Dynamic purine signaling and metabolism during neutrophil-endothelial interactions.

During episodes of hypoxia and inflammation, polymorphonuclear leukocytes (PMN) move into underlying tissues by initially passing between endothelial cells that line the inner surface of blood vessels (transendothelial migration, TEM). TEM creates the potential for disturbances in vascular barrier and concomitant loss of extravascular fluid and resultant edema. Recent studies have demonstrated a crucial role for nucleotide metabolism and nucleoside signaling during inflammation. These studies have implicated multiple adenine nucleotides as endogenous tissue protective mechanisms invivo. Here, we review the functional components of vascular barrier, identify strategies for increasing nucleotide generation and nucleoside signaling, and discuss potential therapeutic targets to regulate the vascular barrier during inflammation.

Introduction

Approximately 70 million PMN exit the vasculature per minute [1]. These inflammatory cells move into underlying tissue by initially passing between endothelial cells that line the inner surface of blood vessels. This process, referred to as transendothelial migration (TEM), is particularly prevalent in inflamed tissues, but also occurs as a natural process of leukocyte mobilization (e.g., bone marrow extravasation). Understanding the biochemical details of leukocyte-endothelial interactions is currently an area of concentrated investigation, and recent studies using genetically modified animals have identified specific molecules which function as ‘bottlenecks’ in the control of the inflammatory response [2]. For example, detailed studies have revealed that the process of leukocyte TEM entails a concerted series of events involving intimate interactions of a series of leukocyte and endothelial glycoproteins that include selectins, integrins, and members of the immunoglobulin supergene family [3-5]. Histologic studies of TEM reveal that PMN initially adhere to endothelium, move to nearby inter-endothelial junctions via diapedesis, and insert pseudopodia into the inter-endothelial paracellular space [6].

Successful TEM is accomplished by temporary PMN self-deformation with localized widening of the inter-endothelial junction. Particularly during episodes of inflammation, TEM has the potential to disturb vascular barrier function and give rise to extravascular fluid extravasation and edema. However, several innate mechanisms have been described to dampen fluid loss during PMN-endothelial interactions [7]. For example, following TEM, adjacent endothelial cells appear to ‘reseal,’ leaving no residual inter-endothelial gaps [6]. These histologic studies are consistent with the observation that leukocyte TEM may result in little or no change in endothelial permeability to macromolecules [8-12]. In the absence of this tight and dynamic control of endothelial morphology and permeability, inter-endothelial gap formation during leukocyte TEM could lead to marked increases in endothelial permeability (Figure 1). However, only limited information exists regarding the biochemical events which maintain and dynamically regulate endothelial permeability in the setting of either PMN activation or TEM [5, 6]. Current studies reveal that activated PMN release soluble factor(s) which support maintenance of endothelial permeability during PMN-endothelial interactions [7, 13, 14]. Several crosstalk pathways have been identified to protect endothelial permeability during inflammation and hypoxia and to dampen excessive fluid loss into the interstitium. Such innate protective pathways share the common strategy to increase intravascular adenosine concentrations and adenosine signaling within the inflamed or hypoxic vasculature [7, 14–18].

Figure 1

Neutrophil (PMN) transendothelial migration (TEM). PMN exit the circulation and move into underlying tissue by passing between endothelial cells. During this process, inter-endothelial gaps have the potential to increase vascular permeability, with resultant tissue edema and organ dysfunction. While the endogenous mechanism(s) which regulate these pathways remain poorly understood, work in recent years has revealed new and previously unappreciated targets for potential therapeutic intervention.

