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Dive into the research topics where Dirk R. Gewert is active.

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Featured researches published by Dirk R. Gewert.


Melanoma Research | 2005

The prevalence of interferon-alpha transcription defects in malignant melanoma.

Karen L. Price; Meenhard Herlyn; Carolyn L. Dent; Dirk R. Gewert; Claire Linge

The type I interferons, interferon-alpha (IFN-&agr;) and interferon-beta (IFN-&bgr;), are situated on the short arm of chromosome 9, specifically 9p21-22. This locus lies very close to an area that is deleted or rearranged in nearly half of all melanomas tested. The identification of 9p rearrangements in both melanoma precursor lesions (dysplastic naevi) and primary lesions has implicated the 9p locus in the early stages of melanoma development. Recent evidence has demonstrated that metastatic melanoma cell lines have a specific loss of IFN-&agr; gene expression, a defect that appears to occur at the level of transcription. In this study, we examined the expression of IFN-&agr; in cell lines isolated from the various stages of melanoma progression, with a view to determine the prevalence of the IFN-&agr; transcription defects exhibited by malignant melanoma, and to assess whether the loss of IFN-&agr; expression was particular to a certain stage of melanoma progression. We showed that all the melanoma cell lines tested (n=20) demonstrated an inability to express IFN-&agr;, a defect that was reflected in the apparent inactivity of the IFN-&agr; promoter. These defects were found to occur in cells isolated from early melanomas, lending support to the hypothesis that IFN-&agr; has a role in the aetiology of malignant melanoma.


FEBS Journal | 1981

Inhibition of cell division by interferons: Changes in the transport and intracellular metabolism of thymidine in human lymphoblastoid (Daudi) cells.

Dirk R. Gewert; Sanjay Shah; Michael J. Clemens


FEBS Journal | 1984

Inhibition of cell proliferation by interferons

Dirk R. Gewert; Graham Moore; Vivienne J. Tilleray; Michael J. Clemens


Virology | 1999

Activation of the Interferon-Inducible (2′-5′) Oligoadenylate Synthetase by the Epstein–Barr Virus RNA, EBER-1☆

Tyson V. Sharp; Daniel A. Raine; Dirk R. Gewert; Bhavesh Joshi; Rosemary Jagus; Michael J. Clemens


FEBS Journal | 1993

Reversal of the double‐stranded‐RNA‐induced inhibition of protein synthesis by a catalytically inactive mutant of the protein kinase PKR

Tyson V. Sharp; Qiurong Xiao; Ian W. Jeffrey; Dirk R. Gewert; Michael J. Clemens


Journal of Interferon and Cytokine Research | 1996

Relative Transcriptional Inducibility of the Human Interferon-α Subtypes Conferred by the Virus-Responsive Enhancer Sequence

Carolyn L. Dent; Sonya J. Macbride; Nigel A. Sharp; Dirk R. Gewert


FEBS Journal | 1984

Inhibition of cell proliferation by interferons. 2. Changes in processing and stability of newly synthesized DNA in human lymphoblastoid (Daudi) cells.

Graham Moore; Dirk R. Gewert; Michael J. Clemens


FEBS Journal | 1996

A Regulatory Domain within the Virus‐Response Element of the Interferon α1 Gene Acts as a Transcriptional Repressor Sequence and Determinant of Cell‐Specific Gene Expression

Carolyn L. Dent; Dirk R. Gewert


Journal of Cellular Biochemistry | 1988

Relationship of cellular oncogene expression to inhibition of growth and induction of differentiation of Daudi cells by interferons or TPA

Michael J. Clemens; Vivienne J. Tilleray; Robert James; Dirk R. Gewert


FEBS Journal | 1995

Regulation of the Interferon‐indueible Protein Kinase PKR and (2′‐5′)oligo(Adenylate) Synthetase by a Catalytically Inactive PKR Mutant Through Competition for Double‐stranded RNA Binding

Tyson V. Sharp; Qiurong Xiao; Just Justesen; Dirk R. Gewert; Michael J. Clemens

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Tyson V. Sharp

Queen Mary University of London

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Carolyn L. Dent

Johns Hopkins University School of Medicine

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