass spectrometry with a plasmaspray interface. In the case of phenolic metabolites the urinary extracts were derivatized with a silylating reagent (with and without prior enzymic hydrolysis) prior to analysis. The structures of metabolites, with the exceptions of mesoridazine N-oxide and phenols, were confirmed by comparison of their chromatographic behaviours and mass spectra with those of authentic standards. 3. Compounds identified in the urine of all three species were mesoridazine, sulforidazine, mesoridazine ring sulphoxide, sulforidazine ring sulphoxide, N-desmethylmesoridazine ring sulphoxide, the lactam of sulforidazine ring sulphoxide and phenolic derivatives of mesoridazine and sulforidazine. Whereas the unconjugated phenolic metabolite of sulforidazine was present in urine of all three species, the conjugated form was identified only in dog and rat urines. Also, the unconjugated phenolic metabolite of mesoridazine was identified only in the urine of dog and human, but rat urine contained only the conjugated form. 4. Other metabolites found were: the lactam of mesoridazine (rat), the lactam of mesoridazine ring sulphoxide (rat and human), mesoridazine N-oxide (human) and sulforidazine N-oxide (dog and human). 5. Mesoridazine and six of its metabolites present in urines of human, rat and dog were quantified by a h.p.l.c.-u.v. method. The mean total excretion of measured analytes in human, rat and dog were 6.3, 2.6 and 29.1%, respectively. The excretion of the lactam of sulforidazine ring sulphoxide was greater in human (0.4%) and rat (0.2%) than dog (0.02%). Moreover, the urinary excretion of the lactam of mesoridazine ring sulphoxide in human and rat constituted 0.4% and 0.2%, respectively. Of the three lactams found in rat the lactam of mesoridazine was present in the least amount (0.05%). 6. Interspecies comparison of the lactam metabolites indicated that both qualitatively and quantitatively human more closely resembled rat than dog. On the other hand, N-oxide metabolites were detected in human and dog but not in rat.

摘要

对雌性大鼠（口服20毫克/千克）、雌性犬（30小时内口服50毫克）和成年男性志愿者（口服25毫克）体内的美索哒嗪代谢情况进行了研究。2. 每个物种尿液的溶剂提取物通过带有等离子体喷雾接口的高效液相色谱-质谱联用仪直接分析。对于酚类代谢物，尿液提取物在分析前用硅烷化试剂进行衍生化处理（有和没有预先的酶水解）。除美索哒嗪N-氧化物和酚类外，通过将代谢物的色谱行为和质谱与标准品的进行比较来确认其结构。3. 在所有三个物种的尿液中鉴定出的化合物有美索哒嗪、舒必利嗪、美索哒嗪环亚砜、舒必利嗪环亚砜、N-去甲基美索哒嗪环亚砜、舒必利嗪环亚砜的内酰胺以及美索哒嗪和舒必利嗪的酚类衍生物。虽然舒必利嗪的未结合酚类代谢物在所有三个物种的尿液中都存在，但结合形式仅在犬和大鼠的尿液中鉴定出。此外，美索哒嗪的未结合酚类代谢物仅在犬和人的尿液中鉴定出，但大鼠尿液中仅含有结合形式。4. 发现的其他代谢物有：美索哒嗪的内酰胺（大鼠）、美索哒嗪环亚砜的内酰胺（大鼠和人）、美索哒嗪N-氧化物（人）和舒必利嗪N-氧化物（犬和人）。5. 通过高效液相色谱-紫外法对人、大鼠和犬尿液中存在的美索哒嗪及其六种代谢物进行了定量。人、大鼠和犬中被测分析物的平均总排泄率分别为6.3%、2.6%和29.1%。舒必利嗪环亚砜内酰胺在人的排泄率（0.4%）和大鼠的排泄率（0.2%）高于犬（0.02%）。此外，美索哒嗪环亚砜内酰胺在人和大鼠尿液中的排泄率分别为0.4%和0.2%。在大鼠中发现的三种内酰胺中，美索哒嗪的内酰胺含量最少（0.05%）。6. 内酰胺代谢物的种间比较表明，在定性和定量方面，人与大鼠比与犬更相似。另一方面，在人和犬中检测到了N-氧化物代谢物，但在大鼠中未检测到。

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The metabolism of piperidine-type phenothiazine antipsychotic agents. III. Mesoridazine in dog, human and rat.哌啶类吩噻嗪抗精神病药物的代谢。III. 美索达嗪在犬、人和大鼠体内的代谢

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哌啶类吩噻嗪抗精神病药物的代谢。III. 美索达嗪在犬、人和大鼠体内的代谢

The metabolism of piperidine-type phenothiazine antipsychotic agents. III. Mesoridazine in dog, human and rat.

作者信息

Lin G, Hawes E M, McKay G, Korchinski E D, Midha K K

机构信息

College of Pharmacy, University of Saskatchewan, Saskatoon, Canada.

出版信息

Xenobiotica. 1993 Jan;23(1):37-52. doi: 10.3109/00498259309059360.

