Terence A. Potter scite author profile

Previous work has established a role for CD40-mediated signals in eliciting helper-dependent CD8 ؉ T cell responses. Here we investigated the effects of in vivo CD40 stimulation on the survival and function of tumor-specific CD8 ؉ T cells in a mouse melanoma model system. We found that agonistic anti-CD40 antibody treatment alone of tumor-bearing mice accelerated the deletion of tumorantigen-specific T cells. However, long-term survival and function of tumor-antigen-specific T cells could be achieved when viral immunization with tumor antigen and anti-CD40 treatment were combined. This rescue of CD8 ؉ T cells could not be easily replicated by inflammatory or antigen-specific stimuli alone, demonstrating the specificity of signals that regulate the deletion or survival of tumor-specific T cells. These results demonstrate that opposing effects can be elicited by CD40 stimulation in vivo and suggest the need for caution in using this treatment for cancer patients.melanoma ͉ MHC tetramer

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The interaction of adenovirus E1A with p300 family members modulates cellular gene expression to reduce tumorigenicity

Miura

Cook

Potter

et al. 2006

J of Cellular Biochemistry

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The use of adenovirus serotype 2 or 5 (Ad2/5) E1A as therapy for human malignancy requires an understanding of the mechanisms involved in E1A-induced tumor suppression. The prevailing use of E1A in the treatment of human malignancy stresses the non-immunologically mediated, anti-tumorigenic activities of E1A. However, the capacity of E1A to elicit a NK-cell and T-cell anti-tumor immune response and to sensitize tumor cells to lysis by immune effector molecules utilized by NK cells and T cells is also an important component of the anti-tumorigenic activity of E1A. This immune-mediated anti-tumorigenic activity of E1A is not shared by functionally similar viral oncoproteins such as the human papillomavirus type 16 (HPV16) E7 oncoprotein and is dependent on the capacity of E1A to interact with transcriptional coadapter, p300. To further define the molecular mechanisms whereby E1A reduces tumorigenicity, we compared total cellular gene expression in H4 cells, a human fibrosarcoma cell line, to gene expression in H4 cells stably expressing E1A, E7, or mutant forms of E1A that do not bind p300. The expression of E1A, but not E7, in H4 cells modulated the expression of cellular genes that may promote apoptosis, enhance immunogenicity and reduce tumor cell metastasis. The difference in the ability of E1A and E7 to modulate the expression of cellular genes that may influence tumorigenicity was largely attributable to distinct interactions of E1A and E7 with p300. Results of this study will be useful in designing novel strategies to augment the anti-tumorigenic activities of E1A.

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Terence A. Potter

CD40 stimulation accelerates deletion of tumor-specific CD8⁺T cells in the absence of tumor-antigen vaccination

The interaction of adenovirus E1A with p300 family members modulates cellular gene expression to reduce tumorigenicity

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Terence A. Potter

CD40 stimulation accelerates deletion of tumor-specific CD8+T cells in the absence of tumor-antigen vaccination

The interaction of adenovirus E1A with p300 family members modulates cellular gene expression to reduce tumorigenicity

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CD40 stimulation accelerates deletion of tumor-specific CD8⁺T cells in the absence of tumor-antigen vaccination