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首页> 外文期刊>Canadian Journal of Veterinary Research >Long-term growth hormone-releasing factor administration on growth hormone, insulin-like growth factor-I concentrations, and bone healing in the Beagle.
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Long-term growth hormone-releasing factor administration on growth hormone, insulin-like growth factor-I concentrations, and bone healing in the Beagle.

机译:长期对Beagle进行生长激素释放因子,胰岛素样生长因子-I浓度和骨愈合的管理。

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Twelve 11 month old male Beagles were assigned to two treatment groups: a control group (saline) and a group receiving human growth hormone (GH)-releasing factor (hGRF) [1-29]NH2 (25 micrograms/kg, SC, TID). Treatment was started 6 days prior to surgery (day 1) and continued until necropsy (3 dogs per group/day) on d 29 or 58. Two porous polyethylene rods were surgically implanted on the lateral diaphysis of the femoral shaft and a 3 mm hole was drilled through the cortex between the two implants of each dog on day 1. Blood and urine were collected on d -6, 27 and 56. Human GRF injections produced a significant (P < 0.05) increase in GH release following each injection. An increase in GH response was also observed (P < 0.05) over time. The concentration of insulin-like growth factor-1 (IGF-1) increased for 5 weeks and then reached a plateau. None of the hematologic or urine measured parameters was affected by the treatment (P > 0.05). Albumin, calcium, and protein concentrations were higher (P < 0.05) on d 27 and 56 in GRF-treated animals. Histological sections of the onlay sites showed that bony ingrowth tended to be greater into the porous polyethylene material in GRF-treated animals than the controls at d 28 and 57, while no difference was observed in the degree of periosteal bone formation around the implants at either time period (P > 0.05). Bone formation into the cortical defect was greater in the GRF-treated dogs when compared to controls at day 57 only. In conclusion, chronic hGRF [1-29]NH2 treatment in Beagle dogs produced an increased GH response over time and increased IGF-1 concentrations. It also appeared to promote bony ingrowth into a porous polyethylene onlay and into a bony deficit.
机译:将十二只11个月大的雄性比格犬分为两个治疗组:对照组(盐水)和接受人生长激素(GH)释放因子(hGRF)[1-29] NH2(25微克/ kg,SC,TID)的组)。在手术前6天(第1天)开始治疗,并持续至第29或58天尸体剖检(每组每天3只狗)。将两根多孔聚乙烯棒通过外科手术植入股骨干的外侧骨干和3 mm的孔中在第1天在每只狗的两个植入物之间的皮质上钻孔。在第-6、27和56天收集血液和尿液。人GRF注射后每次注射产生的GH释放显着增加(P <0.05)。随着时间的推移,还观察到了GH反应的增加(P <0.05)。胰岛素样生长因子-1(IGF-1)的浓度持续5周,然后达到稳定水平。血液学或尿液测量参数均不受治疗影响(P> 0.05)。在接受GRF治疗的动物中,在第27和56天时白蛋白,钙和蛋白质的浓度较高(P <0.05)。覆盖部位的组织学切片显示,在第28和57天时,用GRF处理的动物中的骨向内生长的倾向大于对照组中的多孔聚乙烯材料,而在任一处植入物周围的骨膜骨形成程度均未观察到差异。时间段(P> 0.05)。与仅在第57天的对照组相比,经GRF治疗的狗中形成骨皮质缺损的骨更大。总之,在Beagle犬中进行慢性hGRF [1-29] NH2治疗会导致GH随时间推移而增加,IGF-1浓度也会增加。它也似乎促进骨向内生长成多孔的聚乙烯覆盖物和骨缺损。

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