Structural and functional elements of the vascular barrier

The predominant barrier (∼90%) to movement of macromolecules across a blood vessel wall is presented by the endothelium [19, 20]. Passage of macromolecules across a cellular monolayer can occur via either a paracellular route (i.e., between cells) or a transcellular route (i.e., through cells). In non-pathologic endothelium, macromolecules such as albumin (molecular weight ∼65 kD) appear to cross the cell monolayer by passing between adjacent endothelial cells (i.e., paracellular) although some degree of transcellular passage may also occur [21, 22]. Endothelial permeability is determined by cytoskeletal mechanisms that regulate lateral membrane intercellular junctions [23, 24]. Tight junctions, also known as zona occludens, comprise one type of intercellular junction. Transmembrane proteins found within this region which function to regulate paracellular passage of macromolecules include the proteins occludin, and members of the junctional adhesion molecule (JAM) and claudin families of proteins [18]. Tight junctions form narrow, cell-to-cell contacts with adjacent cells and comprise the predominant barrier to transit of macromolecules between adjacent endothelial cells [25]. Endothelial macromolecular permeability is inversely related to macromolecule size. Permeability is also dependent on the tissue of origin. For example, endothelial cells in the cerebral circulation (i.e., bloodYbrain barrier) demonstrate an exceptionally low permeability [26, 27]. Endothelial permeability may increase markedly upon exposure to a variety of inflammatory compounds (e.g., histamine, thrombin, reactive oxygen species, leukotrienes, bacterial endotoxins) or adverse conditions (e.g., hypoxia, ischemia) [6, 19]. Reversible increases in endothelial permeability are produced by administration of cytochalasin or other agents that disrupt cytoskeletal microfilaments [19, 28]. Likewise, increases in endothelial permeability are accompanied by disruption of peripheral actin microfilaments and formation of gaps between adjacent endothelial cells [19, 28]. Administration of compounds that decrease endothelial permeability result in an irregular endothelial cell contour, greater convolution of cell margins, closer cell-to-cell contact, and increased surface area and cell perimeter [28]. These changes in cell morphology are accompanied by a loss of F-actin in stress fibers, ‘ruffling’ of dense peripheral bands of F-actin, and increase in the polymerized actin pool without significant changes in total F-actin endothelial cell content [23, 24]. Interestingly, these changes in intracellular actin are similar to those observed during PMN transendothelial migration [29]. By comparison, thrombininduced increases in permeability result in a centralization (and peripheral loss) of F-actin. Both of these changes (permeability and F-actin distribution) are inhibited by isoproterenol [30]. Phallacidin, an F-actin-stabilizing compound, also markedly attenuates thrombin-induced increases in permeability and accompanying morphologic changes (Figure 1).

In addition to the above components of the vascular barrier, the glycocalyx may play a role in determining movements of fluid and macromolecules across the endothelium. The endothelial glycocalyx is a dynamic extracellular matrix composed of cell surface proteoglycans, glycoproteins, and adsorbed serum proteins, implicated in the regulation and modulation of capillary tube hematocrit, permeability, and hemostasis [31]. As such, increased paracellular permeability of such molecules as water, albumin and hydroxyethyl starch can be observed following experimental degradation of the functional components of the glycocalyx [32], and functional components of this glycocalyx may be dynamically regulated by endogenous mediators such as adenosine [33].

Vascular barrier during inflammation

Ongoing inflammatory responses are characterized by dramatic shifts in tissue metabolism. These changes include large fluctuations in energy supply and demand and diminished availability of oxygen [34]. Such shifts in tissue metabolism result, at least in part, from profound recruitment of inflammatory cell types, particularly myeloid cells such as neutrophils (PMN) and monocytes. The majority of inflammatory cells are recruited to, as opposed to being resident at, inflammatory lesions, and myeloid cell migration to sites of inflammation are highly dependent on hypoxia-adaptive pathways [34, 35]. Consequently, much recent attention has focused on understanding how metabolic changes (e.g., hypoxia) relate to the establishment and propagation of the inflammatory response (Figure 2).

Figure 2

Proposed model of coordinated nucleotide metabolism and nucleoside signaling in posthypoxic endothelial cells. In areas of ongoing inflammation, diminished oxygen supply coordinates the induction of CD39, CD73, and AdoRA2B. At such sites, activated PMN provide a readily available extracellular source of ATP, that through two enzymatic steps results in the liberation of extracellular adenosine. Activation of surface AdoR functions to promote the re-establishment of vascular integrity. Under such circumstances, PMN appear to “close the door after exiting.”

As outlined above, many parallels exist between hypoxic and inflamed tissues [36]. For example, during episodes of hypoxia, polymorphonuclear leukocytes (PMN) are mobilized from the intravascular space to the interstitium, and such responses may contribute significantly to tissue damage during consequent reperfusion injury [13, 37, 38]. Moreover, emigration of PMN through the endo- and epithelial barrier may lead to a disruption of such tissue barriers [39-41] and such a setting creates the potential for extravascular fluid leakage and subsequent edema formation [42, 43]. In contrast, transcriptional pathways mediated by hypoxia-inducible factor (HIF) may serve as a barrierprotective element during inflammatory hypoxia. For example, experimental studies of murine inflammatory bowel diseases have revealed extensive mucosal hypoxia and concomitant HIF-1 activation during colitis [44]. Mice engineered to express decreased intestinal epithelial HIF-1 exhibit more severe clinical symptoms of colitis, while increased HIF levels were protective in these parameters. Furthermore, colons with constitutive activation of HIF displayed increased expression levels of HIF-regulated barrier-protective genes (multidrug resistance gene-1, intestinal trefoil factor, CD73), resulting in attenuated loss of barrier during colitis in vivo. Such studies identify HIF as a critical factor for barrier protection during mucosal inflammation and hypoxia [44].

