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给予特立帕肽[重组人甲状旁腺激素(1-34)]的F344大鼠的骨肿瘤取决于治疗持续时间和剂量。

Bone neoplasms in F344 rats given teriparatide [rhPTH(1-34)] are dependent on duration of treatment and dose.

作者信息

Vahle John L, Long Gerald G, Sandusky George, Westmore Michael, Ma Yanfei Linda, Sato Masahiko

机构信息

Lilly Research Laboratories, Greenfield, Indiana, USA.

出版信息

Toxicol Pathol. 2004 Jul-Aug;32(4):426-38. doi: 10.1080/01926230490462138.

Abstract

A long-term study was conducted in female F344 rats to determine the relative importance of dose, treatment duration, and age at initiation of treatment on the incidence of teriparatide [rhPTH[1-34)]-induced bone proliferative lesions. Treatment groups consisted of different combinations of dose (0, 5, or 30 microg/kg/d), treatment duration (6, 20, or 24 months) and age at initiation of treatment (2 or 6 months of age). The primary endpoints were the incidence of bone neoplasms and effects on bone mass and structure as evaluated by quantitative computed tomography and histomorphometery. Significant increases in the incidence of bone tumors (osteoma, osteoblastoma, and osteosarcoma) occurred in rats treated with 30 microg/kg for 20 or 24 months. No neoplasms were found when the 5 microg/kg treatment was initiated at 6 months of age and continued for either 6 or 20 months (up to 70% of life span). This treatment regimen defined a "no-effect" dose for neoplasm formation that nevertheless resulted in substantial increases in bone mass. These results demonstrate that treatment duration and administered dose are the most important factors in the teriparatide-induced bone tumors in rats.

摘要

在雌性F344大鼠中进行了一项长期研究,以确定剂量、治疗持续时间和开始治疗时的年龄对特立帕肽[rhPTH(1-34)]诱导的骨增殖性病变发生率的相对重要性。治疗组由剂量(0、5或30微克/千克/天)、治疗持续时间(6、20或24个月)和开始治疗时的年龄(2或6个月龄)的不同组合组成。主要终点是骨肿瘤的发生率以及通过定量计算机断层扫描和组织形态计量学评估的对骨量和结构的影响。接受30微克/千克治疗20或24个月的大鼠骨肿瘤(骨瘤、成骨细胞瘤和骨肉瘤)发生率显著增加。当在6个月龄开始5微克/千克治疗并持续6或20个月(长达寿命的70%)时,未发现肿瘤。这种治疗方案确定了一个肿瘤形成的“无效应”剂量,然而该剂量仍导致骨量大幅增加。这些结果表明,治疗持续时间和给药剂量是大鼠特立帕肽诱导骨肿瘤的最重要因素。

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