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间歇性与持续性给予甲状旁腺激素对骨骼及间充质干细胞的不同影响

[Differential effects on bone and mesenchymal stem cells caused by intermittent and continuous PTH administration].

作者信息

Zhang L X, Balani Y M, Trinh Sophia, Kronenberg Henry M, Mu Yiming

机构信息

Department of Endocrinology, Chinese PLA General Hospital, Beijing 100853, China.

出版信息

Zhonghua Yi Xue Za Zhi. 2018 Mar 13;98(10):781-787. doi: 10.3760/cma.j.issn.0376-2491.2018.10.014.

Abstract

To investigate the distinct effects of intermittent and continuous administration of parathyroid hormone (PTH) on bone and mesenchymal stem cell (MSC). Six weeks old mice with C57/BL6J background and SOX9-creERT/Td-tomato/Osteocalcin-GFP genotype were divided into 6 groups: intermittent administration and withdraw group (subcutaneous injection with PTH 500 μg·kg·d), continuous administration and withdraw group (subcutaneous implantation of PTH pump, 80 μg·kg·d with a rate of 0.25 μl/h), control administration and withdraw group, with 8 mice in each group. Serum calcium level and bone mineral density (BMD) were measured after two weeks' treatment and two weeks after drug withdraw. Histopathology and immunofluorescence analyses were performed to assess the effects of PTH on bone and mesenchymal stem cell. Serum calcium level increased transiently in intermittent group[(1.36±0.03) mmol/L]and increased gradually in continuous group[up to (2.33±0.03) mmol/L], but reduced to normal level (1.12-1.27 mmol/L) 14 days after drug withdraw. BMD of both intermittent[(0.047±0.002) g/cm]and continuous[(0.046±0.001) g/cm]PTH administration groups increased compared with control group[(0.044±0.001) g/cm], but there was no significant difference among three groups 2 weeks after drug withdraw. Femoral histopathology showed that bone mass, trabecular number and little fibrous tissue hyperplasia in intermittent PTH group increased. Osteoblasts number increased, but lining cells decreased. There was no significant difference in osteocyte and osteoclast numbers. After withdrawing of intermittent PTH, osteocyte and osteoblast number declined significantly, but there was an increased number of lining cells. Continuous PTH caused very high amount of fibrosis, and osteoclast number increased significantly, while osteoblast and osteocyte number increased slightly. After withdrawing of continuous PTH, fibrosis disappeared significantly, and lining cell number increased. Immunofluorescence staining in the epiphyseal-metaphyseal regions in fibula showed intermittent PTH increased undifferentiated Td-Tomato MSC, but declined significantly after withdrawing. Undifferentiated Td-Tomato MSC in continuous PTH increased slightly and decreased after drug withdraw. Intermittent PTH increased undifferentiated Td-Tomato MSC and osteoblast number, and might transform lining cell into osteocytes and osteoblasts, and thus lead to bone formation. Continuous PTH increased undifferentiated Td/Tomato MSC, osteoblast and osteocyte number slightly, but high amount of fibrosis and osteoclasts can be seen, leading to metabolic bone disease. However, lining cell ascended after drug withdraw, which may be beneficial to bone remodeling.

摘要

为研究甲状旁腺激素(PTH)间歇性给药和持续给药对骨骼及间充质干细胞(MSC)的不同影响。将6周龄、具有C57/BL6J背景和SOX9-creERT/Td-番茄/Osteocalcin-GFP基因型的小鼠分为6组:间歇性给药后停药组(皮下注射PTH 500 μg·kg·d)、持续给药后停药组(皮下植入PTH泵,80 μg·kg·d,速率为0.25 μl/h)、对照给药后停药组,每组8只小鼠。在治疗两周后及停药两周后测量血清钙水平和骨密度(BMD)。进行组织病理学和免疫荧光分析以评估PTH对骨骼和间充质干细胞的影响。间歇性给药组血清钙水平短暂升高[(1.36±0.03)mmol/L],持续给药组逐渐升高[最高达(2.33±0.03)mmol/L],但停药14天后降至正常水平(1.12 - 1.27 mmol/L)。间歇性[(0.047±0.002)g/cm]和持续[((0.046±0.001)g/cm]PTH给药组的BMD均高于对照组[(0.044±0.001)g/cm],但停药2周后三组之间无显著差异。股骨组织病理学显示,间歇性PTH组骨量、小梁数量增加,纤维组织增生较少。成骨细胞数量增加,但衬里细胞减少。骨细胞和破骨细胞数量无显著差异。间歇性PTH停药后,骨细胞和成骨细胞数量显著下降,但衬里细胞数量增加。持续PTH导致大量纤维化,破骨细胞数量显著增加,而成骨细胞和骨细胞数量略有增加。持续PTH停药后,纤维化明显消失,衬里细胞数量增加。腓骨骨骺-干骺端区域的免疫荧光染色显示,间歇性PTH增加了未分化的Td-番茄MSC,但停药后显著下降。持续PTH组未分化的Td-番茄MSC略有增加,停药后减少。间歇性PTH增加了未分化的Td-番茄MSC和成骨细胞数量,并可能将衬里细胞转化为骨细胞和成骨细胞,从而导致骨形成。持续PTH略微增加了未分化的Td/Tomato MSC、成骨细胞和骨细胞数量,但可见大量纤维化和破骨细胞,导致代谢性骨病。然而,停药后衬里细胞增加,这可能有利于骨重塑。

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