Abstract
Evidence is accumulating that some forms of cell death, like apoptosis, are not only governed by the complex interplay between extracellular and intracellular signals but are also strongly influenced by intercellular communicative networks. The latter is provided by arrays of channels consisting of connexin proteins, with gap junctions directly connecting the cytoplasm of neighboring cells and hemichannels positioned as pores that link the cytoplasm to the extracellular environment. The role of gap junctions in cell death communication has received considerable interest and recently hemichannels have joined in as potentially toxic pores adding their part to the cell death process. However, despite a large body of existing evidence, especially for gap junctions, the exact contribution of the connexin channel family still remains controversial, as both gap junctions and hemichannels may furnish cell death as well as cell survival signals. An additional layer of complexity is formed by the fact that connexin proteins as such, beyond their channel function, may influence the cell death process. We here review the current knowledge on connexins and their channels in cell death and specifically address the molecular mechanisms that underlie connexin-related signaling. We also briefly focus on pannexins, a novel set of connexin-like proteins that have been implicated in cellular responses to pathological insults.
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Main
In multicellular organisms, the maintenance of tissue homeostasis ultimately relies on the critical balance between cell growth and cell death. Among the various cell death types, apoptosis has been most extensively characterized. Being the conceptual counterpart of necrosis, apoptosis is a genetically programmed and well-orchestrated process of selective cell deletion that occurs in all tissues as part of the normal cellular turnover.1 It is also involved in a growing number of pathological conditions, such as in ischemia-related cell injury following stroke.2, 3 Two major apoptotic pathways can be distinguished, the mitochondria-mediated intrinsic cascade and the death receptor-mediated extrinsic pathway.1, 4, 5, 6 Both rely on the proteolytic activity of an evolutionary conserved family of cysteine proteases – the caspases – which form the biochemical basis of the apoptotic phenotype.7 They are responsible for the cleavage of a large number of cellular proteins including major cytoplasmic and nuclear elements. The extrinsic signaling pathway is triggered by the binding of an extracellular death ligand, such as Fas ligand, tumor necrosis factor α (TNFα) or TNF-related apoptosis-inducing ligand (TRAIL) to their corresponding receptors at the plasma membrane (PM).1, 4, 5, 6 In contrast, the intrinsic signaling pathway is mediated by mitochondria and involves a diverse array of non-receptor-mediated stimuli that produce intracellular signals directly acting on targets within the cell. It is regulated by the B-cell lymphoma-2 (Bcl-2) family of pro- and anti-apoptotic proteins.8 Necrotic cell death, on the other hand, has been often considered to be a passive process, lacking underlying signaling events and occurring under extreme physico-chemical conditions, including abrupt anoxia, sudden shortage of nutrients, heat or detergents. Recent evidence, however, suggests that necrotic cell death can also be the morphological manifestation of a molecularly regulated event associated with pathologies such as ischemia-reperfusion injury, neurodegeneration and pathogen infection.9, 10
In contrast to the wealth of knowledge concerning the extracellular and intracellular signaling cascades that govern (apoptotic) cell death, our understanding of the role of intercellular (cell-to-cell) communication in this process is still in its infancy. The most direct form of intercellular communication proceeds through gap junction (GJ) channels. These channels arise from the head-to-head interaction of two hemichannels (HCs) (connexons) on adjacent cells, which are hexameric channels composed of connexins (Cxs). The Cx protein has a four membrane-spanning topology with two extracellular loops, one cytoplasmic loop and a cytoplasmic N- and C-terminal region (Figure 1).11, 12, 13 At present, more than twenty Cx species have been cloned from rodents and human and are named according to their molecular weight.14 Gap junctional intercellular communication (GJIC) is driven by the passive diffusion of small (<1–1.5 kDa) hydrophilic molecules such as glucose, glutamate, glutathione, cyclic adenosine monophosphate (cAMP), adenosine triphosphate (ATP), inositol trisphosphate (IP3) and ions (e.g., Ca2+, K+, Na+).13, 15 The biophysical permeation properties of these substances depend on the nature of the Cx species that form the channel and clear differences in channel permeability have been shown for various ions, reporter dyes and signaling molecules such as cAMP or ATP.16, 17, 18, 19 The gating of GJ channels is controlled by a number of factors, with