Maintenance of CD8+ memory T lymphocytes in the spleen but not in the bone marrow is dependent on proliferation

被引:36
作者
Siracusa, Francesco [1 ]
Alp, Ozen Sercan [1 ]
Maschmeyer, Patrick [1 ]
McGrath, Mairi [1 ]
Mashreghi, Mir-Farzin [1 ]
Hojyo, Shintaro [2 ]
Chang, Hyun-Dong [1 ]
Tokoyoda, Koji [2 ]
Radbruch, Andreas [1 ,3 ]
机构
[1] Inst Leibniz Assoc, German Rheumatism Res Ctr DRFZ, Dept Cell Biol, Berlin, Germany
[2] Inst Leibniz Assoc, German Rheumatism Res Ctr DRFZ, Dept Osteoimmunol, Berlin, Germany
[3] Charite, Berlin, Germany
来源
EUROPEAN JOURNAL OF IMMUNOLOGY | 2017年 / 47卷 / 11期
基金
欧洲研究理事会;
关键词
Bone marrow; CD8(+) memory T lymphocytes; Cyclophosphamide; Homeostatic proliferation; Tissue resident memory; LIVED PLASMA-CELLS; HOMEOSTATIC PROLIFERATION; NAIVE; DEATH; SITE;
D O I
10.1002/eji.201747063
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 current belief that numbers of CD8(+) memory T lymphocytes in the memory phase of an immune response are maintained by homeostatic proliferation. Here, we compare the proliferation of CD8(+) memory T lymphocytes, generated by natural infections and by intentional immunization, in spleen and bone marrow (BM). Fifty percent of CD8(+) memory T lymphocytes in the spleen are eliminated by cyclophosphamide within 14 days, indicating that numbers of at least 50% of splenic CD8(+) memory T lymphocytes are maintained by proliferation. The numbers of CD8(+) memory T lymphocytes in the BM, however, were not affected by cyclophosphamide. This stability was independent of circulating CD8(+) memory T cells, blocked by FTY720, showing that BM is a privileged site for the maintenance of memory T lymphocytes, as resident cells, resting in terms of proliferation.
引用
收藏
页码:1900 / 1905
页数:6
相关论文
共 22 条
[1]   Memory CD8+ T cells colocalize with IL-7+ stromal cells in bone marrow and rest in terms of proliferation and transcription [J].
Alp, Oezen Sercan ;
Durlanik, Sibel ;
Schulz, Daniel ;
McGrath, Mairi ;
Gruen, Joachim R. ;
Bardua, Marcus ;
Ikuta, Koichi ;
Sgouroudis, Evridiki ;
Riedel, Rene ;
Zehentmeier, Sandra ;
Hauser, Anja E. ;
Tsuneto, Motokazu ;
Melchers, Fritz ;
Tokoyoda, Koji ;
Chang, Hyun-Dong ;
Thiel, Andreas ;
Radbruch, Andreas .
EUROPEAN JOURNAL OF IMMUNOLOGY, 2015, 45 (04) :975-987
[2]   CD69 Suppresses Sphingosine 1-Phosophate Receptor-1 (S1P1) Function through Interaction with Membrane Helix 4 [J].
Bankovich, Alexander J. ;
Shiow, Lawrence R. ;
Cyster, Jason G. .
JOURNAL OF BIOLOGICAL CHEMISTRY, 2010, 285 (29) :22328-22337
[3]   Bone marrow is a preferred site for homeostatic proliferation of memory CD8 T cells [J].
Becker, TC ;
Coley, SM ;
Wherry, EJ ;
Ahmed, R .
JOURNAL OF IMMUNOLOGY, 2005, 174 (03) :1269-1273
[4]   Interleukin 15 is required for proliferative renewal of virus-specific memory CD8 T cells [J].
Becker, TC ;
Wherry, EJ ;
Boone, D ;
Murali-Krishna, K ;
Antia, R ;
Ma, A ;
Ahmed, R .
JOURNAL OF EXPERIMENTAL MEDICINE, 2002, 195 (12) :1541-1548
[5]  
Benner R., 1981, IMMUNOLOGICAL METHOD, VII, P247, DOI DOI 10.1016/B978-0-12-442702-0.50020-0
[6]   Homeostatic proliferation and survival of naive and memory T cells [J].
Boyman, Onur ;
Letourneau, Sven ;
Krieg, Carsten ;
Sprent, Jonathan .
EUROPEAN JOURNAL OF IMMUNOLOGY, 2009, 39 (08) :2088-2094
[7]   The immune modulator FTY720 targets sphingosine 1-phosphate receptors [J].
Brinkmann, V ;
Davis, MD ;
Heise, CE ;
Albert, R ;
Cottens, S ;
Hof, R ;
Bruns, C ;
Prieschl, E ;
Baumruker, T ;
Hiestand, P ;
Foster, CA ;
Zollinger, M ;
Lynch, KR .
JOURNAL OF BIOLOGICAL CHEMISTRY, 2002, 277 (24) :21453-21457
[8]  
FREITAS AA, 1982, J IMMUNOL, V128, P54
[9]  
GERDES J, 1984, J IMMUNOL, V133, P1710
[10]   The immunosuppressant FTY720 down-regulates sphingosine 1-phosphate G protein-coupled receptors [J].
Gräler, MH ;
Goetzl, EJ .
FASEB JOURNAL, 2004, 18 (01) :551-+
123