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索立夫定对急性带状疱疹患者二氢嘧啶脱氢酶活性的影响。

The effect of sorivudine on dihydropyrimidine dehydrogenase activity in patients with acute herpes zoster.

作者信息

Yan J, Tyring S K, McCrary M M, Lee P C, Haworth S, Raymond R, Olsen S J, Diasio R B

机构信息

Department of Pharmacology and Toxicology, University of Alabama at Birmingham 35294, USA.

出版信息

Clin Pharmacol Ther. 1997 May;61(5):563-73. doi: 10.1016/S0009-9236(97)90136-3.

Abstract

OBJECTIVE

Bromovinyl-uracil (BVU) is the principal metabolite of sorivudine, a potent anti-zoster nucleoside. BVU binds to, and irreversibly inhibits, the enzyme dihydropyrimidine dehydrogenase (DPD). The objective of this study was to assess the time course of recovery of DPD activity after oral administration of sorivudine in patients with herpes zoster and to correlate restoration of DPD activity and levels of uracil with the elimination of sorivudine and its metabolite BVU from the circulation.

METHODS

Sorivudine was given orally as 40 mg once-daily doses for 10 consecutive days to a total of 19 patients with herpes zoster. Serum sorivudine, BVU, and circulating uracil and DPD activity in peripheral blood mononuclear cells (PBMCs) were determined before, during, and after administration of sorivudine.

RESULTS

BVU was eliminated from the circulation within 7 days after the last sorivudine dose. DPD activity in PBMCs, which was completely suppressed in 18 of the 19 subjects and markedly suppressed in the remaining subject during administration of sorivudine, recovered to baseline levels within 19 days after the last dose of sorivudine in all subjects and within 14 days in all but one of the subjects. The restoration of DPD activity was temporally associated with elimination of BVU from the circulation. The elevated uracil concentrations produced by inhibition of DPD activity fell rapidly after cessation of sorivudine administration and also were temporally associated with elimination of BVU from the circulation. The time course of recovery of DPD activity in three patients with renal impairment was similar to that of the other subjects.

CONCLUSIONS

This study indicates that sorivudine therapy is associated with a profound depression of DPD activity. Recovery of DPD activity occurred within 4 weeks of the completion of sorivudine therapy, which indicates that fluorinated pyrimidines may be safely administered 4 weeks after completion of sorivudine therapy.

摘要

目的

溴乙烯基尿嘧啶(BVU)是索立夫定的主要代谢产物,索立夫定是一种有效的抗带状疱疹核苷。BVU可与二氢嘧啶脱氢酶(DPD)结合并对其产生不可逆抑制作用。本研究的目的是评估带状疱疹患者口服索立夫定后DPD活性恢复的时间进程,并将DPD活性的恢复以及尿嘧啶水平与索立夫定及其代谢产物BVU从循环中的清除情况进行关联。

方法

对总共19例带状疱疹患者连续10天每天口服40mg索立夫定。在索立夫定给药前、给药期间和给药后,测定血清中的索立夫定、BVU、循环尿嘧啶以及外周血单核细胞(PBMC)中的DPD活性。

结果

在最后一剂索立夫定给药后7天内,BVU从循环中清除。在索立夫定给药期间,19名受试者中有18名的PBMC中的DPD活性被完全抑制,其余受试者的DPD活性被显著抑制,在所有受试者中,最后一剂索立夫定给药后19天内DPD活性恢复至基线水平,除一名受试者外,其他所有受试者在14天内恢复至基线水平。DPD活性的恢复在时间上与BVU从循环中的清除相关。索立夫定给药停止后,因DPD活性受抑制而升高的尿嘧啶浓度迅速下降,并且在时间上也与BVU从循环中的清除相关。3例肾功能损害患者的DPD活性恢复时间进程与其他受试者相似。

结论

本研究表明,索立夫定治疗与DPD活性的显著降低有关。索立夫定治疗结束后4周内DPD活性恢复,这表明在索立夫定治疗结束4周后可以安全地给予氟嘧啶类药物。

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