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Stimulation of osteogenesis by means of sustained delivery of various natural androgenic hormones.

机译:通过持续输送各种天然雄激素来刺激成骨作用。

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Sex steroids play an essential role in the maintenance of bone health throughout life, and the mechanisms by which these effects are mediated in a subject of much controversy. Osteoblast cells appear to be stimulated by androgens in vitro, however their use in vivo is limited due to the virilizing side effects as well as alterations in the lipoprotein profiles. The use of targeted sustained release of anabolic steroids may stimulate fracture healing without untoward side effects. The specific aims were: (1) to compare fracture healing in a rat femoral defect model using tricalcium phosphate lysine (TCPL) drug delivery systems to deliver T, DHT and AED for long duration; (2) to quantify the level of steroid delivered from the system; and (3) to use bone histomorphometric techniques to analyze new bone formation at the defect site. A total of 125 adult male Sprague Dawley were obtained and acclimatized for two weeks in the animal care prior surgical procedures. All animals were kept on a 12-hour dayight cycle and were fed Purina rodent chow and water ad libitum. The animals were randomly divided into five equal groups (n = 25 per group). Group 1 animals were used as the intact control. Group 2-5 animals were placed under anesthesia and a standard approach was used to create a 6-mm defect using a dental burr in the midshaft of the femur. Group 2 animals were implanted with a sham TCPL delivery system adjacent to the defect. Animals in groups 3, 4, and 5 received a TCPL delivery system loaded with T, DHT, and AED, respectively. Animals were weighed, x-rayed, and blood samples were drawn on a weekly basis. The rats were sacrificed after 3, 6, 9 12 and 15 weeks and reproductive, vital organs, and fracture calluses were collected and analyzed. Morphometric analysis of the femurs revealed that the use of sustained delivery of DHT induced remarkable bone ingrowth compared to the sham and other experimental groups. All treated femurs appeared healthy and normal bone architecture was observed by the end of the 6 week phase. Measurements of the inner perimeter of the bone on the endosteal side showed significant reduction in the androgens treated animals. The quantitative findings confirms our preliminary studies and endorsing the previous data that the sustained delivery of T or its metabolite (DHT) can stimulate the osteoblastic activities in which eventually causes an increase in the cortical bone density.
机译:性类固醇在维持一生中的骨骼健康中起着至关重要的作用,而在引起争议的受试者中介导这些作用的机制也很重要。成骨细胞似乎在体外受到雄激素的刺激,但是由于其毒副作用以及脂蛋白谱的改变,其在体内的使用受到限制。合成代谢类固醇的靶向持续释放可以刺激骨折愈合,而不会产生不良副作用。具体目的是:(1)在大鼠股骨缺损模型中比较使用磷酸三赖氨酸(TCPL)药物递送系统长期递送T,DHT和AED的骨折愈合; (2)量化从系统中输送的类固醇水平; (3)使用骨组织形态计量学技术分析缺损部位的新骨形成。总共获得了125只成年雄性Sprague Dawley,并在手术前的动物护理中适应了两周。将所有动物维持在12小时的日/夜循环中,并随意喂食Purina啮齿动物食物和水。将动物随机分为五个相等的组(每组n = 25)。第1组动物用作完整对照。将第2-5组的动物置于麻醉下,并使用标准方法通过股骨中轴的牙钻产生6毫米的缺损。第2组动物在缺损处植入假TCPL递送系统。第3组,第4组和第5组的动物分别接受装有T,DHT和AED的TCPL递送系统。称重动物,进行X射线检查,每周抽血一次。 3、6、9、12和15周后处死大鼠,收集并分析生殖,重要器官和老茧。股骨的形态计量学分析显示,与假手术和其他实验组相比,持续递送DHT引起明显的骨向内生长。在第6周阶段结束时,所有接受治疗的股骨均看起来健康,并且骨骼结构正常。骨内膜侧骨内周的测量结果表明,雄激素治疗的动物明显减少。定量结果证实了我们的初步研究并支持先前的数据,即T或其代谢物(DHT)的持续输送可刺激成骨细胞活动,最终导致皮质骨密度增加。

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