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Vascular endothelial cells express isoforms of protein kinase A inhibitor
Authors:Lum, Hazel   Hao, Zengping   Gayle, Dave   Kumar, Priyadarsini   Patterson, Carolyn E.   Uhler, Michael D.
Abstract:First published September 5, 2001;10.1152/ ajpcell.00256.2001.---The expression and function of theendogenous inhibitor of cAMP-dependent protein kinase (PKI) inendothelial cells are unknown. In this study, overexpression of rabbitmuscle PKI gene into endothelial cells inhibited the cAMP-mediatedincrease and exacerbated thrombin-induced decrease in endothelialbarrier function. We investigated PKI expression in human pulmonaryartery (HPAECs), foreskin microvessel (HMECs), and brain microvesselendothelial cells (HBMECs). RT-PCR using specific primers for humanPKIalpha , human PKIgamma , and mouse PKIbeta sequences detectedPKIalpha and PKIgamma mRNA in all three cell types. Sequencing and BLASTanalysis indicated that forward and reverse DNA strands for PKIalpha andPKIgamma were of >96% identity with database sequences. RNaseprotection assays showed protection of the 542 nucleotides in HBMEC andHPAEC PKIalpha mRNA and 240 nucleotides in HBMEC, HPAEC, and HMEC PKIgamma mRNA. Western blot analysis indicated that PKIgamma protein was detectedin all three cell types, whereas PKIalpha was found in HBMECs. Insummary, endothelial cells from three different vascular beds expressPKIalpha and PKIgamma , which may be physiologically important inendothelial barrier function.

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