On the stimulatory effect of microglial cells on angiogenesis
Abstract
ABSTRACT
Angiogenesis, the process by which new vessels sprout from pre-existing
vessels, is fundamental to development, tissue growth and repair. The main
aim of this thesis was to investigate the role of microglia on angiogenesis.
We adapted the rat ex vivo/in vitro aortic ring model to the mouse in a 3-D
culture system. In paper I, we show that ablation of microglia in the retina
leads to a poorly developed vascular network. The aortic ring model,
supplied with microglia, demonstrated that microglia have a direct positive
effect on angiogenic sprouting. The angiogenic effect was mediated by
soluble factor/factors, and cell-cell contacts were not required. We also
show that the microglia-derived angiogenic factor(s) is distinct from
vascular endothelial growth factor-A. Moreover, the sprouting aortic ring
induces oriented migration of microglia towards the aortic ring. In paper II,
we analysed the microglia transcriptome. We found that microglia express
known activators and inhibitors of angiogenesis that might have a role in
retinal blood vessel development. The aortic ring system was also used as a
complement to in vivo analyses to address the function of sphingosine-1-
phosphate receptor 1 (S1P1) on angiogenesis (paper III). The results
indicate that S1P1 is required within endothelial cells to counteract VEGFA-
signalling and prevent endothelial hyper-sprouting. In paper IV,
expression of green fluorescent protein in endothelial/hematopoietic cells
using Tie2-Cre was used to mark transplanted bone marrow-derived cells.
The study aimed to address if grafted bone marrow derived cells can
differentiate into pancreatic β-cells in mice. The major part of the thesis
concerns the establishment and use of the mouse aortic ring as a model for
angiogenesis. Importantly, application of the system enabled us to identify
a direct positive effect of microglia on angiogenesis and to test putative
modifiers. This could be further pursued by microarray analyses. The
presented work might therefore provide a platform for the identification of
molecules that regulate angiogenesis.
Key words: microglia, angiogenesis, aortic ring.
ISBN: 978-91-628-8285-3
Parts of work
I. Rymo SF, Gerhardt H, Wolfhagen Sand F, Lang R, Uv A, Betsholtz C. (2011). A two-way communication between microglial cells and angiogenic sprouts regulates angiogenesis in aortic ring cultures.PLoS One. 2011 Jan 10;6(1):e15846.::PMID::21264342 II. Simin F. Rymo, Zulfeghar A. Syed, Anne Uv and Christer Betsholtz.
A transcriptional profiling approach to identify microglia-derived factors that stimulate
angiogenesis in aortic ring cultures.
Manuscript III. Konstantin Gaengel, Kazuhiro Hagikura, Colin Niaudet, Lars Muhl, Staffan Nyström, Simin
F. Rymo, Bàrbara Laviňa Siemsen, Jennifer Hofmann, Lwaki Ebarasi, Long Long Chen,
Karin Strittmatter, Guillem Genove, Pernilla Roswall, Peter Lönneberg, Per Uhlen, Anne
Uv, Arindam Majumdar, Richard L. Proia and Christer Betsholtz.
S1P1 is a critical regulator of angiogenesis.
Manuscript IV.Rosengren AH, Taneera J, Rymo S, Renström E. (2009). Bone marrow transplantation stimulates pancreatic β-cell replication after tissue damage.Islets. 2009 Jul-Aug;1(1):10-8.::PMID::21084844
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Biomedicine. Department of Medical Biochemistry and Cell Biology
Disputation
Tid: 2011-06-16 kl 13:00, Plats: Medicinarberget - Arvid Carlsson, Medicinaregatan 3
Date of defence
2011-06-16
simin.rymo@medkem.gu.se
Date
2011-05-26Author
Rymo, Simin
Keywords
microglia
angiogenesis
aortic ring
Publication type
Doctoral thesis
ISBN
978-91-628-8285-3
Language
eng