DOI:10.3109/00498259309059360

PMID:8097900

Abstract

The metabolism of mesoridazine was studied in female rats (20 mg/kg, oral), female dogs (50 mg over 30 h, oral) and adult male volunteers (25 mg, oral). 2. Solvent extracts of urines from each species were directly analysed by h.p.l.c.-mass spectrometry with a plasmaspray interface. In the case of phenolic metabolites the urinary extracts were derivatized with a silylating reagent (with and without prior enzymic hydrolysis) prior to analysis. The structures of metabolites, with the exceptions of mesoridazine N-oxide and phenols, were confirmed by comparison of their chromatographic behaviours and mass spectra with those of authentic standards. 3. Compounds identified in the urine of all three species were mesoridazine, sulforidazine, mesoridazine ring sulphoxide, sulforidazine ring sulphoxide, N-desmethylmesoridazine ring sulphoxide, the lactam of sulforidazine ring sulphoxide and phenolic derivatives of mesoridazine and sulforidazine. Whereas the unconjugated phenolic metabolite of sulforidazine was present in urine of all three species, the conjugated form was identified only in dog and rat urines. Also, the unconjugated phenolic metabolite of mesoridazine was identified only in the urine of dog and human, but rat urine contained only the conjugated form. 4. Other metabolites found were: the lactam of mesoridazine (rat), the lactam of mesoridazine ring sulphoxide (rat and human), mesoridazine N-oxide (human) and sulforidazine N-oxide (dog and human). 5. Mesoridazine and six of its metabolites present in urines of human, rat and dog were quantified by a h.p.l.c.-u.v. method. The mean total excretion of measured analytes in human, rat and dog were 6.3, 2.6 and 29.1%, respectively. The excretion of the lactam of sulforidazine ring sulphoxide was greater in human (0.4%) and rat (0.2%) than dog (0.02%). Moreover, the urinary excretion of the lactam of mesoridazine ring sulphoxide in human and rat constituted 0.4% and 0.2%, respectively. Of the three lactams found in rat the lactam of mesoridazine was present in the least amount (0.05%). 6. Interspecies comparison of the lactam metabolites indicated that both qualitatively and quantitatively human more closely resembled rat than dog. On the other hand, N-oxide metabolites were detected in human and dog but not in rat.

摘要

对雌性大鼠（口服20毫克/千克）、雌性犬（30小时内口服50毫克）和成年男性志愿者（口服25毫克）体内的美索哒嗪代谢情况进行了研究。2. 每个物种尿液的溶剂提取物通过带有等离子体喷雾接口的高效液相色谱-质谱联用仪直接分析。对于酚类代谢物，尿液提取物在分析前用硅烷化试剂进行衍生化处理（有和没有预先的酶水解）。除美索哒嗪N-氧化物和酚类外，通过将代谢物的色谱行为和质谱与标准品的进行比较来确认其结构。3. 在所有三个物种的尿液中鉴定出的化合物有美索哒嗪、舒必利嗪、美索哒嗪环亚砜、舒必利嗪环亚砜、N-去甲基美索哒嗪环亚砜、舒必利嗪环亚砜的内酰胺以及美索哒嗪和舒必利嗪的酚类衍生物。虽然舒必利嗪的未结合酚类代谢物在所有三个物种的尿液中都存在，但结合形式仅在犬和大鼠的尿液中鉴定出。此外，美索哒嗪的未结合酚类代谢物仅在犬和人的尿液中鉴定出，但大鼠尿液中仅含有结合形式。4. 发现的其他代谢物有：美索哒嗪的内酰胺（大鼠）、美索哒嗪环亚砜的内酰胺（大鼠和人）、美索哒嗪N-氧化物（人）和舒必利嗪N-氧化物（犬和人）。5. 通过高效液相色谱-紫外法对人、大鼠和犬尿液中存在的美索哒嗪及其六种代谢物进行了定量。人、大鼠和犬中被测分析物的平均总排泄率分别为6.3%、2.6%和29.1%。舒必利嗪环亚砜内酰胺在人的排泄率（0.4%）和大鼠的排泄率（0.2%）高于犬（0.02%）。此外，美索哒嗪环亚砜内酰胺在人和大鼠尿液中的排泄率分别为0.4%和0.2%。在大鼠中发现的三种内酰胺中，美索哒嗪的内酰胺含量最少（0.05%）。6. 内酰胺代谢物的种间比较表明，在定性和定量方面，人与大鼠比与犬更相似。另一方面，在人和犬中检测到了N-氧化物代谢物，但在大鼠中未检测到。

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哌啶类吩噻嗪抗精神病药物的代谢。III. 美索达嗪在犬、人和大鼠体内的代谢

The metabolism of piperidine-type phenothiazine antipsychotic agents. III. Mesoridazine in dog, human and rat.

作者信息

机构信息

出版信息

相似文献

哌啶类吩噻嗪抗精神病药物的代谢。III. 美索达嗪在犬、人和大鼠体内的代谢

The metabolism of piperidine-type phenothiazine antipsychotic agents. III. Mesoridazine in dog, human and rat.

作者信息

机构信息

出版信息

相似文献