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Logo of arthrestherBioMed Centralbiomed central web sitesearchsubmit a manuscriptregisterthis articleArthritis Research & Therapy
Arthritis Res Ther. 2009; 11(4): 237.
Published online Aug 4, 2009. doi:  10.1186/ar2752
PMCID: PMC2745781

Is there a feudal hierarchy amongst regulatory immune cells? More than just Tregs

Abstract

Nature has provided the developing immune system with several checkpoints important for the maintenance of tolerance and the prevention of autoimmunity. The regulatory mechanisms operating in the periphery of the system are mediated by subsets of regulatory cells, now considered principal contributors to peripheral tolerance. Regulatory T cells (Tregs) have received titanic interest in the past decade, placing them at the centre of immuno-suppressive reactions. However, it has become clearer that other immune suppressive cells inhibit auto-reactivity as effectively as Tregs. The function of Tregs and other regulatory cells in rheumatoid arthritis will be discussed in this review.

Introduction

Rheumatoid arthritis (RA) is an autoimmune disorder characterized by chronic systemic and synovial tissue inflammation that, if not therapeutically tackled, ultimately leads to bone and cartilage destruction. Like other auto-immune diseases, RA results from a cascade of reactions, beginning with the breakdown of tolerance and leading to dysregulated chronic inflammation in one or multiple organs [1]. During synovial inflammation, critical events include neo-angiogenesis, cellular hyperplasia, and a massive influx of inflammatory cells such as T cells, B cells, fibroblast-like syno-viocytes, macrophages, and dendritic cells (DCs). Cellular infiltration, and subsequent cellular proliferation, is largely orchestrated by a complex interplay of pro-inflammatory cytokines, chemokines, and matrix metalloproteinases [1,2]. In addition to expressing a variety of pro-inflammatory cytokines, the joint hosts immunosuppressive cells producing anti-inflammatory cytokines (that is, IL-10 and transforming growth factor (TGF)β) [3]. The balance between the various regulatory CD4+ T cell subsets, collectively termed regulatory T cells (Tregs), IL-10-producing regulatory B cells (Bregs), regulatory DCs and suppressive macrophages on the one hand, and pro-inflammatory effector lymphocytes and monocyte-derived cells on the other, is likely to dictate the choice between tolerance and autoimmunity. In this review we have collated data from models that demonstrate the existence of different regulatory cells to generate a more unified view of how immunoregulatory cells may cooperate in the choice between maintenance and breakdown of tolerance in chronic inflammation.

Regulatory cells: is there only one immunoregulatory queen? Regulatory T cells

Regulatory CD4+ T cells can be divided into two main subsets, natural Tregs (nTregs) and induced Tregs (iTregs), which develop in the thymus and the periphery, respectively. nTregs express the transcription factor forkhead box protein 3 (FoxP3) during development in the thymus [4]. FoxP3 plays a key role in a sophisticated developmental program that nudges the immature T cell lineage into a regulatory pathway during positive selection on high affinity T cell receptor ligands [4]. Via the T cell receptor, activated Tregs can exert non-antigen specific bystander suppression of other T cells [5]. Tregs have been shown to require cell-to-cell contact to suppress target cells in vitro [6]. Binding of CTLA-4 on Tregs to CD80 and CD86 on effector T cells (Teffs), infusion of cyclic AMP through gap junctions or direct cytolic mechanisms have been reported to be involved in Treg-mediated suppression [7]. In addition, Treg expression of glucocorticoid-induced tumour necrosis factor receptor (GITR) and Neuropillin-1 facilitate cell contact-mediated suppression of non-T cells such as endothelial cells and antigen-presenting cells (GITR) or DCs (Neuropillin-1) [8,9]. Efficient regulatory function requires an initial burst, followed by consumption, of endogenous IL-2 followed by the release of other soluble factors such as IL-10 and/or TGFβ and IL-35 [10-13].

