人脐带间充质干细胞治疗杜氏肌营养不良:印度的安全性和可行性研究。

Q4 Biochemistry, Genetics and Molecular Biology
Journal of Stem Cells Pub Date : 2015-01-01
B S Rajput, Swarup K Chakrabarti, Vaishali S Dongare, Christina M Ramirez, Kaushik D Deb
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引用次数: 0

摘要

目的:杜氏肌营养不良症(DMD)是一种以肌营养不良蛋白缺乏为特征的肌肉退行性疾病,目前尚无明确的治疗方法。废弃脐带是非免疫原性间充质干细胞的潜在来源,可用于同种异体移植。鉴于间充质干细胞(MSCs)的再生和抗炎特性,我们在这里研究了它在DMD患者细胞治疗中的作用。设计:这是一项在印度孟买、德里和勒克瑙的多家医院进行的单盲研究。纳入研究患者的标准是年龄在5 - 18岁之间的男孩,肌肉活检的免疫组化检查中没有肌营养不良蛋白,细胞遗传学分析中有肌营养不良蛋白基因突变。排除标准为肌肉活检中存在肌营养不良蛋白,患者使用皮质类固醇等。UC-MSCs(200万个/kg体重)通过静脉注射和IM注射给药。对11例UC-MSCs移植后的DMD患者的上肢近端、上肢远端、下肢近端、下肢远端、髋关节屈肌、髋关节伸肌、髋关节外展肌和棘旁肌的肌力进行了测量,随访时间长达3年(平均随访时间为1.5年)。5例DMD患者未接受UC-MSCs移植,作为对照组。结果:治疗组(基线时N = 11)上肢近端和远端肌肉移植前强度分别为3.45±1.0357和4.090±0.8312。1年后(N = 9),这些优势保持稳定,平均为3.78(1.03)和4.22(0.83)。对照组(N = 5)的上肢近端和远端移植前强度分别为3.6(0.54)和4(1)。1年后,(N = 5) 3/5的受试者上肢近端有轻微但无统计学意义的下降,平均3.0(1.0),5/5的受试者力量下降,平均3.0(1.0)。治疗组移植前下肢远端和近端肌肉强度分别为2.0909±0.8312和3.1181±0.8738。1年后(N = 9), 4/9的受试者下肢远端力量增加了1个单位(平均3.78(0.97)),8/9的受试者下肢近端力量增加了1个单位,平均3.11(1.05)。对照组下肢远端和近端基线平均值分别为3.41(0.54)和3.0(1.0)。1年后,3/5的受试者下肢远端和近端强度下降1个单位(平均2.8(0.45)),5/5的受试者下肢远端和近端强度下降1个单位,平均2.0(1.0)。与未治疗组相比,髋关节屈肌、髋关节伸肌、髋关节外展肌和棘旁肌的肌肉功能在一年内也实现了稳定。结论:UC-MSCs给药不仅导致肌肉力量的稳定,而且没有显示出GVHD或对患者的任何有害影响,因此与对照组相比,可能被认为是治疗DMD的安全选择,尽管需要进一步的更大规模的双盲研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Human Umbilical Cord Mesenchymal Stem Cells in the Treatment of Duchenne Muscular Dystrophy: Safety and Feasibility Study in India.

Objective: Duchenne muscular dystrophy (DMD) is a musculo-degenerative disease characterized by lack of dystrophin production with no definite cure available currently. Discarded umbilical cord is a potential source of mesenchymal stem cells which are non-immunogenic and can be used for transplantation in allogenic set ups. Given the regenerative and anti-inflammatory properties of mesenchymal stem cells (MSCs), here we investigated its role in the cellular therapy of DMD patients.

Design: This is a single-blinded study conducted in various hospitals of India situated in Mumbai, Delhi, and Lucknow. Inclusion criteria for enrolling the patients in the study were boys aged between 5 to 18 years, absence of dystrophin in the immunohistochemistry of muscle biopsy and mutation in dystrophin gene in cytogenetic analysis. The exclusion criteria were presence of dystrophin in the muscle biopsy, patients on corticosteroids etc. UC-MSCs (2 millions/kg body weight) were administered through IV and IM injection. Muscle power in muscles of proximal upper limb, distal upper limb, proximal lower limb, distal lower limb, hip flexors, hip extensors, hip abductors, and paraspinal muscles were measured in 11 DMD patients after UC-MSCs transplantation and were followed for up to 3 years (average follow up 1.5 years). 5 DMD patients did not receive any UC-MSCs transplantation and served as the control group.

Results: The treatment group (N = 11 at baseline) had a pretransplantation strength of 3.45 ± 1.0357 and 4.090 ± 0.8312 in muscles of proximal upper limb and distal upper limb respectively. After 1 year (N = 9) these strengths remained stable with an average of 3.78 (1.03) and 4.22 (0.83). In contrast, the control group (N = 5) has a pre-transplantation strength of 3.6 (0.54) and 4 (1) in the proximal and distal upper limb respectively. After 1 year, (N = 5) 3/5 subjects had a slight but not statistically significant decrease in the proximal upper limb, mean 3.0 (1.0) and 5/5 had a lunit decrease in strength, mean 3.0 (1.0). The treatment group had a pre-transplantation strength of 2.0909 ± 0.8312 and 3.1181 ± 0.8738 in muscles of distal and proximal lower limbs respectively. At 1 year (N = 9), 4/9 subjects had a 1 unit increase in strength in the distal lower limb (mean 3.78 (0.97)) and 8/9 subjects had a lunit increase in strength in the proximal lower limb, mean 3.11 (1.05). The control group has a mean of 3.41 (0.54) and 3.0 (1.0) at baseline in the distal and proximal lower limb respectively. By 1 year, 3/5 subjects had a 1 unit decrease (mean 2.8 (0.45)) and 5/5 had a lunit decrease, mean 2.0 (1.0) in distal and proximal lower limb strength. Stability in muscle function was also achieved in muscles of hip flexors, hip extensors, hip abductors, and paraspinal muscles at one year as compared to untreated group.

Conclusion: UC-MSCs administration not only resulted in the stabilization of muscle power but also did not show GVHD or any deleterious effects on the patients and thus may be considered as safe option for treatment of DMD as compared to control untreated group although further larger double-blinded studies are needed.

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来源期刊
Journal of Stem Cells
Journal of Stem Cells Medicine-Transplantation
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