as prominent players the transmembrane voltage (over the PM), transjunctional voltage (over the GJ), Ca2+ and the phosphorylation status.20, 21, 22 With the notable exception of Cx26, all Cxs are phosphoproteins that are targeted, particularly at their C-terminal tail, by a broad panel of kinases. HCs reside as closed channels in the PM but open by a process of ‘loop gating’ when their extracellular loops interact to form a functional GJ channel.20, 23 Before being incorporated into GJs, HCs can also be opened by various signals or conditions, including membrane depolarization,24 a decrease of extracellular Ca2+,25 cytoplasmic Ca2+ changes,26 mechanical stimulation,27 changes in phosphorylation status,28 changes in redox status,29 reactive oxygen species (ROS),30 nitrosylation of the Cx protein,31 ischemia/hypoxia,3, 32, 33 and also certain Cx mutations.34, 35, 36, 37 Open HCs allow the entry of below 1 to 1.5 kDa substances (e.g., Ca2+, Na+)38 or the escape of essential metabolites such as nicotinamide adenine dinucleotide (NAD+),39 ATP,40 glutamate,41 prostaglandins42 and glutathione.43
Another family of GJ channel-forming proteins, the ‘innexins’, was first reported in invertebrates and later renamed ‘pannexins’ (Panxs) after their orthologs were discovered in vertebrates.44 Thus far, three Panxs (Panx1, Panx2 and Panx3) have been characterized in rodents and human. Despite the lack of sequence homology between Cxs and Panxs, they share a similar topology and also display cell-specific expression patterns.45 They appear to be endowed with several other Cx-like properties such as the ability to form homomeric Panx1 or heteromeric Panx1/Panx2 HCs46 and functionally competent GJ channels,47, 48 although some controversy still exists concerning the latter.49, 50 Furthermore, Panx channels are also permeable to small molecules,51, 52, 53 release ATP,54, 55 open in response to mechanical stimulation,54 and intracellular Ca2+,56 and are blocked by certain Cx-based GJ blockers.46, 53
Numerous physiological processes are driven by regulatory molecules that pass through GJs and HCs, which are therefore considered as major gatekeepers in the control of tissue homeostasis. Many efforts in this respect have been focused on their roles in the regulation of cellular proliferation and differentiation.12, 15, 57 The exploration of Cx- and Panx-related signaling in cell death, however, has only been initiated in recent years, nevertheless reporting some striking observations in this newly arisen research field.12, 45, 58, 59 In this review, we will focus on the role of Cxs and their channels as both positive and negative modulators of cell death, mainly apoptosis. We additionally demonstrate the involvement of the recently discovered Panxs in cellular responses to insults.
Connexin-Based Gap Junction Channels and Cell Death
A substantial body of evidence indicates a positive correlation between GJIC and apoptotic activity (Figure 2). Indirect data come from the observation that chemical GJ inhibitors, such as carbenoxolone and 18-beta-glycyrrhetinic acid, prevent apoptosis.60, 61, 62, 63 Vice versa, tumor promoters, including peroxisome proliferators and phenobarbital which are known to counteract apoptosis, also inhibit GJIC.64, 65 Furthermore, exogenous introduction of Cxs in a plethora of experimental models was found to facilitate apoptotic cell death (Table 1).30, 63, 66, 67, 68, 69, 70, 71, 72, 73, 74, 75, 76, 77, 78 Various cell death models have demonstrated the clustering of dying cells, indicating the spread of death signals to neighboring cells through GJs.63, 79, 80 This phenomenon of ‘bystander death’ (the ‘kiss of death’) has gained a great deal of attention for it opens up the possibility to therapeutically limit the wave of secondary injury in the context of stroke or brain trauma,3, 80, 81, 82, 83, 84 and to amplify the potency of cancer treatment. With respect to the latter, the ‘suicide gene/prodrug therapy’ is a well-known model whereby malignant cells are transfected with the herpes simplex virus-thymidine kinase (HSV-tk) gene, followed by treatment with the prodrug ganciclovir (GCV). Following phosphorylation to GCV-triphosphate, this cytotoxic compound competitively inhibits the incorporation of endogenous deoxyguanosine triphosphate into the DNA, resulting in the termination of DNA synthesis and the onset of apoptosis.85, 86 In several tumor cell models, cells that lack the suicide gene and that surround a HSV-tk+ cell are also killed by GCV treatment because of diffusion of GCV-triphosphate through GJs connecting those cells.85, 86, 87 Another form of bystander killing is mediated by the transfer of viral peptides through Cx-related communication. Neijssen et al.88 discovered that a cell expressing viral proteins and its closest neighbors are killed by cytotoxic T-cells, because the adjacent cells receive the viral peptides through GJs. Thus, GJ immunological coupling could mediate the elimination of uninfected bystander cells or those in the earliest phases of infection.
