Literature DB >> 17208541

Induction of cytolytic T lymphocytes against pediatric solid tumors in vitro using autologous dendritic cells pulsed with necrotic primary tumor.

Joel Shilyansky1, Paulette Jacobs, Kara Doffek, Sonia L Sugg.   

Abstract

PURPOSE: Effective and generally applicable methods for generating cancer vaccines in children have not been defined. Dendritic cells (DCs) are the most potent professional antigen-presenting cells capable of activating primary cytolytic T cells. We tested the ability of DCs generated from pediatric patients' peripheral blood monocytes and pulsed with a necrotic tumor to activate autologous tumor-specific cytolytic T cells.
METHODS: Tumor and peripheral blood cells were obtained from pediatric patients undergoing biopsy or resection for advanced solid tumors according to an institutional research board-approved protocol and after acquiring informed consent from them. To generate DCs, we treated peripheral blood monocytes with granulocyte-macrophage colony stimulating factor and interleukin (IL)-4. Maturation was induced with a cytokine cocktail (CC) containing tumor necrosis factor-alpha, IL-6, IL-1beta, and prostaglandin E2. The DC phenotype was assayed using flow cytometry. Tumor necrosis was induced by exposure to UV-B irradiation (1000 mJ). Dendritic cells pulsed with a UV-B-treated primary tumor and matured with CC were used to stimulate autologous peripheral blood lymphocytes weekly. Tumor-specific cytolytic activity was assayed using 4-hour 51Cr release.
RESULTS: Peripheral blood monocytes isolated from pediatric patients differentiated into immature DCs (CD14-, MHCII+ [major histocompatibility complex], CD80(low), CD86(low)) in the presence of granulocyte-macrophage colony stimulating factor and IL-4. Cytokine cocktail induced maturation of DCs, as characterized by increased expressions of MHCII, CD83, CD80, and CD86. Patients' peripheral blood lymphocytes stimulated in vitro with DCs loaded with a necrotic primary tumor and matured with CC specifically lysed autologous neuroblastoma in 7 of 9 patients.
CONCLUSION: Dendritic cells generated from the peripheral blood of children with advanced solid tumors and pulsed with a necrotic primary tumor undergo maturation and effectively stimulate autologous tumor-specific cytolytic T cells in vitro. We describe a simple method for generating a vaccine capable of activating cytotoxic T cells against pediatric solid tumors that does not require the genetic identification of tumor-associated antigens.

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Year:  2007        PMID: 17208541     DOI: 10.1016/j.jpedsurg.2006.09.008

Source DB:  PubMed          Journal:  J Pediatr Surg        ISSN: 0022-3468            Impact factor:   2.545


  8 in total

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Journal:  J Neurooncol       Date:  2015-08-27       Impact factor: 4.130

Review 2.  Dendritic cell vaccines: A review of recent developments and their potential pediatric application.

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3.  Phenotype and polarization of autologous T cells by biomaterial-treated dendritic cells.

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4.  Lack of T-cell responses following autologous tumour lysate pulsed dendritic cell vaccination, in patients with relapsed osteosarcoma.

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Review 5.  Cellular immunotherapy for neuroblastoma: a review of current vaccine and adoptive T cell therapeutics.

Authors:  C U Louis; M K Brenner
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6.  Induction of protective cytotoxic T-cell responses by a B-cell-based cellular vaccine requires stable expression of antigen.

Authors:  S Guo; J Xu; W Denning; Z Hel
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Review 7.  Recent developments in cell-based immune therapy for neuroblastoma.

Authors:  Michael R Verneris; John E Wagner
Journal:  J Neuroimmune Pharmacol       Date:  2007-03-02       Impact factor: 7.285

Review 8.  Cell death-based treatment of neuroblastoma.

Authors:  Kadri Valter; Boris Zhivotovsky; Vladimir Gogvadze
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  8 in total

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