Jolette Jacquelin, Wilker Clynn E, Smith Susan Y, Doyle Nancy, Hardisty Jerry F, Metcalfe Anna J, Marriott Thomas B, Fox John, Wells David S
Charles River Laboratories, Senneville, Quebec H9X 3R3, Canada.
Toxicol Pathol. 2006;34(7):929-40. doi: 10.1080/01926230601072301.
The carcinogenic potential of human parathyroid hormone 1-84 (PTH) was assessed by daily subcutaneous injection (0, 10, 50, 150 microg/kg/day) for 2 years in Fischer 344 rats. Histopathological analyses were conducted on the standard set of soft tissues, tissues with macroscopic abnormalities, selected bones, and bones with abnormalities identified radiographically. All PTH doses caused widespread osteosclerosis and significant, dose-dependent increases in femoral and vertebral bone mineral content and density. In the mid-and high-dose groups, proliferative changes in bone increased with dose. Osteosarcoma was the most common change, followed by focal osteoblast hyperplasia, osteoblastoma, osteoma and skeletal fibrosarcoma. The incidence of bone neoplasms was comparable in control and low-dose groups providing a noncarcinogenic dose for PTH of 10 microg/kg/day at a systemic exposure to PTH that is 4.6-fold higher than for a 100 microg dose in humans. The ability of PTH to interact with and balance the effects of both the PTH-1 receptor and the putative C-terminal PTH receptor, may lead to the lower carcinogenic potential observed with PTH than reported previously for teriparatide.
通过在Fischer 344大鼠中每日皮下注射(0、10、50、150微克/千克/天),持续2年,评估了人甲状旁腺激素1-84(PTH)的致癌潜力。对一组标准软组织、有宏观异常的组织、选定的骨骼以及经X线检查发现有异常的骨骼进行了组织病理学分析。所有PTH剂量均导致广泛的骨硬化,以及股骨和椎骨骨矿物质含量和密度显著的剂量依赖性增加。在中、高剂量组中,骨的增殖性变化随剂量增加。骨肉瘤是最常见的变化,其次是局灶性成骨细胞增生、成骨细胞瘤、骨瘤和骨骼纤维肉瘤。对照组和低剂量组的骨肿瘤发生率相当,这表明PTH的非致癌剂量为10微克/千克/天,此时PTH的全身暴露量比人类服用100微克剂量时高4.6倍。PTH与PTH-1受体和假定的C端PTH受体相互作用并平衡其效应的能力,可能导致观察到的PTH致癌潜力低于先前报道的特立帕肽。
