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患有干燥综合征的aly/aly小鼠的唾液腺中自然杀伤T细胞数量丰富,但肝脏和胸腺中则没有。

Abundance of NKT cells in the salivary glands but absence thereof in the liver and thymus of aly/aly mice with Sjögren syndrome.

作者信息

Narita J, Kawamura T, Miyaji C, Watanabe H, Honda S, Koya T, Arakawa M, Abo T

机构信息

Department of Immunology, Niigata University School of Medicine, Niigata, 951-8510, Japan.

出版信息

Cell Immunol. 1999 Mar 15;192(2):149-58. doi: 10.1006/cimm.1998.1450.

DOI:10.1006/cimm.1998.1450
PMID:10087183
Abstract

It is known that ALY/Nsc Jcl-aly/aly (aly/aly) mice that congenitally lack lymph nodes fall victim to Sjögren syndrome as a function of age. We investigated how TCRint cells of extrathymic origin and TCRhigh cells of thymic origin are distributed in various organs of these mice. Although the distribution of T-cell subsets was not different between control aly/+ and aly/aly mice in youth in any of the tested organs, the proportion of TCRint cells in the liver and spleen of aly/aly mice increased with aging. Usually, TCRint cells in the liver comprise a half-and-half mixture of a NK1. 1(+) subset (i.e., NKT cells) and a NK1.1(-) subset. In constrast, almost all expanding TCRint cells in various immune organs of aly/aly mice were found to be NK1.1(-). A large proportion of lymphocytes, including NK cells and TCRint cells, were also present in the salivary glands of aly/aly mice. Interestingly, these TCRint cells in the salivary glands contained an NK1.1(+) subset (i.e., NKT cells) that used an invariant chain of Valpha14Jalpha281 for TCRalphabeta (>50%). Moreover, gammadeltaT cells that used Vgamma 1, 2, 4/Vdelta 1, 4, 6 mRNAs, different from those of gammadeltaT cells in the liver and intestine, were abundant. Possibly reflecting the in situ generation of these T cells in the salivary glands, the expression of RAG-2 mRNA was evident by the RT-RCR method. These results suggest that (i) inflammatory lymphocytes that evoke Sjögren syndrome in aly/aly mice are NK cells or TCRint cells (both NK1.1(+) and NK1.1(-) subsets) and (ii) TCRint cells in the salivary glands might be generated in situ.

摘要

已知先天性缺乏淋巴结的ALY/Nsc Jcl-aly/aly(aly/aly)小鼠会随着年龄增长患上干燥综合征。我们研究了胸腺外起源的TCRint细胞和胸腺起源的TCRhigh细胞在这些小鼠的各种器官中的分布情况。尽管在年轻时,对照aly/+小鼠和aly/aly小鼠的T细胞亚群在任何测试器官中的分布都没有差异,但aly/aly小鼠肝脏和脾脏中TCRint细胞的比例会随着年龄增长而增加。通常,肝脏中的TCRint细胞由NK1.1(+)亚群(即NKT细胞)和NK1.1(-)亚群各占一半混合而成。相比之下,在aly/aly小鼠的各种免疫器官中几乎所有扩增的TCRint细胞都被发现是NK1.1(-)。aly/aly小鼠的唾液腺中也存在大量淋巴细胞,包括NK细胞和TCRint细胞。有趣的是,这些唾液腺中的TCRint细胞包含一个NK1.1(+)亚群(即NKT细胞),其TCRαβ使用不变链Valpha14Jalpha281(>50%)。此外,使用Vgamma 1、2、4/Vdelta 1、4、6 mRNA的γδT细胞数量丰富,与肝脏和肠道中的γδT细胞不同。通过RT-RCR方法明显检测到RAG-2 mRNA的表达,这可能反映了这些T细胞在唾液腺中的原位生成。这些结果表明:(i)在aly/aly小鼠中引发干燥综合征的炎性淋巴细胞是NK细胞或TCRint细胞(NK1.1(+)和NK1.1(-)亚群);(ii)唾液腺中的TCRint细胞可能是原位生成的。

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