In-depth studies have revealed that Cx-related communication is modified during the cell death process (Table 2). Particularly the early phases of apoptosis require GJIC,62, 70, 89, 90, 91 but with progression of cell death, GJIC drastically declines culminating in the absence of cell coupling between apoptotic bodies. The abolishment of GJIC thus coincides with the typical morphological transformations that occur in apoptosis and results from an increased removal of GJ channels from the PM and not from their functional closure.70 In a recent study, Theiss et al.92 exposed primary bovine lens epithelial cells and mouse NIH-3T3 fibroblasts to a number of well-established apoptosis-inducing agents. The authors noticed a decrease in GJIC that was associated with caspase 3-mediated degradation of Cx43. Similarly, activation of apoptosis in primary cultures of chick lenses resulted in caspase 3-mediated truncation of Cx45.6, a reaction that was inhibited by casein kinase 2-mediated phosphorylation of Cx45.6.93 As a matter of fact, phosphorylation is likely to be a major mechanism responsible for GJIC alterations during apoptosis (Table 2). In rabbit lens epithelial cells, H2O2 induced caspase 3-dependent apoptosis that was associated with activation of protein kinase Cγ, the phosphorylation of Cx43 and Cx50, and the disassembly of GJ plaques abolishing GJIC.94, 95 Induction of apoptosis in rat liver epithelial WB-F344 cells by the hydrophobic platinum IV complex LA-12 was also linked to suppression of GJIC and the disappearance of Cx clusters from the cell membrane surface. LA-12 thereby triggered rapid Cx43 hyperphosphorylation mediated by the mitogen-activated protein kinase kinase/extracellular signal-regulated kinase (MEK/ERK) pathway.96 Increased Cx phosphorylation does not always go hand in hand with a loss of GJIC. Indeed, in the WB-F344 rat liver epithelial cell model, serum deprivation91 and exposure to the histone deacetylase inhibitor suberoylanilide hydroxamic acid97 enhanced GJIC, particularly during the early phases of apoptosis, and simultaneously increased Cx43 phosphorylation. Inversely, inhibition of GJIC in primary bovine lens epithelial cells and primary human corneal fibroblasts by staurosporine92 and TNFα98 was accompanied by a decrease in the Cx43 phosphorylation status. Of note, alterations in Cx phosphorylation are frequently allied with modifications in cellular localization. The drastic decrease in GJIC that is observed during mitosis, for instance, results from the cytoplasmic redistribution of a unique Cx43 phosphoform called ‘Cx43m’ or ‘Cx43P3’.99, 100, 101 The latter is generated by the cyclin-dependent kinase 1/cyclin B1 complex, which not only controls the G2/M transition of the cell cycle, but also plays a crucial role in the initiation of apoptosis.91, 99, 100, 101 In fact, induction of apoptosis by choline deficiency increased Cx43 immunoreactivity in the cytoplasm of rat liver epithelial cells. Restoration of the Cx43 membrane localization, and consequently of GJIC, as well as enhanced cell survival was brought about by 8-bromo-cAMP,102 a well-known inductor of Cx43 phoshorylation.22
Contradictory to the paradigm that GJIC facilitates apoptosis are a number of investigations showing that GJs may impede the occurrence of cell death (Figure 2).103, 104, 105, 106, 107, 108, 109, 110, 111, 112, 113, 114, 115, 116 In line with this notion are a number of reports describing induction of apoptosis by chemical GJIC inhibitors107, 108, 117, 118, 119 as well as by Cx mimetic peptides,120 which are peptides identical to a short Cx sequence that act as GJ blockers.121 Healthy cells may indeed provide their dying neighbors with rescue signals3 or cells in danger may dilute toxic substances toward healthy neighbors through GJs.3, 103 This event whereby cell survival is promoted has been designated the ‘good Samaritan’ effect or the ‘kiss of life’, as opposed to the ‘bystander death’ phenomenon.85 Thus, there seems to be a clear two-way traffic between (early) apoptotic and non-apoptotic cells80 and, depending on the status and environmental context of the cell that receives the signal, two opposite biological outcomes can be achieved, namely cell death or cell survival.3