Unlike FoxP3+ nTregs, which are fully functional upon thymic exit, iTregs are generated from naïve CD4+ T cells in the periphery, where they acquire suppressive capacity [14]. iTRegs can acquire the expression of FoxP3 (FoxP3+ iTregs) in response to antigens presented on non-inflammatory antigen-presenting cells coupled to TGFβ and IL-2. FoxP3+ iTregs also require Foxp3 for their suppressive activity and phenotypic stability [7,14]. Data from several studies support the notion that iTregs are as important as nTregs in peripheral tolerance. In mice, FoxP3+ iTregs effectively control experimental autoimmune encephalomyelitis (EAE), colitis and type 1 diabetes [15-17]. Early thymectomised mice display impaired nTreg development but normal Foxp3+iTreg numbers, and these mice develop a less severe disease than Foxp3-deficient mice, suggesting that, early in life, iTreg cells may be vital due to the delay in nTreg development [18]. In addition, the foetal peripheral adaptive immune system generates FoxP3+ iTregs, in response to cross placenta maternal cells, that inhibit anti-maternal immunity. These iTregs persist at least into early adulthood [19]. iTregs are also important in adult life as they have been identified in situ and positively correlate with a clinical improvement of allergy symptoms [20]. Nonetheless, it remains difficult to dissect the relative contributions of iTregs and nTregs in the maintenance of tolerance, since once in the periphery they are phenotypically undistinguishable.

FoxP3- iTregs can be identified based on their specific cytokine profile, producing only IL-10 and/or TGFβ [21,22]. FoxP3-iTregs display a low proliferative capacity and inhibit the development of both Th1-mediated experimental autoimmune diseases and Th2-mediated allergy [21,23]. They are induced in vitro and in vivo by sustained stimulation with IL-10, immature DCs or a combination of vitamin D3 and dexamethasone [24,25]. FoxP3- iTregs also include TGFβ-producing Th3 cells and CD4+CD25- latency-associated peptide (LAP)+ T cells, which are central in mediating oral tolerance [26]. Th3 regulatory cells depend on IL-2 for survival and exert suppression primarily via TGFβ, but also via IL-10 [27,28]. LAP+CD4+CD25- T cells are important in the inhibition of diabetes and colitis, and suppression is TGFβ-dependent but IL-10-independent [21,29].

Other lymphocytes, including CD8+FoxP3+ cells, γδ and invariant natural killer T cells are immunosuppressive [30-32], but since their functions in RA remain largely elusive they have not been included in this review.

Regulatory cells in human rheumatoid arthritis and in experimental arthritis

The first clues that Tregs are critical in mediating protection from arthritis were provided by the observations that depletion of CD4+CD25+ cells in a collagen-induced arthritis (CIA) model, which closely mimics RA, resulted in increased severity and incidence of CIA [33] and that adoptive transfer of CD4+CD25+ cells in the early stages of disease slowed CIA progression [34]. The transferred Tregs migrated to the arthritic joint where they acted locally to reduce inflammation [34]. However, it could not be definitively concluded that exacerbation of the disease seen following depletion of CD4+CD25+ cells was exclusively due to Treg depletion, as it may also be a result of the depletion of other regulatory CD25+-expressing cells, such as CD8+ T cells, Tr1, or Bregs [35]. Several other studies, using a variety of experimental models for arthritis, have now confirmed the importance of Tregs in 'dampening' arthritogenic responses [36-38] and their relevance in the maintenance of a 'stable' non-immuno-genic environment.

Translation of data from experimental models to patients with RA has proved to be challenging. Our laboratory originally reported that Tregs are dysfunctional in RA as they cannot suppress tumour necrosis factor (TNF)α and interferon (IFN)γ released by responder CD4+ T cells [39]. We and others have also described that therapies that target TNFα, such as infliximab, increase the percentage of Tregs in circulation, and that Tregs isolated from patients responding to anti-TNFα therapy reacquire suppressive capacity [39,40]. Valencia and colleagues [40] elegantly demonstrated that TNFα directly suppresses human Tregs via signalling through TNF receptor II and inhibition of FoxP3 transcription. van Amelsfort and colleagues [41] have also shown that Tregs cultured with pro-inflammatory cytokines lose their capacity to inhibit responder T cell proliferation and cytokine production. However, paradoxically, TNFα is a potent immuno-modulator of CD4+ T cells and can, in some cases, prevent experimental autoimmune diseases such as type I diabetes and lupus [42,43]. In addition, TNF receptor II is chiefly expressed on both human and murine Tregs and is associated with higher suppressive capacity [44,45]. The dual functions of TNFα suggest that the mechanisms driving the induction of Tregs after TNFα blockade have not been completely elucidated.

