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烟酰胺在人和小鼠体内的药代动力学:比较评估及其对放射治疗的意义。

Nicotinamide pharmacokinetics in humans and mice: a comparative assessment and the implications for radiotherapy.

作者信息

Horsman M R, Høyer M, Honess D J, Dennis I F, Overgaard J

机构信息

Danish Cancer Society, Department of Experimental Clinical Oncology, Aarhus.

出版信息

Radiother Oncol. 1993 May;27(2):131-9. doi: 10.1016/0167-8140(93)90133-s.

Abstract

Healthy human volunteers orally ingested escalating doses of up to 6 g nicotinamide in capsule form on an empty stomach. Some side-effects were seen although these were mild and transient. HPLC analysis of blood samples showed peak plasma levels, typically within 45 min after ingestion, which were linearly dependent on dose ingested. The elimination half-life and AUC were also found to increase with drug dose, although these increases were non-linear. Pharmacokinetic studies were also performed in female CDF1 mice with C3H mammary carcinomas grown in the right rear foot. Analysis of blood and tumour samples taken from mice injected i.p. with nicotinamide doses between 100-1000 mg/kg showed similar characteristics as the human data, although the elimination half-lives were not dose-dependent. The average peak plasma concentration of 160 micrograms/ml measured in humans after taking 6 g of nicotinamide was equivalent to that seen in mice after injecting 171 mg/kg. Using a regrowth delay assay the enhancement of radiation damage by nicotinamide in this mouse tumour was found to be independent of drug dose from 100-1000 mg/kg, resulting in a constant 1.3-fold increase in radiation response. Doses of nicotinamide that can be tolerated clinically should therefore produce adequate enhancements of radiation damage in human tumours.

摘要

健康的人类志愿者空腹口服递增剂量的胶囊形式的烟酰胺,最高剂量达6克。尽管出现了一些副作用,但都很轻微且短暂。对血样的高效液相色谱分析显示,血浆峰值水平通常在摄入后45分钟内出现,且与摄入剂量呈线性相关。还发现消除半衰期和药时曲线下面积也随药物剂量增加,尽管这些增加是非线性的。对右后足生长有C3H乳腺癌的雌性CDF1小鼠也进行了药代动力学研究。对腹腔注射100 - 1000毫克/千克烟酰胺剂量的小鼠采集的血液和肿瘤样本进行分析,结果显示与人类数据具有相似特征,尽管消除半衰期与剂量无关。人类服用6克烟酰胺后测得的平均血浆峰值浓度为160微克/毫升,这与小鼠注射171毫克/千克后测得的浓度相当。使用再生长延迟试验发现,在该小鼠肿瘤中,100 - 1000毫克/千克剂量范围内烟酰胺对辐射损伤的增强作用与药物剂量无关,辐射反应持续增加1.3倍。因此,临床上能够耐受的烟酰胺剂量应该能在人类肿瘤中产生足够的辐射损伤增强作用。

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