The biochemical nature of the signals that actually mediate these effects, in particular those that propagate the cell death message, are largely unknown. Ca2+ has been proposed as a ‘master’ cell death messenger (Figure 2). The onset of apoptosis is indeed frequently accompanied by drastic alterations in cytoplasmic Ca2+ concentration, and several crucial apoptosis effectors are known to depend on Ca2+.3, 58, 63, 80, 89, 122 However, Ca2+ diffusion through GJs may be limited by its interactions with more slowly mobile Ca2+-binding proteins. The Ca2+ messenger IP3, produced by phospholipase C activation and triggering Ca2+ release from the endoplasmic reticulum (ER), is probably a better suited candidate as it can pass through GJs,123 its ER IP3-receptor is modulated by Bcl-2124, 125 and the ensuing Ca2+ changes may trigger cytochrome C (CytC) release from mitochondria.126 Released CytC on its turn can interact with IP3 receptors to potentiate ER Ca2+ release and to exacerbate mitochondrial Ca2+-driven CytC release in a vicious circle.127 Recent work further suggests that the pattern of Ca2+ changes – steady or oscillatory changes – may determine the outcome towards either cell death (sustained Ca2+ change) or survival (Ca2+ oscillations).128 The signature of the Ca2+ signal is largely influenced by the level of IP3 and the sensitivity of its receptor.129 As a consequence, the modulation of IP3 receptors by Bcl-2 family proteins125 will determine the Ca2+ load of mitochondria and will thus be expected to be decisive in initiating apoptosis through mitochondrial CytC release. CytC has too high a molecular weight (12.4 kDa) to pass as a death messenger through GJs or HCs, so IP3 remains as a very likely candidate to communicate the cell death message. Other proposed candidate ‘killer messengers’ that can pass through GJs include cAMP and cyclic guanosine monophosphate (cGMP).58, 74 Potential ‘rescue messengers’ on the other hand include the energy molecules glucose and ATP or the free radical scavengers ascorbic acid and reduced glutathione that are all able to flow through GJs and favor cell survival.3 GJ channels display selective permeability towards the proposed messengers and this typically depends on their Cx composition.15, 16, 17, 18, 19 Seul et al.74 found that adenoviral delivery of Cx37, but not of the other vascular Cx40 and Cx43, induces apoptotic cell death in human umbilical vein endothelial cells. This effect was cell- and species-specific as Cx37 did not trigger cell death in mouse N2A neuroblastoma cells and rat NRK kidney epithelial cells. These findings demonstrate that conveying a cell death or survival response through GJ channels is a selective and well-coordinated process, involving specific Cxs and biochemical messengers rather than just the movement of common noxious or vital molecules between cells.
Connexin-Based Hemichannels and Cell Death
For a long time, HCs were classified as mere structural precursors of GJs. A large body of recent evidence, however, suggests that they must be considered as functional channels controlled by various extracellular and intracellular signals, thereby providing a unique pathway for transport and signaling. Of note, many of the signals that trigger HC opening, or responses attributed to HCs, are also involved in the signaling cascades leading to cell death,11 including cytoplasmic Ca2+ changes and oxidation or nitrosylation reactions. Being a pore permeable to quite a large range of substances, HC opening may furthermore help in setting off cell death by causing membrane depolarization, the collapse of ionic gradients, loss of small metabolites and elevation of cytoplasmic Ca2+.130
As holds for GJs, cell death may have a profound influence on the status of the HCs (Table 2). This has been well exemplified in the case of ischemia-related cell injury where the involvement of HCs as ‘pathogenic pores’ has been demonstrated.3, 33 Indeed, metabolic inhibition of astrocytes was found to accelerate cell death, which was directly associated with Cx43 HC opening. The molecular mechanism by which it activates HCs is, however, not entirely known, but may involve dephosphorylation and/or oxidation.31, 32 With respect to the latter, Retamal et al.31 showed that nitrosylation of intracellular Cx43 cysteine residues by nitric oxide (NO), a protein modification likely to occur under oxidative stress, could be at the heart of HC opening. Along the same line, NO was found to mediate Cx43 HC activation in astrocytes under proinflammatory conditions.131 The importance of oxidative stress as a key trigger is underscored by the observation that cigarette smoke extract and H2O2 may open HCs by depolarizing the cells, thereby facilitating ROS entry into the cell.30 HC function may also be drastically affected by genetic factors. Mutations in Cx32, Cx30 and Cx26 genes result in hereditary peripheral neuropathy, hidrotic ectodermal dysplasia, and nonsyndromic hereditary hearing impairments and skin disease, respectively. In all cases, the phenotype is caused by abnormal HC opening which could adversely affect cell viability.34, 35, 36, 37, 132, 133 Gomez-Hernandez et al.35 revealed that HC dysregulation in inherited peripheral neuropathy, caused by a Cx32 mutation, is due to alterations in a Ca2+-binding site that interacts with extracellular Ca2+ to keep the HCs closed under physiological conditions. A similar mechanism could account for aberrant HC gating and cell death caused by a Cx26 mutation located right next to this putative Ca2+-binding site, a mutation that is known to lead to nonsyndromic hereditary deafness.34
