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重组人骨形成蛋白-1对非人灵长类动物节段性缺损愈合的影响。

Effect of recombinant human osteogenic protein-1 on healing of segmental defects in non-human primates.

作者信息

Cook S D, Wolfe M W, Salkeld S L, Rueger D C

机构信息

Department of Orthopaedic Surgery, Tulane University School of Medicine, New Orleans, Louisiana 70112-2699, USA.

出版信息

J Bone Joint Surg Am. 1995 May;77(5):734-50. doi: 10.2106/00004623-199505000-00010.

Abstract

The effect of recombinant human osteogenic protein-1 on the healing of segmental bone defects was studied in twenty-eight African green monkeys (Cercopithecus aethiops). A 2.0-centimeter osteoperiosteal defect was created in the middle of the ulnar shaft in fourteen animals and in the diaphysis of the tibia in the other fourteen. The ulnar defect was filled with an implant consisting of 1000 micrograms of recombinant human osteogenic protein-1 in 400 milligrams of bovine bone-collagen carrier in six animals, with collagen carrier alone in two animals, and with autogenous cancellous bone graft from the contralateral tibia and femur in six animals. The tibial defect was filled with 250, 500 (two tibiae), 1000, or 2000 micrograms of recombinant human osteogenic protein-1 in 400 milligrams of collagen carrier in five animals, with collagen carrier alone in one animal, and with autogenous cancellous bone graft in six animals; in the two remaining animals (controls), the tibial defect was left unfilled. The tibial defects were stabilized with an intramedullary Steinmann pin. All animals were killed at twenty weeks postoperatively. Healing of the defects was evaluated with biweekly radiographs, with histological examination, and with mechanical testing. Radiographically, all of the defects that had been treated with recombinant human osteogenic protein-1 exhibited new-bone formation, but they differed in the degree of healing and remodeling. Five of the six ulnae treated with recombinant human osteogenic protein-1 and four of the five tibiae treated with this substance exhibited complete healing at six to eight weeks, with bridging of the defect by new bone first observed at four weeks. The two unhealed defects both exhibited new-bone formation but incomplete union, which precluded mechanical testing. No defect that had been filled with collagen carrier or that had been left unfilled exhibited any signs of healing or major new-bone formation. None of the six ulnae that had been filled with autogenous bone graft exhibited complete healing, compared with five of the six tibiae that had been so treated. Histological evaluation of the defects treated with recombinant human osteogenic protein-1 revealed the formation of new cortices with areas of woven and lamellar bone and normal-appearing marrow elements at twenty weeks postoperatively. The tibial defects that had been treated with autogenous bone graft had a similar appearance. All control ulnar and tibial defects and all ulnar defects that had been treated with autogenous bone graft had fibrous union with little new-bone formation.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在28只非洲绿猴(猕猴)中研究了重组人骨生成蛋白-1对节段性骨缺损愈合的影响。在14只动物的尺骨干中部制造了一个2.0厘米的骨膜骨缺损,在另外14只动物的胫骨干制造了骨缺损。在6只动物中,尺骨缺损填充了一种植入物,该植入物由1000微克重组人骨生成蛋白-1与400毫克牛骨胶原载体组成;2只动物填充胶原载体;6只动物填充来自对侧胫骨和股骨的自体松质骨移植。在5只动物中,胫骨缺损填充了250、500(两根胫骨)、1000或2000微克重组人骨生成蛋白-在400毫克胶原载体中;1只动物填充胶原载体;6只动物填充自体松质骨移植;在其余2只动物(对照组)中,胫骨缺损未填充。胫骨缺损用髓内斯氏针固定。所有动物在术后20周处死。通过每两周一次的X线片、组织学检查和力学测试评估缺损的愈合情况。X线片显示,所有用重组人骨生成蛋白-1治疗的缺损均有新骨形成,但愈合和重塑程度不同。用重组人骨生成蛋白-1治疗的6只尺骨中的5只和用该物质治疗的5只胫骨中的4只在6至8周时完全愈合,在4周时首次观察到新骨桥接缺损。2个未愈合的缺损均有新骨形成但未完全愈合,无法进行力学测试。填充胶原载体或未填充的缺损均未显示任何愈合迹象或大量新骨形成。与6只接受自体骨移植的胫骨中的5只相比,6只接受自体骨移植的尺骨均未完全愈合。术后20周,用重组人骨生成蛋白-1治疗的缺损的组织学评估显示有新皮质形成,有编织骨和板层骨区域以及外观正常骨髓成分。接受自体骨移植治疗的胫骨缺损有类似表现。所有对照尺骨和胫骨缺损以及所有接受自体骨移植治疗的尺骨缺损均为纤维性愈合,几乎没有新骨形成。(摘要截短至400字)

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