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EDITORIAL FOCUS

RENAL HEMODYNAMICS AND CARDIORENAL INTEGRATION

Inward rectifier currents in pericytes

University of Calgary Smooth Muscle Research Group, Calgary, Alberta, Canada

THE HETEROGENEITY OF THE VASCULATURE in regard to regional variations in the properties of vascular smooth muscle is an area of major interest and is of primary importance in understanding circulatory regulation. The renal microcirculation represents a rather remarkable example of such heterogeneity. In cortical nephrons, the activating mechanisms of the smooth muscle myocytes comprising preglomerular afferent and postglomerular efferent arterioles are strikingly different. Membrane potential and voltage-gated Ca entry play a prominent role in the afferent arteriole but have no apparent influence on the vasoconstrictor responses of the cortical efferent arteriole (13). Major differences also exist between the ion channel expression patterns and properties of cortical versus juxtamedullary efferent arterioles (11). The heterogeneity of renal microvascular mechanism extends beyond the juxtamedullary efferent arterioles to the vascular pericytes regulating the conductance of the descending vasa recta capillaries and medullary blood flow. Unlike the rest of the "postglomerular" circulation, this segment exhibits features similar to the afferent arteriole, and tone is regulated by voltage-gated Ca entry and modulated by factors influencing membrane potential (18). In the present issue, Cao and coworkers (2) report on their continuing investigations of the ionic channels and biophysical properties of the descending vasa recta pericytes, and they present evidence that these smooth muscle-like cells express an inward rectifier potassium conductance.

Potassium channels play an essential role in controlling membrane potential and in regulating cellular functions that are triggered by electrical signaling. This, of course, includes vasoconstrictor responses that are dependent on the activation of voltage-gated calcium channels. Four classes of potassium channels are recognized to be of primary importance in vascular myocytes, voltage-gated (K_V), calcium activated (K_Ca), ATP-sensitive (K_ATP), and inward rectifier (K_IR) K channels. These differing K channel types have unique biophysical characteristics, differing patterns of distribution within the circulation, and play distinct roles in regulating vascular function (5, 6, 10, 14, 19). For example, K_V is activated when the myocyte is depolarized to membrane potentials more positive than that of relaxed perfused arterioles [–45 mV (6)]. The activity of K_Ca is similarly increased by positive shifts in membrane potential, but the activation range is additionally modulated by intracellular Ca²⁺ (14). Thus a physiological role of both K_V and K_Ca is thought to involve a modulation of the agonist- and or pressure-induced membrane depolarization. The activity of K_ATP is not affected by voltage but is altered by intracellular metabolic events, suggesting a role in vascular responses to physiological signals, such as hypoxia (10, 19). The activities of some members of the K_V, K_Ca, and K_ATP families are stimulated by cyclic nucleotide-dependent kinases and inhibited by protein kinase C, contributing to the actions of vasodilator and vasoconstrictor agonists (6, 14, 19). Accordingly, an understanding of physiological regulation of blood vessel function requires knowledge of the individual contributions of diverse K channel types to the membrane potential and information on the regulation of these channels by cell signaling pathways.

In this regard, the study by Cao and coworkers in the present issue (2) represents a significant advance to our understanding of this important region of the renal microcirculation. Previous work from this innovative group has established that membrane depolarization and the activation of voltage-gated Ca channels play major roles in the contractile responses of descending vasa recta pericytes (17, 20, 25), underscoring the importance of the present report. For example, ANG II, which constricts this segment, inhibits pericyte K currents (16), in addition to stimulating a chloride current (24). As discussed in the present article, this group had previously demonstrated that K_ATP exerts a basal influence on the pericyte membrane potential (3), and in the present study, they show an additional significant contribution of K_IR. The bulk of this work is important, not only to our understanding of the renal medullary circulation but, in more general terms, to our understanding of the properties of contractile vascular pericytes. Pericytes are a heterogeneous cell type, exhibiting diverse properties and roles in regard to capillary development and function. We have only begun to appreciate the role of the contractile smooth muscle-like pericytes in blood flow regulation. However, a physiological function of pericytes in regulating renal medullary blood flow is clearly indicated (18), and a similar role is suggested in the retinal circulation (1). To my knowledge, the report by Cao et al. (2) is the first to demonstrate that vascular pericytes express K_IR.

