2004
DOI: 10.1016/j.prostaglandins.2003.11.002
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Effects of platelet-activating factor and thromboxane A2 on isolated perfused guinea pig liver

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Cited by 21 publications
(17 citation statements)
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“…Although PAF substantially increased P pv in isolated perfused mouse livers (Fig. 3), the increase was much smaller than that in rats (6), dogs (29), and guinea pigs (22): the peak R t after PAF was 1.4 times baseline in mice, 3.7 times baseline in rats (6), 3.3 times baseline in dogs (29), and 5.1 times baseline in guinea pigs (22). Further studies on structural and functional mechanisms for weak reactivity of the mouse hepatic vessels are required to determine the amount and distribution of vascular smooth muscle cells and receptors for anaphylactic vasoactive substances and vasoreactivity to those individual substances in the mouse portal and hepatic veins.…”
Section: Discussionmentioning
confidence: 75%
“…Although PAF substantially increased P pv in isolated perfused mouse livers (Fig. 3), the increase was much smaller than that in rats (6), dogs (29), and guinea pigs (22): the peak R t after PAF was 1.4 times baseline in mice, 3.7 times baseline in rats (6), 3.3 times baseline in dogs (29), and 5.1 times baseline in guinea pigs (22). Further studies on structural and functional mechanisms for weak reactivity of the mouse hepatic vessels are required to determine the amount and distribution of vascular smooth muscle cells and receptors for anaphylactic vasoactive substances and vasoreactivity to those individual substances in the mouse portal and hepatic veins.…”
Section: Discussionmentioning
confidence: 75%
“…For example, with respect to PAF, which caused a substantial increase in PPV in isolated perfused mouse livers, 1,4 the increase was much smaller than that in rats, 6 dogs, 18 and guinea pigs 9 : the peak portal-to-hepatic vein resistance levels after PAF injection were 1.4-fold the baseline in mice, 1 3.7-fold in rats, 6 3.3-fold in dogs, 19 and 5.1-fold in guinea pigs. 9 One of the limitations of the present study is that the same size catheter was used for PPV measurement in different size of mouse and rats. Although the resistance due to catheter itself at the insert portion of the portal vein should be relatively larger in mouse than in rat, the length of the catheter inserted was as short as 5 mm.…”
Section: Discussionmentioning
confidence: 93%
“…1 In addition, we previously demonstrated that the response of PPV in isolated perfused mouse liver to the vasoactive substances of norepinephrine (NE), 3 histamine, 3 PAF, 1,4 and thromboxane A 2 analogue 5 was much weak as compared with that in other mammals such as rat, 4-7 rabbit, 8 and guinea pig. 4,5,7,9 The passive blood mobilization to and from the liver, which influences the venous return to the heart, is critically dependent on the location and magnitude of intrahepatic vascular resistances, the changes of which could be produced by hepatic venoconstriction. 10 Thus, it is important to investigate the characteristics of the hepatic venoconstriction in response to physiological vasoactive agonists in mice.…”
Section: Introductionmentioning
confidence: 99%
“…In guinea pig livers, the anaphylactic presinusoidal constriction may be caused mainly by PAF, whereas the postsinusoidal constriction is caused by cysteinyl leukotrienes (19). Actually, PAF predominantly contracts presinusoidal vessels in guinea pig livers (17). However, effects of anaphylaxis-related vasoactive substances are not currently known on the segmental vascular resistances of rat livers.…”
Section: Discussionmentioning
confidence: 98%