Direct reprogramming of terminally differentiated B cells into erythroid lineage

SadahiraK.; FukuchiY.; KunimonoH.; SakuraiM.; IkedaY.; OkamotoS.; NakajimaH.

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Direct reprogramming of terminally differentiated B cells into erythroid lineage

机译：将终末分化B细胞直接重编程为红系

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Hematopoietic progenitors have been shown to retain plasticity and switch lineages by appropriate stimuli. However, mature blood cells hardly showed such differentiation plasticity. In this paper, we tried to reprogram mature B cells into erythroid lineage by expressing various hematopoietic transcription factors. Among various factors, GATA-1, SCL together with CCAAT/enhancer binding protein (C/EBP) α turned out to be a minimal set of factors that efficiently reprogrammed terminally differentiated mature B cells into erythroid lineage, as evidenced by colony forming assays and erythroid-specific gene expressions. This study sets an avenue to generate autologous erythrocytes from peripheral B cells.

机译：造血祖细胞已显示可通过适当刺激保持可塑性并转换血统。但是，成熟的血细胞几乎没有表现出这种分化可塑性。在本文中，我们试图通过表达各种造血转录因子将成熟的B细胞重编程为类红细胞谱系。在各种因素中，GATA-1，SCL以及CCAAT /增强子结合蛋白（C / EBP）α成为有效地将最终分化的成熟B细胞重编程为红系谱系的最小因素，如集落形成试验和红系特异性基因表达。这项研究为从外周B细胞产生自体红细胞提供了一条途径。

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《FEBS letters.》 |2012年第20期|共8页
作者
SadahiraK.; FukuchiY.; KunimonoH.; SakuraiM.; IkedaY.; OkamotoS.; NakajimaH.;
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正文语种 eng
中图分类生物化学;
关键词
B cell; Erythroid; Lineage conversion; Reprogramming;

机译：B细胞;类红素;谱系转换;重编程;

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1. Direct reprogramming of terminally differentiated B cells into erythroid lineage [J] . SadahiraK., FukuchiY., KunimonoH., FEBS letters. . 2012,第20期

机译：将终末分化B细胞直接重编程为红系
2. Inhibition of Human Erythropoiesis during Inflammation Is Mediated By High Mobility Group Box Protein 1 (HMGB1) through Decreased Commitment of Hematopoietic Stem Cells to the Erythroid Lineage and By Increased Apoptosis of Terminally Differentiating Erythroblasts [J] . Dulmovits Brian M., Papoin Julien, Hale John, Blood: The Journal of the American Society of Hematology . 2016,第22期

机译：高迁移率族框蛋白1（HMGB1）通过减少造血干细胞对红系谱系的承诺和增加终末分化的成红细胞的凋亡来介导炎症过程中对人类红细胞生成的抑制作用
3. Inhibition of Human Erythropoiesis during Inflammation Is Mediated By High Mobility Group Box Protein 1 (HMGB1) through Decreased Commitment of Hematopoietic Stem Cells to the Erythroid Lineage and By Increased Apoptosis of Terminally Differentiating Erythroblasts [J] . Dulmovits Brian M., Papoin Julien, Hale John, Blood: The Journal of the American Society of Hematology . 2016,第22期

机译：高迁移率族框蛋白1（HMGB1）通过减少造血干细胞对红系谱系的承诺和增加终末分化的成红细胞的凋亡来介导炎症过程中对人类红细胞生成的抑制作用
4. Lineage potential, plasticity and environmental reprogramming of epithelial stem/progenitor cells [C] . Alessandro W. Amici, Fatai O. Onikoyi, Paola Bonfanti Biochemical Society Annual Symposium . 2014

机译：上皮茎/祖细胞的谱系潜力，可塑性和环境重新编程
5. Construction of an Xpo7 Protein Expression Plasmid and PCR Focused Array Studies of Cell Cycle Related Genes During Erythroid Terminal Differentiation. [D] . Maher, Varun. 2012

机译：Xpo7蛋白表达质粒的构建和类红细胞末端分化过程中细胞周期相关基因的PCR聚焦阵列研究。
6. Cellular Reprogramming toward the Erythroid Lineage [O] . Laura J. Norton, Alister P. W. Funnell, Richard C. M. Pearson, 2011

机译：对红系谱系进行细胞重编程
7. Direct reprogramming of terminally differentiated B cells into erythroid lineage [O] . Sadahira Ken, Fukuchi Yumi, Kunimono Hiroyoshi, 2012

机译：将终末分化B细胞直接重编程为红系谱系

Direct reprogramming of terminally differentiated B cells into erythroid lineage

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