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IMPORTANCE OF CONTROLLED ICE FORMATION FOR EFFICIENT CELL BIOBANKING

机译:受控冰形成对于有效细胞发酵的重要性

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摘要

Effective long-term storage of rare and clinically relevant cells depends on the cell type and thus requires optimization of the main process parameters involved in cryopreservation. Among these parameters, the cooling and thawing rates, as well as the temperature of nucleation can be adjusted by a specific cryopreservation method. In this work, we reveal the optimal conditions for cryopreservation of human fibroblasts (HF), human pulmonary microvascular endothelial cells (HPMECs), amnion (aMSCs), and bone marrow stem cells (bMSCs) using an electro-freezing method and applying 2.5 %, 5 % or 10 % (v/v) dimethyl sulfoxide (Me2SO) as a cryoprotective agent. The optimal nucleation temperature for freezing of HF was −10 ℃ for a cooling rate of 1 K·min~(-1) and −7.5 ℃ for 5 K·min~(-1) using 5 % Me2SO. Application of a cooling rate of 5 K·min~(-1) and induction of the ice formation at −12 ℃ resulted in 90 % of viable HPMECs. The aMSCs and bMSCs reflected the highest viability of 75 % after freezing using a two-step freezing protocol utilizing a cooling rate of 7.5 K·min~(-1)down to −30 ℃ and 3 K·min~(-1) down to −80 ℃. The highest cell viability was observed while inducing the ice formation at −10 ℃ for both aMSCs and bMSCs.
机译:稀有和临床相关细胞的有效长期存储取决于细胞类型,因此需要优化冷冻保存中涉及的主要过程参数。在这些参数中,冷却和解冻速率以及成核温度可以通过特定的低温保存方法进行调节。在这项工作中,我们揭示了冷冻保存人成纤维细胞(HF),人肺微血管内皮细胞(HPMECs),羊膜(aMSCs)和骨髓干细胞(bMSCs)的最佳条件,采用的是电冻结方法并应用2.5% ,5%或10%(v / v)的二甲基亚砜(Me2SO)作为冷冻保护剂。使用5%Me2SO冷却HF的最佳成核温度为-10℃(冷却速率为1 K·min〜(-1))和-7.5℃(5 K·min〜(-1))。施加5 K·min〜(-1)的冷却速率和在-12℃诱导结冰,可产生90%的高效HPMEC。 aMSCs和bMSCs通过两步冷冻方案冷冻后的最高存活率达到75%,该过程采用7.5 K·min〜(-1)降至-30℃和3 K·min〜(-1)的冷却速率至-80℃。对于aMSCs和bMSCs,在-10℃诱导结冰时观察到最高的细胞活力。

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  • 会议地点 Dresden(DE)
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    Institute for Multiphase Processes, Leibniz Universität Hannover, Callinstrasse 36, Hannover, 30167, Germanylauterboeck@imp.uni-hannover.de;

    Institute for Multiphase Processes, Leibniz Universität Hannover, Callinstrasse 36, Hannover, 30167, Germany;

    Institute for Multiphase Processes, Leibniz Universität Hannover, Callinstrasse 36, Hannover, 30167, Germany;

    Institute for Multiphase Processes, Leibniz Universität Hannover, Callinstrasse 36, Hannover, 30167, Germany;

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