Equally, the data relating to Treg number and function in RA are a complex jigsaw that remains to be assembled. In contrast to the lack of inhibition exerted by Tregs identified as CD4+CD25high and isolated from peripheral blood, other studies have shown that CD4+CD25+ Tregs isolated from joints of patients with active arthritis had a more powerful suppressor activity than peripheral CD4+CD25+ Tregs [46]. There is a disparity between the number of Tregs found in the peripheral blood of RA patients compared to the numbers of Tregs isolated from the joint of the same individuals, with more Tregs in the inflamed joints than in circulation, suggesting that compensatory mechanisms take place at the site of inflammation [46,47]. The discordance between different studies could be due to different methods of Treg purification (inclusion of all CD25 [46] versus the inclusion of only CD4+CD25high T cells [39]) and/or a difference between the choices of the patients enrolled in each study. Whereas in our study only patients who failed all the conventional treatments and, hence, had more active RA were assessed, RA patients with a broader range of clinical scores were included in the van Amelsfort study [39,41]. These results suggest that the overall degree of inflammation, the balance between pro- and anti-inflammatory cells and the amount of cytokines they produce might influence Treg suppressive capacity.

CD4+ T cells producing IL-17 (Th17) play a pivotal role in the induction of arthritic diseases and should also be included in this complex 'balancing equation' [48,49]. Aberrant Th17 responses have been found in several experimental autoimmune models, including CIA [50] and EAE [51]. Patients with juvenile idiopathic arthritis displayed an increased number of IL-17+ cells in both their synovial fluid and peripheral blood compared to the numbers in the peripheral blood of healthy volunteers [52]. It has been recently reported that disease severity in juvenile idiopathic arthritis is positively correlated with the numbers of Th17 cells and inversely correlated with Treg number, although not with their function, suggesting that the balance of Th17 cells and Tregs may be critical for disease outcome [52]. At the moment it remains to be formally proven whether functionally active Tregs can limit Th17 expansion or whether an uncontrolled Th17 expansion observed in patients with RA is responsible for the lack of Treg suppression.

The first evidence for the existence of IL-10-producing CD4+ T cells in inflamed synovia was provided in 1994 by Feldman and collaborators [53], who showed that IL-10 was spontaneously produced in most synovial tissues isolated from RA patients. The major producers of IL-10 were T cells in the mononuclear cell aggregates and monocytes in the lining layer. The authors also showed that neutralization of endogenously produced IL-10 in the RA synovial membrane cultures resulted in increased levels of the pro-inflammatory cytokines TNFα and IL-1β, thus demonstrating the active anti-inflammatory role of IL-10.

The discovery of new and more specific markers has allowed better discrimination of the various Treg subsets in vivo. Comprehensive studies comparing different Treg subsets should be carried out in the same cohorts of patients to give an overview of how the inflammatory environment influences all Treg responses in patients with RA. Fundamentally, a more 'holistic' approach should be considered for shaping future therapies as it is likely that the effect of anti-inflammatory cytokines released by Tregs, such as IL-10 and TGFβ, is antagonised by the myriad pro-inflammatory factors present in the synovia. Perfusion of Tregs is unlikely to provide a long standing clinical benefit to patients with active autoimmune disease unless the pro-inflammatory environment is reconditioned to a 'neutral state', where Tregs can effectively maintain tolerance rather than re-condition existing inflammation (Figure (Figure11).

Figure 1
The balance between pro- and anti-inflammatory cell types and cytokines dictates arthritic disease development. (a) During inflammation the joint is overwhelmed by an influx of pro-inflammatory cell types. This activates the immune cells such as macrophages ...

Are other immune regulatory cells the 'vassals' of regulation?