Barrier disruptive pathways

Macromolecule transit across blood vessels has evolved to be tightly controlled. Relatively low macromolecular permeability of blood vessels is essential for maintenance of a physiologically optimal equilibrium between intravascular and extravascular compartments [45, 46]. Endothelial cells are primary targets for leukocytes during episodes of infection, ischemic or traumatic injury, which all together can result in an altered barrier function. Disturbance of endothelial barrier during these disease states can lead to deleterious loss of fluids and plasma protein into the extravascular compartment. Such disturbances in endothelial barrier function are prominent in disorders such as shock and ischemia-reperfusion and contribute significantly to organ dysfunction [47-51]. Previous studies have indicated that activated PMN release a number of soluble mediators, which dynamically influence vascular permeability during transmigration. As such, PMN have been shown to liberate factors that can either disrupt or protect the endothelial barrier: For example, it was recently shown that activation of PMN through β2-integrins elicits the release of soluble factor(s) which induce endothelial cytoskeletal rearrangement, gap formation and increased permeability [52]. This PMN-derived permeabilizing factor was subsequently identified as heparin-binding protein (HBP), also called azurocidin or CAP37 [52], a member of the serprocidin family of cationic peptides [53]. HBP, but not other neutrophil granule proteins (e.g., elastase, cathepsin G), was shown to induce Ca2+-dependent cytoskeletal changes in cultured endothelia and to trigger macromolecular leakage in vivo. Interestingly, HBP regulation of barrier may not be selective for PMN, and in fact, endothelial cells themselves are now a reported source of HPB [54]. It is therefore possible that endothelia may self-regulate permeability through HBP under some conditions, and that mediators found within the inflammatory milieu may also increase endothelial permeability.

Similarly, PMNs were observed to significantly alter endothelial permeability by release of glutamate, following FMLP activation. This crosstalk pathway appears to be of particular importance for the regulation of the vascular barrier of the brain (“blood-brain barrier”). In fact, treatment of human brain endothelia with glutamate or selective, mGluR group I or III agonists resulted in a time-dependent loss of phosphorylated vasodilator-stimulated phosphoprotein (VASP) and significantly increased endothelial permeability. Glutamate-induced decreases in brain endothelial barrier function and phosphorylated VASP were significantly attenuated by pretreatment of human brain endothelia with selective mGluR antagonists. Even in an in vivo hypoxic mouse model, the pretreatment with mGluR antagonists significantly decreased fluorescein isothiocyanate-dextran flux across the blood-brain barrier, suggesting that activated human PMNs release glutamate and that endothelial expression of group I or III mGluRs function to decrease human brain endothelial VASP phosphorylation and barrier function [13].

A recently described gene regulatory pathway revealed a critical role for BMK1/ERK5 in maintaining the endothelial barrier and blood vessel integrity: A targeted deletion of big mitogen-activated protein kinase1 gene (BMK1) (also known as ERK5, member of the MAPK family), in adult mice leads to disruption of the vascular barrier. Histological analysis of these mice revealed that, after BMK1 ablation, hemorrhages occurred in multiple organs in which endothelial cells lining the blood vessels became round, irregularly aligned, and, eventually, apoptotic. In vitro removal of BMK1 protein also led to the death of endothelial cells partially due to the deregulation of transcriptional factor MEF2C, which is a direct substrate of BMK1. Additionally, endothelial-specific BMK1-deletion leads to cardiovascular defects identical to that of global BMK1-deletion. Taken together, these studies identify the BMK1 pathway as critical for endothelial function and for maintaining blood vessel integrity [55].

Barrier protective pathways

Acute increases in vascular permeability to macromolecules closely coincides with tissue injury of many etiologies, and can result in fluid loss, edema, and organ dysfunction [19, 56, 57]. Previous studies have indicated that extracellular nucleotide metabolites may function as an endogenous protective mechanism during hypoxia and ischemia [58-60]. One important factor may be increased production of endogenous adenosine, a naturally occurring anti-inflammatory agent [60-62]. Several lines of evidence support this assertion. First, adenosine receptors are widely expressed on target cell types as diverse as leukocytes, vascular endothelia, and mucosal epithelia and have been studied for their capacity to modulate inflammation [63]. Second, murine models of inflammation provide evidence for adenosine receptor signaling as a mechanism for regulating inflammatory responses in vivo. For example, mice deficient in the A2A-adenosine receptor (AdoRA2A) show increased inflammation-associated tissue damage [64]. Third, hypoxia is a common feature of inflamed tissues [34] and is accompanied by significantly increased levels of adenosine [65-67]. At present, the exact source of adenosine is not well defined, but likely results from a combination of increased intracellular metabolism and amplified extracellular phosphohydrolysis of adenine nucleotides via surface ecto-nucleotidases.

