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骨髓干细胞与聚合物水凝胶——脊髓损伤修复的两种策略。

Bone marrow stem cells and polymer hydrogels--two strategies for spinal cord injury repair.

作者信息

Syková Eva, Jendelová Pavla, Urdzíková Lucia, Lesný Petr, Hejcl Ales

机构信息

Institute of Experimental Medicine ASCR, Videnská, 1083 142 20, Prague 4, Czech Republic.

出版信息

Cell Mol Neurobiol. 2006 Oct-Nov;26(7-8):1113-29. doi: 10.1007/s10571-006-9007-2. Epub 2006 Apr 22.

Abstract
  1. Emerging clinical studies of treating brain and spinal cord injury (SCI) led us to examine the effect of autologous adult stem cell transplantation as well as the use of polymer scaffolds in spinal cord regeneration. We compared an intravenous injection of mesenchymal stem cells (MSCs) or the injection of a freshly prepared mononuclear fraction of bone marrow cells (BMCs) on the treatment of an acute or chronic balloon-induced spinal cord compression lesion in rats. Based on our experimental studies, autologous BMC implantation has been used in a Phase I/II clinical trial in patients (n=20) with a transversal spinal cord lesion. 2. MSCs were isolated from rat bone marrow by their adherence to plastic, labeled with iron-oxide nanoparticles and expanded in vitro. Macroporous hydrogels based on derivatives of 2-hydroxyethyl methacrylate (HEMA) or 2-hydroxypropyl methacrylamide (HPMA) were prepared, then modified by their copolymerization with a hydrolytically degradable crosslinker, N,O-dimethacryloylhydroxylamine, or by different surface electric charges. Hydrogels or hydrogels seeded with MSCs were implanted into rats with hemisected spinal cords. 3. Lesioned animals grafted with MSCs or BMCs had smaller lesions 35 days postgrafting and higher scores in BBB testing than did control animals and also showed a faster recovery of sensitivity in their hind limbs using the plantar test. The functional improvement was more pronounced in MSC-treated rats. In MR images, the lesion populated by grafted cells appeared as a dark hypointense area and was considerably smaller than in control animals. Morphometric measurements showed an increase in the volume of spared white matter in cell-treated animals. In the clinical trial, we compared intraarterial (via a. vertebralis, n=6) versus intravenous administration of BMCs (n=14) in a group of subacute (10-33 days post-SCI, n=8) and chronic patients (2-18 months, n=12). For patient follow-up we used MEP, SEP, MRI, and the ASIA score. Our clinical study revealed that the implantation of BMCs into patients is safe, as there were no complications following cell administration. Partial improvement in the ASIA score and partial recovery of MEP or SEP have been observed in all subacute patients who received cells via a. vertebralis (n=4) and in one out of four subacute patients who received cells intravenously. Improvement was also found in one chronic patient who received cells via a. vertebralis. A much larger population of patients is needed before any conclusions can be drawn. The