Memory CD8+ T cells colocalize with IL-7+ stromal cells in bone marrow and rest in terms of proliferation and transcription

被引:93
|
作者
Alp, Oezen Sercan [1 ]
Durlanik, Sibel [2 ]
Schulz, Daniel [1 ]
McGrath, Mairi [1 ]
Gruen, Joachim R. [3 ]
Bardua, Marcus [1 ]
Ikuta, Koichi [4 ]
Sgouroudis, Evridiki [1 ]
Riedel, Rene [1 ]
Zehentmeier, Sandra [5 ]
Hauser, Anja E. [5 ]
Tsuneto, Motokazu [6 ]
Melchers, Fritz [6 ]
Tokoyoda, Koji [7 ]
Chang, Hyun-Dong [1 ]
Thiel, Andreas [2 ]
Radbruch, Andreas [1 ]
机构
[1] German Rheumatism Res Ctr DRFZ, Dept Cell Biol, D-10117 Berlin, Germany
[2] Charite, Berlin Brandenburger Ctr Regenerat Therapies BCRT, D-13353 Berlin, Germany
[3] German Rheumatism Res Ctr, Dept Bioinformat, Berlin, Germany
[4] Kyoto Univ, Inst Virus Res, Dept Biol Responses, Kyoto 606, Japan
[5] German Rheumatism Res Ctr, Dept Immunodynam, Berlin, Germany
[6] Max Plank Inst Infect Biol, Dept Lymphocyte Dev, Berlin, Germany
[7] German Rheumatism Res Ctr, Dept Osteoimmunol, Berlin, Germany
基金
欧洲研究理事会;
关键词
Bone marrow; CD8 T cell; Gene expression; Interleukin-7; Memory cells; PLASMA-CELLS; HOMEOSTATIC PROLIFERATION; IMMUNOLOGICAL MEMORY; LYMPHOID ORGANS; RM CELLS; SITE; SURVIVAL; TISSUE; NAIVE; MAINTENANCE;
D O I
10.1002/eji.201445295
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
It is believed that memory CD8(+) Tcells are maintained in secondary lymphoid tissues, peripheral tissues, and BM by homeostatic proliferation. Their survival has been shown to be dependent on IL-7, but it is unclear where they acquire it. Here we show that in murine BM, memory CD8(+) Tcells individually colocalize with IL-7(+) reticular stromal cells. The Tcells are resting in terms of global transcription and do not express markers of activation, for example, 4-1BB (CD137), IL-2, or IFN-, despite the expression of CD69 on about 30% of the cells. Ninety-five percent of the memory CD8(+) Tcells in BM are in G(0) phase of cell cycle and do not express Ki-67. Less than 1% is in S/M/G(2) of cell cycle, according to propidium iodide staining. While previous publications have estimated the extent of proliferation of CD8(+) memory Tcells on the basis of BrdU incorporation, we show here that BrdU itself induces proliferation of CD8(+) memory Tcells. Taken together, the present results suggest that CD8(+) memory Tcells are maintained as resting cells in the BM in dedicated niches with their survival conditional on IL-7 receptor signaling.
引用
收藏
页码:975 / 987
页数:13
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