The vascular endothelium is the primary interface between a hypoxic insult and the surrounding tissues. At the same time, the endothelium is central to the orchestration of leukocyte trafficking in response to chemotactic stimuli. This critical anatomic location places vascular endothelial cells in an ideal position to coordinate extracellular metabolic events important to endogenous anti-inflammatory responses. We recently identified a neutrophilYendothelial cell crosstalk pathway that is coordinated by hypoxia. This pathway utilizes extracellular nucleotide substrates, liberated from different cell types. Extracellular ATP release has been shown from endothelial cells, particularly under sheer conditions or hypoxia. In addition, fMLP activated neutrophils can release ATP, however the exact mechanism through that these cells release ATP remains currently unknown (see below) [14, 47]. Activated platelets comprise an additional source for extracellular adenine nucleotides [68, 69]. The role of endothelial CD39 (Ecto-apyrase, conversion of ATP/ADP to AMP) has been viewed as a protective, thromboregulatory mechanism for limiting the size of the hemostatic plug [69, 70]. Metabolism of adenine nucleotides derived from activated platelets is crucial in limiting excessive platelet aggregation and thrombus formation [71, 72]. Similarly, excessive platelet accumulation and recruitment can be treated with the use of soluble forms of CD39 [73, 74]. Moreover, a thromboregulatory role was demonstrated in a model of stroke, where cd39-null mice showed increased infarction size that was reduced by treatment with soluble CD39 [75]. Surprisingly, targeted disruption of cd39 resulted in prolonged bleeding and increased vascular leak and fibrin deposition in hypoxemia [76], suggesting a dual role for ATP metabolism by CD39 in modulating hemostasis and thrombotic reactions. Moreover, this observation may be related to an activation and desensitization of the purinergic typeP2Y1 receptor. Activation of the P2Y1-platelet receptor appears to be crucial in the activation process of platelets. As such, P2Y1 deficient mice exhibit signs of prolonged bleeding time and resistance to thromboembolism [77]. In contrast to these studies, we observed a barrier-protective influence during hypoxia that was not related to the activation of PX receptors, but to a downstream metabolism and signaling of ATP metabolites (esp. adenosine).

Extracellular ATP is readily converted on the endothelial surface to adenosine, due to the enzymatic function of CD39 and CD73 (5′-ecto-nucleotidase, conversion of AMP to adenosine). Such adenosine binds to surface expressed PMN adenosine receptors to limit excessive accumulation of PMN within tissues, and as such, functions as a feedback loop to attenuate potential tissue injury [14]. With regard to this latter point, it was recently shown that hypoxia coordinates both, transcriptional and metabolic control of the surface ecto-nucleotidases CD39 and CD73 [14, 15, 78], and as such, significantly amplifies the extracellular production of adenosine from adenine nucleotide precursors. In fact when using cd39- and cd73-null animals we found that extracellular adenosine, produced through adenine nucleotide metabolism during hypoxia, is a potent anti-inflammatory signal for PMN in vitro and in vivo. These findings identify CD39 and CD73 as critical control points for endogenous adenosine generation and implicate this pathway as an innate mechanism to attenuate excessive tissue PMN accumulation [14].

In addition to a role in limiting excessive neutrophil tissue accumulation,CD39andCD73are also critical control points for vascular permeability. For the purpose of investigating overall organ vascular permeability, we usedEvan’s blue dye, which tightly binds to plasma albumin [79]. To do this, mice were administered 0.2% Evan’s blue dye (0.5% in PBS) by intravenous tail vein injection, subjected to room air (normoxia) or normobaric hypoxia (8% O2/92% N2). At the end of exposure, animals were anesthetized, heparinized (50 U by i.p. injection) and fluid overloaded (3 cc normal Ringer’s solution i.p.). Animals were then exsanguinated by femoral cut-down to flush all vascular beds, and tissues were harvested. Tissues were rinsed in PBS, and Evan’s blue was extracted with formamide at 56 °C for 2 h, and quantified at 610 nm with subtraction of reference absorbance at 450 nm. This model entails the quantification of formamide-extractable Evans blue [80] from tissues of mice as a readout for overall vascular permeability of different organs. In fact we found that vascular permeability in tissues derived from animals subjected to normobaric hypoxia (8% O2/92% N2) ranged from two to four-fold more permeant to Evans blue than normoxic controls [14].

In order to identify the role of CD73 in vascular permeability, we used this model in wild-type or cd73−/− mice administered either vehicle or the CD73 inhibitor α,β-methylene ADP (APCP). These studies revealed a profound increase of hypoxia-elicited dysfunction of the vascular barrier in different organs (lung, heart, intestine, kidneys) following CD73 inhibition or deletion. Vascular leak associated with hypoxia was, at least in part, reversed by reconstitution with soluble 5′-nucleotidase and adenosine receptor agonists in the cd73-null mice. Histological examination of lungs from hypoxic cd73−/− revealed perivascular interstitial edema associated with inflammatory infiltrates surrounding larger pulmonary vessels [81]. Taken together, these studies identify CD73 as a critical mediator of vascular permeability in vivo. When measuring vascular permeability during hypoxia in mice with targeted deletion of CD39, similar increases in vascular barrier function could be observed in different organs [14]. Taken together, these studies have identified adenosine generation of the hypoxic vasculature via nucleotide-phosphohydrolysis as a critical cellular strategy to generate adenosine and maintain vascular barrier function.