Overall, there are at least four possible mechanisms by which HCs could contribute to cell death or survival (Figure 2). First, the bidirectionally permeable HC pathway may facilitate the uptake of toxic or survival-enhancing substances, and may contribute to the loss of essential metabolites.30, 38, 59, 70, 134, 135, 136, 137 As well-documented ATP release channels, HCs may lower the intracellular ATP content and play as such a decisive role in the balance between cell death through necrosis or apoptosis.63, 70, 138 ATP is also necessary for the phosphorylation of Cxs which, on its turn, influences HC gating.28, 32, 139, 140, 141 In Shigella infection, hemichannel ATP release may promote bacterial invasion and dissemination.142 Another compound released through HCs is glutathione.43 The loss of intracellular glutathione may compromise the antioxidant defense at the cells’ inside but its consequent accumulation outside the cells may as well act beneficially as it can intercept in a more direct manner invading free radicals threatening the cell.43 Another potentially beneficial role of Cx43 HCs is suggested from experiments in astrocytes that demonstrated increased open probability of Cx43 HCs and glucose uptake in response to exposure to proinflammatory cytokines.131
A second level where HCs can influence the balance between cell death and survival involves a paracrine communication component. The release of metabolites such as ATP, glutamate or prostaglandins through HCs combined with their extracellular diffusion and action (directly or through breakdown products like adenosine)143, 144 on corresponding receptors on remotely located cells may exert toxic as well as survival effects.145, 146, 147, 148, 149, 150, 151 Ligand-receptor binding of these messengers is often accompanied by a rise in cytoplasmic Ca2+,126, 145, 152, 153, 154 that on its turn may trigger a new cycle of HC responses or is even influenced by HC activity.26, 35, 38, 126, 152 In a model of cochlear explant cultures, the local infliction of a cell-damaging stimulus caused a spatiotemporal spread of cell death in hair cells that was related to ERK1/2 activation, dependent on the associated intercellular Ca2+ wave and ATP release, and inhibited by carbenoxolone.155 Once released, ATP is rapidly degraded to adenosine which displays both neuroprotective and -toxic properties.143, 144 Combined in vitro and in vivo studies have demonstrated that ischemic pre-conditioning in the brain promotes ATP efflux through HCs and thereby protects against a second exposure to ischemic conditions through adenosine.156 Another messenger released through HCs is glutamate, a well-documented paracrine messenger of cell death in the brain. The presence of this substance, released by HCs, in conditioned media from microglia and macrophages treated with proinflammatory molecules resulted in marked neuronal cell death when neurons were exposed to it.136, 157 Conditioned media from activated microglia also affected astrocytes as it reduced their GJIC and induced HC opening.131 The latter can have a drastic influence on neuronal survival as well, as the capacity of ‘spatial buffering’, which is provided by coupling of astrocytes through GJ channels and is essential for the control of the composition of the extracellular environment, decreases.3, 158 This is observed in an ex vivo model for spinal cord injury where Cx43 channels appeared to play a dual role; HCs seemed to be involved in cell swelling and the spread of neurotoxins early after injury, whereas GJs were required for spatial buffering between astrocytes and long-term survival of neurons.159 A paracrine signaling component may not only be of importance for the expansion of cell death or survival but could also assist in the recruitment of both innate and adaptive components of the inflammatory response system.160 Certain types of dead cells can trigger inflammation by release of danger signals or ‘damage-associated molecular patterns’ that are normally located inside the cells.161, 162 At a more speculative level, it is conceivable that these endogenous danger signals (e.g., uric acid, 168 Da) may be shared through GJs with neighboring cells and released through HCs.
