il -2缺陷小鼠胸腺基质细胞异常和t细胞发育失调。

T Reya, H Bassiri, R Biancaniello, S R Carding
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引用次数: 21

摘要

白细胞介素-2 (IL-2)在t细胞发育中的作用尚不清楚。为了解决这个问题,我们研究了在IL-2缺陷(IL-2-/-)小鼠中发生的胸腺发育异常和自身免疫性疾病的本质。出生4至5周后,IL-2-/-小鼠逐渐发展为胸腺疾病,导致胸腺细胞成熟中断。这种疾病的特点是细胞数量急剧减少,未成熟CD4-8-(双阴性;DN)和CD4+8+(双阳性;胸腺细胞和胸腺间质细胞室的缺陷。不同年龄的特异性无病原体和无细菌的IL-2-/-小鼠胸腺切片的免疫组织化学染色显示皮质上皮细胞、MHCⅱ类表达细胞、单核细胞和巨噬细胞的逐渐丧失。早在出生后1周,巨噬细胞数量就明显减少。由于IL-2-/-胸腺细胞祖细胞群在转移到正常胸腺后可以正常成熟,IL-2-/-小鼠的胸腺缺陷似乎是由于胸腺基质细胞的异常所致。这些结果强调了IL-2在维持功能微环境中的作用,这是支持胸腺细胞生长、发育和选择所必需的。
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Thymic stromal-cell abnormalities and dysregulated T-cell development in IL-2-deficient mice.

The role that interleukin-2 (IL-2) plays in T-cell development is not known. To address this issue, we have investigated the nature of the abnormal thymic development and autoimmune disorders that occurs in IL-2-deficient (IL-2-/-) mice. After 4 to 5 weeks of birth, IL-2-/- mice progressively develop a thymic disorder resulting in the disruption of thymocyte maturation. This disorder is characterized by a dramatic reduction in cellularity, the selective loss of immature CD4-8- (double negative; DN) and CD4+8+ (double positive; DP) thymocytes and defects in the thymic stromal-cell compartment. Immunohistochemical staining of sections of thymuses from specific pathogen-free and germ-free IL-2-/- mice of various ages showed a progressive loss of cortical epithelial cells, MHC class II-expressing cells, monocytes, and macrophages. Reduced numbers of macrophages were apparent as early as 1 week after birth. Since IL-2-/- thymocyte progenitor populations could mature normally on transfer into a normal thymus, the thymic defect in IL-2-/- mice appears to be due to abnormalities among thymic stromal cells. These results underscore the role of IL-2 in maintaining functional microenvironments that are necessary to support thymocyte growth, development, and selection.

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