Of the four types of K channel mentioned above, K_IR is unique in that its expression is generally restricted to resistance vessels, and this channel is rarely seen in larger conduit arteries or other smooth muscle types (10, 19). This pattern of distribution suggests a primary importance in regard to physiological responses governing tissue perfusion and blood flow regulation. In this regard the report by Cao et al. (2) is consistent with the role that pericytes are suggested to play in regulating the medullary circulation. Of the vascular K channel types, K_IR is the least characterized, in part, because of its limited distribution and the difficulties of investigating ion channel regulation in microvessels. For example, although protein kinase C is known to inhibit the activities of other smooth muscle K-channel types, the potential role of this signaling pathway in the regulation of microvascular K_IR channels is not fully resolved (5). However, the unique biophysical characteristics of K_IR suggest mechanisms contributing to some of its proposed physiological roles. As the name implies, the outward or hyperpolarizing current through this channel is impeded by its rectification properties. Elevations in extracellular K⁺ at the outer vestibule of the channel alter this property, reducing a polyamine block of K⁺ efflux and increasing the outward current passed by the channel (15). The resultant effect is that modest elevations in interstitial K⁺ concentrations are capable of evoking a K-induced hyperpolarization and vasodilation through this mechanism in vessels expressing K_IR (19).

A physiological importance of this phenomenon relates to local regulatory mechanisms. For example in the cerebral microcirculation, increased neural activity can result in modest elevations in extracellular K⁺, eliciting hyperpolarization and vasodilation in the microvasculature feeding this region (19). Whether such a function underlies the role of K_IR in the renal circulation is unexplored. Another potential role for this phenomenon concerns the suggestion that extracellular K⁺ might be the long-sought endothelium-derived hyperpolarizing factor (EDHF). EDHF responses are more prominent in small resistance vessels than in larger conduit vessels, and a major component of this response is dependent on charybdotoxin- and apamin-sensitive endothelial K_Ca channels (12). It has been suggested that endothelial K⁺ efflux via these channels sufficiently elevates K⁺ in the vicinity of K_IR and the electrogenic Na⁺-K⁺-ATPase of the underlying vascular myocytes to trigger a K⁺-induced hyperpolarization and vasodilation (7). For a number of reasons, this postulate, however, remains controversial. For example, many vessels exhibiting EDHF responses do not express K_IR or exhibit K⁺-induced vasodilation (12). Moreover, the EDHF responses seen in vessels exhibiting a strong dependence on K_IR are often not affected by barium. A prime example is the renal afferent arteriole. Barium blockade of K_IR fully prevents K⁺-induced vasodilation (4) but does not affect the charybdotoxin and apamin-sensitive EDHF response of this vessel (23). Whether K_IR contributes to endothelium-dependent responses of the vasa recta is, however, a very interesting question that is prompted by the report by Cao et al. (2).

Another important characteristic of small resistance vessels expressing K_IR is that electrical responses originating at one location can be transmitted along the vessel to evoke vasomotor responses at remote sites. These conducted responses occur over relatively large distances and are generally thought to be mediated by a passive electrotonic current spread through gap junction communications in both the endothelium and underlying myocytes (22). However, the excessive length constants that are often observed also suggest the possibility that a regenerative process may be involved. In this regard, recent studies implicating an essential role of K_IR in conducted hyperpolarization and vasodilation are of considerable interest. As first shown by Rivers et al. (21), the ability of a local application of hyperpolarizing stimuli to elicit remote vasodilatory responses in coronary arterioles is prevented by micromolar concentrations of barium but not other K-channel blocking agents. Horiuchi et al. (9) and Goto et al. (8) demonstrated similar effects of barium in cerebral-penetrating arterioles and small mesenteric arteries, respectively. In each case, K_IR blockade prevented or impaired conducted vasodilation or hyperpolarization, and evidence was presented suggesting a role of K_IR in the underlying myocytes. Of interest, Goto et al. (8) further reported that the effects of barium were not seen in hypertensive animals, and this group exhibited impaired conductance. The mechanisms underlying this apparent dependence of conducted responses on K_IR are not fully understood, but if this represents a general phenomenon, it would be of major importance in regard to our understanding of the specific roles of K_IR in the microcirculation. It is interesting to speculate that if conducted responses are seen in the descending vasa recta and play a physiological role in regulating the medullary circulation, the recent finding by Cao and coworkers (2) that K_IR is a prominent outward current in vasa recta pericytes may have further significance.

FOOTNOTES

Address for reprint requests and other correspondence: R. Loutzenhiser, Dept. of Pharmacology and Therapeutics, Univ. of Calgary Faculty of Medicine, Calgary, Alberta T2N 4N1 Canada (E-mail: rloutzen{at}ucalgary.ca)

