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Hyperbaric oxygen improves engraftment of ex-vivo expanded and gene transduced human CD34+ cells in a murine model of umbilical cord blood transplantation

机译:高压氧可改善脐带血移植鼠模型中离体扩增和基因转导的人CD34 +细胞的植入

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摘要

Delayed engraftment and graft failure represent major obstacles to successful umbilical cord blood (UCB) transplantation. Herein, we evaluated the use of hyperbaric oxygen (HBO) therapy as an intervention to improve human UCB stem/progenitor cell engraftment in an immune deficient mouse model. Six-to eight-week old NSG mice were sublethally irradiated 24 hours prior to CD34+ UCB cell transplant. Irradiated mice were separated into a non-HBO group (where mice remained under normoxic conditions) and the HBO group (where mice received two hours of HBO therapy; 100% oxygen at 2.5 atmospheres absolute). Four hours after completing HBO therapy, both groups intravenously received CD34+ UCB cells that were transduced with a lentivirus carrying luciferase gene and expanded for in vivo imaging. Mice were imaged and then sacrificed at one of 10 times up to 4.5 months post-transplant. HBO treated mice demonstrated significantly improved bone marrow, peripheral blood , and spleen (p=0.0293) retention and subsequent engraftment. In addition, HBO significantly improved peripheral, spleen and bone marrow engraftment of human myeloid and B-cell subsets. In vivo imaging demonstrated that HBO mice had significantly higher ventral and dorsal bioluminescence values. These studies suggest that HBO treatment of NSG mice prior to UCB CD34+ cell infusion significantly improves engraftment.
机译:延迟移植和移植失败是成功脐带血(UCB)移植的主要障碍。在本文中,我们评估了高压氧(HBO)治疗作为在免疫缺陷小鼠模型中改善人UCB干细胞/祖细胞植入的干预措施。在CD34 + UCB细胞移植前24小时,对6至8周大的NSG小鼠进行了致命的辐照。将受辐照的小鼠分为非HBO组(其中小鼠保持常氧条件)和HBO组(其中小鼠接受2小时的HBO治疗;在2.5个大气压下绝对100%的氧气)。在完成HBO治疗后四个小时,两组都静脉接受CD34 + UCB细胞,这些细胞用携带萤光素酶基因的慢病毒转导并扩增用于体内成像。对小鼠进行成像,然后在移植后最多4.5个月的10次中之一处死。经HBO处理的小鼠表现出显着改善的骨髓,外周血和脾脏(p = 0.0293)保留和随后的植入。此外,HBO显着改善了人类骨髓和B细胞亚群的外周,脾脏和骨髓移植。体内成像表明,HBO小鼠的腹侧和背侧生物发光值明显更高。这些研究表明,在输注UCB CD34 +细胞之前,HBO对NSG小鼠的治疗显着改善了植入。

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