Functional data are summarized in Table 2. contraction [25, 28, 8, 27] graded effect [54]; contraction [52] No resistance to U46619, ET-1, and 5HT [55] ATP-induced in resistance attenuated [55] No change (PGI2 induced tone) [55] U46619-induced contraction [70] No basal tone [9, 10] No sensitivity to SNP [70] Relaxation in pressurized vessels [68] Dilatation of large placental arteries [16] No contraction to U46619 [70] sensitivity to SNP [70] Contraction in pressurized vessels

[68] 4AP mimics contraction effect of hypoxia [25] 4AP perfusion pressure [4] 4AP basal tone in control only [69] 4AP basal tone and ET-1-induced contraction [58] ScTX-1; MgTX; COR no basal tone effect [36] ScTX-1; MgTX U46619-induced contraction [36] 4AP basal tone in control only [69] ScTX-1; MgTX; COR no basal tone effect Dasatinib chemical structure [36] COR U46619-induced

contraction [36] 4AP sig. IK [25]; hypoxia did NOT IK further in presence of 4AP [25] 4AP sig. IK in CPA VSMC [5] PIN basal tone (low/control) and relaxes U46619-induced contraction (high/low; not control) [69, 72] GLIB U46619-, 3-deazaneplanocin A order AVP- and ET-1-induced contraction [72] GLIB no effect on SNAP –induced relaxation [58] KRN2391 basal tone; U46619-induced contraction [33] CROM no basal tone effect; desensitized U46619-induced contraction [33] KRN4884 no basal tone effect; desensitized U46619-induced contraction [33] PIN basal tone and U46619 contraction (high/low; not control) [69] KRN2391 basal tone (control) and U46619-induced contraction [33] CROM

no basal tone effect; U46619-induced contraction [33] KRN4884 no basal tone effect; U46619-induced contraction [33] No whole-cell KATP currents observed [25] GLIB-sensitive alteration in VSMC but not EC Vm [20] IbTX no effect on basal tone [69] IbTX max U46619 contraction in control only; no effect high/low [69] CTX SNAP-induced relaxation [58] IbTX slightly IK in small and large arteries [25] TEA; IbTX; CTX; 1-EBIO; TRAM-34 modify IK in CPA VSMC [5] In support of the Pyruvate dehydrogenase placental perfusion data, the presence of KATP channels was demonstrated by inhibition of agonist-induced contraction with glibenclamide [72]. Subsequent studies found reduced basal tone of chorionic plate arteries and veins with pinacidil and KRN2391; in addition, precontracted vessels were demonstrated to significantly relax upon exposure to pinacidil, KRN2391, and cromakalim [69, 33]. The observation that calcitonin gene-related peptide-induced alterations in isolated placental artery and venous reactivity are also partially mediated by KATP channel activation [13] lends further weight to the notion that KATP channel activation modifies blood vessel tone in both arms of the fetoplacental circulation.