B cells are critical to t-cell–mediated antitumor immunity induced by a combined immune-stimulatory/ conditionally cytotoxic therapy for glioblastoma

Candolfi, Marianela; Curtin, James F.; Yagiz, Kader; Assi, Hikmat; Wibowo, Mia K.; Alzadeh, Gabrielle E.; Foulad, David; Muhammad, AKM G.; Salehi, Sofia; Keech, Naomi; Puntel, Mariana; Liu, Chunyan; Sanderson, Nicholas R.; Kroeger, Kurt; Dunn, Robert; Martins, Gislaine; Castro; Lowenstein, Pedro R.; Castro, Maria G

doi:10.1593/neo.11024

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Candolfi, Marianela Se ha confirmado la validez de este valor de autoridad por un usuario

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Curtin, James F.

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Yagiz, Kader

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Assi, Hikmat

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Wibowo, Mia K.

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Alzadeh, Gabrielle E.

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Foulad, David

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Muhammad, AKM G.

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Salehi, Sofia

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Keech, Naomi

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Puntel, Mariana Se ha confirmado la validez de este valor de autoridad por un usuario

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Liu, Chunyan

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Sanderson, Nicholas R.

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Kroeger, Kurt

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Dunn, Robert

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Martins, Gislaine

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Castro

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Lowenstein, Pedro R.

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Castro, Maria G

dc.date.available

2017-04-17T21:56:45Z

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2011-10

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Candolfi, Marianela; Curtin, James F.; Yagiz, Kader; Assi, Hikmat; Wibowo, Mia K.; et al.; B cells are critical to t-cell–mediated antitumor immunity induced by a combined immune-stimulatory/ conditionally cytotoxic therapy for glioblastoma; Elsevier Inc; Neoplasia; 13; 10; 10-2011; 947-960

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1522-8002

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http://hdl.handle.net/11336/15348

dc.description.abstract

We have demonstrated that modifying the tumor microenvironment through intratumoral administration of adenoviral vectors (Ad) encoding the conditional cytotoxic molecule, i.e., HSV1-TK and the immune-stimulatory cytokine, i.e., fms-like tyrosine kinase 3 ligand (Flt3L) leads to T-cell-dependent tumor regression in rodent models of glioblastoma. We investigated the role of B cells during immune-mediated glioblastoma multiforme regression. Although treatment with Ad-TK+Ad-Flt3L induced tumor regression in 60% of wild-type (WT) mice, it completely failed in B-cell-deficient Igh6-/- mice. Tumor-specific T-cell precursors were detected in Ad-TK+Ad-Flt3L-treated WT mice but not in Igh6-/- mice. The treatment also failed in WT mice depleted of total B cells or marginal zone B cells. Because we could not detect circulating antibodies against tumor cells and the treatment was equally efficient in WT mice and in mice with B-cell-specific deletion of Prdm 1 (encoding Blimp-1), in which B cells are present but unable to fully differentiate into antibody-secreting plasma cells, tumor regression in this model is not dependent on B cells’ production of tumor antigen-specific immunoglobulins. Instead, B cells seem to play a role as antigen-presenting cells (APCs). Treatment with Ad-TK+Ad-Flt3L led to an increase in the number of B cells in the cervical lymph nodes, which stimulated the proliferation of syngeneic T cells and induced clonal expansion of antitumor T cells. Our data show that B cells act as APCs, playing a critical role in clonal expansion of tumor antigen-specific T cells and brain tumor regression.

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application/pdf

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eng

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Elsevier Inc Se ha confirmado la validez de este valor de autoridad por un usuario

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info:eu-repo/semantics/openAccess

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https://creativecommons.org/licenses/by-nc-nd/2.5/ar/

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Adenovirus Gene Therapy

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Hsv1 Thymidine Kinase +Flt3l

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B Cells

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Glioblastoma

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Otros Tópicos Biológicos Se ha confirmado la validez de este valor de autoridad por un usuario

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Ciencias Biológicas Se ha confirmado la validez de este valor de autoridad por un usuario

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CIENCIAS NATURALES Y EXACTAS Se ha confirmado la validez de este valor de autoridad por un usuario

dc.title

B cells are critical to t-cell–mediated antitumor immunity induced by a combined immune-stimulatory/ conditionally cytotoxic therapy for glioblastoma

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info:eu-repo/semantics/article

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info:ar-repo/semantics/artículo

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info:eu-repo/semantics/publishedVersion

dc.date.updated

2017-04-07T14:28:41Z

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13

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10

dc.journal.pagination

947-960

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Estados Unidos Se ha confirmado la validez de este valor de autoridad por un usuario

dc.description.fil

Fil: Candolfi, Marianela. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Houssay. Instituto de Investigaciones Biomédicas; Argentina

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Fil: Curtin, James F.. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Yagiz, Kader. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Assi, Hikmat. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

dc.description.fil

Fil: Wibowo, Mia K.. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Alzadeh, Gabrielle E.. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

dc.description.fil

Fil: Foulad, David. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Muhammad, AKM G.. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

dc.description.fil

Fil: Salehi, Sofia. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

dc.description.fil

Fil: Keech, Naomi. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Puntel, Mariana. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina

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Fil: Liu, Chunyan. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Sanderson, Nicholas R.. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Kroeger, Kurt. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos

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Fil: Dunn, Robert. Biogen Idec; Estados Unidos

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Fil: Martins, Gislaine. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos

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Fil: Castro. Cedars Sinai Medical Center. Gene Therapeutics Research Institute; Estados Unidos

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Fil: Lowenstein, Pedro R.. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos. University of Michigan; Estados Unidos

dc.description.fil

Fil: Castro, Maria G. Cedars Sinai Medical Center. Gene Therapeutics Research Institute. Department Of Biomedical Sciences; Estados Unidos. University of California at Los Angeles; Estados Unidos. University of Michigan; Estados Unidos

dc.journal.title

Neoplasia

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info:eu-repo/semantics/altIdentifier/doi/http://dx.doi.org/10.1593/neo.11024

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info:eu-repo/semantics/altIdentifier/url/http://www.sciencedirect.com/science/article/pii/S1476558611800825

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info:eu-repo/semantics/altIdentifier/url/https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3201571/

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