A third cell survival/cell death regulatory platform includes HCs as a transmembrane signal transduction pathway. The prototypic example here is the involvement of HCs in the anti-apoptotic actions of alendronate, a drug used to counteract osteoporosis. Alendronate induces the opening of Cx43 HCs in dexamethasone-treated osteoblasts and osteocytes, which activates Src kinase and ERK. Subsequent phosphorylation by the p90 ribosomal S6 kinase (p90RSK) leads to an inactivation of the cytoplasmic pro-apoptotic Bcl-2 protein Bad and binding of pro-caspases by the phosphorylated CCAAT/enhancer-binding protein β (pC/EBPβ), both favoring survival of osteoblasts and osteocytes.163
A fourth possible link between HCs and cell survival/cell death relates to modifications in the subcellular localization of HCs. Upon ischemic pre-conditioning, a form of cardioprotection, Cx43 translocates from the PM to the inner mitochondrial membrane through a heat-shock protein 90-dependent pathway.164, 165, 166 The functional relevance of mitochondrial Cx43, however, is not clear. It has been postulated that Cx43 is part of a multiprotein complex that somehow controls mitochondrial homeostasis.117 Mitochondrial Cx43 could also form HCs that serve as a conduit for ion fluxes,59, 165, 166, 167 a function reminiscent of the apoptosis-regulating Bcl-2 family proteins.117 Mitochondrial Cx43 was recently found to be a major regulator of cardiomyocyte apoptosis.117
Non-Channel Aspects of Connexins in Relation to Cell Death
Several studies have shown that Cx proteins as such can influence tissue homeostasis independent of their channel-forming capabilities. In most cases, the evidence is based on experiments in which Cx expression was artificially modified (Table 1). Cx overexpression was found to trigger cell cycle arrest168, 169, 170, 171, 172, 173 and cellular differentiation174 without influencing Cx channel activity in any way. In a similar manner, transfection of C6 rat glioma cells with Cx43, Cx40 or Cx32 genes resulted in an increased resistance to exogenously induced cellular injury, independently of GJIC.110 Forced expression of Cx43 in U251 human glioblastoma cells, on the other hand, did not increase GJ coupling but enhanced the apoptotic response to chemotherapeutics.69 Furthermore, research in a model of apoptosis-primed primary quail granulosa cells showed that Cx43 expression was inversely related to both the apoptotic index and the level of GJIC, suggesting distinct roles for GJIC and Cx43 in cell death and cell survival, respectively.89
The mechanisms that underlie non-channel Cx protein contributions to cell death remain to be elucidated (Figure 2). It has been suggested that Cxs participate in cell death pathways through direct interaction with apoptotic factors. The cytoplasmic co-localization of Cx26 and Cx43 with the Bcl-2 proteins Bak, Bcl-xL and Bax, in human breast cancer cells and human colorectal cancer cells, respectively, could be in favor of this idea.175, 176 More recently, Cx43 was reported to directly interact with apoptosis signal-regulating kinase 1 (ASK1).106 Cxs may also be involved in the control of cell death-related gene expression. A number of papers have reported changes in the expression of individual subsets of apoptotic factors while interfering with Cx expression.67, 68, 69, 72, 75, 76, 168, 177 Microarray analysis of heart tissue from Cx43 knockout mice showed altered expression of a wide spectrum of apoptotic genes, including Bok, Bax, Bid, Diablo, caspase 6 and caspase 9.114 Iacobas et al.178 performed a similar in-depth study, by analyzing the transcriptome of Cx43-null astrocytes in mice. Interestingly, they showed that both pro-apoptotic (e.g., Map4k) and anti-apoptotic (e.g., Bcl-xL) genes are affected, a finding that might explain the often contradictory reports, associating both induction and inhibition of apoptotic cell death with the presence of Cxs. The exact nature of the link between Cxs and apoptosis-related gene expression is still a matter of debate. An attractive hypothesis is that Cxs are directly involved in transcriptional control. In this respect, ‘Cx response elements’ have been proposed to modulate gene expression in rat osteocytes.179, 180 An active role for Cxs in the regulation of gene expression is further supported by the observation that (transfected) Cxs, or at least specific parts of these molecules (i.e. the C-terminal region), can reside in the nuclear compartment.170, 181, 182 The latter may, however, also be a result of the well-known interaction of Cxs with transcriptional regulators and/or mediators of crucial signaling pathways. A broad range of Cx-binding partners have actually been characterized, some of which are acknowledged regulators of gene expression.183, 184 Cx43, for instance, interacts with β-catenin, a key player in Wnt signaling.185 In the cell nucleus, β-catenin forms a complex with the T-cell factor that facilitates the transcription of a number of target genes that are relevant to apoptosis, including survivin,186 Bcl-xL187 and Bcl-2.188 Cx43 expression itself is also controlled by Wnt signaling.185 In fact, TNFα and TRAIL not only increase Cx43 degradation but also augment the Cx43 mRNA content in human osteosarcoma cells. The enhanced Cx43 gene transcription is thought to represent a reflexive response to apoptosis and is likely to be mediated by β-catenin.189
Pannexins and Cell Death
The structural and functional similarities between Cxs and Panxs raise the possibility that Panxs might be implicated in cell responses to several pathological insults as well, for example ischemic neuronal cell death. Exposure of pyramidal neurons from cortex or hippocampus to oxygen and glucose deprivation (OGD), a condition that mimics some aspects of ischemia, triggered opening of a large conductance and the bidirectional transfer of small fluorescent tracer molecules.52 Long OGD exposures resulted in irreversible current activation, neuronal swelling and membrane breakdown. Based on the absence of Cxs but presence of Panx1 in these neurons, the large single channel conductance and the effect of the (non-specific) blockers carbenoxolone and the HC-inhibiting La3+ ions, the authors concluded that these responses are likely to be mediated by Panx1 HCs. The mechanism by which OGD leads to Panx HC opening is not clear but may involve an increase in cytoplasmic Ca2+, which is known to occur in hippocampal neurons after ischemic injury and to activate Panx HCs.56, 152, 153 The proposed mechanism of dephosphorylation-induced opening of Cx43 HCs in metabolically inhibited astrocytes could also account for Panx HC opening as multiple phosphorylation sites have been predicted in both the cytoplasmic loop and the C-terminal tail of the Panx protein.45 There is, however, no clear evidence yet of functional modulation of Panx HCs by this covalent modification.
