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Fibroblast Growth Factor 9 Imparts Hierarchy and Vasoreactivity to the Microcirculation of Renal Tumors and Suppresses Metastases
Authors:Hao Yin  Matthew J Frontini  John-Michael Arpino  Zengxuan Nong  Caroline O'Neil  Yiwen Xu  Brittany Balint  Aaron D Ward  Subrata Chakrabarti  Christopher G Ellis  Robert Gros  J Geoffrey Pickering
Institution:From the Robarts Research Institute and ;Departments of §Biochemistry.;Medical Biophysics.;Pathology.;**Physiology and Pharmacology, and ;‡‡Medicine, University of Western Ontario.;§§London Health Sciences Centre, London, Ontario N6A 5A5, Canada
Abstract:Tumor vessel normalization has been proposed as a therapeutic paradigm. However, normal microvessels are hierarchical and vasoreactive with single file transit of red blood cells through capillaries. Such a network has not been identified in malignant tumors. We tested whether the chaotic tumor microcirculation could be reconfigured by the mesenchyme-selective growth factor, FGF9. Delivery of FGF9 to renal tumors in mice yielded microvessels that were covered by pericytes, smooth muscle cells, and a collagen-fortified basement membrane. This was associated with reduced pulmonary metastases. Intravital microvascular imaging revealed a haphazard web of channels in control tumors but a network of arterioles, bona fide capillaries, and venules in FGF9-expressing tumors. Moreover, whereas vasoreactivity was absent in control tumors, arterioles in FGF9-expressing tumors could constrict and dilate in response to adrenergic and nitric oxide releasing agents, respectively. These changes were accompanied by reduced hypoxia in the tumor core and reduced expression of the angiogenic factor VEGF-A. FGF9 was found to selectively amplify a population of PDGFRβ-positive stromal cells in the tumor and blocking PDGFRβ prevented microvascular differentiation by FGF9 and also worsened metastases. We conclude that harnessing local mesenchymal stromal cells with FGF9 can differentiate the tumor microvasculature to an extent not observed previously.
Keywords:angiogenesis  fibroblast growth factor (FGF)  hypoxia  metastasis  tumor microenvironment  vascular biology  microvascular flow  vasoreactivity
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