Regulatory B cells

Traditionally, B cells have been seen as antibody secreting 'machines', but recently their capacity to produce distinct arrays of cytokines during chronic inflammation has been explored. Several groups have described B cells with regulatory function (Bregs) that can restrain immune responses and prevent autoimmune diseases, including arthritis [35,54]. Bregs were originally identified by Charles Janeway, who showed that B cell-deficient mice immunized with myelin basic protein in complete Freund's adjuvant were unable to recover from EAE [55]. These original data were confirmed and extended by Fillatreau and colleagues [56], who revealed that resolution of disease depends upon the presence of IL-10-producing B cells. Further, we have demonstrated that in vitro activation of arthritogenic B cells with an agonistic anti-CD40 induces the differentiation of IL-10-producing B cells. When adoptively transferred, these activated B cells can control CIA development via the suppression of the autoreactive Th1 response [57]. These results were consistent with the inhibition of the spontaneous Th1 response of Palmerston North mice with lupus-like disease after the adoptive transfer of CpG-activated IL-10-producing B cells [58]. In addition, it has been reported that treatment of DBA/1 mice with apoptotic cells at the time of immunization with collagen type II (CII) suppresses Th1 differentiation and antibody production, and protected mice from arthritis via the induction of IL-10+ Bregs [59].

Unlike the Treg field, there is a lack of overall consensus about the combinations of markers that identify Bregs. We recently demonstrated that the IL-10+ B cells in the CIA model are confined within the immature transitional 2-marginal zone precursor (T2-MZP) B cell subset and are CD19+, CD21high, CD23high, CD24high and CD1dhigh[60]. Adoptive transfer of T2-MZP B cells from naïve or convalescent mice prevented the recipient syngenic DBA/1 mice from developing arthritis. Although the mechanism of action of these T2-MZP Bregs has not been completely elucidated, we demonstrated that the protection is IL-10-mediated, since T2-MZP B cells isolated from IL-10 knockout mice failed to protect against the Th1-driven autoimmune response in recipient mice. Analysis of T cells isolated from T2-MZP B cell-treated mice revealed a reduction in proliferation following in vitro CII stimulation, confirming that Bregs can reduce autoreactive T cell responses [60]. Unlike other autoimmune models, depletion of Tregs using anti-CD25 antibodies did not alter the capacity of Bregs to suppress arthritis, suggesting that Bregs, at least in CIA, are not dependent on natural Tregs for their suppressive effects.

We have also identified B regs with similar phenotype (T2-MZP) in the MRL/lpr mice lupus-like disease model, and demonstrated that they can be enriched upon short term in vitro culture with agonistic anti-CD40 [61]. Transfer of anti-CD40-generated T2 B cells (T2-like Bregs) to syngeneic mice significantly improved renal disease and survival by an IL-10-dependent mechanism. In this model, T2-like Bregs not only suppressed Th1 responses, but induced the differentiation of FoxP3-IL-10+CD4+ T cells, which could regulate other CD4+ T cells. Interestingly, the therapeutic effect of Breg transfer could be recapitulated by administration of agonistic anti-CD40 [61]. Although the therapeutic use of agonistic anti-CD40 monoclonal antibodies is not a viable therapy for autoimmune diseases, enrichment of Bregs in vitro followed by their transfer might represent a feasible alternative for autoimmune patients who have failed other biological therapies.

Marginal zone B cells have been also proposed as candidates for Bregs in experimental models of rheumatic diseases due to their capacity to up-regulate IL-10 in response to CpG [62] or after exposure to apoptotic cells [59]. However, it remains to be formally proven whether their IL-10 production is paralleled by functional suppressive capacity. B-1 cells are also known to release IL-10 and IgM natural autoantibody and they have been proposed to play a protective role in individuals predisposed to autoimmunity and in patients with atherosclerosis via enhancing the clearance of apoptotic cells [63-65].

Despite increased interest in Breg biology, the existence of an equivalent population in humans has not yet been fully proven. Populations of IL-10-producing B cells have been identified in healthy individuals as well as in patients with multiple sclerosis [66]. However, their phenotype, suppressive functions and whether they can be exploited for immune therapy of autoimmune disease are the subject of current investigations.

