首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >A block in both early T lymphocyte and natural killer cell development in transgenic mice with high-copy numbers of the human CD3E gene.
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A block in both early T lymphocyte and natural killer cell development in transgenic mice with high-copy numbers of the human CD3E gene.

机译:在具有高拷贝数的人CD3E基因的转基因小鼠中早期T淋巴细胞和自然杀伤细胞的发育均受阻。

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摘要

A severe immunodeficiency involving a complete loss of T lymphocytes and natural killer cells was observed in independent lines of transgenic mice containing > 30 copies of the human CD3E gene (pL12). T-cell- natural killer (NK)- mice could also be generated by using a gene fragment pL12 delta 1 (without exons 4A and 5) coding for the CD3-epsilon transmembrane region and its 55-amino acid nonenzymatic cytoplasmic tail. The abnormally small thymus gland in the homozygous transgenic animals, which was approximately 1% the size of a wild-type thymus, contained only a few (2-4%) prethymocytes with a Thy-1+Pgp-1+IL-2R alpha- CD3-4-8- phenotype. In mice with lower copy numbers of the transgene thymocyte development was blocked at the Thy-1+Pgp-1-IL-2R alpha+CD3-4-8- stage, and normal NK activity was detected. Mice generated with high-copy numbers of a transgene pL12 delta 2 (pL12 delta 1 minus exons 6), coding for a truncated protein from which the CD3-epsilon extracellular domain, its transmembrane region, and most of its cytoplasmic region were absent, contained normal numbers of T lymphocytes and NK cells. These transgene effects suggested that recruitment of signal-transduction molecules by the cytoplasmic tail of this protein played an important role in the abrogation of both lineages. Taken together these observations support the notion that T lymphocytes and NK cells stemmed from a common precursor.
机译:在包含> 30个人类CD3E基因(pL12)拷贝的转基因小鼠的独立品系中观察到严重的免疫缺陷,涉及T淋巴细胞和自然杀伤细胞的完全丧失。 T细胞自然杀手(NK)-小鼠也可以通过使用编码CD3-ε跨膜区及其55个氨基酸的非酶细胞质尾的基因片段pL12 delta 1(无外显子4A和5)生成。纯合转基因动物中的异常小胸腺,大约是野生型胸腺的1%,仅包含少数(2-4%)胸腺前体细胞,其中Thy-1 + Pgp-1 + IL-2R alpha -CD3-4-8-表型。在转基因拷贝数较低的小鼠中,胸腺细胞的发育在Thy-1 + Pgp-1-IL-2Rα+ CD3-4-8-期受阻,并且检测到正常的NK活性。含有高拷贝数的转基因pL12 delta 2(pL12 delta 1减去外显子6)产生的小鼠,该小鼠编码一种截短的蛋白,其中不存在CD3-ε胞外域,其跨膜区和大部分胞质区。正常数量的T淋巴细胞和NK细胞。这些转基因效应表明,该蛋白的细胞质尾部募集信号转导分子在两个谱系的废除中都起着重要作用。综上所述,这些观察结果支持了T淋巴细胞和NK细胞起源于共同的前体的观点。

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