M. Kunz scite author profile

M. Kunz

5Publications

25Citation Statements Received

91Citation Statements Given

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University of California, Berkeley

Publications

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A Herpesviral induction of RAE-1 NKG2D ligand expression occurs through release of HDAC mediated repression

Greene

Tokuyama

Knudsen

et al. 2016

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Natural Killer (NK) cells are essential for control of viral infection and cancer. NK cells express NKG2D, an activating receptor that directly recognizes NKG2D ligands. These are expressed at low level on healthy cells, but are induced by stresses like infection and transformation. The physiological events that drive NKG2D ligand expression during infection are still poorly understood. We observed that the mouse cytomegalovirus encoded protein m18 is necessary and sufficient to drive expression of the RAE-1 family of NKG2D ligands. We demonstrate that RAE-1 is transcriptionally repressed by histone deacetylase inhibitor 3 (HDAC3) in healthy cells, and m18 relieves this repression by directly interacting with Casein Kinase II and preventing it from activating HDAC3. Accordingly, we found that HDAC inhibiting proteins from human herpesviruses induce human NKG2D ligand ULBP-1. Thus our findings indicate that virally mediated HDAC inhibition can act as a signal for the host to activate NK-cell recognition.DOI: http://dx.doi.org/10.7554/eLife.14749.001

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Role of microRNA in melanoma progression

Kunz¹,

Schultz²,

Ibrahim³

2006

Melanoma Research

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Abstracts

Silginer¹,

S²,

Hasenbach³

et al. 2012

Neuro-Oncology

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Integrins have become a target for novel therapeutic strategies against malignant gliomas. Cilengitide, a synthetic Arg-Gly-Asp (RGD)-motif peptide, interferes with ligand binding to avb3 and avb5 integrins and is currently investigated in clinical trials. Integrins may also be involved in the activation of transforming growth factor (TGF)-b, a mediator of invasiveness and immune escape of glioma cells. Using flow cytometry, we demonstrate that the target integrins of cilengitide are expressed not only in glioblastoma blood vessels, but also by tumor cells. After exposure of glioma cells to cilengitide, we noticed reduced phosphorylation of Smad2 in most glioma cell lines, including stem-like glioma cells. Phophorylation of Smad2, but not cilengitide-induced detachment, is rescued by addition of recombinant TGF-b. Administration of cilengitide to glioma cells results in reduced TGF-b-mediated reporter gene activity. Furthermore, exposure to cilengitide leads to decreased TGF-b 1 and TGF-b 2 mRNA and protein expression. These effects are mimicked by blocking av, b3 or b5 antibodies or by silencing of integrins av, b3, b5 or b8 using RNA interference. Treatment of mice bearing experimental LN-308 glioma xenografts with cilengitide results in reduced pSmad2 levels. Taken together, cilengitide may exert anti-invasive and immune stimulatory activity in human glioblastoma patients by its anti-TGF-b properties.

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Author response: A Herpesviral induction of RAE-1 NKG2D ligand expression occurs through release of HDAC mediated repression

Greene

Tokuyama

Knudsen

et al. 2016

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Identification of osteopontin-dependent cell cycle molecules in malignant melanoma

Kunz¹,

Schultz²,

Gross³

et al. 2006

Melanoma Research

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M. Kunz

A Herpesviral induction of RAE-1 NKG2D ligand expression occurs through release of HDAC mediated repression

Role of microRNA in melanoma progression

Abstracts

Author response: A Herpesviral induction of RAE-1 NKG2D ligand expression occurs through release of HDAC mediated repression

Identification of osteopontin-dependent cell cycle molecules in malignant melanoma

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