Purinergic mechanism in the immune system: A signal of danger for dendritic cells.

There is increasing appreciation that injured or stressed cells release molecules endowed with the ability to modulate dendritic cell maturation. The role of these molecules is thought to be that of alerting the body of an impending danger, and initiate and shape the subsequent immune response. Nucleotides are perfectly suited for this task as they are easily released upon damage of the cell membrane, rapidly diffuse in the extracellular environment and ligate specific plasma membrane receptors expressed by dendritic cells and other mononuclear phagocytes. A better knowledge of the modulation of dendritic cell responses by extracellular nucleotides may provide novel routes to enhance the immune response and increase the efficacy of vaccination.

Introduction

One of the fundamental tenets in immunology is that our body reacts against foreign (non-self) antigens. Antigenic molecules, that signal invasion by pathogenic microrganisms, or simply the presence of cells that carry a foreign genome (as in transplants) are initally sensed by first line defense immune cells (such as the dendritic cells, DCs, the prototypic antigen presenting cells, APCs) that initiate inflammation and the native and adaptive immune responses [1]. Albeit generally accepted and largely validated by countless experimental and clinical findings, the theory that we exclusively or mainly react to non-self molecules is unable to explain a number of observations that have bothered immunologists for many years. As pointed out by Matzinger [2], why we do not react against proteins that are synthesized late in the life and therefore are not exposed to lymphocytes during maturation of the immune system? Or, why do we all harbour auto-reactive B and T cells, and yet autoimmune diseases are rare? Or, why are some tissues easier to transplant than others? Over the last years, the view has emerged that we do not react to nonself (‘foreign’) molecules but rather to molecules that cause damage to our tissues. In other words, our body reacts to ‘danger’ rather than to ‘stranger’ [3]. While it is clear that the ‘danger hypothesis’ does not rule out but rather complements non-self recognition in immunity, it is also clear that this novel way to look at the very first phases of the immune response gives some powerful weapons for the interpretation of many key events in immunity and inflammation.

Every physician and every pathologist knows well that the strongest stimulus for inflammation is tissue damage, to such an extent that cell injury is thought to be the common event whereby conditions as different as cancer, chemical irritants, UV light, closed traumas or biological agents trigger inflammation [4]. The pro-inflammatory (‘flogistic’) activity of tissue trauma was long thought to reside in the release of normally segregated intracellular molecules that once exteriorized into the extracellular environment would have the ability to switch on quiescent immune cells. Not surprisingly, it is well known that necrotic cells are more likely than apoptotic cells to initiate inflammation [5]. However, the identity of these intracellular molecules has been ill defined for many years, and the pathways leading to stimulation of native and adaptive immunity were purely hypothetical. The merit of the ‘danger signal’ hypothesis as put forward by Matzinger lays in the description of the basic features of a danger signal and in the identification of their role in the initiation of inflammation and in the modulation of DCs [6]. We will see that extracellular nucleotides have all the essential features of a ‘danger signal’, and in fact they may be a type of primordial signal of tissue distress ubiquitous in the biological world. Accordingly, nucleotide receptors (P2R) in the immune system can be viewed as receptors for danger signals.

Danger signals: What are they?

According to the current generally accepted definition, we may define a danger signal as something that is released by injured or dying cells, is perceived as a sign of tissue distress, and is endowed with the ability to stimulate DCs and induce their differentiation [6]. Danger signals can be endogenous (originating from the host’s cells) or exogenous (released into the body by invading pathogens). Danger signals can also be generated by tissue destruction or activation of classical inflammatory pathways [7, 8]. Endogenous danger signals can further be classified into constitutive or inducible. A key feature of the constitutive danger signals is their ability to stimulate the release of the inducible ones. Constitutive danger signals are normally segregated inside all cells and, so far as they are intracellular, they have no stimulatory activity on the immune system. Several intracellular constituents are candidates to this role (see Table 1), among which are extracellular nucleotides.

Table 1

Intracellular molecules candidates for the role of constitutive danger signals.