Similar to Cxs, Panx1 was found to be critical for inflammatory responses in lipopolysaccharide-stimulated macrophages pulsed with ATP53 or exposed to the pore-forming toxins nigericin and maitotoxin,190 through HC-dependent or HC-independent mechanisms respectively. With respect to the former, studies further demonstrated that Panx1 HC opening can be induced by ATP stimulation of P2X7 receptors (P2X7R) and thereby provides an entry pathway for bacterial inflammatory proteins to make their way to the cytosol.191 P2X receptors are a family of ionotropic receptors that open non-selective cation channels when activated by pyrimidine nucleotides. Interestingly, during prolonged agonist exposure, certain of these receptors like the P2X7R lead to the opening of a non-selective pore capable of passing large hydrophilic molecules, leading to cell death by apoptosis or necrosis.147, 148, 192, 193, 194 In fact, many of the characteristics of the P2X7R-activated pore seem to match those of HCs, including blockade by prototypical GJ channel blockers.195 A number of studies have demonstrated that the large permeabilization pore may correspond to Panx1 HCs being recruited by prolonged P2X7R activation.53, 190, 193, 196 Binding of the tyrosine kinase Src to the P2X7R seems to be a crucial step in this process.196 In support of this finding is the observation that prolonged stimulation of the P2X7R by ATP or an agonist induced cell death in oocytes and human astrocytoma cells, a process that was affected by carbenoxolone. Thus, Panx1 appears to be the molecular substrate for the permeabilization pore or ‘death receptor channel’ recruited into the P2X7R-signaling complex.193 Panx1 HCs can also be activated by ATP through the metabotropic P2Y1 and P2Y2 receptors, presumably through increases in cytoplasmic Ca2+.56 This, however, is not accompanied by subsequent membrane permeabilization and is therefore thought to serve more physiological functions, such as the communication of Ca2+ signals between cells,55 a communication pathway that may be further supported by Panx1 GJs connecting the cells.48, 55, 56 In addition, a recent study suggests that Panx1 may also be present in the ER, forming Ca2+-permeable channels and representing one of the mechanisms responsible for ER Ca2+ leak.48 The latter may on its turn trigger apoptotic cell death by facilitating Ca2+-induced opening of the mitochondrial permeability transition pore, which has been implicated in the release of CytC from mitochondria.126, 197
In contrast to Panx1, a neuroprotective role was proposed for Panx2. De novo and transient expression of Panx2 in astrocytes was observed in the brain of adult rats following ischemia-reperfusion and in co-cultures of hippocampal neurons and astrocytes. The authors hypothesized that Panx2 mediates its neuroprotective effect through the formation of HCs allowing the release of signaling molecules devoted to influence the cellular metabolism and the redox status of the surrounding environment.198
Conclusions and Perspectives
The maintenance of the homeostatic balance is controlled by the global interplay between three major communicative networks that make use of extracellular, intracellular and intercellular signaling pathways. Direct intercellular communication is mainly mediated by GJ channels composed of Cxs. The key roles of GJs in the control of cellular proliferation and differentiation have been demonstrated at numerous occasions over the last few decades.12, 15, 57 Their participation as mediators of cell death communication, particularly of apoptotic cell death, has only gained interest in recent years but has already brought up the important insight that not only GJs but also their structural precursors, the HCs and the Cx proteins as such, influence the cell death process. Strikingly, Cx-related communication has been found to both facilitate or counteract the cell death process. Such opposed functions may, to some extent, relate to differences in the model systems used, including the mode of cell death induction. Different cell death activators may indeed recruit distinct signaling cascades and messengers that may or may not be able to pass or activate Cx channels. An additional factor that may complicate the situation is the fact that