Influence of adenosine receptor activation on endothelial barrier function

In vitro studies of endothelial permeability suggested, that activation of a specific endothelial adenosine receptor, the AdoRA2B, leads to a barrier resealing response following PMN transmigration [7]. Thus we were able to show that of the four different adenosine receptors that are expressed by endothelia, only the AdoRA2B is selectively induced by hypoxia [14]. Activation of the AdoRA2B is associated with increases in intracellular cAMP concentration due to the activation of the adenylate cyclase [60]. By inhibition of cAMP formation, the resealing of the endothelial barrier during PMN transmigration can be obviated [7]. Such increases in cAMP following activation of the AdoRA2B lead to an activation of protein kinase A (PKA) [18]. Further studies revealed a central role of PKA-induced phosphorylation of vasodilator-stimulated phosphoprotein (VASP), a protein responsible for controlling the geometry of actin-filaments [82]. Adenosine-receptor mediated phosphorylation of VASP is responsible for changes in the geometry and distribution of junctional proteins, thereby affecting the characteristics of the junctional complex and promoting increases in barrier function [18, 83].

Inflammatory hypoxia

Hypoxia and vascular barrier function

A number of studies have identified perturbations of endothelial permeability associated with hypoxia [84, 85]. In addition, tissue hypoxia has been implicated as a contributing factor to inflammatory diseases initiated at the vascular surface. For example, ongoing inflammatory responses are characterized by dramatic shifts in tissue metabolism, including lactate accumulation, increased nucleotide metabolism, and diminished availability of oxygen [86-88]. However, the exact mechanism by which hypoxia causes changes in vascular permeability remains the center of debate. In addition to the observation that hypoxia causes a disruption of the vascular barrier, several studies were able to identify hypoxia-elicited crosstalk pathways, that are involved in maintaining the vascular barrier and limiting excessive inflammatory responses. As outlined above, targeted disruption of such pathways is associated with dramatic increases in vascular permeability during hypoxia exposure and increases in myeloid cell accumulation within the hypoxic tissues [14, 15, 47, 81].

Increases in inflammatory cell accumulation during hypoxia

During episodes of hypoxia or during ischemia-reperfusion, the PMN influx across the protective endothelium creates the potential of endothelial barrier dysfunction, loss of fluid and edema formation [40, 89]. The myeloid cell migration to sites of inflammation are highly dependent on hypoxia adaptive pathways [34] and HIF-1α plays a critical role in this process. This transcription factor consists of two subunits HIF-1α and HIF-1β. Under conditions such as normoxia, the HIF-1α subunit undergoes mechanisms of enzymatic degradation. In contrast to its degradation during non-hypoxic states, degradation of the a subunit is inhibited under hypoxic conditions, leading to rapid accumulation of the protein. HIF-1α and HIF-1β dimerize to the active protein that translocates to the nucleus and binds to an hypoxia response element within the promoter region of target genes, thereby altering the transcription and translation of specific hypoxia elicited gene products [90].

Moreover, previous studies demonstrate, that HIF-1α is essential for myeloid cell-mediated inflammation. As outlined above, metabolic shifts during inflammation can result in significant tissue hypoxia, with resultant induction of hypoxia-responsive genes. As such, recent studies show that leukocyte functional responses are influenced by hypoxia on a transcriptional level. Increases of leukocyte accumulation within hypoxic tissues are transcription-dependent and can be specifically blocked by antibodies directed against β2-integrins. In addition, analysis of the β2-integrin mRNA and protein shows a dramatic increase with hypoxia. Subsequent studies identified a binding site for hypoxia-inducible factor 1 (HIF-1) in the CD18 gene. This gene encodes the subunit common to all four known types of β2-integrin heterodimer. HIF-1 binding was demonstrated in vivo, and mutational analysis of the HIF-1 site within the CD18 promoter resulted in a loss of hypoxia inducibility, suggesting that hypoxia induces leukocyte β2-integrin expression and function by transcriptional mechanisms dependent upon HIF-1 [35]. Moreover, myeloid cellular ATP-pools are significantly reduced in the absence of HIF-1α, leading to profound impairment of myeloid cell aggregation, motility, invasiveness and bacterial killing [34]. Shifts in tissue metabolism result, at least in part, from extensive recruitment of inflammatory cells, particularly myeloid cells such as neutrophils (PMN) and monocytes [36]. However, the direct relationship between PMN activation and increased endothelial permeability is not clear. While PMN accumulation and increased vascular permeability are often coincidental, particularly at sites of inflammation/hypoxia, PMN activation can occur with limited or no net changes in endothelial permeability [8–10, 12]. Moreover, while PMN depletion has been demonstrated to decrease organ injury in some models of ischemia and reperfusion [91], PMN have been demonstrated to exert a protective effect in other models. Therefore, further information regarding PMN-endothelial cell interactions and their influence on endothelial permeability may provide a better understanding of the regulation of endothelial permeability.

