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Short-term intermittent PTH 1–34 administration and bone marrow blood vessel ossification in Mature and Middle-Aged C57BL/6 mice

机译:成熟和中年C57BL / 6小鼠的短期间歇性PTH 1–34给药和骨髓血管骨化

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摘要

Intermittent parathyroid hormone (PTH) administration augments bone and progressive bone marrow blood vessel (BMBV) ossification occurs with advancing age. Since intermittent PTH administration augments bone, it may also serve to increase BMBV ossification. We assessed the influence of 5- and 10-days of intermittent PTH 1–34 administration on trabecular and cortical bone and BMBV ossification in mature (6–8 mon; n = 30) and middle-aged (10–12 mon; n = 30) male and female C57BL/6 mice. Mice were divided accordingly: control (CON) and 5-days (5dPTH) and 10-days (10dPTH) of PTH. Mice were given PBS (50 μl) or PTH 1–34 (43 μg/kg/d) for 5- and 10-consecutive days. Trabecular bone microarchitecture (i.e., BV/TV [%], Tb.Th [μm], Tb.N [/mm], and Tb.Sp [μm]) was assessed in the distal femoral metaphysis and cortical bone parameters (i.e., Ct.Th [μm] and CSMI [mm4]) at the femoral mid-shaft. BMBV ossification (i.e., ossified vessel volume [OsVV, %] and ossified vessel thickness [OsV.Th, μm]) was assessed in the medullary cavity of the femoral shaft. All parameters were determined by μCT. At this sample size, no gender-related differences were observed so female and male data were pooled. There were no main effects nor interactions for trabecular microarchitecture and Ct.Th. However, CSMI was larger (p < 0.05) in Middle-Age vs. Mature and larger (p < 0.05) in CON and 10dPTH vs. 5dPTH. OsVV tended (p = 0.057) to be higher (0.18 ± 0.04% vs. 0.09 ± 0.02%, respectively) and OsV.Th was higher (p < 0.05; 17.4 ± 1.6 μm vs. 12.1 ± 1.4 μm, respectively) in Middle-Aged vs. Mature mice. OsVV was not altered, but ossified vessels tended (p = 0.08) to be thicker in 10dPTH (17.6 ± 2.0 μm) vs. CON (12.5 ± 1.7 μm). No interactions were observed for OsVV and OsV.Th. In conclusion, this is the first report of ossified BMBV in C57BL/6 mice. The increased OsV.Th in Middle-Aged mice coincides with previous reports of increased OsVV in aged rats. The tendency of augmented OsV.Th in 10dPTH suggests that this treatment may ultimately impair the patency of bone marrow blood vessels.
机译:间歇性甲状旁腺激素(PTH)给药可增强骨骼,并且随着年龄的增长,进行性骨髓血管(BMBV)会发生骨化。由于间歇性PTH给药可增强骨骼,因此也可能会增加BMBV的骨化。我们评估了在成人(6-8个月; n = 30)和中年(10-12星期一; n = 30)雄性和雌性C57BL / 6小鼠。相应地将小鼠分为:对照(CON)和5天(5dPTH)和10天(10dPTH)。连续5天和10天给小鼠PBS(50μl)或PTH 1–34(43μg/ kg / d)。在股骨远端干meta端和骨皮质参数(即,BV / TV [%],Tb.Th [μm],Tb.N [/ mm]和Tb.Sp [μm])中评估骨小梁的微结构。 Ct.Th [μm]和CSMI [mm 4 ])在股骨中轴。在股骨干髓腔中评估BMBV骨化(即骨化血管体积[OsVV,%]和骨化血管厚度[OsV.Th,μm])。所有参数均通过μCT确定。在此样本量下,未观察到性别相关差异,因此汇总了男性和女性数据。小梁微结构和Ct.Th没有主要作用,也没有相互作用。然而,CSMI在中年期相对于成熟期较大(p <0.05),在CON和10dPTH与5dPTH中较大(p <0.05)。在中部,OsVV倾向于(p = 0.057)更高(分别为0.18±0.04%和0.09±0.02%)和OsV.Th较高(p <0.05; 17.4±1.6μm与12.1±1.4μm)。 -老年鼠与成熟鼠。 OsVV并未改变,但在10dPTH(17.6±2.0微米)中,骨化的血管趋于(p = 0.08)较CON(12.5±1.7微米)更厚。没有观察到OsVV和OsV的相互作用。总之,这是C57BL / 6小鼠骨化BMBV的首次报道。 OsV.Th在中年小鼠中的增加与以前的报告中在老年大鼠中OsVV的增加相吻合。 OsV.Th在10dPTH中升高的趋势表明,这种治疗可能最终损害骨髓血管的通畅性。

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