人胸腺细胞二肽基肽酶IV (CD26)活性随个体发育阶段的改变而改变

Phillip Ruiz , Natalia Zacharievich , Lei Hao , Ana L. Viciana , Mark Shenkin
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引用次数: 13

摘要

非整合素受体CD26,也被称为二肽基肽酶IV (DPP IV),是一种110- 120 kda的跨膜丝氨酸氨基肽酶糖蛋白,具有多种功能,包括通过细胞外基质的细胞运输和T细胞活化过程中的共刺激电位,并影响胸腺成熟过程中的T细胞分化。为了进一步确定这种膜外肽酶在人胸腺中的表达和功能活性,我们使用了一种非破坏性的细胞荧光测定法,使用荧光染料共轭肽底物同时测量细胞内DPP IV的活性,并对质膜相关T淋巴细胞谱系抗原CD4和CD8以及CD26进行表面染色。使用三色法检测人类胸腺,发现由CD4/CD8表型定义的胸腺细胞亚群在时间依赖性DPP IV活性方面存在显著差异。在这方面,CD4−/CD8−胸腺细胞表现出最低的DPP IV活性,而比较小尺寸的CD26+细胞具有更高的活性。胸腺细胞中凋亡细胞的比例高于活细胞,表达的DPP IV活性低于活细胞。因此,随着胸腺细胞的成熟,DPP IV似乎上调,而在经历程序性细胞死亡的胸腺细胞群中,DPP IV的表达减少,这表明cd26相关的酶活性在T细胞成熟过程中受到致瘤性控制,可能与新生克隆的胸腺缺失有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Human Thymocyte Dipeptidyl Peptidase IV (CD26) Activity Is Altered with Stage of Ontogeny

The nonintegrin receptor CD26, also known as dipeptidyl peptidase IV (DPP IV) is a transmembrane 110- to 120-kDa serine aminopeptidase glycoprotein with multiple functions, including cellular trafficking through extracellular matrix, and costimulatory potential during T cell activation, and is an influence upon T cell differentiation during their maturation in the thymus. In order to further define the expression and functional activity of this membrane exopeptidase in human thymus, we utilized a nondisruptive, cytofluorogenic assay which allowed simultaneous measurement of intracellular DPP IV activity using a fluorochrome-conjugated peptide substrate with surface staining of plasma membrane-associated T lymphocyte lineage antigens CD4 and CD8, as well as CD26. Human thymi were examined using the three-color assay, and significant differences in time-dependent DPP IV activity were found among the thymocyte subsets defined by their CD4/CD8 phenotype. In this regard, CD4/CD8thymocytes displayed the lowest DPP IV activity and had higher activity than the smaller-sized CD26+cells. Thymocytes containing greater percentages of apoptotic cells expressed lower DPP IV activity than viable cells. Thus, DPP IV appears to be upregulated as thymocytes mature and is reduced among thymocyte populations enriched for cells undergoing programmed cell death, suggesting that CD26-associated enzymatic activity is ontogenically controlled during T cell maturation and may be involved in thymic deletion of emerging clones.

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