| Literature DB >> 22642643 |
Er-Ning Su1, Stephen J Cringle, Ian L McAllister, Dao-Yi Yu.
Abstract
BACKGROUND: Vascular endothelial growth factor (VEGF) plays an important role in ocular physiology. Anti-VEGF agents are now used for treatment of common retinal diseases. This study characterises the vasoactive properties of VEGF in isolated perfused pig retinal arterioles under normal tone or endothelin-1 (ET-1) pre-contracted conditions and determines the influence of an anti VEGF agent on VEGF induced vasoactivity.Entities:
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Year: 2012 PMID: 22642643 PMCID: PMC3395563 DOI: 10.1186/1471-2415-12-10
Source DB: PubMed Journal: BMC Ophthalmol ISSN: 1471-2415 Impact factor: 2.209
Figure 1Schematic representation of the isolated perfused vessel system. The isolated pig retinal arteriole is cannulated at both ends and perfused intraluminally whilst maintained in a temperature controlled bath on the stage of an inverted microscope. VEGF can be administered intraluminally via an HPLC valve. ET-1 and bevacizumab are delivered extraluminally by addition to the bathing solution. Vessel diameter is monitored every two seconds by an automated frame grabbing and vessel diameter measurement routine.
Figure 2Concentration response curve of VEGF in retinal arterioles with normal tone. With intraluminal delivery over a concentration range (10-16 – 10-7 M) the level of contraction reduced at higher VEGF concentration, producing a significant dilatation when compared to the maximally contracted state at 10-11 M VEGF. * Denotes a significant contraction compared to initial baseline (p < 0.05).
Figure 3Concentration response curve of VEGF from ET-1 pre-contracted retinal arterioles. In isolated pig retinal arterioles pre-contracted with ET-1 (3 x 10-9 M) VEGF exhibited a concentration dependent vasodilatation response. * Denotes a significant dilatation compared to contracted baseline (p < 0.05).
Figure 4Concentration response curve of VEGF from ET-1 pre-contracted retinal arterioles with extraluminal bevacizumab. In isolated pig retinal arterioles pre-contracted with ET-1 (3 x 10-9 M) VEGF induced a concentration dependent vasodilation response was significantly inhibited by bevacizumab. For ease of comparison the data showing the VEGF induced dilatation in the absence of bevacizumab is also included (grey symbols). * Denotes a significant dilatation compared to contracted baseline (p < 0.05).