1 Eects of the prostanoids on the growth of cultured aortic vascular smooth muscle cells (VSMCs) were examined using mice lacking prostanoid receptors. 3 In VSMCs from wild-type mice, expressions of mRNAs for the EP 4 and TP were most abundant, followed by those for the IP, EP 3 and FP, when examined by competitive reverse transcriptase-PCR. Those for the EP 1 , EP 2 and DP, however, could not be detected. 4 AE1-329, an EP 4 agonist, and cicaprost, an IP agonist, inhibited platelet derived growth factor (PDGF)-induced proliferation of VSMCs from wild-type mice; these inhibitory eects disappeared completely in VSMCs from EP 4 7/7 and IP 7/7 mice, respectively. In accordance with these eects, AE1-329 and cicaprost stimulated cAMP production in VSMCs from wild-type mice, which were absent in VSMCs from EP 4 7/7 and IP 7/7 mice, respectively. 5 Eects of PGE 2 on cell proliferation and adenylate cyclase were almost similar with those of AE1-329 in VSMCs from wild-type mice, which disappeared in VSMCs from EP 4 7/7 mice. 6 PGD 2 inhibited PDGF-induced proliferation of VSMCs from both wild-type and DP 7/7 mice to a similar extent. This action of PGD 2 was also observed in VSMCs from EP4 7/7 and IP 7/7 mice. 7 In VSMCs from wild-type mice, I-BOP, a TP agonist, showed potentiation of PDGF-induced hypertrophy. I-BOP failed to show this action in VSMCs from TP 7/7 mice. 8 The speci®c agonists for the EP 1 , EP 2 or EP 3 , and PGF 2 a showed little eect on the growth of VSMCs. 9 These results show that PGE 2 , PGI 2 and TXA 2 modulate PDGF-induced proliferation or hypertrophy of VSMCs via the EP 4 , IP and TP, respectively, and that the inhibitory eect of PGD 2 on PDGF-induced proliferation is not mediated by the DP, EP 4 or IP.
