间充质干细胞
生物
低温保存
免疫系统
免疫学
间质细胞
移植
促炎细胞因子
造血
体外
干细胞
川地34
男科
补体系统
细胞疗法
炎症
癌症研究
细胞生物学
医学
内科学
胚胎
生物化学
作者
Guido Moll,Jessica J. Alm,Lindsay C. Davies,Lena von Bahr,Nina Heldring,Lillemor Stenbeck-Funke,Osama A. Hamad,Robin Hinsch,Lech Ignatowicz,Matthew Locke,Helena Lönnies,John D. Lambris,Yuji Teramura,Kristina Nilsson‐Ekdahl,Bo Nilsson,Katarina Le Blanc
出处
期刊:Stem Cells
[Oxford University Press]
日期:2014-05-08
卷期号:32 (9): 2430-2442
被引量:405
摘要
We have recently reported that therapeutic mesenchymal stromal cells (MSCs) have low engraftment and trigger the instant blood mediated inflammatory reaction (IBMIR) after systemic delivery to patients, resulting in compromised cell function. In order to optimize the product, we compared the immunomodulatory, blood regulatory, and therapeutic properties of freeze-thawed and freshly harvested cells. We found that freeze-thawed MSCs, as opposed to cells harvested from continuous cultures, have impaired immunomodulatory and blood regulatory properties. Freeze-thawed MSCs demonstrated reduced responsiveness to proinflammatory stimuli, an impaired production of anti-inflammatory mediators, increased triggering of the IBMIR, and a strong activation of the complement cascade compared to fresh cells. This resulted in twice the efficiency in lysis of thawed MSCs after 1 hour of serum exposure. We found a 50% and 80% reduction in viable cells with freshly detached as opposed to thawed in vitro cells, indicating a small benefit for fresh cells. In evaluation of clinical response, we report a trend that fresh cells, and cells of low passage, demonstrate improved clinical outcome. Patients treated with freshly harvested cells in low passage had a 100% response rate, twice the response rate of 50% observed in a comparable group of patients treated with freeze-thawed cells at higher passage. We conclude that cryobanked MSCs have reduced immunomodulatory and blood regulatory properties directly after thawing, resulting in faster complement-mediated elimination after blood exposure. These changes seem to be paired by differences in therapeutic efficacy in treatment of immune ailments after hematopoietic stem cell transplantation.
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