PROGRESSION OF A VESICULAR STOMATITIS-VIRUS INFECTION IN PRIMARY LYMPHOCYTES IS RESTRICTED AT MULTIPLE LEVELS DURING B-CELL ACTIVATION

被引：0

作者：

SCHMIDT, MR

GRAVEL, KA

WOODLAND, RT

机构：

来源：

JOURNAL OF IMMUNOLOGY | 1995年 / 155卷 / 05期

关键词：

D O I：

暂无

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Small resting B cells do not support a productive vesicular stomatitis virus (VSV) infection, but are induced by B cell activators to become fully permissive for VSV replication. Nonpermissive B cell populations restrict VSV expression at multiple points: transcript levels, translation, and maturation. Unstimulated resting G(0) B cells can be infected by VSV and support the synthesis of all VSV mRNAs. Steady-state levels of viral transcripts are selectively enhanced by T cell-derived cytokines to an extent comparable with that seen for cytokine-regulated cellular mRNAs. However, viral proteins are not detected in immunoprecipitates from unstimulated or cytokine-stimulated B cells despite the fact that viral mRNAs are associated with polysomes and can be translated in vitro. This translational block is released by stimulation of infected B cells with mitogenic anti-Ig or LPS, or non-mitogenic PMA. VSV virion maturation is also regulated by activation signals, because neither anti-Ig- nor PMA-stimulated B cells produce high levels of infectious VSV particles. Because anti-Ig stimulation supports viral genome replication, maturational arrest is apparently at virus assembly or release. PMA and ionomycin induces changes beyond those seen with anti-Ig, because these B cells produce PFUs at levels comparable with those seen with LPS-activated B cells and VSV-permissive cell lines. Activation-dependent regulation of virus expression provides a new paradigm for assessing activator-induced events in B cell differentiation not revealed by previous assessments of proliferation or Ab synthesis.

引用

页码：2533 / 2544

页数：12

共 50 条

[41] Evidence for B cell-mediated activation of V delta 1(+) T lymphocytes during progression of HIV infection
Hyjek, EM
Bartkowiak, J
Drozdz, R
Wasik, TJ
Jasinski, M
Kaneko, Y
Lischner, HW
Kozbor, D
JOURNAL OF IMMUNOLOGY, 1997, 158 (01): : 464 - 474
[42] MEASLES-VIRUS INFECTION OF LYMPHOCYTES-B PERMITS CELLULAR ACTIVATION BUT BLOCKS PROGRESSION THROUGH THE CELL-CYCLE
MCCHESNEY, MB
KEHRL, JH
VALSAMAKIS, A
FAUCI, AS
OLDSTONE, MBA
JOURNAL OF VIROLOGY, 1987, 61 (11) : 3441 - 3447
[43] CYTOLYTIC LYMPHOCYTES-T FROM THE BALB C-H-2DM2 MOUSE RECOGNIZE THE VESICULAR STOMATITIS-VIRUS GLYCOPROTEIN AND ARE RESTRICTED BY CLASS-II MHC ANTIGENS
BROWNING, MJ
HUANG, AS
REISS, CS
JOURNAL OF IMMUNOLOGY, 1990, 145 (03): : 985 - 994
[44] Chronic hepatitis C virus infection and primary cutaneous B-cell lymphoma
Prati, D
Zanella, A
De Mattei, C
Farma, E
Boschetti, C
Sirchia, G
Venegoni, L
Berti, E
BRITISH JOURNAL OF HAEMATOLOGY, 1999, 105 (03) : 841 - 841
[45] ANTIGEN-PRESENTING B-CELLS - EFFICIENT UPTAKE AND PRESENTATION BY ACTIVATED B-CELLS FOR INDUCTION OF CYTO-TOXIC LYMPHOCYTES-T AGAINST VESICULAR STOMATITIS-VIRUS
CIAVARRA, RP
BURGESS, DH
CELLULAR IMMUNOLOGY, 1988, 114 (01) : 27 - 40
[46] PTK72 ACTIVITY DURING B-CELL ACTIVATION AND CELL-CYCLE PROGRESSION
BURG, DL
GEAHLEN, RL
JOURNAL OF IMMUNOLOGY, 1993, 150 (08): : A263 - A263
[47] HIV-1-SPECIFIC B-CELL ACTIVATION - A MAJOR CONSTITUENT OF SPONTANEOUS B-CELL ACTIVATION DURING HIV-1 INFECTION
AMADORI, A
ZAMARCHI, R
CIMINALE, V
DELMISTRO, A
SIERVO, S
ALBERTI, A
COLOMBATTI, M
CHIECOBIANCHI, L
JOURNAL OF IMMUNOLOGY, 1989, 143 (07): : 2146 - 2152
[48] POLYCLONAL B-CELL ACTIVATION DURING THE COURSE OF ANGIOSTRONGYLUS-CANTONENSIS INFECTION
TAKAI, A
SATO, Y
OTSURU, M
DEVELOPMENTAL AND COMPARATIVE IMMUNOLOGY, 1985, 9 (03): : 485 - 495
[49] Apoptosis and polyclonal B-cell activation during HIV-1 infection
Samuelsson, A
De Milito, A
Hassani, H
Broström, C
Chiodi, F
ADVANCES IN ANIMAL VIROLOGY, 2000, : 265 - 280
[50] POLYCLONAL B-CELL LYMPHOMA DURING INFECTION WITH EPSTEIN-BARR VIRUS
SCHUMACHER, HR
DUVALARNOULD, BJ
FORMAN, DS
THOMAS, WJ
CREEGAN, WJ
STRONG, DM
NEW ENGLAND JOURNAL OF MEDICINE, 1980, 303 (18): : 1064 - 1064

← 1 2 3 4 5 →