Mohammed Eman E A, El-Zawahry Mohamed, Farrag Abdel Razik H, Aziz Nahla N Abdel, Sharaf-ElDin Wessam, Abu-Shahba Nourhan, Mahmoud Marwa, Gaber Khaled, Ismail Taher, Mossaad Mohamed M, Aleem Alice K Abdel
Medical Molecular Genetics Department, Human Genetics and Genome Research Division, National Research Center, Cairo, Egypt.
Stem Cell Research Group, Medical Research Centre of Excellence, National Research Centre, Cairo, Egypt.
Open Access Maced J Med Sci. 2019 Feb 14;7(4):507-515. doi: 10.3889/oamjms.2019.124. eCollection 2019 Feb 28.
Cell therapies offer a promising potential in promoting bone regeneration. Stem cell therapy presents attractive care modality in treating degenerative conditions or tissue injuries. The rationale behind this is both the expansion potential of stem cells into a large cell population size and its differentiation abilities into a wide variety of tissue types, when given the proper stimuli. A progenitor stem cell is a promising source of cell therapy in regenerative medicine and bone tissue engineering.
This study aimed to compare the osteogenic differentiation and regenerative potentials of human mesenchymal stem cells derived from human bone marrow (hBM-MSCs) or amniotic fluid (hAF-MSCs), both and studies.
Human MSCs, used in this study, were successfully isolated from two human sources; the bone marrow (BM) and amniotic fluid (AF) collected at the gestational ages of second or third trimesters.
The stem cells derived from amniotic fluid seemed to be the most promising type of progenitor cells for clinical applications. In a pre-clinical experiment, attempting to explore the therapeutic application of MSCs in bone regeneration, Rat lumbar spines defects were surgically created and treated with undifferentiated and osteogenically differentiated MSCs, derived from BM and second trimester AF. Cells were loaded on gel-foam scaffolds, inserted and fixed in the area of the surgical defect. X-Ray radiography follows up, and histopathological analysis was done three-four months post- operation. The transplantation of AF-MSCs or BM-MSCs into induced bony defects showed promising results. The AF-MSCs are offering a better healing effect increasing the likelihood of achieving successful spinal fusion. Some bone changes were observed in rats transplanted with osteoblasts differentiated cells but not in rats transplanted with undifferentiated MSCs. Longer observational periods are required to evaluate a true bone formation. The findings of this study suggested that the different sources; hBM-MSCs or hAF-MSCs exhibited remarkably different signature regarding the cell morphology, proliferation capacity and osteogenic differentiation potential.
AF-MSCs have a better performance bone healing than that of BM-MSCs. Hence, AF derived MSCs is highly recommended as an alternative source to BM-MSCs in bone regeneration and spine fusion surgeries. Moreover, the usage of gel-foam as a scaffold proved as an efficient cell carrier that showed bio-compatibility with cells, bio-degradability and osteoinductivity .
细胞疗法在促进骨再生方面具有广阔的潜力。干细胞疗法为治疗退行性疾病或组织损伤提供了有吸引力的治疗方式。其背后的原理是,在给予适当刺激时,干细胞具有扩展为大量细胞群体的潜力以及分化为多种组织类型的能力。祖干细胞是再生医学和骨组织工程中有前景的细胞治疗来源。
本研究旨在比较源自人骨髓(hBM-MSCs)或羊水(hAF-MSCs)的人间充质干细胞的成骨分化和再生潜力,同时进行体内和体外研究。
本研究中使用的人间充质干细胞成功从两个人类来源分离;在妊娠中期或晚期收集的骨髓(BM)和羊水(AF)。
羊水来源的干细胞似乎是临床应用中最有前景的祖细胞类型。在一项临床前实验中,试图探索间充质干细胞在骨再生中的治疗应用,通过手术制造大鼠腰椎缺损,并用源自骨髓和妊娠中期羊水的未分化和成骨分化的间充质干细胞进行治疗。将细胞加载到凝胶泡沫支架上,插入并固定在手术缺损区域。术后进行X线摄影随访,并在三到四个月后进行组织病理学分析。将AF-MSCs或BM-MSCs移植到诱导的骨缺损中显示出有前景的结果。AF-MSCs提供了更好的愈合效果,增加了实现成功脊柱融合的可能性。在移植有成骨细胞分化细胞的大鼠中观察到一些骨变化,但在移植有未分化间充质干细胞的大鼠中未观察到。需要更长的观察期来评估真正的骨形成。本研究结果表明,不同来源;hBM-MSCs或hAF-MSCs在细胞形态、增殖能力和成骨分化潜力方面表现出明显不同的特征。
AF-MSCs在骨愈合方面的表现优于BM-MSCs。因此,强烈推荐将AF衍生性间充质干细胞作为骨再生和脊柱融合手术中BM-MSCs的替代来源。此外,使用凝胶泡沫作为支架被证明是一种有效的细胞载体,显示出与细胞的生物相容性、生物降解性和骨诱导性。
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