Katy Hayward scite author profile

Aims/hypothesis This study used proteomics and biochemical approaches to identify novel glucose-regulated proteins and to unveil their role in pancreatic beta cell function. Translationally controlled tumour protein (TCTP) was identified to be one such protein, and further investigations into its function and regulation were carried out. Methods Global protein profiling of beta cell homogenates following glucose stimulation was performed using twodimensional gel electrophoresis. Proteins were identified by mass spectroscopy analysis. Immunoblotting was used to investigate alterations in TCTP protein levels in response to glucose stimulation or cell stress induced by palmitate. To investigate the biological function of TCTP, immunolocalisation, gene knockdown and overexpression of Tctp (also known as Tpt1) were performed. Apoptosis was measured in Tctp knockdown or Tctp-overexpressing cells. Glucosestimulated insulin secretion was carried out in Tctp knockdown cells. Results TCTP was identified as a novel glucose-regulated protein, the level of which is increased at stimulatory glucose concentration. Glucose also induced TCTP dephosphorylation and its partial translocation to the mitochondria and the nucleus. TCTP protein levels were downregulated in response to cell stress induced by palmitate or thapsigargin treatments. Gene knockdown by small interfering RNA led to increased apoptosis, whereas overproduction of TCTP prevented palmitate-induced cell death. Conclusions/interpretation Regulation of TCTP protein levels by glucose is likely to be an important cyto-protective

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MyRIP interaction with MyoVa on secretory granules is controlled by the cAMP-PKA pathway

Brozzi

Lajus

Diraison

et al. 2012

MBoC

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Katy Hayward

Translationally controlled tumour protein (TCTP) is a novel glucose-regulated protein that is important for survival of pancreatic beta cells

MyRIP interaction with MyoVa on secretory granules is controlled by the cAMP-PKA pathway

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