Ligand (danger signal)	Receptor (danger sensor)
Heat shock proteins (HSP60, HSP70, HSP90)	CD91, TLR4, TLR4/TLR2, LOX-1
Uric acid crystals	?
DNA	TLR9
ssRNA	TLR3, TLR7, TLR8
Nucleotides	P2Y11,2,4,6,11, P2X4,7
Sugar metabolites	P2Y14
(UDPglucose)

A danger signal must be in the first place a good extracellular messenger because, in case of tissue damage, it must efficiently travel across the intercellular space to alert nearby cells. Ideally, any good extracellular messenger should have the following features:

It should be easily and quickly generated in the extracellular space. This would require the presence of a large pool of intracellular molecules.

Under resting conditions its concentration should be close to zero to allow a high signal-to-noise ratio upon release. Maintenance of a large pool and a low steady-state value of messenger molecules is an essential feature of signalling in biological systems because it allows a rapid, many-fold change in messenger concentration.

It should be highly mobile in the pericellular aqueous environment, therefore small and hydrophilic molecules are better suited to this task.

It should be recognized by specific receptors expressed by immune cells.

It should be easy to destroy once it reaches the extracellular space. This ensures a quick termination of the response once the causative agent is removed.

Extracellular nucleotides fulfill all these pre-requisites as:

They are present at a high concentration intracellularly (ATP 5–10 mM, UTP 0.5–1 mM), and are quickly released following cell death, damage, or even simple plasma membrane stretching. The mechanism by which ATP can be released in the absence of overt cell damage is unclear: it is well documented that some cell types (e.g. platelets [9], neurons [10] or epithelia [11]) secrete ATP most likely by exocytosis of nucleotide-laden vesicles. Evidence mostly based on inhibitor studies suggests that channels or transporters might also participate in ATP release (see [12] for recent review). More controversial is the evidence that pro-inflammatory factors may to drive non-lytic ATP release from immune cells [13-16].

The extracellular ATP concentration under resting conditions is very low, in the 1–10 nM range. Paradoxically, before the purinergic signalling hypothesis became accepted, this was taken as evidence against the role of ATP as an extracellular messenger. On the contrary, a very low resting level is a fundamental feature of any messenger, danger signals included.

ATP is a small solute (molecular mass 650 Da) bearing from two to four negative charges, depending on the pH and the Ca2+ and Mg2+ concentration. Thus, it is highly diffusible in the extracellular aqueous milieu.

As of now 15 receptors for extracellular nucleotides have been identified [17]. The widely differing range of nucleotide specificity and affinity makes this receptor family very flexible and efficient in translating information delivered by the ligands.

All cells express plasma membrane ecto-nucleotidases that quickly hydrolyze extracellular nucleoside tri-, di- and mono-phosphates [18]. Interestingly, these enzymes by generating nucleoside diphosphates from triphosphates (e.g. ADP from ATP, or UDP from UTP) and thus additional ligands also modulate activation of P2 receptors with different specificities.

Are extracellular nucleotides released at sites of tissue damage?

This may sound as a very naive question. We all believe that an acutely injured cell will release all its ATP content, as can be clearly shown in the test tube when a cell suspension (or a cell monolayer in a Petri dish) is lysed with a detergent or by freeze-thawing, and the ATP concentration in the supernatant is measured by the usual luciferin-luciferase assay. However, in vivo measurements that document an increase in the extracellular ATP concentration at sites of inflammation or tissue damage are few. An early in vivo report by Forrester [19] suggested that cell membrane stretching can cause ATP secretion. This author showed that the ATP concentration in the venous effluent from human exercising muscle increased from 20 to about 200 pmol/ml, mainly due to release from contracting muscle fibers. Other measurements following vessel injury show that the free ATP concentration in the blood can rise up to 20 µM from a basal level of 10–20 nM [20]. The origin of this ATP is identified as the damaged vessel wall cells (endothelium and muscle cells), platelets and other circulating blood cells. Platelets are without doubt an important source of ATP since they store near molar amounts of this nucleotide inside their dense granules. It is worth pointing out that, although nucleotide release from platelets is generally viewed in the context of clot formation, we should not forget that platelets are also one of the most important sources of inflammatory mediators, thus ATP release from activated platelets is certainly proof for ATP release during inflammation. Implications for a typical inflammatory lesion in which platelets have a key role, such as the atheromatous plaque, could be far reaching [21].