Purine signaling during inflammation and hypoxia

PMN release nucleotides

As stated earlier, the transendothelial migration of PMN during episodes of inflammation and hypoxia can be associated with fluid accumulation, edema and organ dysfunction as a cause of increased vascular permeability. During TEM, neutrophils primarily interact with endothelial cells and it is well documented that transmigration of neutrophils may lead to an alteration of barrier function. However their interactions with the endothelium do not inevitably result in endothelial barrier dysfunction: there is also evidence that PMN do not affect vascular permeability despite extensive non-inflammatory PMN-endothelial adhesion and subsequent transendothelial PMN migration. Although many studies indicate that activated PMN lead rather to disruption of the endothelial barrier, an increase of endothelial barrier permeability upon exposure to activated PMN has also been demonstrated [7, 14]. These studies show that PMN derived soluble mediators like adenosine and AMP are capable to increase the endothelial barrier function via activation of the AdoRA2B adenosine-receptor [59]. In addition, we showed that neutrophils also release ATP following activation, and such ATP is coordinately hydrolyzed to adenosine at the endothelial cell surface particularly under hypoxic conditions by hypoxia-induced CD39 and CD73 [14]. Several mechanisms for ATP release have been proposed, including direct transport through ATP-binding cassette (ABC) proteins, transport through connexin hemichannels, as well as vesicular release [92]. At present, the mechanism by which leukocytes release ATP remains unclear and is the subject of ongoing studies. Moreover, studies directed at understanding extracellular metabolism of nucleotides in cell and tissue responses now suggest that a number of different cells can release ATP in an active manner [93]. In addition to PMN, also activated platelets comprise an important source for extracellular adenine nucleotides [68, 69]. However, their relative contribution to regulating the vascular barrier or inflammation is currently not clear.

Nucleotide phosphohydrolysis is increased during hypoxia

The major pathway for extracellular hydrolysis of ATP and ADP is the ecto-nucleoside triphosphate diphosphohydrolase (NTPDase) [94], previously identified as ecto-ATPase, ecto-ATPDase or CD39 [95, 96]. In addition to modulating extracellular nucleoside generation, CD39 has been considered in the modulation of platelet purinoreceptor activity by the sequential hydrolysis of extracellular ATP or ADP to AMP [96, 97]. This thromboregulatory potential of CD39 has been demonstrated by the generation of mutant mice with disruption of the CD39 gene [76], and by a series of experiments where high levels ATPDase expression are attained by adenoviral vectors in the injured vasculature [98-100].

Ecto-5′-nucleotidase (CD73) is a membrane bound glycoprotein which functions to convert the adenine nucleotide AMP into adenosine, which in turn can activate transmembrane adenosine receptors or can be internalized through dipyridamole-sensitive carriers [60]. These pathways have been shown to result in such diverse endpoints as regulation of endothelial barrier [7], stimulation of epithelial electrogenic chloride secretion (responsible for mucosal hydration) [101], and promotion of lymphocyte-endothelial adhesion [102]. Targeted over expression of lymphocyte CD73 has recently revealed that increased adenosine resulting from enhanced CD73 expression could contribute to thymocyte apoptosis in adenosine deaminase deficiency [103]. Endothelial cells of many origins express constitutive CD73. The primary function attributed to endothelial CD73 has been catabolism of extracellular nucleotides, although CD73 may also mediate lymphocyte binding under some circumstances [102].

As outlined above, multiple cell types release adenine nucleotides under conditions of limited oxygen availability. Extracellular nucleotides are metabolized to adenosine by CD39 and CD73 and subsequent activation of surface adenosine receptors has been shown to regulate endothelial and epithelial barrier function [7]. Microarray RNA analysis revealed an increase in CD73 and CD39 in hypoxic endothelial and epithelial cells [14, 15]. Metabolic studies of CD39/CD73 function revealed that hypoxia enhances CD39/CD73 function as much as six-fold over normoxia. Examination of the CD73 gene promoter identified a binding site for hypoxia-inducible factor-1 (HIF-1) and inhibition of HIF-1alpha expression by antisense oligonucleotides resulted in significant inhibition of hypoxia-inducible CD73 expression. Studies using luciferase reporter constructs showed a significant increase in activity in cells subjected to hypoxia, which was lost in truncated constructs lacking the HIF-1 site. Mutagenesis of the HIF-1alpha binding site resulted in a nearly complete loss of hypoxiainducibility. In vivo studies in a murine hypoxia model revealed that hypoxia-induced CD73 may serve to protect the epithelial [15] and endothelial [81] barrier, since the CD73 inhibitor alpha,beta-methylene ADP (APCP) promotes increased intestinal permeability and cd73−/− mice show increased vascular permeability during hypoxia exposure. These results identify a HIF-1-dependent regulatory pathway for CD73 and indicate the likelihood that CD39/CD73 protects the epithelial and vascular barrier during hypoxia [14, 15, 81].

