ANTIGEN PRESENTATION FOR T-CELL INTERLEUKIN-2 SECRETION IS A LATE ACQUISITION OF NEONATAL B-CELLS

被引:24
|
作者
MORRIS, JF [1 ]
HOYER, JT [1 ]
PIERCE, SK [1 ]
机构
[1] NORTHWESTERN UNIV, DEPT BIOCHEM MOLEC BIOL & CELL BIOL, EVANSTON, IL 60208 USA
来源
EUROPEAN JOURNAL OF IMMUNOLOGY | 1992年 / 22卷 / 11期
关键词
D O I
10.1002/eji.1830221125
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
The ability of B lymphocytes to process and present antigen to helper T cells is essential to initiate T cell-B cell interactions in humoral immune responses. Here we describe the developmental acquisition of the antigen-presenting function of B cells as measured by the ability of B cells to stimulate a T cell hybrid to interleukin (IL)-2 secretion. Neonatal splenic B cells are not adult-like in their ability to process and present the model protein antigen pigeon cytochrome (Pc). which enters the B cell through fluid-phase pinocytosis, until 21 to 28 days of life. The ability of neonatal B cells to process and present antigen which enters the cell bound to surface Ig is not adult-like until 28 days of age. When neonatal B cells acquire antigen-presenting cell (APC) function, surface IgM facilitates antigen processing. The delayed acquisition of APC function cannot be accounted for solely by a deficiency in major histocompatibility complex MHC class II, ICAM-1, or LFA-1 as neonatal B cells express adult levels of these molecules by 7-14 days after birth. Moreover, the ability of neonatal B cells to present a peptide fragment of Pc which does not require processing is adult like by day 14. Furthermore, neonatal B cells are capable of binding, internalizing and degrading radiolabeled antigen, suggesting a more subtle level of regulation. In contrast to neonatal B cells, immature B cells in the adult bone marrow and adult B cells undergoing antigen-driven differentiation to memory B cells, as defined by the loss of the J11D marker, are competent to process and present antigen resulting in T cell IL-2 secretion. Thus, developing B cell subpopulations in the adult and in the neonate can be distinguished. Only neonatal B cells are deficient in their ability to stimulate T cells to IL-2 production.
引用
收藏
页码:2923 / 2928
页数:6
相关论文
共 50 条
  • [21] MALIGNANT HUMAN B-CELLS INHIBIT INTERLEUKIN-2 PRODUCTION BY HUMAN T-CELLS
    BURTON, J
    KAY, NE
    CLINICAL RESEARCH, 1985, 33 (04): : A840 - A840
  • [22] INTERLEUKIN-2 - A CENTRAL T-CELL LYMPHOKINE
    ROLLINGHOFF, M
    LOHOFF, M
    SOLBACH, W
    ALLERGOLOGIE, 1988, 11 (10) : 422 - 424
  • [23] CD3-INDUCED T-CELL PROLIFERATION AND INTERLEUKIN-2 SECRETION IS MODULATED BY THE CD45 ANTIGEN
    ORAVECZ, T
    MONOSTORI, E
    KURUCZ, E
    TAKACS, L
    ANDO, I
    SCANDINAVIAN JOURNAL OF IMMUNOLOGY, 1991, 34 (05) : 531 - 537
  • [24] INTERLEUKIN-2 REGULATES ANTIGEN-SPECIFIC IMMUNOGLOBULIN RESPONSE OF NAIVE MURINE B-CELLS
    ISAKOV, N
    MORROW, PR
    CELLULAR IMMUNOLOGY, 1989, 120 (02) : 366 - 374
  • [25] INTERLEUKIN-2 REGULATES ANTIGEN-SPECIFIC IMMUNOGLOBULIN RESPONSE OF NAIVE MURINE B-CELLS
    MORROW, PR
    ISAKOV, N
    LYMPHOKINE RESEARCH, 1988, 7 (03): : 314 - 314
  • [26] CAPACITY TO INTERACT WITH T-CELL REPLACING FACTOR CORRELATES WITH ACQUISITION BY B-CELLS OF MURINE DIFFERENTIATION ANTIGEN-1
    BATTISTO, JR
    FINKE, JH
    YEN, B
    IMMUNOLOGY, 1979, 37 (03) : 623 - 629
  • [27] EXPRESSION OF INTERLEUKIN-2 RECEPTOR ON T-CELL CHRONIC LYMPHOCYTIC-LEUKEMIA CELLS AND THEIR RESPONSE TO INTERLEUKIN-2
    TSUDO, M
    UCHIYAMA, T
    UMADOME, H
    WANO, Y
    HORI, T
    TAMORI, S
    UCHINO, H
    KITA, K
    CHIBA, S
    MITSUTANI, S
    NESUMI, N
    BLOOD, 1986, 67 (02) : 316 - 321
  • [28] ANTIGEN PRESENTATION BY HUMAN B-CELLS - T-CELL PROLIFERATION INDUCED BY EPSTEIN-BARR VIRUS-B LYMPHOBLASTOID-CELLS
    ISSEKUTZ, T
    CHU, E
    GEHA, RS
    JOURNAL OF IMMUNOLOGY, 1982, 129 (04): : 1446 - 1450
  • [29] IMMUNOSUPPRESSION BY LYMPHOCYTIC CHORIOMENINGITIS VIRUS-INFECTION - COMPETENT EFFECTOR T-CELL AND B-CELLS BUT IMPAIRED ANTIGEN PRESENTATION
    ALTHAGE, A
    ODERMATT, B
    MOSKOPHIDIS, D
    KUNDIG, T
    HOFFMANROHRER, U
    HENGARTNER, H
    ZINKERNAGEL, RM
    EUROPEAN JOURNAL OF IMMUNOLOGY, 1992, 22 (07) : 1803 - 1812
  • [30] B-CELLS AND THE DEVELOPMENT OF THE T-CELL REPERTOIRE
    GRAY, D
    IMMUNOLOGY TODAY, 1984, 5 (11): : 316 - 317
12345