Regulatory dendritic cells

DCs are mainly regarded as specialized professional antigen presenting cells. In a resting environment, in the absence of any inflammation or pathogenic elements, most DCs are at an immature stage of development, characterized by a high endocytic capacity and low surface expression of major histocompatibility (MHC) and co-stimulatory molecules. In the presence of microbial infections or inflammation, DCs rapidly mature and become activated [67]. The outcome of DC-T cell interactions is regulated by several factors, including the state of DC maturation and/or the presence of cytokines. Immature, or semi-matured DCs with low expression of CD40 and MHCII can tolerize T cells and prevent unwanted immune reactions. In the CIA model, stimulation of DCs with TNFα generates DCs with a strong suppressive capacity. Transfer of these TNFα-induced DCs suppressed arthritis in recipient syngeneic mice [68]. It is clear that the micro-environmental stimuli that condition DCs are important and numerous strategies based on immunosuppressive agents, such as vitamin-D3, IL-10, TGFβ, glucocorticoids, detaxomethasone, and N-acetyl-l-cysteine, have been used to induce tolerogenic DCs [69,70]. Amongst them, induction of regulatory DCs via stimulation with vasoactive intestinal peptide (VIP) holds therapeutic promise. Gonzalez-Rey and Delgado have shown that exposure of immature DCs to VIP induces the differentiation of tolerogenic DCs, which efficiently controlled the development of arthritis in an adoptive transfer system [71]. It is possible that maturing DCs exposed in vivo to VIP might differentiate into regulatory DCs that help to keep the regulatory pool 'topped up'.

Regulatory DCs also appear to be the mediators of oral tolerance, a process that refers to the immunological hypo-responsiveness initiated by ingestion of protein antigens [72]. Since oral tolerance is initiated in the gut-associated lymphoid tissue, DCs in the Peyer's Patches are believed to be responsible for priming CD4+ T cells that secrete IL-10 and IL-4 or TGFβ in response to oral tolerance regimes; thus, DCs appear to be inducing iTreg (Tr1 or Th3) differentiation [73]. Repeated oral administration of CII to susceptible strains induces tolerance and prevents the induction of CIA, which has been ascribed to a specific subset of DCs that are CD11c+ and CD11b+ [74]. The transfer of CII-pulsed regulatory DCs prevented arthritis development and promoted the differentiation of IL-10 and/or TGFβ-producing Tregs (Th3) [74-76] Unfortunately, despite positive results in both experimental arthritis and phase II trials, no effect was observed in phase III trials of CII in RA [77]. The possibility of harnessing DCs for the generation of both induced Tregs and adaptive Tr1 cells represents one of the major goals in immunotherapy at the moment as it could potentially replace non-specific immunosuppressive drugs.

Suppressor macrophages

Macrophages are present at sites of inflammation and have previously been shown to play a pivotal role in the induction and perpetuation of RA [78]. Recently emigrated monocytes mature into macrophages in the RA synovial membrane. Subsets of monocytes differentially colonize the synovial sublining and lining layer as well as the superficial and deep layers of the lining. A possible functional diversity of monocytes in these areas, which is emphasized by the expression of different activation markers and adhesion molecules, is believed to contribute to disease progression [79].

Like many other immune cells, the role of macrophages cannot be simply associated with inflammation, and a distinct subset of macrophages can also act as suppressive cells via immunomodulatory factors, including IL-10, reactive oxygen species (ROS), and tryptophan and arginine catabolism [80-82]. Macrophages can be divided into specific subsets according to functional and phenotypical criteria. 'Classically' activated macrophages are monocytes stimulated with IFNγ, alone or in combination with IL-12 and IL-23, which differentiate into M1-polarised cells that induce the differentiation of Th1 type responses. Conversely, monocytes activated in the presence of IL-4 and IL-13 differentiate into M2-polarized cells producing IL-10, which favours a Th2 type response [83]. Although not yet extended to arthritis, it is interesting to note that monocytes differentiating in the presence of Tregs acquire a suppressive phenotype and function [84]. Monocytes entering tissues can undergo phenotypic switches between M1 and M2 macrophage phenotypes due to soluble micro-environmental factors (cytokines, chemokines, growth factors, and tissue cells), and the balance of activated Teffs and Tregs affects their maturation [85]. In addition, macrophages differentiating upon stimulation with macrophage colony-stimulating factor express indoleamine 2,3-dioygenase and inhibit T cell proliferation in vitro by depleting the important amino acid tryptophan from co-cultures in response to T cell activation [86]. The adoptive transfer of in vitro TGFβ-generated antigen presenting F4/80+ peritoneal macrophages induced the differentiation of TGFβ-producing Tregs in primed and naïve mice. Interestingly, whereas in naïve mice the majority of induced Tregs were CD4+ and produced TGFβ, in primed mice the induced Tregs were CD8+ Tregs and the response involved Fas-mediated deletion of Teffs [87]. Macrophages derived from myeloid suppressor cells from tumour-bearing mice and cancer patients could suppress T cell proliferation in vitro and induce the differentiation of FoxP3+ Tregs in vivo using IL-10/IFNγ-dependent mechanisms [88]. In humans, monocyte-derived macrophages can convert CD4+ naïve T cells, but not activated T cells, into Tregs, suggesting that macrophages might curb immune responses during tolerogenic conditions but not during inflammation [89].