A widely held opinion is that the main source of ATP release in the setting of trauma is the damaged cells. While this is very likely to occur, a recent study by Nedergaard and co-workers has documented that shortly (10 min) after the trauma the main site of ATP release is not the traumatized region itself, but rather the perilesional area [22]. It appears that cells that surround the traumatized tissue are driven into an activated state that persists for several hours after the injury. Quite interestingly, blockade of the P2X7 receptor subtype, a main mediator of the proinflammatory effects of ATP, decreased tissue injury and enhanced functional recovery after the insult. This finding lends further support to the view that ATP might be one of the most important early pro-inflammatory signals released at injury sites. The view that local accumulation of ATP (and ADP) might have a long lasting action is further supported by the observation that in mice lacking the main Langerhans cell ecto-ATPase (CD39) local irritants cause nucleotide release and an exacerbated skin inflammation [23]. Furthermore, local accumulation of nucleotides also affects the outcome of contact dermatitis caused by topical administrations of allergens. This again concurs to support the view that nucleotide release at site of injury or inflammation can have far reaching effects on immunomodulation.

Do nucleotides activate DCs?

As summarized above, the main distinguishing feature of a danger signal resides in its ability to activate DCs and drive their differentiation. DCs are the most efficient APCs for activation of naïve T cells [24]. Thus, they are the key elements in the initiation of primary immune response. DCs reside in the tissues as immature cells, but when activated by a variety of extracellular agents (pathogens, cytokines, neurotransmitters), they mature and migrate to the lymphonodes where they stimulate T cell differentiation [1, 24]. DCs have become a focus of attention as a possible target for extracellular nucleotides only very recently, nonetheless a wealth of data is already available on the pattern of P2R expression and the functional responses associated with their stimulation.

DCs express both P2YRs (P2Y1, P2Y2, P2Y4, P2Y6, P2Y11 and P2Y14) and P2XRs (P2X1 , P2X4, P2X7) [25-30]. Acute, transient, stimulation with ATP or UTP causes many of the responses typically associated with P2Y or P2X activation (phosphatidyl inositol breakdown, release of Ca2+ from intracellular stores, Ca2+ influx across the plasma membrane, and even opening of the P2X7 large conductance pore if a high ATP concentration is used).

Nucleotide effects on DC responses are dramatically different whether they are due to exposure to chronic low (10–250 µM) or acute high (500 µM to millimolar) concentrations. Chronic stimulation triggers a process of DC maturation that enhances their ability to stimulate Th2 lymphocytes and thus initiate a type 2 immune response. In the presence of ATP the expression of typical markers (CD54, CD80, CD83, CD86) of DC maturation is increased, furthermore endocytic activity is reduced and the capacity to promote proliferation of allogeneic lymphocytes enhanced. ATP alone, at variance with classical maturation factors, does not induce cytokine or chemokine secretion [31, 32]. However, in the presence of maturating factors (e.g. bacterial endotoxin, LPS, or CD40L), ATP strongly distorts the pattern of cytokine produced. LPS or CD40L-dependent release of IL-1β, IL-1α, TNF-α, IL-6 and IL-12 is inhibited, while release of the IL-1 receptor antagonist and IL-10 is not affected. As a result, when co-cultured with naïve Th lymphocytes these DCs promote a Th2 polarization, witnessed by the typical pattern of cytokines produced by the stimulated lymphocytes (low interferon γ, high IL-4, IL-5 and IL-10). The pattern of chemokine receptors expressed by DCs is also strongly modified by chronic exposure to low ATP concentrations. Receptors for inflammatory chemokines such as CC chemokine receptor 5 (CCR5) are down modulated while those for lymphoid chemokines such as CXC chemokine receptor 4 (CXC4R) and CCR7 are upregulated [33]. This has far reaching consequences in recirculation of dendritic cells from tissues to the lymphonodes, and from blood into tissues. In fact, following exposure to pathogens or tissue damage, resident immature DCs respond to inflammatory chemokines to become activated, concentrate in the inflamed tissue, take up antigens, mature and migrate to the regional lymphonodes. During maturation DCs upmodulate receptors for lymphoid chemokines, that allow lymphonode localization and enhance their ability to interact with naïve T cells. ATP priming also affects the pattern of chemokines secreted by DCs: constitutive production of the lymphoid chemokine CCL22 is increased, while the LPS-stimulated secretion of the inflammatory chemokines CXCL10 and CCL5 is inhibited [33]. This shift in chemokine release favours recruitment of Th2 rather than Th1 lymphocytes. Thus, in summary chronic exposure to low ATP concentrations has a strong modulatory activity on DC maturation by enhancing their ability to localize in the lymphonodes and to initiate a type 2 rather than a type 1 immune response (see Figure 1 for a schematic rendering). The P2Rs responsible for such an immunomodulatory effect have not been conclusively identified, but convergent data point to P2Y11 as the most likely candidate [29] (despite an early suggestion that P2XRs were involved [31]). However, at this very preliminary stage we cannot exclude that other P2YRs or P2XRs may also participate in DC maturation. Involvement of different P2Rs in DC maturation is also suggested by a recent work of Schnurr and co-workers [34] showing that ATP-primed DCs have a differential ability to activate naive or memory T cells. This further stresses the complexity and the potential relevance of purinergic signalling in the manipulation of DC responses.

