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Protective effect of liposome-mediated glial cell line. derived neurotrophic factor gene transfer in vivo on motoneurons following spinal cord injury in rats
引用本文:鲁凯伍,陈哲宇,侯铁胜. Protective effect of liposome-mediated glial cell line. derived neurotrophic factor gene transfer in vivo on motoneurons following spinal cord injury in rats[J]. 中华创伤杂志(英文版), 2004, 7(5): 275-279
作者姓名:鲁凯伍  陈哲宇  侯铁胜
作者单位:Department of Orthopedic and Spine Surgery,Nanfang Hospital,First Military Medical University,Guangzhou 510515,China,Department of Orthopedic and Spine Surgery,Nanfang Hospital,First Military Medical University,Guangzhou 510515,China,Department of Orthopedic and Spine Surgery,Nanfang Hospital,First Military Medical University,Guangzhou 510515,China
基金项目:ThisworkwassupportedbyNationalNaturalScienceFoundationofChina (30 0 0 0 0 4 8)andtheNationalBasicResearchProgram (G 19990 5 4 0 0 0 )ofChina
摘    要:
IDepartmentofOrthopedicandSpineSurgery ,NanfangHospital,FirstMilitaryMedicalUniversity ,Guangzhou 5 10 5 15 ,China (LuKW ,ChenZYandHouTS) Correspondingauthor:Tel:86 2 0 6 136 0 0 4 6 ,E mail:lukaiwu @sohu .comThisworkwassupportedbyNationalNaturalScienceFoundationofChina (30 0 0 0 0 4 8)andtheNationalBasicResearchProgram (G 19990 5 4 0 0 0 )ofChina.nrecentyears ,substantialevidencehassuggestedthatearlyadministrationofexogenousneurotrophicfactors (NTFs)intoinjuredregioncanfacilit…

关 键 词:保护作用 脂质体 神经胶质细胞系统 神经营养 基因因素转移 体内作用 运动神经元 脊椎麻醉 老鼠 组织化学

Protective effect of liposome-mediated glial cell line-derived neurotrophic factor gene transfer in vivo on motoneurons following spinal cord injury in rats
LU Kai-wu ,CHEN Zhe-yu and HOU Tie-sheng. Protective effect of liposome-mediated glial cell line-derived neurotrophic factor gene transfer in vivo on motoneurons following spinal cord injury in rats[J]. Chinese journal of traumatology, 2004, 7(5): 275-279
Authors:LU Kai-wu   CHEN Zhe-yu  HOU Tie-sheng
Affiliation:Department of Orthopedic and Spine Surgery, Nanfang Hospital, First Military Medical University, Guangzhou 510515,China
Abstract:
OBJECTIVE: To investigate the effect of liposome-mediated glial cell line-derived neurotrophic factor (GDNF) gene transfer in vivo on spinal cord motoneurons after spinal cord injury (SCI) in adult rats. METHODS: Sixty male Sprague-Dawley rats were divided equally into two groups: GDNF group and control group. The SCI model was established according to the method of Nystrom, and then the DC-Chol liposomes and recombinant plasmid pEGFP-GDNF cDNA complexes were injected into the injured spinal cord. The expression of GDNF cDNA 1 week after injection was detected by RT-PCR and fluorescence microscope. We observed the remaining motoneurons in the anterior horn and the changes of cholinesterase (CHE) and acid phosphatase (ACP) activity using Nissl and enzyme histochemistry staining. The locomotion function of hind limbs of rats was evaluated using inclined plane test and BBB locomotor scale. RESULTS: RT-PCR and fluorescence observation confirmed the presence of expression of GDNF cDNA 1 week and 4 weeks after injection. At 1, 2, 4 weeks after SCI, the number of motoneurons in the anterior horn in GDNF group (20.4+/-3.2, 21.7+/-3.6, 22.5+/-3.4) was more than that in control group (16.8+/-2.8, 17.3+/-2.7, 18.2+/-3.2, P<0.05). At 1, 2 weeks after SCI, the mean gray of the CHE-stained spinal motoneurons in GDNF group (74.2+/-25.8, 98.7+/-31.6) was less than that in control group (98.5+/-32.2, 134.6+/-45.2, P<0.01), and the mean gray of ACP in GDNF group (84.5+/-32.6, 79.5+/-28.4) was more than that in control group (61.2+/-24.9, 52.6+/-19.9, P<0.01). The locomotion functional scales in GDNF group were higher than that in control group within 1 to 4 weeks after SCI (P<0.05). CONCLUSIONS: GDNF gene transfer in vivo can protect motoneurons from death and degeneration induced by incomplete spinal cord injury as well as enhance locomotion functional restoration of hind limbs. These results suggest that liposome-mediated delivery of GDNF cDNA might be a practical method for treating traumatic spinal cord injury.
Keywords:Spinal cord injury  Motor neurons  Liposome  Gene therapy
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