Adult Stem Cells
Adult Stem Cells
Institute of Cell and Molecular Science Centre for Diabetes & Metabolic Medicine - London PDF Print E-mail
Centre for Diabetes & Metabolic Medicine
Institute of Cell and Molecular Science
Barts and The London School of Medicine and Dentistry
4 Newark Street
London
E1 2AT

Director:



Professor Malcolm R. Alison, BSc, PhD, DSc, FRCPath

Background of Director:

After receiving his PhD in Newcastle, Dr. Alison spent over 20 years at Hammersmith Hospital (RPMS and Imperial) moving from lecturer to professor of Experimental Pathology. Heavily involved in undergraduate and postgraduate teaching throughout, Dr. Alison developed interests in endodermal (particularly liver) stem cells and wound healing. In September 2004, as part of a 'stem cell initiative' he was appointed professor of Stem Cell Biology within the Centre for Diabetes and Metabolic Medicine at QMUL with a remit to study stem cells in diabetes.

Current Projects:

Our research covers liver and pancreatic stem cell biology with particular reference to diabetes, end-stage fibrotic disease and cancer.
  • With regard to stem cell identity and location in pancreas and liver, we aim to employ a series of novel markers to aid stem cell identification which is presently proving intractable, particularly in the pancreas.
  • Concurrently we aim to identify the stem cell niche through examination of signaling pathways (Wnts, Hhs and Notch/Delta) at the mRNA and protein level; and study the role of particular non-parenchymal sub-populations through their selective deletion (collaboration with Stuart Forbes and John Iredale, Edinburgh). These endeavors will be supported by our studies of mitochondrial (mt) DNA mutations that accumulate with age within our cells, elucidating patterns of cellular inheritance and clonal expansion in the normal and diseased human pancreas and liver, and high-resolution synchotron radiation-based Fourier transform infrared microspectroscopy that detects subtle intracellular changes in macromolecules based upon variations in levels of absorption of infrared radiation, appearing to be a robust means of identifying stem cells - collaboration with The University of Lancaster.
  • We are currently generating a transgenic mouse model using an inducible Cre-loxP system based upon the CK19 promoter to investigate the possible ductal origin of b–cells.
  • We have several collaborations with groups both within and outwith ICMS, including investigations into the Accelerator Hypothesis in the NOD mouse model of T1D and the potential of transplanted bone marrow cells to undergo vasculogenesis in tissue regeneration in inflammatory bowel disease and diabetes.
  • In collaboration with David Fine (Southampton) we are developing a murine model of pancreatitis and fibrosis, building upon our previous studies in the liver that proposed that the bone marrow was a major source of fibrogenic cells and that the genotype of the bone marrow could influence the liver's fibrogenic response to injury.
  • We are also investigating cancer stem cells in human pancreatic cell lines, and are looking at the roles of stellate (niche) cells (from both pancreas and liver) in modulating cancer stem cell behavior (collaboration with Albert Geerts, Vrije Universiteit, Brussels).


Website:

http://www.icms.qmul.ac.uk/Profiles/Diabetes/Alison%20Malcolm.htm

 
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Adult Stem Cells
Adult Stem Cells

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