Figure 1

Cell damage caused by physical trauma or pathogens causes an initial wave of ATP release (red) from injured cells. This first wave of ATP release diffuses through the pericellular space and activates adjacent cells (e.g. epithelial cells, macrophages, fibroblasts). P2 receptors expressed on the plasma membrane of the bystander cells will be activated and trigger the release of several bioactive agents, among which ATP itself (ATP-induced ATP release, dark blue). Accumulation of ATP into the extracellular milieu will prime Langerhans/dendritic cells (DC) and modify their responses to bacterial endotoxin (LPS) or T lymphocyte-derived CD40 ligand (CD40L). The combined action of these agents drives DC maturation and the secretion of cytokines and chemokines.

We are faced with a completely different scenario when DCs are acutely challenged with high ATP doses in association with a bacterial pathogen. In this case secretion of pro-inflammatory cytokines is potently stimulated and, if exposure to ATP is not discontinued, cell death occurs [27, 35]. This pro-inflammatory activity is non dissimilar from that elicited by ATP in many other mononuclear phagocytes [36, 37]. The IL-1β-releasing activity of ATP is particularly striking: in cells primed with LPS the addition of this nucleotide causes an explosive acceleration of pro- IL-1β processing and the consequent exteriorization of the mature cytokine embedded into plasma membrane-derived microvesicles [38]. It is of interest that ATP is unable to drive IL-1β release in phagocytes that have not been previously primed with LPS, thus reinforcing ATP’s role as danger signal that acts in concert with bacterial pathogens to initiate inflammation. On the other hand, the inability of LPS to drive IL-1β secretion in the absence of ATP further supports the view that bacterial factors are incomplete stimuli in the absence of endogenously-released danger signals.

Nucleotides may shape the immune response also by having a differential effect on DC recruitment. Idzko and co-workers have shown that immature but not mature DCs chemotact in response to a nucleotide gradient [39]. This would allow recruitment of immature DCs to the ATP-rich inflammatory site, but would not prevent migration of mature DCs to regional lymph nodes. Many other immune cells, such as mast cells, macrophages and microglia, are sensitive to the chemotactic activity of ATP, UTP or ADP, thus reinforcing the role of nucleotides as powerful activators of inflammation [40-42]. As of now there are no reports of an in vivo modulatory activity of extracellular ATP on dendritic cell function, but the observations reported in mice deleted of the main ecto-ATPase of immune cells (CD39) point in this direction [23].

Conclusion

The danger model for the initiation of the immune response is enjoying increasing appreciation. Although overenthusiastic generalizations should be avoided, we think that it provides a useful guidance to comprehension of the initial phases of inflammation. In this context, nucleotides are an outstanding example of how an intracellular molecule, with no obvious links to immunity, can modulate the immune response if released extracellularly.