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人胸腺胎儿发育过程中CD44分子及其配体的表达:CD44亚型的表达受发育调控。

Expression of CD44 molecules and CD44 ligands during human thymic fetal development: expression of CD44 isoforms is developmentally regulated.

作者信息

Patel D D, Hale L P, Whichard L P, Radcliff G, Mackay C R, Haynes B F

机构信息

Department of Medicine, Duke University Medical Center, Durham, NC 27710, USA.

出版信息

Int Immunol. 1995 Feb;7(2):277-86. doi: 10.1093/intimm/7.2.277.

Abstract

It has recently been recognized that CD44 comprises a large family of alternatively spliced forms. In the thymus, CD44 has been postulated to play an important role in immature T cell migration and maturation. In this paper, we have studied the expression of CD44 molecules and two CD44 ligands, hyaluronan (HA) and fibronectin (FN), during human thymic fetal development. We found that mAbs against all CD44 isoforms (A3D8 or A1G3) reacted with both thymic epithelial (TE) cells and thymocytes beginning at the time of initial colonization of the human thymus by hematopoietic stem cells at 8.2 weeks of fetal gestation. However, mAbs specific for splice variants of CD44 containing membrane-proximal inserts (11.24, 11.10 and 11.9) reacted only with terminally differentiated TE cells in and around Hassall's bodies beginning at 16-19 weeks of fetal gestation. Studies of differentiated versus undifferentiated TE cells in vitro confirmed the selective expression of CD44 variant isoforms on terminally differentiated TE cells. Expression of HA and FN was determined by fluorescence microscopy using either biotinylated-HA binding protein or an anti-FN mAb. We found that whereas FN was present throughout the human fetal thymus beginning at 8.2 weeks, HA was not present until 16 weeks of gestational age. These data demonstrate the differential expression of standard versus variant CD44 isoforms during thymic ontogeny and implicate CD44 interactions with ligands other than HA as important in the earlier stages of human thymus development.

摘要

最近人们认识到,CD44由大量可变剪接形式组成的大家族。在胸腺中,CD44被认为在未成熟T细胞迁移和成熟过程中发挥重要作用。在本文中,我们研究了人胎儿胸腺发育过程中CD44分子以及两种CD44配体,即透明质酸(HA)和纤连蛋白(FN)的表达情况。我们发现,针对所有CD44异构体的单克隆抗体(A3D8或A1G3)在胎儿妊娠8.2周造血干细胞首次定植于人胸腺时,就与胸腺上皮(TE)细胞和胸腺细胞发生反应。然而,针对含有膜近端插入片段的CD44剪接变体(11.24、11.10和11.9)的单克隆抗体,从胎儿妊娠16 - 19周开始,仅与哈氏小体及其周围的终末分化TE细胞发生反应。体外对分化和未分化TE细胞的研究证实了CD44变体异构体在终末分化TE细胞上的选择性表达。HA和FN的表达通过使用生物素化HA结合蛋白或抗FN单克隆抗体的荧光显微镜进行测定。我们发现,虽然FN在胎儿妊娠8.2周时就存在于整个人类胎儿胸腺中,但HA直到妊娠16周才出现。这些数据表明,在胸腺个体发育过程中标准型与变体型CD44异构体存在差异表达,并暗示CD44与HA以外的配体的相互作用在人类胸腺发育的早期阶段很重要。

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