AI Article Synopsis

  • In previous studies, HSP70-peptide complexes (HSP70.PCs) from fused dendritic cells and tumor cells (HSP70.PC-F) were found to be more effective in stimulating dendritic cell maturation and inducing cytotoxic T lymphocytes (CTLs) than those derived solely from tumor cells.
  • HSP70.PC-F was extracted from dendritic cells fused with ovarian or breast cancer cells and demonstrated significant potential as a tumor vaccine, leading to T cells that produced higher levels of IFN-gamma and exhibited enhanced tumor cell-killing abilities.
  • The improved performance of HSP70.PC-F as a vaccine was linked to its better composition, including a higher content of tumor antigens and the presence of additional

Article Abstract

In previous studies, we have shown that heat shock protein 70-peptide complexes (HSP70.PCs) derived from the fusion of dendritic cells (DCs) to tumor cells (HSP70.PC-F) possess superior properties compared with HSP70.PCs from tumor cells. HSP70.PC-F are more effective in stimulation of DC maturation and induction of CTL that are able to provide protection of mice against challenge with tumor cells. To develop an improved formulation of HSP70.PC-based tumor vaccine for patient use, we extracted HSP70.PC-F from DCs fused to patient-derived ovarian cancer cells or established human breast cancer cells and examined their properties as tumor vaccines. HSP70.PC-F induced T cells that expressed higher levels of IFN-gamma and exhibited increased levels of killing of tumor cells, compared with those induced by HSP70.PC derived from tumor cells. Enhanced immunogenicity of HSP70.PC-F was associated with improved composition of the vaccine, including increased content of tumor Ags and their processed intermediates, and the detection of other heat shock proteins (HSPs) such as HSP90 and HSP110. The present study has therefore provided an alternative approach to preparation of HSP-based vaccines using DC/tumor fusion technology and gentle and rapid isolation of HSP peptide complexes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2911119PMC
http://dx.doi.org/10.4049/jimmunol.0902255DOI Listing

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