In the context of arthritis, it has been shown that macrophages control disease development via ROS. Mice with a mutation in the neutrophil cytosolic factor 1 (Ncf1) gene develop exacerbated arthritis, an enhanced IgG response and delayed-type hypersensitivity responses against CII [90]. Further work by the same group demonstrated that resistance to the disease relies upon the ROS produced by macrophages. Transgenic mice over-expressing functional Ncf1 in macrophages develop a significantly milder disease compared to wild-type mice and suppress T cell responses during antigen presentation [91]. Interestingly, whilst a significant reduction of IL-2 and proliferation was observed, the levels of IFNγ remained unchanged despite the reduced severity of the disease. Unequivocally, these studies challenge the common dogma that antioxidants are anti-inflammatory and provide an additional class of drugs with strong potential as therapeutics [92].

Conclusion

Our findings and those from others challenge the paradigm of Tregs as the sole co-ordinating cell type directly involved in the regulation of autoimmunity. Further study is needed to understand the interaction between different immunoregu-latory cells and unravel the outcomes of these interactions. A more cohesive approach aimed at the expansion of multiple regulatory cells could be the key to designing better therapies for RA. The interpretation of the collective data discussed in this review suggests that therapies aimed at drastically depleting or entirely eliminating T or B cells from patients with autoimmunity need to be carefully re-evaluated, since the depletion of regulatory subsets could have long-lasting deleterious effects.

Outstanding questions

It is well documented that deletion of FoxP3+ cells either in adult or neonatal mice can cause catastrophic autoimmunity [93] and FoxP3 mutations in humans cause lethal diseases [94,95]. Recent data have shown that the ablation of all DCs, although not only those with regulatory functions, leads to development of autoimmunity, which was, however, much milder than the aggressive rapidly fatal disease that occurs when Foxp3+ Tregs are deleted [96]. However, although it remains to be revealed whether the selective deletion of regulatory B cells, DCs or macrophages also leads to the development of severe forms of autoimmunity, until then regulatory T cells should be placed at the top of the putative 'regulatory pyramid'.

Abbreviations

Breg: regulatory B cell; CIA: collagen-induced arthritis; CII: type II collagen; DC: dendritic cell; EAE: experimental autoimmune encephalomyelitis; FoxP3: forkhead box protein 3; GITR: glucocorticoid-induced tumour necrosis factor receptor; IFN: interferon; IL: interleukin; iTreg: induced Treg; LAP: latency-associated peptide; MHC: major histocompatibility; nTreg: natural Treg; RA: rheumatoid arthritis; ROS: reactive oxygen species; T2-MZP: transitional 2-marginal zone precursor; Teff: effector T cell; TGF: transforming growth factor; TNF: tumour necrosis factor; Treg: regulatory T cell; VIP: vasoactive intestinal peptide.

Competing interests

The authors declare that they have no competing interests.

Acknowledgements

We would like to acknowledge Drs Paul Blair and Clare Notley for their critical evaluation of this manuscript. NC and our work are funded by the Arthritis Research Campaign (ARC) Programme grant MP/17707 to CM.

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