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假异胞苷的生化、药理学及I期临床评估

Biochemical, pharmacological, and phase I clinical evaluation of pseudoisocytidine.

作者信息

Woodcock T M, Chou T C, Tan C T, Sternberg S S, Philips F S, Young C W, Burchenal J H

出版信息

Cancer Res. 1980 Nov;40(11):4243-9.

PMID:7471064
Abstract

Pseudoisocytidine (psi ICyd) is a C-nucleoside with enhanced stability and resistance to enzymatic deamination when compared to 5-azacytidine and 1-beta-D-arabinofuranosylcytosine. Elimination kinetics in plasma using [14C]psi ICyd showed a beta-phase for t1/2 for 14C of 2 hr and a beta-phase t1/2 of unchanged psi ICyd of 1.5 hr. Net recovery of radioactivity in urine over 24 hr varied between 40 and 80% of the administered dose; 50 to 90% was unchanged drug and the rest was pseudouridine. Human leukemic cells in vitro deaminated psi ICyd very slowly, formed appreciable quantities of pseudoisocytidine triphosphate, and incorporated small amounts into RNA and DNA. Clinical trials were done using a daily i.v. injection for 5 consecutive days. Hematological or intestine toxicities were not seen, nor was depression of white blood cell count observed in leukemic patients. Hepatic toxicity proved to be dose limiting; this was characterized by an early phase with elevation of prothrombin time and aspartate aminotransferase. A later phase with cirrhosis was observed in two patients. Autopsy showed massive hepatic necrosis in patients dying of acute toxicity and micronodular cirrhosis in one patient dying with the chronic form.

摘要

假异胞苷(psi ICyd)是一种C核苷,与5-氮杂胞苷和1-β-D-阿拉伯呋喃糖基胞嘧啶相比,具有更高的稳定性和抗酶促脱氨能力。使用[14C]psi ICyd进行的血浆消除动力学显示,14C的t1/2的β相为2小时,未变化的psi ICyd的β相t1/2为1.5小时。24小时内尿液中放射性的净回收率在给药剂量的40%至80%之间变化;50%至90%为未变化的药物,其余为假尿苷。体外人白血病细胞对psi ICyd的脱氨作用非常缓慢,形成了相当数量的假异胞苷三磷酸,并少量掺入RNA和DNA中。临床试验采用每日静脉注射,连续注射5天。未观察到血液学或肠道毒性,白血病患者也未观察到白细胞计数降低。肝毒性被证明是剂量限制性的;其特征是早期阶段凝血酶原时间和天冬氨酸转氨酶升高。在两名患者中观察到后期出现肝硬化。尸检显示,死于急性毒性的患者有大量肝坏死,一名死于慢性形式的患者有小结节性肝硬化。

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