在动物模型中，通过逆转录病毒递送头蛋白可抑制由骨形态发生蛋白-4、脱矿骨基质和创伤诱导的异位骨化的形成。

Hannallah David, Peng Hairong, Young Brett, Usas Arvydas, Gearhart Brian, Huard Johnny

Department of Orthopaedic Surgery, University of Pittsburgh, PA 15213-2582, USA.

J Bone Joint Surg Am. 2004 Jan;86(1):80-91. doi: 10.2106/00004623-200401000-00013.

BACKGROUND

The heterotopic ossification of muscles, tendons, and ligaments is a common problem faced by orthopaedic surgeons. We investigated the ability of Noggin (a BMP [bone morphogenetic protein] antagonist) to inhibit heterotopic ossification.

METHODS

Part 1: A retroviral vector carrying the gene encoding human Noggin was developed and used to transduce muscle-derived stem cells. Part 2: Cells transduced with BMP-4 were implanted into both hind limbs of mice along with either an equal number, twice the number, or three times the number of Noggin-expressing muscle-derived stem cells (treated limb) or with nontransduced muscle-derived stem cells (control limb). At four weeks, the mice were killed and radiographs were made to look for evidence of heterotopic ossification. Part 3: Eighty milligrams of human demineralized bone matrix was implanted into the hind limbs of SCID (severe combined immunodeficiency strain) mice along with 100,000, 500,000, or 1,000,000 Noggin-expressing muscle-derived stem cells (treated limbs) or nontransduced muscle-derived stem cells (control limbs). At eight weeks, the mice were killed and radiographs were made. Part 4: Immunocompetent mice underwent bilateral Achilles tenotomy along with the implantation of 1,000,000 Noggin-expressing muscle-derived stem cells (treated limbs) or nontransduced muscle-derived stem cells (control limbs). At ten weeks, the mice were killed and radiographs were made.

RESULTS

Part 1: An in vitro BMP inhibition assay demonstrated that Noggin was expressed by muscle-derived stem cells at a level of 280 ng per million cells per twenty-four hours. Part 2: Three varying doses of Noggin-expressing muscle-derived stem cells inhibited the heterotopic ossification elicited by BMP-4-expressing muscle-derived stem cells. Heterotopic ossification was reduced in a dose-dependent manner by 53%, 74%, and 99%, respectively (p < 0.05). Part 3: Each of three varying doses of Noggin-expressing muscle-derived stem cells significantly inhibited the heterotopic ossification elicited by demineralized bone matrix. Heterotopic ossification was reduced by 91%, 99%, and 99%, respectively (p < 0.05). Part 4: All eleven animals that underwent Achilles tenotomy developed heterotopic ossification at the site of the injury in the control limbs. In contrast, the limbs treated with the Noggin-expressing muscle-derived stem cells had a reduction in the formation of heterotopic ossification of 83% and eight of the eleven animals had no radiographic evidence of heterotopic ossification (p < 0.05).

CONCLUSIONS

The delivery of Noggin mediated by muscle-derived stem cells can inhibit heterotopic ossification caused by BMP-4, demineralized bone matrix, and trauma in an animal model.

CLINICAL RELEVANCE

Gene therapy to deliver Noggin may become a powerful method to inhibit heterotopic ossification in targeted areas of the body.

背景

肌肉、肌腱和韧带的异位骨化是骨科医生面临的常见问题。我们研究了Noggin（一种骨形态发生蛋白[BMP]拮抗剂）抑制异位骨化的能力。

方法

第1部分：构建携带编码人Noggin基因的逆转录病毒载体，并用于转导肌肉来源的干细胞。第2部分：将用BMP-4转导的细胞与等量、两倍数量或三倍数量的表达Noggin的肌肉来源干细胞（处理组肢体）或未转导的肌肉来源干细胞（对照组肢体）一起植入小鼠的双后肢。四周时，处死小鼠并拍摄X线片以寻找异位骨化的证据。第3部分：将80毫克人脱矿骨基质与100,000、500,000或1,000,000个表达Noggin的肌肉来源干细胞（处理组肢体）或未转导的肌肉来源干细胞（对照组肢体）一起植入严重联合免疫缺陷（SCID）小鼠的后肢。八周时，处死小鼠并拍摄X线片。第4部分：对具有免疫活性的小鼠进行双侧跟腱切断术，并植入1,000,000个表达Noggin的肌肉来源干细胞（处理组肢体）或未转导的肌肉来源干细胞（对照组肢体）。十周时，处死小鼠并拍摄X线片。

结果

第1部分：体外BMP抑制试验表明，肌肉来源的干细胞表达Noggin的水平为每百万细胞每24小时280纳克。第2部分：三种不同剂量的表达Noggin的肌肉来源干细胞抑制了由表达BMP-4的肌肉来源干细胞引起的异位骨化。异位骨化分别以剂量依赖的方式减少了53%、74%和99%（p<0.05）。第3部分：三种不同剂量的表达Noggin的肌肉来源干细胞中的每一种都显著抑制了由脱矿骨基质引起的异位骨化。异位骨化分别减少了91%、99%和99%（p<0.05）。第4部分：所有11只接受跟腱切断术的动物在对照组肢体的损伤部位均发生了异位骨化。相比之下，用表达Noggin的肌肉来源干细胞处理的肢体异位骨化形成减少了83%，11只动物中有8只没有异位骨化的X线证据（p<0.05）。

结论

在动物模型中，由肌肉来源干细胞介导的Noggin递送可抑制由BMP-4、脱矿骨基质和创伤引起的异位骨化。

临床意义

递送Noggin的基因治疗可能成为抑制身体靶向区域异位骨化的有力方法。

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