G. Gobe scite author profile

G. Gobe

5Publications

55Citation Statements Received

75Citation Statements Given

How they've been cited

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137

Affiliations

University of Queensland, Griffith University, Kitasato University

Publications

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Comparative alterations in p53 expression and apoptosis in the irradiated rat small and large intestine

Arai

Kida²,

Harmon³

et al. 1996

Br J Cancer

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Summary Temporal and spatial relationships between radiation-induced apoptosis and expression of p53 mRNA and protein were compared in rat small and large intestine. Apoptosis was quantified using morphological criteria, and p53 expression determined by immunohistochemistry or whole-tissue Northern analysis. In the small intestine, peak levels of apoptosis appeared earlier (4 h) than in the large intestine (6 h). p53 mRNA transcript levels in small and large intestine were not significantly altered from control levels at any time after treatment. However, in treated small and large intestine, cells showed increased positivity for p53 protein, increasing 10-fold over control levels 4-5 h after irradiation. A strong spatial relationship was found between high incidence apoptosis and p53 protein positivity. We compared published data of stem cell population positions for small and large intestine with our results. Target cells for apoptosis and p53 expression occurred at approximately fifth position from the crypt base of the small intestine, a zone coincident with stem cell population. Target cell position for apoptosis and p53 expression in the large intestine was again at fifth or sixth position from the base, but this zone is not the reported stem cell position (first or second position) for large intestine. Results from our model of radiation-induced intestinal apoptosis indicate that p53 protein is closely associated both temporally and spatially with the induction of apoptosis, and support the work of others in suggesting that p53 expression is modulated post-transcriptionally. Furthermore, our results support a hypothesis that apoptotic targeting of damaged stem cell populations, early response for apoptotic removal of DNA-damaged cells and/or early repair of these damage cells are all important parameters that determine differences in levels of tumorigenesis in the small and large intestine.

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Interrelationship between Epstein–Barr virus infection in gastric carcinomas and the expression of apoptosis‐associated proteins

et al. 2001

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Renal cell carcinoma: Resistance to therapy, role of apoptosis, and the prognostic and therapeutic target potential of TRAF proteins

et al. 2012

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P1-94 Adult chronic kidney disease patients have lower birth weight than the general Australian population

Salmi¹,

Hoy²,

Kondalsamy‐Chennakesavan³

et al. 2007

Early Human Development

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Epstein-Barr Virus Infection Is Associated with Increased Apoptosis in Untreated and Phorbol Ester-Treated Human Burkitt′s Lymphoma (AW-Ramos) Cells

Ishii

Gobe

1993

Biochemical and Biophysical Research Communications

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G. Gobe

Comparative alterations in p53 expression and apoptosis in the irradiated rat small and large intestine

Interrelationship between Epstein–Barr virus infection in gastric carcinomas and the expression of apoptosis‐associated proteins

Renal cell carcinoma: Resistance to therapy, role of apoptosis, and the prognostic and therapeutic target potential of TRAF proteins

P1-94 Adult chronic kidney disease patients have lower birth weight than the general Australian population

Epstein-Barr Virus Infection Is Associated with Increased Apoptosis in Untreated and Phorbol Ester-Treated Human Burkitt′s Lymphoma (AW-Ramos) Cells

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