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The transcription factor Gli3 promotes B cell development in fetal liver through repression of Shh

机译：转录因子Gli3通过抑制Shh促进胎儿肝脏B细胞发育

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摘要

Before birth, B cells develop in the fetal liver (FL). In this study, we show that Gli3 activity in the FL stroma is required for B cell development. In the Gli3-deficient FL, B cell development was reduced at multiple stages, whereas the Sonic hedgehog (Hh [Shh])–deficient FL showed increased B cell development, and Gli3 functioned to repress Shh transcription. Use of a transgenic Hh-reporter mouse showed that Shh signals directly to developing B cells and that Hh pathway activation was increased in developing B cells from Gli3-deficient FLs. RNA sequencing confirmed that Hh-mediated transcription is increased in B-lineage cells from Gli3-deficient FL and showed that these cells expressed reduced levels of B-lineage transcription factors and B cell receptor (BCR)/pre-BCR–signaling genes. Expression of the master regulators of B cell development Ebf1 and Pax5 was reduced in developing B cells from Gli3-deficient FL but increased in Shh-deficient FL, and in vitro Shh treatment or neutralization reduced or increased their expression, respectively.

机译：出生前，B细胞在胎儿肝脏（FL）中发育。在这项研究中，我们表明FL基质中的Gli3活性是B细胞发育所必需的。在缺乏Gli3的FL中，B细胞发育在多个阶段减少，而缺乏音速刺猬（Hh [Shh]）的FL显示出B细胞发育增加，而Gli3起到抑制Shh转录的作用。使用转基因Hh-reporter小鼠显示，Shh直接向发育中的B细胞发出信号，并且从缺乏Gli3的FL发育中的B细胞中，Hh途径的激活增加。 RNA测序证实，Hh介导的转录在Gli3缺陷型FL的B谱系细胞中增加，并显示这些细胞表达的B谱系转录因子和B细胞受体（BCR）/ BCR前信号基因水平降低。 B细胞发育的主要调节因子Ebf1和Pax5的表达在来自Gli3缺失的FL的发育中B细胞中降低，但在Shh缺失的FL中升高，并且体外Shh处理或中和分别降低或增加了它们的表达。

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Solanki Anisha; Lau Ching-In; Saldaña José Ignacio; Ross Susan; Crompton Tessa;
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专利

1. The transcription factor Gli3 promotes B cell development in fetal liver through repression of Shh [J] . Anisha Solanki, Ching-In Lau, José Ignacio Salda?a, The Journal of Experomental Medicine . 2017,第7期

机译：转录因子Gli3通过抑制Shh促进胎儿肝脏B细胞发育
2. Gli3 in fetal thymic epithelial cells promotes thymocyte positive selection and differentiation by repression of Shh [J] . Solanki Anisha, Yanez Diana C., Ross Susan, Development . 2018,第3期

机译：胎儿胸腺上皮细胞的Gli3促进胸腺细胞阳性选择和抑制Shh的分化
3. Hoxa3 and pax1 transcription factors regulate the ability of fetal thymic epithelial cells to promote thymocyte development. [J] . Su DM, Manley NR The Journal of Immunology: Official Journal of the American Association of Immunologists . 2000,第11期

机译：Hoxa3和pax1转录因子调节胎儿胸腺上皮细胞促进胸腺细胞发育的能力。
4. Effect of EMP on mice polydactylia and related genes expression (Gli3, Shh and Fgf4) during the development of mice limbs [C] . Chen Yongbin, Zhang Liyan, Guo Guozhen Asia-Pacific Conference on Environmental Electromagnetics (CEEM'2006) . 2006

机译：EMP对小鼠四肢发育过程中小鼠多乳及相关基因表达（Gli3，Shh和Fgf4）的影响
5. Retinoic acid-mediated regulation of GLI3 enables high yield motoneuron derivation from human embryonic stem cells independent of extrinsic activation of SHH signaling [D] . Calder, Elizabeth Lane 2015

机译：视黄酸介导的GLI3调控可独立于SHH信号的外在激活，从人胚胎干细胞中获得高产的运动神经元。
6. The transcription factor Gli3 promotes B cell development in fetal liver through repression of Shh [O] . Anisha Solanki, Ching-In Lau, José Ignacio Saldaña, 2017

机译：转录因子Gli3通过抑制Shh促进胎儿肝脏B细胞发育
7. In the fetal thymus, Gli3 in thymic epithelial cells promotes thymocyte positive selection and differentiation by repression of Shh [O] . Anisha Solanki, Diana C. Yanez, Susan Ross, 2018

机译：在胎儿胸腺中，在胸腺上皮细胞中GLI3促进胸腺细胞阳性选择和通过抑制SHH的分化

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