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在由储存的人类脐带血制成的细胞治疗产品中,促进髓鞘再生的基因产物上调。

Gene products promoting remyelination are up-regulated in a cell therapy product manufactured from banked human cord blood.

作者信息

Scotland Paula, Buntz Susan, Noeldner Pamela, Saha Arjun, Gentry Tracy, Kurtzberg Joanne, Balber Andrew E

机构信息

Robertson Clinical and Translational Cell Therapy Program, Duke Translational Medicine Institute, Duke University Medical Center, Durham, North Carolina, USA.

Robertson Clinical and Translational Cell Therapy Program, Duke Translational Medicine Institute, Duke University Medical Center, Durham, North Carolina, USA.

出版信息

Cytotherapy. 2017 Jun;19(6):771-782. doi: 10.1016/j.jcyt.2017.03.004. Epub 2017 Apr 5.

Abstract

BACKGROUND AIMS

DUOC-01, a cell product being developed to treat demyelinating conditions, is composed of macrophages that arise from CD14 monocytes in the mononuclear cell (MNC) population of banked cord blood (CB). This article demonstrates that expression of multiple gene products that promote remyelination is rapidly up-regulated during manufacturing of DUOC-01 from either MNC or purified CB CD14 monocytes.

METHODS

Cell cultures were initiated with MNC or with immunoselected CD14 monocytes isolated from the same CB unit. Cell products present in these cultures after 2 and 3 weeks were compared by three methods. First, quantitative polymerase chain reaction was used to compare expression of 77 transcripts previously shown to be differentially expressed by freshly isolated, uncultured CB CD14 monocytes and DUOC-01. Second, accumulation of 16 soluble proteins in the culture medium was measured by Bioplex methods. Third, whole transcriptomes of the cell products were compared by microarray analysis.

RESULTS

Key transcripts in multiple pathways that promote remyelination were up-regulated in DUOC-01, and substantial secretion of proteins corresponding to many of these transcripts was detected. Cell products manufactured from MNC or from CD14 monocytes were similar with regard to all metrics. Upregulation of gene products characteristic of DUOC-01 was largely completed within 14 days of culture.

CONCLUSION

We demonstrate that expression of multiple gene products that promote remyelination is up-regulated during the first 2 weeks of manufacturing of DUOC-01. Measuring these mechanistically important transcripts and proteins will be useful in monitoring manufacturing, evaluating manufacturing changes, and developing mechanism-based product potency assays.

摘要

背景目的

DUOC-01是一种正在研发用于治疗脱髓鞘疾病的细胞产品,由来自库存脐带血(CB)单核细胞(MNC)群体中CD14单核细胞产生的巨噬细胞组成。本文证明,在从MNC或纯化的CB CD14单核细胞生产DUOC-01的过程中,多种促进髓鞘再生的基因产物的表达迅速上调。

方法

用MNC或从同一CB单位分离的免疫选择的CD14单核细胞启动细胞培养。通过三种方法比较培养2周和3周后这些培养物中存在的细胞产物。第一,使用定量聚合酶链反应比较77种转录本的表达,这些转录本先前已显示在新鲜分离的、未培养的CB CD14单核细胞和DUOC-01中差异表达。第二,通过Bioplex方法测量培养基中16种可溶性蛋白质的积累。第三,通过微阵列分析比较细胞产物的全转录组。

结果

促进髓鞘再生的多个途径中的关键转录本在DUOC-01中上调,并检测到与许多这些转录本相对应的蛋白质的大量分泌。从MNC或CD14单核细胞制造的细胞产物在所有指标方面都相似。DUOC-特异性基因产物的上调在培养14天内基本完成。

结论

我们证明,在DUOC-01生产的前2周内,多种促进髓鞘再生的基因产物的表达上调。测量这些具有重要机制意义的转录本和蛋白质将有助于监测生产、评估生产变化以及开发基于机制的产品效价测定。 1的特征

请注意,原文最后一句“DUOC-特异性基因产物的上调在培养14天内基本完成。”中的“DUOC-特异性”表述可能有误,推测原文想表达的是“DUOC-01特异性”,译文已按照推测进行修正。你可根据实际情况进行调整。

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