the two channel types, although composed of the same protein, are differentially regulated. Under normal conditions, GJs are open and HCs are closed and two recent papers indicate that these two channels can be differentially influenced by the same stimulus,28, 131 for example by arachidonic acid which inhibits GJs and potentiates HC responses. The decision to stay alive or die may further depend on the condition of the cell receiving the message carried through Cx channels. Thus, if the concerned cell is concomitantly exposed to stress stimuli, then Cx-related communication may switch from a survival program to a death mode. Furthermore, the contributions of Cxs to cell death communication may be adjoined by the Panx channel family. The specifics and possible differences in the regulation of Cx versus Panx channels are currently largely unknown and a major challenge for future work is to elucidate the exact contribution of GJs and HCs composed of either Cxs or Panxs, to cell death processes of both the apoptotic or non-apoptotic type. An equally important challenge concerns the development of specific blockers that affect HCs or GJs only. Comparisons between Cx-expressing cells and cells treated with protocols to silence the concerned gene or obtained from knockout animals are necessary to unequivocally determine the involvement of Cx HCs.195 Knockout animal models can, however, not be used to establish the involvement of Cx HCs in vivo because both GJs and HCs are suppressed in that case. The quest is still open but progress is, as expected from channels composed of the same building blocks, not in immediate sight. The molecular principles to distinguish GJs from HCs are still hazy. For instance, Cx mimetic peptides composed of a short stretch from one of the extracellular Cx loops are actually expected to open the HCs by a process similar to ‘loop gating’ but these substances turn out to inhibit the responses attributed to HCs. Clearly, further work is needed to bring progress in this complex but tantalizing field: two distinct channels formed by a single protein that in addition (and beyond its channel function) has intrinsic signaling functions is not a simple case at all! In summary, Cxs and Panxs as well as their corresponding channels represent multilevel platforms for cell death-related signaling. It is expected that, upon the introduction of appropriate experimental tools, more insight will be gained into the exact molecular mechanisms that underlie Cx- and Panx-inherent communication in (apoptotic) cell death.
Abbreviations
- ATP:
-
adenosine triphosphate
- Bcl-2:
-
B-cell lymphoma-2
- cAMP:
-
cyclic adenosine monophosphate
- cGMP:
-
cyclic guanosine monophosphate
- Cx:
-
connexin
- CytC:
-
cytochrome C
- ER:
-
endoplasmic reticulum
- GCV:
-
ganciclovir
- GJ:
-
gap junction
- GJIC:
-
gap junctional intercellular communication
- HC:
-
hemichannel
- HSV-tk:
-
herpes simplex virus-thymidine kinase
- IP3:
-
inositol trisphosphate
- MEK/ERK:
-
mitogen-activated protein kinase kinase/extracellular signal-regulated kinase
- NAD+:
-
nicotinamide adenine dinucleotide
- NO:
-
nitric oxide
- OGD:
-
oxygen/glucose deprivation
- P2X7R:
-
P2X7 receptor
- p90RSK:
-
p90 ribosomal S6 kinase
- Panx:
-
pannexin
- pC/EBPβ:
-
phosphorylated CCAAT/enhancer-binding protein β
- PM:
-
plasma membrane
- ROS:
-
reactive oxygen species
- TNFα:
-
tumor necrosis factor α
- TRAIL:
-
TNF-related apoptosis-inducing ligand
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Acknowledgements
This work is supported by the Fund for Scientific Research Flanders (FWO-Vlaanderen), Belgium (grant nos. G.0354.07 and G.0140.08 and G.0134.09 to LL) and the Interuniversity Attraction Poles Program (Belgian Science Policy, project P6/31) and the Research Council of the Vrije Universiteit Brussel (OZR-VUB). Special thanks go to the European FP6 projects carcinoGENOMICS and LIINTOP.
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Decrock, E., Vinken, M., De Vuyst, E. et al. Connexin-related signaling in cell death: to live or let die?. Cell Death Differ 16, 524–536 (2009). https://doi.org/10.1038/cdd.2008.196
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DOI: https://doi.org/10.1038/cdd.2008.196
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