D. McAndrew
University of Queensland
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Publication
Featured researches published by D. McAndrew.
Nature Reviews Cancer | 2007
Gregory R. Monteith; D. McAndrew; Helen M. Faddy; Sarah J. Roberts-Thomson
Ca2+ is a ubiquitous cellular signal. Altered expression of specific Ca2+ channels and pumps are characterizing features of some cancers. The ability of Ca2+ to regulate both cell death and proliferation, combined with the potential for pharmacological modulation, offers the opportunity for a set of new drug targets in cancer. However, the ubiquity of the Ca2+ signal is often mistakenly presumed to thwart the specific therapeutic targeting of proteins that transport Ca2+. This Review presents evidence to the contrary and addresses the question: which Ca2+ channels and pumps should be targeted?
Molecular Cancer Therapeutics | 2011
D. McAndrew; Desma Grice; Amelia A. Peters; Felicity M. Davis; Teneale A. Stewart; Michelle Rice; Chanel E. Smart; Melissa A. Brown; Paraic A. Kenny; Sarah J. Roberts-Thomson; Gregory R. Monteith
The entry of calcium into the mammary epithelial cell from the maternal plasma (i.e., calcium influx mechanisms) during lactation is poorly understood. As alterations in calcium channels and pumps are a key feature of some cancers, including breast cancer, understanding these calcium influx pathways may have significance beyond mammary biology. We show that the store-operated calcium influx protein, Orai1, is increased during lactation whereas the Orai1 activator Stim1, but not Stim2, is downregulated. Stim2 siRNA reduced basal calcium levels in a lactation model. Our results suggest that calcium influx is remodeled in mammary epithelial cells during lactation, with calcium influx increased through Orai1, activated by Stim2. Breast cancer cell lines had increased levels of ORAI1. ORAI1 siRNA in breast cancer cells reduced store-operated calcium entry and remodeled the calcium influx associated with invasive stimuli. Analysis of microarray data from 295 breast cancers showed that the transcriptional breast cancer subtype with the poorest prognosis (basal) was associated with an altered relationship between the ORAI1 regulators STIM1 and STIM2, and that women with breast cancers with STIM1high/STIM2low tumors had a significantly poorer prognosis. Our studies show that during lactation there is a remodeling in the nature of calcium influx and that alteration in the ORAI1 influx pathway may be a feature of some breast cancers, particularly those with the poorest prognosis. Our studies suggest that this pathway may be a novel therapeutic target for breast cancer treatment in these women. Mol Cancer Ther; 10(3); 448–60. ©2011 AACR.
Archive | 2008
Gregory R. Monteith; Sarah J. Roberts-Thomson; D. McAndrew
ComBio 2007 | 2007
D. McAndrew; Sarah J. Roberts-Thomson; Gregory R. Monteith
Archive | 2013
Gregory R. Monteith; Sarah J. Roberts-Thomson; D. McAndrew
11th Meeting of the European Calcium Society | 2010
Nicole Luk; D. McAndrew; Amelia A. Peters; Desma Grice; Gregory R. Monteith; Sarah J. Roberts-Thomson
Combio2009 | 2009
D. McAndrew; Paraic A. Kenny; Melissa A. Brown; Chanel E. Smart; Sarah J. Roberts-Thomson; Gregory R. Monteith
ASCEPT 43rd Annual Scientific Meeting 2009 | 2009
Johnathon Bassett; Amelia A. Peters; D. McAndrew; Sarah J. Roberts-Thomson; Gregory R. Monteith
ASCEPT 43rd Annual Scientific Meeting 2009 | 2009
Nicole Luk; D. McAndrew; Amelia A. Peters; Gregory R. Monteith; Sarah J. Roberts-Thomson
The American Society for Cell Biology, 48th Annual Meeting (ASCB 2008) | 2008
D. McAndrew; Sarah J. Roberts-Thomson; Gregory R. Monteith