Adenosine concentrations in hypoxia

Extracellular adenosine has been widely implicated in adaptive responses to hypoxia. Thus, it is well documented that adenosine tissue and plasma levels are increased during hypoxia, however, mechanisms of this response have yet to be further elucidated [66, 104]. For example, in human volunteers exposed to ambient hypoxia (SpO2 = 80% over 20 min), plasma adenosine concentrations increased from 21 to 51 nM in the presence of dipyridamole, an inhibitor of adenosine reuptake [105]. Similarly, when measuring adenine nucleotide concentrations in neurally and vascularly isolated, perfused skeletal muscles of anesthetized dogs, normobaric hypoxia is associated with increases of adenosine in the venous blood, but not of AMP, ADP or ATP [106]. A possible role for adenosine during hypoxia may include vasodilatory characteristics. For instance, it has been suggested that elevations in intracellular nitric oxide as a result of AdoRA1 activation may be responsible for the vasodilatory properties of adenosine [107-109]. Due to its vasodilator properties, increases in adenosine tissue concentrations during hypoxia may promote blood flow to hypoxic tissues, thereby providing an innate adaptive pathway to hypoxia. In addition, there is evidence that hypoxia-induced vascular leak is, at least in part, controlled by adenosine. In vitro and in vivo studies indicated that endogenously generated adenosine, through activation of PMN adenosine AdoRA2A/2B receptors, functions as an anti-adhesive signal for PMN binding to microvascular endothelia [47, 64, 110]. Other studies revealed that adenosine derived via nucleotide phosphohydrolysis is critical in eliciting decreases in endothelial paracellular permeability [7] and that such responses are dramatically enhanced by hypoxia [14, 15]. In addition, some studies have suggested that uptake of adenosine by equilibrative nucleoside transporters (ENTs) in cultured myocardial cells are decreased during hypoxia. This might resemble an additional cellular strategy to increase extracellular levels of adenosine during hypoxia [111]. However, this has not yet been investigated within the endothelium or the vasculature, and the physiological relevance of this adaptive pathway currently remains unclear.

Increased adenosine signaling by hypoxia

Several studies had demonstrated a functional role for hypoxia-regulated CD39 and CD73 in promoting endothelial permeability [14, 15, 47], however, the role of signal transduction via endothelial adenosine receptors in the post-hypoxic vasculature remained unclear until recently. In order to identify changes in endpoint signaling (i.e., adenosine receptor activation) in the post-hypoxic endothelium, we profiled the relative expression of adenosine receptors in normoxic and hypoxic endothelial cells. Interestingly, these experiments demonstrated that the AdoRA2B was selectively induced by hypoxia, and that all other isoforms were either not changed (AdoRA3) or significantly down-regulated (AdoRA1 and AdoRA2A) [14]. Such microarray results were verified by real-time PCR and measurement of surface protein levels and consistently confirmed selective induction of the AdoRA2B receptor by hypoxia. To determine whether such hypoxia-induced AdoRA2B expression was functional, endothelial permeability assays were employed using the selective AdoRA2B antagonist MRS 1754 [112] and demonstrated a significantly shift in the adenosine dose-response curve suggesting that AdoRA2B responses are amplified in posthypoxic endothelia. However, further studies in vivo to verify these in vitro findings in genetically engineered animals using targeted deletion of individual adenosine receptors have yet to be performed to follow up on these observations.

Nucleotide and inosine signaling

Purine signaling is presently a field of intense investigation. Adenosine as an extracellular nucleoside interacts via P1 receptors. Four P1 receptor subtypes have been identified until now, namely AdoRA1, AdoRA2A, AdoRA2B and AdoRA3 and the growth hormone secretagogue receptor GHSR [60]. Extracellular nucleotides as signaling molecules interact through to different categories of P2-types of cell surface receptors: P2Y type G protein coupled receptors, and P2X type ligand gated ion channels. Eight subtypes of P2Y receptors have been characterized at present, which are either activated by the adenine nucleotides ATP or ADP or respectively by the uridine nucleotides UTP or UDP. One P2Y subtype is activated by both, adenine and uridine nucleotides [113-116]. However, there can be large differences between different species (e.g., between human and rat) with regard to P2 receptor selectivity for adenine or uridine nucleotides [117]. Despite of the fact that the vascular endothelium and multiple cell types of the immune system (including PMN) express different P2 receptors [113, 118], only very little is known about the effect of nucleotide signaling on neutrophilY endothelial interaction. In fact, the cell physiology of these receptors and the precise function of the multiple P2 receptor subtypes remains to be understood. As currently selective blockers of these receptors are being synthesized, we can soon hope for a more precise understanding of how nucleotide signaling modulates immune function [119].

