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1. Murine B cell development and antibody responses to model antigens are not impaired in the absence of the TNF receptor GITR.

Author

Lenka Sinik Teodorovic, Carlo Riccardi, Raul M Torres, and Roberta Pelanda

Subjects
Medicine, Science
Abstract

The Glucocorticoid-Induced Tumor necrosis factor Receptor GITR, a member of the tumor necrosis factor receptor superfamily, has been shown to be important in modulating immune responses in the context of T cell immunity. B lymphocytes also express GITR, but a role of GITR in humoral immunity has not been fully explored. To address this question, we performed studies to determine the kinetics of GITR expression on naïve and stimulated B cells and the capacity of B cells to develop and mount antibody responses in GITR(-/-) mice. Results of our studies indicate that all mature B cells express GITR on the cell surface, albeit at different levels. Expression of GITR on naïve mature B cells is upregulated by BCR signaling, but is counteracted by helper T cell-related factors and other inflammatory signals in vitro. In line with these findings, expression of GITR on germinal center and memory B cells is lower than that on naïve B cells. However, the expression of GITR is strongly upregulated in plasma cells. Despite these differences in GITR expression, the absence of GITR has no effect on T cell-dependent and T cell-independent antibody responses to model antigens in GITR(-/-) mice, or on B cell activation and proliferation in vitro. GITR deficiency manifests only with a slight reduction of mature B cell numbers and increased turnover of naïve B cells, suggesting that GITR slightly contributes to mature B cell homeostasis. Overall, our data indicate that GITR does not play a significant role in B cell development and antibody responses to T-dependent and independent model antigens within the context of a GITR-deficient genetic background.

Published
2012
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4. Supplemental Figure 7 from Inhibition of MERTK Promotes Suppression of Tumor Growth in BRAF Mutant and BRAF Wild-Type Melanoma

Author

Douglas K. Graham, Deborah DeRyckere, H. Shelton Earp, Stephen V. Frye, Xiaodong Wang, S. Gail Eckhardt, Tal Burstyn-Cohen, Rotem Kami, William A. Robinson, Stacey M. Bagby, Jacqueline Carrico, John J. Tentler, Katherine A. Minson, and Lenka Sinik

Abstract

Supplemental Figure 7 shows combined UNC2025 and vemurafenib treatment is tolerated in mice.

Published
2023

7. Inhibition of MERTK Promotes Suppression of Tumor Growth in BRAF Mutant and BRAF Wild-Type Melanoma

Author

Jacqueline Carrico, Katherine A. Minson, Stephen V. Frye, Rotem Kami, S. Gail Eckhardt, John J. Tentler, Douglas K. Graham, Tal Burstyn-Cohen, Stacey M. Bagby, Deborah DeRyckere, Lenka Sinik, H. Shelton Earp, Xiaodong Wang, and William A. Robinson

Subjects
Proto-Oncogene Proteins B-raf, 0301 basic medicine, MAPK/ERK pathway, Neuroblastoma RAS viral oncogene homolog, Cancer Research, Cell Survival, Article, Piperazines, Receptor tyrosine kinase, GTP Phosphohydrolases, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Piperidines, Cell Line, Tumor, Animals, Humans, Medicine, Phosphorylation, Vemurafenib, Melanoma, neoplasms, Protein kinase B, Cell Proliferation, Cobimetinib, c-Mer Tyrosine Kinase, biology, business.industry, Adenine, Membrane Proteins, Drug Synergism, MERTK, medicine.disease, digestive system diseases, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Mutation, biology.protein, Cancer research, Azetidines, Female, business, Signal Transduction, medicine.drug
Abstract

Molecularly-targeted agents have improved outcomes for a subset of patients with BRAF-mutated melanoma, but treatment of resistant and BRAF wild-type tumors remains a challenge. The MERTK receptor tyrosine kinase is aberrantly expressed in melanoma and can contribute to oncogenic phenotypes. Here we report the effect of treatment with a MERTK-selective small molecule inhibitor, UNC2025, in preclinical models of melanoma. In melanoma cell lines, treatment with UNC2025 potently inhibited phosphorylation of MERTK and downstream signaling, induced cell death, and decreased colony formation. In patient-derived melanoma xenograft models, treatment with UNC2025 blocked or significantly reduced tumor growth. Importantly, UNC2025 had similar biochemical and functional effects in both BRAF-mutated and BRAF wild-type models and irrespective of NRAS mutational status, implicating MERTK inhibition as a potential therapeutic strategy in tumors that are not amenable to BRAF-targeting and for which there are limited treatment options. In BRAF-mutated cell lines, combined treatment with UNC2025 and the BRAF inhibitor vemurafenib provided effective inhibition of oncogenic signaling through ERK, AKT, and STAT6, increased induction of cell death, and decreased colony-forming potential. Similarly, in NRAS-mutated cell lines, addition of UNC2025 to cobimetinib therapy increased cell death and decreased colony-forming potential. In a BRAF-mutated patient-derived xenograft, treatment with combined UNC2025 and vemurafenib was well-tolerated and significantly decreased tumor growth compared with vemurafenib alone. These data support the use of UNC2025 for treatment of melanoma, irrespective of BRAF or NRAS mutational status, and suggest a role for MERTK and targeted combination therapy in BRAF and NRAS-mutated melanoma.

Published
2019

8. Murine B Cell Development and Antibody Responses to Model Antigens Are Not Impaired in the Absence of the TNF Receptor GITR.

Author

Teodorovic, Lenka Sinik, Riccardi, Carlo, Torres, Raul M., and Pelanda, Roberta

Subjects
*B cells, *ANTIBODY formation, *ANTIGENS, *GLUCOCORTICOIDS, *TUMOR necrosis factor receptors, *LABORATORY mice
Abstract

The Glucocorticoid-Induced Tumor necrosis factor Receptor GITR, a member of the tumor necrosis factor receptor superfamily, has been shown to be important in modulating immune responses in the context of T cell immunity. B lymphocytes also express GITR, but a role of GITR in humoral immunity has not been fully explored. To address this question, we performed studies to determine the kinetics of GITR expression on naïve and stimulated B cells and the capacity of B cells to develop and mount antibody responses in GITR-/- mice. Results of our studies indicate that all mature B cells express GITR on the cell surface, albeit at different levels. Expression of GITR on naïve mature B cells is upregulated by BCR signaling, but is counteracted by helper T cell-related factors and other inflammatory signals in vitro. In line with these findings, expression of GITR on germinal center and memory B cells is lower than that on naïve B cells. However, the expression of GITR is strongly upregulated in plasma cells. Despite these differences in GITR expression, the absence of GITR has no effect on T cell-dependent and T cell-independent antibody responses to model antigens in GITR-/- mice, or on B cell activation and proliferation in vitro. GITR deficiency manifests only with a slight reduction of mature B cell numbers and increased turnover of naïve B cells, suggesting that GITR slightly contributes to mature B cell homeostasis. Overall, our data indicate that GITR does not play a significant role in B cell development and antibody responses to T-dependent and independent model antigens within the context of a GITR-deficient genetic background. [ABSTRACT FROM AUTHOR]

Published
2012
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