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帕米膦酸盐对成骨不全患儿的骨内在材料特性没有不利影响。

Pamidronate does not adversely affect bone intrinsic material properties in children with osteogenesis imperfecta.

作者信息

Weber Markus, Roschger Paul, Fratzl-Zelman Nadja, Schöberl Thomas, Rauch Frank, Glorieux Francis H, Fratzl Peter, Klaushofer Klaus

机构信息

Ludwig Boltzmann Institute of Osteology at the Hanusch Hospital of WGKK and AUVA Trauma Centre Meidling, 4th Med. Dept., Hanusch Hospital, Heinrich Collin Str. 30, A-1140 Vienna, Austria.

出版信息

Bone. 2006 Sep;39(3):616-22. doi: 10.1016/j.bone.2006.02.071. Epub 2006 Apr 27.

Abstract

Cyclical intravenous pamidronate therapy increases bone mass in children with osteogenesis imperfecta (OI), but the effect on the intrinsic material properties of bone is unknown at present. Thus, a possible influence of pamidronate treatment on bone quality at the material level might negate the beneficial effects of the gain in bone mass and lead to bone fragility in the long term. In the present study, we used transiliac bone biopsy samples and assessed the intrinsic material properties of the bone tissue at the micron-level by combined backscattered electron imaging and nanoindentation. Paired iliac bone samples from 14 patients (age 3 to 17 years) with severe OI before and after 2.5 +/- 0.5 years (mean +/- SD) of pamidronate treatment as well as age-matched controls were examined. Bone histomorphometry was performed in all samples and confirmed an increase of bone mass in treated patients. Backscattered electron imaging was used to measure the weighted mean calcium content (Ca(Mean)), the most frequent calcium content (Ca(Peak)), the variation in mineralization (Ca(Width)) and the amount of lowly mineralized areas (Ca(Low)) that correspond to sites of primary mineralization. Nanoindentation was performed in a subgroup of 6 patients and 6 controls to determine hardness and elastic modulus. Compared to controls, untreated OI patients had a significantly higher degree of bone matrix mineralization (Ca(Peak) +7%, P < 0.001) and a strong reduction of Ca(Low) (-38%, P < 0.001) despite enhanced bone formation, as well as increased hardness (+21%, P < 0.01) and elastic modulus (+13%, P < 0.01). However, none of these parameters was significantly altered by the subsequent pamidronate treatment. This shows that OI bone is stiffer and more mineralized and that, despite the enhanced bone formation rate in these patients, areas of primary mineralization are hardly visible. We also conclude that pamidronate treatment in children with OI does not have an adverse effect on the intrinsic material properties of bone and, as a consequence, that a long-term administration of the drug might not increase brittleness and fragility of the bone matrix. The antifracture effectiveness of pamidronate treatment in OI, as shown in previous clinical studies, has to be explained by the increase of mainly cortical bone volume.

摘要

周期性静脉注射帕米膦酸盐治疗可增加成骨不全(OI)患儿的骨量,但目前对骨的内在材料特性的影响尚不清楚。因此,帕米膦酸盐治疗在材料水平上对骨质量的可能影响可能会抵消骨量增加的有益效果,并长期导致骨脆性增加。在本研究中,我们使用了经髂骨活检样本,并通过背散射电子成像和纳米压痕相结合的方法在微米水平评估了骨组织的内在材料特性。对14例(年龄3至17岁)严重OI患者在接受2.5±0.5年(平均±标准差)帕米膦酸盐治疗前后的配对髂骨样本以及年龄匹配的对照组进行了检查。对所有样本进行了骨组织形态计量学分析,并证实治疗患者的骨量增加。背散射电子成像用于测量加权平均钙含量(Ca(Mean))、最常见钙含量(Ca(Peak))、矿化变化(Ca(Width))以及对应于初级矿化部位的低矿化区域的量(Ca(Low))。对6例患者和6例对照组的亚组进行了纳米压痕试验,以确定硬度和弹性模量。与对照组相比,未经治疗的OI患者尽管骨形成增强,但骨基质矿化程度显著更高(Ca(Peak) +7%,P < 0.001),Ca(Low)显著降低(-38%,P < 0.001),硬度增加(+21%,P < 0.01),弹性模量增加(+13%,P < 0.01)。然而,随后的帕米膦酸盐治疗并未使这些参数中的任何一个发生显著改变。这表明OI骨更硬且矿化程度更高,并且尽管这些患者的骨形成率增强,但初级矿化区域几乎不可见。我们还得出结论,OI患儿的帕米膦酸盐治疗对骨的内在材料特性没有不利影响,因此,长期使用该药物可能不会增加骨基质的脆性和易碎性。如先前临床研究所示,帕米膦酸盐治疗在OI中的抗骨折有效性必须通过主要皮质骨体积的增加来解释。

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