Characterization of the P<sub>2</sub> receptors in rabbit pulmonary artery

Qasabian, Raffi; Schyvens, Christopher G.; Owe-Young, R; Killen, James; Macdonald, Peter S.; Conigrave, Arthur D.; Williamson, Dominic J.

doi:10.1038/sj.bjp.0700924

Cited by 24 publications

(22 citation statements)

References 40 publications

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“…Exchange systems were mediated by P-2 purinoceptors (Jeffrey et al 1994;Bhagwat & Williams 1997). Suramin is an antagonist ligand for P-2 purinoceptors located on endothelial cell and brain astrocyte membranes (King et al 1996;Centemeri et al 1997;Qasabian et al 1997), and could have altered this selective transport for the passage of some molecules including megazol. In the trypanosome, megazol is recognized by another P2 purine transporter (Carter et al cells in the parenchymal perivascular spaces (Figure 1a,c).…”

Section: Resultsmentioning

confidence: 99%

Megazol combined with suramin: a chemotherapy regimen which reversed the CNS pathology in a model of human African trypanosomiasis in mice

Enanga

Keita

Chauvière

et al. 1998

Tropical Med Int Health

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SummaryChemotherapy for human African trypanosomiasis (HAT), or sleeping sickness, is unreliable because of resistance, refraction and toxic and adverse side-effects. Using a long-term experimental model of HAT with involvement of the central nervous system (CNS), we tested the ability of a megazol and suramin combination treatment to eliminate CNS trypanosomes. This consisted of 20 mg suramin per kg body weight administered intraperitoneally (IP), followed 24 h later by 4 daily doses (80 mg/kg) of megazol given either IP or per os. One week post-treatment, neurological disorders had disappeared. One of 15 mice relapsed in each application group at 81 and 98 days after treatment, respectively. At six months, no signs of relapse were seen in remaining mice, indicating that this chemotherapy regimen was curative. Immunohistochemical (astrocytosis) and histological (inflammatory lesions) examinations of brain tissues showed that animals returned to normal from 2 months post-treatment. These results suggest that the megazol-suramin combination reversed the CNS pathology in this model. keywords megazol, suramin, CNS-trypanosomiasis correspondence B. Bouteille,

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Section: Resultsmentioning

confidence: 99%

Megazol combined with suramin: a chemotherapy regimen which reversed the CNS pathology in a model of human African trypanosomiasis in mice

Enanga

Keita

Chauvière

et al. 1998

Tropical Med Int Health

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“…In rabbit pulmonary arteries, relaxation to UTP was endothelium dependent, whereas relaxation to ATP was only partially inhibited by removing the endothelium (Qasabian et al, 1997). In contrast, ATP and 2-MeSATP evoked endothelium-dependent vasodilatation in the rat isolated pulmonary circulation, suggesting an involvement of P2Y 1 receptors; this involved NO but there was no evidence for a role of prostanoids (Hasséssian and Burnstock, 1995;Hakim et al, 1997).…”

Section: J Pulmonary Vesselsmentioning

confidence: 99%

Purinergic Signaling and Blood Vessels in Health and Disease

2013

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“…ATP and UTP, acting via endothelial P2Y 1 , P2Y 2 , and/or P2Y 4 receptors, elicits vasodilation of bovine and rabbit pulmonary arteries, partly via mobilization of intracellular Ca 2ϩ and subsequent prostacyclin release (Lustig et al, 1992;Chen et al, 1996;Qasabian et al, 1997). Shear stress evokes release of ATP from endothelial cells, which causes NO release and pulmonary vasodilation (Hasséssian et al, 1993;Kiefmann et al, 2009).…”

Section: E Vasculaturementioning

confidence: 99%