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人类胸腺微环境:胸腺上皮含有与表皮角质形成细胞成熟早期和晚期相关的特定角蛋白。

The human thymic microenvironment: thymic epithelium contains specific keratins associated with early and late stages of epidermal keratinocyte maturation.

作者信息

Laster A J, Itoh T, Palker T J, Haynes B F

出版信息

Differentiation. 1986;31(1):67-77. doi: 10.1111/j.1432-0436.1986.tb00385.x.

Abstract

Normal T-cell development is dependent on interactions with the thymic microenvironment; thymic epithelial cells are thought to play a key role in the induction of thymocyte maturation, both through direct contact and, indirectly, via thymic hormone secretion. It has been postulated that thymic epithelial cells progress through an antigenically defined pathway of differentiation similar to that of epidermal keratinocytes. As keratins vary according to epithelial cell type and the stage of epithelial cell maturation, we used a panel of monoclonal antibodies against keratins to study specific types of keratin intermediate filaments within human thymic epithelium. The demonstration in human thymus of keratins previously shown to be associated with distinct stages of epidermal keratinocytic maturation would support the hypothesis that thymic epithelial cells undergo sequential stages of differentiation. Two-dimensional immunoblot analysis of cytoskeletal extracts from human thymus revealed that thymic epithelium contains the following keratins: 1-2, 5, 6, 7, 8, 10, 13, 14, 15, 16, and 17 (molecular masses, 65-67, 58, 56, 54, 52, 56.5, 51, 50, 50', 48, and 46 kilodaltons, respectively). Thus, in thymic epithelium, we found keratins previously observed in epidermal basal cells (5, 14, 15), as well as keratins specific for terminally differentiated keratinocytes in supra-basal epidermis (1-2, 10). Indirect immunofluorescence (IF) performed on fetal and postnatal human thymus demonstrated that keratin epitopes recognized by antibodies AE-3, 35 beta H11, and RTE-23 are present on epithelial cells of the subcapsular cortex, the cortex, the medulla, and Hassall's bodies. In contrast, antibodies AE-1 and RTE-22 reacted primarily with neuroendocrine thymic epithelium (subcapsular cortex, medulla, Hassall's bodies). The epithelial reactivity of antibody AE-2 was limited to epithelial cells in Hassall's bodies and did not appear until 16 weeks of fetal gestation i.e., when Hassall's bodies first formed. Two-dimensional gel analysis of thymic keratins demonstrated that antibody AE-2 identified only the keratins with molecular masses of 56.6 and 65-67 kilodaltons (10 and 1-2 respectively) in thymus. These data, together with the selective reactivity of AE-2 with Hassall's bodies in fluorescence assays, demonstrate the localization in Hassall's bodies of the high-molecular-weight keratins associated with the late stages of epidermal cell maturation. In summary, we demonstrated that human thymic epithelium contains specific keratins found in multiple epithelial types as well as keratins associated with both early and late stages of epidermal cell differentiation.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

正常T细胞的发育依赖于与胸腺微环境的相互作用;胸腺上皮细胞被认为在诱导胸腺细胞成熟过程中起关键作用,这一过程既通过直接接触,也通过分泌胸腺激素间接实现。据推测,胸腺上皮细胞通过一条抗原定义的分化途径发育,这一途径类似于表皮角质形成细胞的分化途径。由于角蛋白根据上皮细胞类型和上皮细胞成熟阶段的不同而有所差异,我们使用一组抗角蛋白的单克隆抗体来研究人胸腺上皮内特定类型的角蛋白中间丝。在人胸腺中证实存在先前已表明与表皮角质形成细胞不同成熟阶段相关的角蛋白,将支持胸腺上皮细胞经历连续分化阶段这一假说。对人胸腺细胞骨架提取物进行的二维免疫印迹分析显示,胸腺上皮含有以下角蛋白:1 - 2、5、6、7、8、10、13、14、15、16和17(分子量分别为65 - 67、58、56、54、52、56.5、51、50、50'、48和46千道尔顿)。因此,在胸腺上皮中,我们发现了先前在表皮基底细胞中观察到的角蛋白(5、14、15),以及在基底上层表皮终末分化角质形成细胞中特有的角蛋白(1 - 2、10)。对胎儿和出生后人胸腺进行的间接免疫荧光(IF)检测表明,抗体AE - 3、35βH11和RTE - 23识别的角蛋白表位存在于被膜下皮质、皮质、髓质和哈氏小体的上皮细胞上。相比之下,抗体AE - 1和RTE - 22主要与神经内分泌胸腺上皮(被膜下皮质、髓质、哈氏小体)发生反应。抗体AE - 2的上皮反应性仅限于哈氏小体中的上皮细胞,且直到胎儿妊娠16周时才出现,即哈氏小体首次形成时。胸腺角蛋白的二维凝胶分析表明,抗体AE - 2在胸腺中仅识别分子量为56.6和65 - 67千道尔顿的角蛋白(分别为10和1 - 2)。这些数据以及在荧光检测中AE - 2与哈氏小体的选择性反应性,证明了与表皮细胞成熟后期相关的高分子量角蛋白定位于哈氏小体中。总之,我们证明了人胸腺上皮含有在多种上皮类型中发现的特定角蛋白,以及与表皮细胞分化早期和晚期相关的角蛋白。(摘要截短至400字)

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