Your search keyword '"Castle, John"' showing total 6 results

1. Enhanced protection of C57 BL/6 vs Balb/c mice to melanoma liver metastasis is mediated by NK cells.

Author

Foerste, Friedrich, Boegel, Sebastian, Heck, Rosario, Pickert, Geetha, Rüssel, Nina, Rosigkeit, Sebastian, Bros, Matthias, Strobl, Stephanie, Kaps, Leonard, Aslam, Misbah, Diken, Mustafa, Castle, John, Sahin, Ugur, Tuettenberg, Andrea, Bockamp, Ernesto, and Schuppan, Detlef

Subjects

MELANOMA treatment, KILLER cells, METASTASIS

Abstract

The B16F10 murine melanoma cell line displays a low expression of MHC class I molecules favoring immune evasion and metastases in immunocompetent C57 BL/6 wild-type mice. Here, we generated metastases to the liver, an organ that is skewed towards immune tolerance, by intrasplenic injection of B16F10 cells in syngeneic C57 BL/6 compared to allogeneic Balb/c mice. Surprisingly, Balb/c mice, which usually display a pronounced M2 macrophage and Th2 T cell polarization, were ~3 times more susceptible to metastasis than C57 BL/6 mice, despite a much higher M1 and Th1 T cell immune response. The anti-metastatic advantage of C57 BL/6 mice could be attributed to a more potent NK-cell mediated cytotoxicity against B16F10 cells. Our findings highlight the role of NK cells in innate anti-tumor immunity in the context of the liver - particularly against highly aggressive MHC I-deficient cancer cells. Moreover, the B16F10 model of melanoma liver metastasis is suited for developing novel therapies targeting innate NK cell related immunity in liver metastases and liver cancer. [ABSTRACT FROM AUTHOR]

Published

2018

2. Designing a Path to an Economically, Socially and Environmentally Sustainable Plan for Accessible Storage at Winterthur Museum, Garden and Library.

Author

Wickens, Joelle D. J., Parker Miller, Beth J., Castle, John W., and Eaton, Linda

Subjects

HENRY Francis du Pont Winterthur Museum Gardens (Del.), SUSTAINABLE architecture, PROTECTION of cultural property, PRESERVATION of museum architecture, PRESERVATION of historic buildings, GOVERNMENT policy

Abstract

The article focuses on the development of a sustainable project for improving the storage at the historic site Winterthur Museum, Garden and Library created by Henry Francis du Port. Topics include the history of the museum building acquired by the du Pont family in 1810, the architectural features of the museum building, and the initiatives for the preservation of the Winterthur Museum, Garden and Library. It offers information on the application of the Collection Policy for the preservation of the historic site.

Published

2018

3. Designing a Path to an Economically, Socially and Environmentally Sustainable Plan for Accessible Storage at Winterthur Museum, Garden and Library.

Author

Parker Miller, Beth J., Castle, John W., Eaton, Linda, and Wickens, Joelle D. J.

Subjects

*MUSEUM collection accessibility, *ART conservation & restoration, *CULTURAL property, *SUSTAINABILITY

Abstract

The article focuses on the sustainability for accessible storage in the Winterthur Museum, Garden and Library made by Henry Francis du Pont. It discusses the history of this cultural property which has research library, collection of decorative arts objects, historic home and museum galleries, the need for developing the method for collection care, trying to improve the accessibility to storage spaces and attaining viability for the institution by accessing social sustainability. It also talks about the process led by project leadership team for curatorial, registration and conservation fellows.

Published

2018

4. Monitoring changes in greater Yellowstone lake water quality following the 1988 wildfires.

Author

Lathrop, Richard G., Vande Castle, John D., and Brass, James A.

Published

1994

5. Responsiveness to anti-PD-1 and anti-CTLA-4 immune checkpoint blockade in SB28 and GL261 mouse glioma models.

Author

Genoud, Vassilis, Marinari, Eliana, Nikolaev, Sergey I, Castle, John C., Bukur, Valesca, Dietrich, Pierre-Yves, Okada, Hideho, and Walker, Paul R.

Subjects

GLIOBLASTOMA multiforme treatment, CANCER immunotherapy, CYTOTOXIC T lymphocyte-associated molecule-4

Abstract

Immune checkpoint blockade (ICB) is currently evaluated in patients with glioblastoma (GBM), based on encouraging clinical data in other cancers, and results from studies with the methylcholanthrene-induced GL261 mouse glioma. In this paper, we describe a novel model faithfully recapitulating some key human GBM characteristics, including low mutational load, a factor reported as a prognostic indicator of ICB response. Consistent with this observation, SB28 is completely resistant to ICB, contrasting with treatment sensitivity of the more highly mutated GL261. Moreover, SB28 shows features of a poorly immunogenic tumor, with low MHC-I expression and modest CD8+ T-cell infiltration, suggesting that it may present similar challenges for immunotherapy as human GBM. Based on these key features for immune reactivity, SB28 may represent a treatment-resistant malignancy likely to mirror responses of many human tumors. We therefore propose that SB28 is a particularly suitable model for optimization of GBM immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2018

6. A catalog of HLA type, HLA expression, and neo-epitope candidates in human cancer cell lines.

Author

Boegel, Sebastian, Löwer, Martin, Bukur, Thomas, Sahin, Ugur, and Castle, John C

Subjects

CANCER cells, HLA histocompatibility antigens, SOMATIC mutation, IMMUNOTHERAPY, RNA sequencing, CELL lines, GENE expression

Abstract

Cancer cell lines are a tremendous resource for cancer biology and therapy development. These multipurpose tools are commonly used to examine the genetic origin of cancers, to identify potential novel tumor targets, such as tumor antigens for vaccine devel­opment, and utilized to screen potential therapies in preclinical studies. Mutations, gene expression, and drug sensitivity have been determined for many cell lines using next-generation sequencing (NGS). However, the human leukocyte antigen (HLA) type and HLA expression of tumor cell lines, characterizations necessary for the development of cancer vaccines, have remained largely incomplete and, such information, when available, has been distributed in many publications. Here, we determine the 4-digit HLA type and HLA expression of 167 cancer and 10 non-cancer cell lines from publically available RNA-Seq data. We use standard NGS RNA-Seq short reads from “whole transcriptome” sequencing, map reads to known HLA types, and statistically determine HLA type, heterozygosity, and expression. First, we present previously unreported HLA Class I and II genotypes. Second, we determine HLA expression levels in each cancer cell line, providing insights into HLA downregulation and loss in cancer. Third, using these results, we provide a fundamental cell line “barcode” to track samples and prevent sample annotation swaps and contamination. Fourth, we integrate the cancer cell-line specific HLA types and HLA expression with available cell-line specific mutation information and existing HLA binding prediction algorithms to make a catalog of predicted antigenic mutations in each cell line. The compilation of our results are a fundamental resource for all researchers selecting specific cancer cell lines based on the HLA type and HLA expression, as well as for the development of immunotherapeutic tools for novel cancer treatment modalities. [ABSTRACT FROM PUBLISHER]

Published

2014