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人新生儿T细胞上CD45异构体的表达:激活后新生儿与成人T细胞上CD45异构体的表达及更新

CD45 isoform expression on human neonatal T cells: expression and turnover of CD45 isoforms on neonatal versus adult T cells after activation.

作者信息

Yamada A, Kaneyuki T, Hara A, Rothstein D M, Yokoyama M M

机构信息

Department of Immunology, Kurume University School of Medicine, Japan.

出版信息

Cell Immunol. 1992 Jun;142(1):114-24. doi: 10.1016/0008-8749(92)90273-r.

Abstract

Neonatal T cells are phenotypically similar to "naive" T cells from adult donors in the CD45 isoform expression. Despite the phenotypic similarity, large differences were found between neonatal and adult T cells when T cells were activated. After activation with PHA, adult CD45RA+ T cells began to express CD45RO and no loss of CD45RA expression had yet occurred at Day 3 post-stimulation. Three days after activation, CD45RA+ neonatal T cells also coexpressed CD45RO; however, in contrast to adult T cells, a marked loss of CD45RA was observed. We analyzed the rapid loss of CD45RA found in neonatal T cells. The de novo synthesis of CD45 isoforms in neonatal T cells was essentially the same as that in the adult T cells. Turnover of the CD45RA was very rapid in both resting adult and neonatal T cells. After activation with PHA, the turnover of CD45RA on adult T cells was decreased significantly, while the turnover of CD45RA on neonatal T cells was not changed after activation. Therefore, the regulation of CD45 isoform expression not only involves switches in alternative splicing, but also involves different regulation of turnover of these isoforms from the cell membrane.

摘要

新生儿T细胞在CD45异构体表达方面,其表型与成年供体的“初始”T细胞相似。尽管表型相似,但在激活T细胞时,发现新生儿和成年T细胞之间存在很大差异。用PHA激活后,成年CD45RA+ T细胞开始表达CD45RO,且在刺激后第3天尚未发生CD45RA表达的丢失。激活三天后,CD45RA+新生儿T细胞也共表达CD45RO;然而,与成年T细胞不同的是,观察到CD45RA明显丢失。我们分析了新生儿T细胞中发现的CD45RA的快速丢失情况。新生儿T细胞中CD45异构体的从头合成与成年T细胞基本相同。在静息的成年和新生儿T细胞中,CD45RA的周转都非常快。用PHA激活后,成年T细胞上CD45RA的周转显著降低,而新生儿T细胞上CD45RA的周转在激活后没有变化。因此,CD45异构体表达的调控不仅涉及可变剪接的转换,还涉及这些异构体从细胞膜周转的不同调控。

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