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Optimization of Targeted Cell Replacement Therapy: A New Approach for Lung Disease

机译:靶向细胞替代疗法的优化:肺疾病的一种新方法

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摘要

Cell replacement therapy is a promising approach for treatment of lung disease such as cystic fibrosis, although rates of engraftment need to be improved. We previously showed improved cell retention in the lung using transtracheal delivery compared to intravenous injection. Here, we optimized other parameters of cell delivery using 7-day cultured bone marrow cells (BMCs). Retention of BMC in the lung was dose-dependent. Naphthalene treatment had maximal effects on BMC retention when given 2 days before cell delivery. Naphthalene treatment of the donor amplified a CCSP+ population and increased retention efficiency in the recipient. Repeated naphthalene treatment and repeated cell delivery both resulted in greater retention. The contribution of the second cell dose was minimal suggesting that a second delivery of BMC promotes proliferation of the first. Busulfan-induced myelosuppression augmented retention of exogenous BMC by up to 20-fold. These BMC helped CCSP reconstitution. Using the optimal delivery techniques and cytokeratin-18-driven green fluorescent protein (GFP) reporter mice, we detected threefold more GFP suggesting more BMC differentiated to epithelial cells. We propose that improved engraftment in the lung will increase cell replacement and thus be a more efficient therapeutic approach for various lung diseases.
机译:尽管需要提高植入率,但是细胞替代疗法是治疗诸如囊性纤维化等肺部疾病的有前途的方法。与静脉注射相比,我们以前显示了通过气管递送改善了肺中的细胞保留。在这里,我们使用7天培养的骨髓细胞(BMC)优化了细胞递送的其他参数。肺中BMC的保留是剂量依赖性的。在细胞递送前2天给予萘治疗,对BMC的保留作用最大。供体的萘处理扩增了CCSP + 种群,并提高了受体的保留效率。重复的萘处理和重复的细胞递送均导致更大的保留。第二细胞剂量的贡献极小,表明第二次BMC传递促进了第一细胞的增殖。白消安诱导的骨髓抑制使外源BMC的保留增加了20倍。这些BMC帮助CCSP重组。使用最佳的传递技术和细胞角蛋白18驱动的绿色荧光蛋白(GFP)报告基因小鼠,我们检测到GFP的三倍多,表明更多的BMC分化为上皮细胞。我们建议改善肺部植入,将增加细胞置换,因此是治疗各种肺部疾病的更有效方法。

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