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首页> 外文期刊>Cytometry, Part A: the journal of the International Society for Analytical Cytology >Cryopreservation of canine cardiosphere-derived cells: Implications for clinical application
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Cryopreservation of canine cardiosphere-derived cells: Implications for clinical application

机译:Canine心脏影像孢子源细胞的冷冻保存:临床应用的影响

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The clinical application of cardiosphere-derived cells (CDCs) to treat cardiac disease has gained increasing interest over the past decade. Recent clinical trials confirm their regenerative capabilities, although much remains to be elucidated about their basic biology. To develop this new treatment modality, in a cost effective and standardized workflow, necessitates the creation of cryopreserved cell lines to facilitate access for cardiac patients requiring urgent therapy. Cryopreservation may however lead to alterations in cell behavior and potency. The aim of this study was to investigate the effect of cryopreservation on canine CDCs. CDCs and mesenchymal stem cells (MSCs) isolated from five dogs were characterized. CDCs demonstrated a population doubling time that was unchanged by cryopreservation (fresh vs. cryopreserved; 57.13 +/- 5.27 h vs. 48.94 +/- 9.55 h, P=0.71). This was slower than for MSCs (30.46 h, P0.05). The ability to form clones, self-renew, and commit to multiple lineages was unaffected by cryopreservation. Cryopreserved CDCs formed larger cardiospheres compared to fresh cells (P0.0001). Fresh CDCs showed a high proportion of CD105(+) (89.0%+/- 4.98) and CD44(+) (99.68%+/- 0.13) cells with varying proportions of CD90(+) (23.36%+/- 9.78), CD34(+) (7.18%+/- 4.03) and c-Kit(+) (13.17%+/- 8.67) cells. CD45(+) (0.015%+/- 0.005) and CD29(+) (2.92%+/- 2.46) populations were negligible. Increasing passage number of fresh CDCs correlated with an increase in the proportion of CD34(+) and a decrease in CD90(+) cells (P=0.003 and 0.03, respectively). Cryopreserved CDCs displayed increased CD34(+) (P0.001) and decreased CD90(+) cells (P=0.042) when compared to fresh cells. Overall, our study shows that cryopreservation of canine CDCs is feasible without altering their stem characteristics, thereby facilitating their utilization for clinical trials. (c) 2017 International Society for Advancement of Cytometry
机译:心脏源细胞(CDC)治疗心脏病的临床应用已经在过去十年中获得了越来越多的利益。最近的临床试验证实了他们的再生能力,虽然其基本生物学有很多仍有待措施。为了开发这种新的治疗方式,在成本效益和标准化的工作流程中,需要创建冷冻保存的细胞系,以便于进入需要紧急治疗的心脏患者。然而,冷冻保存可能导致细胞行为和效力的改变。本研究的目的是探讨冷冻保存对犬CDC的影响。特征在于从五只狗中分离的CDC和间充质干细胞(MSCs)。 CDCS展示了通过冷冻保存(新鲜与冷冻保存; 57.13 +/- 5.27小时,48.94 +/- 9.55,P = 0.71)的人口倍增时间。这比MSCs慢(30.46小时,P <0.05)慢。能够形成克隆,自我更新和提交多个谱系的能力不受冷冻保存的影响。与新鲜细胞相比(P <0.0001)相比,冷冻保存的CDCS形成较大的心肌。新鲜CDC表现出高比例的CD105(+)(89.0%+ / - 4.98)和CD44(+)(99.68%+ / - 0.13)细胞,其CD90(+)的不同比例(23.36%+ / - 9.78), CD34(+)(7.18%+ / - 4.03)和C-kit(+)(13.17%+ / - 8.67)细胞。 CD45(+)(0.015%+ / - 0.005)和CD29(+)(2.92%+ / - 2.46)群体可忽略不计。增加随着CD34(+)比例的增加和CD90(+)细胞的减少(分别为0.003和0.03)的增加,增加新鲜CDC的数量。与新鲜细胞相比,冷冻保存的CDCS显示CD34(+)(P <)(P <0.001)和降低CD90(+)细胞(P = 0.042)。总体而言,我们的研究表明,在不改变它们的茎特征的情况下,犬CDC的冷冻保存是可行的,从而促进它们对临床试验的利用率。 (c)2017年国际促进细胞计量学会

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