REFERENCES

1. Anderson DR. Glaucoma, capillaries and pericytes. 1. Blood flow regulation. Ophthalmologica 210: 257–262, 1996.[ISI][Medline]
2. Cao C, Goo JH, Lee-Kwon W, and Pallone TL. Vasa recta pericytes express a strong inward rectifier K⁺ conductance. Am J Physiol Regul Integr Comp Physiol 290: R1601–R1607, 2006.[Abstract/Free Full Text]
3. Cao C, Lee-Kwon W, Silldorff EP, and Pallone TL. K_ATP channel conductance of descending vasa recta pericytes. Am J Physiol Renal Physiol 289: F1235–F1245, 2005.[Abstract/Free Full Text]
4. Chilton L and Loutzenhiser R. Functional evidence for an inward rectifier potassium current in rat renal afferent arterioles. Circ Res 88:152–158, 2001.[Abstract/Free Full Text]
5. Chrissobolis S and Sobey CG. Inwardly rectifying potassium channels in the regulation of vascular tone. Curr Drug Targets 4: 281–289, 2003.[CrossRef][ISI][Medline]
6. Cole WC, Clement-Chomienne O, and Aiello EA. Regulation of 4-aminopyridine-sensitive, delayed rectifier K⁺ channels in vascular smooth muscle by phosphorylation. Biochem Cell Biol 74: 439–447, 1996.[ISI][Medline]
7. Edwards G and Weston AH. Potassium and potassium clouds in endothelium-dependent hyperpolarizations. Pharmacol Res 49: 535–541, 2004.[CrossRef][ISI][Medline]
8. Goto K, Rummery NM, Grayson TH, and Hill CE. Attenuation of conducted vasodilatation in rat mesenteric arteries during hypertension: role of inwardly rectifying potassium channels. J Physiol 561: 215–231, 2004.[Abstract/Free Full Text]
9. Horiuchi T, Dietrich HH, Hongo K, and Dacey RG Jr. Mechanism of extracellular K⁺-induced local and conducted responses in cerebral penetrating arterioles. Stroke 33: 2692–2699, 2002.[Abstract/Free Full Text]
10. Jackson WF. Potassium channels in the peripheral microcirculation. Microcirculation 12: 113–127, 2005.[ISI][Medline]
11. Jensen BL, Friis UG, Hansen PB, Andreasen D, Uhrenholt T, Schjerning J, and Skott O. Voltage-dependent calcium channels in the renal microcirculation. Nephrol Dial Transplant 19: 1368–1373, 2004.[Free Full Text]
12. McGuire JJ, Ding H, and Triggle CR. Endothelium-derived relaxing factors: a focus on endothelium-derived hyperpolarizing factor(s). Can J Physiol Pharmacol 79: 443–470, 2001.[CrossRef][ISI][Medline]
13. Navar LG. Integrating multiple paracrine regulators of renal microvascular dynamics. Am J Physiol Renal Physiol 274: F433–F444, 1998.[Abstract/Free Full Text]
14. Nelson MT and Quayle JM. Physiological roles and properties of potassium channels in arterial smooth muscle. Am J Physiol Cell Physiol 268: C799–C822, 1995.[Abstract/Free Full Text]
15. Nichols CG and Lopatin AN. Inward rectifier potassium channels. Annu Rev Physiol 59: 171–191, 1997.[CrossRef][ISI][Medline]
16. Pallone TL, Cao C, and Zhang Z. Inhibition of K⁺ conductance in descending vasa recta pericytes by ANG II. Am J Physiol Renal Physiol 287: F1213–F1222, 2004.[Abstract/Free Full Text]
17. Pallone TL and Huang JM. Control of descending vasa recta pericyte membrane potential by angiotensin II. Am J Physiol Renal Physiol 282: F1064–F1074, 2002.[Abstract/Free Full Text]
18. Pallone TL, Zhang Z, and Rhinehart K. Physiology of the renal medullary microcirculation. Am J Physiol Renal Physiol 284: F253–F266, 2003.[Abstract/Free Full Text]
19. Quayle JM, Nelson MT, and Standen NB. ATP-sensitive and inwardly rectifying potassium channels in smooth muscle. Physiol Rev 77: 1165–1232, 1997.[Abstract/Free Full Text]
20. Rhinehart K, Zhang Z, and Pallone TL. Ca²⁺ signaling and membrane potential in descending vasa recta pericytes and endothelia. Am J Physiol Renal Physiol 283: F852–F860, 2002.[Abstract/Free Full Text]
21. Rivers RJ, Hein TW, Zhang C, and Kuo L. Activation of barium-sensitive inward rectifier potassium channels mediates remote dilation of coronary arterioles. Circulation 104: 1749–1753, 2001.[Abstract/Free Full Text]
22. Segal SS. Regulation of blood flow in the microcirculation. Microcirculation 12: 33–45, 2005.[ISI][Medline]
23. Wang X and Loutzenhiser R. Determinants of renal microvascular response to ACh: afferent and efferent arteriolar actions of EDHF. Am J Physiol Renal Physiol 282: F124–F132, 2002.[Abstract/Free Full Text]
24. Zhang Z, Huang JM, Turner MR, Rhinehart KL, and Pallone TL. Role of chloride in constriction of descending vasa recta by angiotensin II. Am J Physiol Regul Integr Comp Physiol 280: R1878–R1886, 2001.[Abstract/Free Full Text]
25. Zhang Z, Rhinehart K, and Pallone TL. Membrane potential controls calcium entry into descending vasa recta pericytes. Am J Physiol Regul Integr Comp Physiol 283: R949–R957, 2002.[Abstract/Free Full Text]

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