implantation of hydrogels into hemisected rat spinal cords showed that cellular ingrowth was most pronounced in copolymers of HEMA with a positive surface electric charge. Although most of the cells had the morphological properties of connective tissue elements, we found NF-160-positive axons invading all the implanted hydrogels from both the proximal and distal stumps. The biodegradable hydrogels degraded from the border that was in direct contact with the spinal cord tissue. They were resorbed by macrophages and replaced by newly formed tissue containing connective tissue elements, blood vessels, GFAP-positive astrocytic processes, and NF-160-positive neurofilaments. Additionally, we implanted hydrogels seeded with nanoparticle-labeled MSCs into hemisected rat spinal cords. Hydrogels seeded with MSCs were visible on MR images as hypointense areas, and subsequent Prussian blue histological staining confirmed positively stained cells within the hydrogels. 4. We conclude that treatment with different bone marrow cell populations had a positive effect on behavioral outcome and histopathological assessment after SCI in rats; this positive effect was most pronounced following MSC treatment. Our clinical study suggests a possible positive effect in patients with SCI. Bridging the lesion cavity can be an approach for further improving regeneration. Our preclinical studies showed that macroporous polymer hydrogels based on derivatives of HEMA or HPMA are suitable materials for bridging cavities after SCI; their chemical and physical properties can be modified to a specific use, and 3D implants seeded with different cell types may facilitate the ingrowth of axons.
摘要
  1. 新兴的脑和脊髓损伤(SCI)临床研究促使我们研究自体成体干细胞移植以及聚合物支架在脊髓再生中的作用。我们比较了静脉注射间充质干细胞(MSCs)或注射新鲜制备的骨髓细胞(BMCs)单核部分对大鼠急性或慢性球囊诱导脊髓压迫损伤的治疗效果。基于我们的实验研究,自体BMC植入已用于横贯性脊髓损伤患者(n = 20)的I/II期临床试验。2. 通过贴壁法从大鼠骨髓中分离MSCs,用氧化铁纳米颗粒标记并在体外扩增。制备了基于甲基丙烯酸2-羟乙酯(HEMA)或甲基丙烯酰胺2-羟丙酯(HPMA)衍生物的大孔水凝胶,然后通过与可水解降解的交联剂N,O-二甲基丙烯酰羟胺共聚或通过不同的表面电荷进行改性。将水凝胶或接种有MSCs的水凝胶植入脊髓半切的大鼠体内。3. 移植MSCs或BMCs的损伤动物在移植后35天损伤较小,BBB测试得分高于对照动物,并且使用足底试验显示后肢感觉恢复更快。功能改善在MSC治疗的大鼠中更为明显。在磁共振图像中,移植细胞填充的损伤表现为暗的低信号区,并且比对照动物中的损伤小得多。形态学测量显示细胞治疗动物中 spared白质体积增加。在临床试验中,我们比较了一组亚急性(SCI后10 - 33天,n = 8)和慢性患者(2 - 18个月,n = 12)中动脉内(通过椎动脉,n = 6)与静脉内给予BMCs(n = 14)的情况。对于患者随访,我们使用了运动诱发电位(MEP)、体感诱发电位(SEP)、磁共振成像(MRI)和美国脊髓损伤协会(ASIA)评分。我们的临床研究表明,将BMCs植入患者体内是安全的,因为细胞给药后没有并发症。在所有通过椎动脉接受细胞的亚急性患者(n = 4)以及四分之一通过静脉接受细胞的亚急性患者中观察到ASIA评分部分改善以及MEP或SEP部分恢复。在一名通过椎动脉接受细胞的慢性患者中也发现了改善。在得出任何结论之前,需要更多的患者群体。将水凝胶植入脊髓半切的大鼠体内表明,细胞向内生长在表面电荷为正的HEMA共聚物中最为明显。尽管大多数细胞具有结缔组织成分的形态学特性,但我们发现NF - 160阳性轴突从近端和远端残端侵入所有植入的水凝胶。可生物降解的水凝胶从与脊髓组织直接接触的边界开始降解。它们被巨噬细胞吸收并被含有结缔组织成分、血管、GFAP阳性星形胶质细胞突起和NF - 160阳性神经丝的新形成组织所取代。此外,我们将接种有纳米颗粒标记的MSCs的水凝胶植入脊髓半切的大鼠体内。接种有MSCs的水凝胶在磁共振图像上表现为低信号区,随后普鲁士蓝组织学染色证实水凝胶内有阳性染色的细胞。4. 我们得出结论,用不同的骨髓细胞群体进行治疗对大鼠SCI后的行为结果和组织病理学评估有积极影响;这种积极影响在MSC治疗后最为明显。我们的临床研究表明对SCI患者可能有积极影响。桥接损伤腔可能是进一步改善再生的一种方法。我们的临床前研究表明,基于HEMA或HPMA衍生物的大孔聚合物水凝胶是SCI后桥接腔隙的合适材料;它们的化学和物理性质可以根据特定用途进行修改,并且接种不同细胞类型的3D植入物可能促进轴突向内生长。

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