Title of article
Priming Antiviral Cytotoxic T Lymphocytes: Requirement for CD4+ Cells Is Dependent on the Antigen Presenting Cell in Vivo
Author/Authors
Ciavarra، نويسنده , , Richard P. and Tedeschi، نويسنده , , Bruce، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 1994
Pages
12
From page
132
To page
143
Abstract
We have analyzed cytotoxic thymus-derived lymphocyte (CTL) responses to vesicular stomatitis virus (VSV) to determine whether VSV precursor CTL (pCTL) can be primed in vivo in the absence of CD4+ cells. Our studies demonstrated that secondary anti-VSV CTL responses in vitro were markedly reduced by CD4-depletion prior to priming in vivo with VSV. Limiting dilution analysis indicated that the vast majority (>90%) of VSV pCTL failed to become primed when exposed to VSV in the absence of CD4+ cells. A second minor population (5-10%) of pCTL was identified that was reproducibly primed in CD4-deficient mice. In contrast to CD4-depleted mice infected with free, infectious virus, CD4-deficient mice primed with VSV-infected, activated B cells mounted normal secondary anti-VSV CTL responses in vitro . Precursor estimates indicated that virtually all VSV pCTL became primed using this cellular immunogen. CD4-independent priming could not be achieved using VSV-infected, activated T cells, another permissive cell type for VSV replication. Thus, most VSV pCTL require inductive signals from classical CD4+ helper T cells in order to become primed in vivo and this requirement may be regulated in vivo by the antigen presenting cell.
Journal title
Cellular Immunology
Serial Year
1994
Journal title
Cellular Immunology
Record number
1850451
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