Inhibition of the P2X7 Receptor Reduces Cystogenesis in PKD
Author(s) -
MingYang Chang,
Jenn-Kan Lu,
YaChung Tian,
YungChang Chen,
Cheng-Chieh Hung,
Yihui Huang,
YauHung Chen,
Mai-Szu Wu,
ChihWei Yang,
YiChuan Cheng
Publication year - 2011
Publication title -
journal of the american society of nephrology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 4.451
H-Index - 279
eISSN - 1533-3450
pISSN - 1046-6673
DOI - 10.1681/asn.2010070728
Subject(s) - zebrafish , morpholino , pronephros , biology , agonist , medicine , endocrinology , gene knockdown , polycystic kidney disease , autosomal dominant polycystic kidney disease , microbiology and biotechnology , purinergic receptor , receptor , cancer research , kidney , cell culture , adenosine , biochemistry , genetics , gene
The P2X7 receptor participates in purinergic signaling, which may promote the progression of ADPKD. We examined the effects of a P2X7 receptor antagonist and a P2X7 receptor agonist on cyst development in a zebrafish model of polycystic kidney disease in which we knocked down pkd2 by morpholinos. We used live wt-1b pronephric-specific GFP-expressing zebrafish embryos to directly observe changes in the pronephros. Exposure of pkd2-morphant zebrafish to a P2X7 receptor antagonist (oxidized ATP [OxATP]) significantly reduced the frequency of the cystic phenotype compared with either exposure to a P2X7 receptor agonist (BzATP) or with no treatment (P < 0.01). Histology confirmed improvement of glomerular cysts in OxATP-treated pkd2 morphants. OxATP also reduced p-ERK activity and cell proliferation in pronephric kidneys in pkd2 morphants. Inhibition of P2X7 with an additional specific antagonist (A-438079), and through morpholino-mediated knockdown of p2rx7, confirmed these effects. In conclusion, blockade of the P2X7 receptor reduces cyst formation via ERK-dependent pathways in a zebrafish model of polycystic kidney disease, suggesting that P2X7 antagonists may have therapeutic potential in ADPKD.
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