There is no unequivocal evidence that AMP can function as a signaling molecule. Recently, Inbe et al. suggested that the orphan receptor GPR80/99 may function as an AMP receptor [120]. In contrast, there is now convincing evidence that GPR80/99 binds α-ketoglutarate, thereby functioning as receptor for citric acid cycle intermediates [121]. In addition, other studies demonstrated that GPR80/99 does not bind adenosine or AMP [122]. Therefore, there is now consensus that GPR80/99 is not a nucleotide receptor [123].

In contrast to adenosine, which has for long been considered an important modulator of immune function and inflammation, its major degradation product inosine was originally thought to have no biological effects. However, some recent studies have suggested that inosine itself may influence immune function and tissue protection [61]. Similar to adenosine, inosine concentrations are increased during hypoxia and during ischemia/reperfusion [124]. As such, inosine was found to bind to the adenosine AdoRA3 receptor subtype and cause mast cell degranulation [125] or cutaneous vasodilatation [126]. In addition, inosine was found to be involved in the down-regulation of tissue damage under different inflammatory conditions in vivo via activation of AdoRA2A and AdoRA3 adenosine receptors [127]. However, specific inosine receptors have not yet been described. In addition, it remains unclear whether endogenously produced inosine is sufficient to exert tissue protective influences in vivo, particularly since the AdoRA3 receptors show only a low affinity for inosine. However, interstitial concentrations of inosine may be high enough to activate AdoRA3 receptors during pathophysiological states such as tissue hypoxia [125]. In addition, it is possible that inosine signaling may contribute to the effects of adenosine signaling, since exogenous administration of large doses of inosine were found to decrease ischemia reperfusion injury in several tissues [61, 125, 128]. Taken together, the overall contribution of inosine signaling to the regulation of the vascular function remains to be seen.

Potential therapeutic developments

Several inflammatory diseases (e.g., sepsis, acute respiratory failure, colitis) are characterized by vascular barrier dysfunction, leading to fluid extravasation and edema formation [129-131]. As outlined above, endothelial nucleoside signaling creates the potential for therapeutically modulating the vascular barrier function. For example, promoting vascular adenosine signaling by increasing extracellular adenosine generation, activation of specific vascular adenosine receptors, or impeding with adenosine breakdown may potentially dampen vascular barrier impairment during hypoxia and inflammation. Several experimental studies have examined this approach. Cohen et al. investigated the influence of the adenosine deaminase inhibitor 2′-deoxy-coformycin (pentostatin) in an animal model of sepsis (cecal ligation and puncture model) [132]. Using intravital microscopy, the authors demonstrated that septic mice treated with pentostatin revealed decreased leukocyte rolling and adhesion. In addition, circulating levels of interleukin-6 and tumor-necrosis-factor-α were decreased, and survival was increased after 48 h. At the same time, leakage of fluorescein-isothiocyanate-labeled albumin was decreased following pentostatin treatment, suggesting that inhibition of adenosine breakdown during sepsis is associated with improved vascular barrier function and decreased inflammatory activation. An alternate strategy to promote vascular adenosine signaling may include administration of soluble nucleotidase. As outlined above, nucleotidases convert AMP to adenosine, thereby increasing adenosine levels. Using this principle, it was recently shown that administration of 5-nucleotidase to mice during hypoxia significantly diminished vascular leak syndrome [81]. Moreover, we recently demonstrated that administration of the specific AdoRA2B antagonist MRS 1754 is associated with decreased endothelial adenosine responses, causing increased leakage of 70 kD dextran molecules [14]. These studies were confirmed using an in vivo model of pulmonary barrier function, showing increased albumin leakage after hypoxia exposure in mice treated with MRS 1754 [81]. These experiments suggest that therapeutic use of a specific agonist of the AdoRA2B may dampen edema and fluid extravasation in patients suffering from inflammatory vascular leak syndrome(s). Despite of the fact that our understanding of neutrophil-endothelial interaction during inflammation and hypoxia has considerably advanced over the last years, and purine metabolism and signaling clearly offers novel therapeutic targets in the treatment of inflammation, these experimentally derived ideas have yet to be fully integrated into clinical practice.