Surface molecule loss and bleb formation by human germinal center B cells undergoing apoptosis:: Role of apoptotic blebs in monocyte chemotaxis

被引:86
作者
Segundo, C
Medina, F
Rodríguez, C
Martínez-Palencia, R
Leyva-Cobián, F
Brieva, JA
机构
[1] Hosp Univ Puerto del Mar, Serv Inmunol, Cadiz 11009, Spain
[2] Hosp Univ Marques Valdecilla, Serv Inmunol, Santander, Spain
关键词
D O I
10.1182/blood.V94.3.1012.415k05_1012_1020
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Human tonsil germinal center (GC) B cells rapidly undergo apoptosis in culture. Annexin-V binding shows an early event in this process. In the present study, this method has been used to label apoptotic GC B cells and to analyze additional surface molecules. The expression of all of the molecules studied was reduced in apoptotic (annexin-V+) GC B cells, and the reduction was more marked for CD11a, CD21, CD22, CD49d, and CD54, molecules that participate in survival interaction for GC B cells. The analysis of CD54, one of the molecules that was more drastically reduced, showed that GC, but not mantle zone, B cells actively secrete CD54 to the culture supernatant (SN). The secreted CD54 was partly released from the GC B cells in a particulate form as demonstrated by centrifugation. Further experiments using filtration, fluorescence microscopy, electron microscopy, and flow cytometry analysis showed that GC B cells released to the culture SN a population of spherical membranous vesicles of about 0.18 mu m in size, similar to the blebs described in other apoptosis systems. Bleb formation depended on active metabolism, Ca2+, and, in part, on microfilament integrity. GC B-cell-derived blebs were clearly associated with apoptosis, as antiapoptotic stimuli prevented their formation. In addition, GC B-cell-derived blebs contained the adhesion molecules previously studied. Consequently, bleb formation might contribute to the surface molecule loss occurring in apoptotic GC B cells. Finally, a chemotaxis assay showed that GC B-cell blebs were chemotactic for human monocytes, suggesting that this mechanism might operate in vivo. (C) 1999 by The American Society of Hematology.
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页码:1012 / 1020
页数:9
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