Cynthia Osmanian scite author profile

Apoptosis is a genetically encoded programme of cell death that can be activated under physiological conditions and may be an important safeguard against tumour development. Regions of low oxygen (hypoxia) and necrosis are common features of solid tumours. Here we report that hypoxia induces apoptosis in oncogenically transformed cells and that further genetic alterations, such as loss of the p53 tumour-suppressor gene or overexpression of the apoptosis-inhibitor protein Bcl-2, substantially reduce hypoxia-induced cell death. Hypoxia also selects for cells with defects in apoptosis, because small numbers of transformed cells lacking p53 overtake similar cells expressing wild-type p53 when treated with hypoxia. Furthermore, highly apoptotic regions strongly correlate with hypoxic regions in transplanted tumours expressing wild-type p53, whereas little apoptosis occurs in hypoxic regions of p53-deficient tumours. We propose that hypoxia provides a physiological selective pressure in tumours for the expansion of variants that have lost their apoptotic potential, and in particular for cells acquiring p53 mutations.

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142 The role of hypoxia, p53, and apoptosis in human cervical carcinoma pathogenesis

Kim¹,

Tsai²,

Osmanian³

et al. 1997

International Journal of Radiation Oncology*Biology*Physics

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Hypoxia in a tumor may promote emergence of clones with p53 gene mutation

Kw¹,

Vogelstein²,

Tg³

et al. 1996

Advances in Anatomic Pathology

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