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Heat Shock Proteins as Endogenous Adjuvants in Sterile and Septic Inflammation¹

Department of Immunology, Weizmann Institute of Science, Rehovot, Israel

	Abstract

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

 
Heat shock proteins (HSPs) have been reported to stimulate the immune system via innate receptors. However, the role of HSPs as endogenous adjuvants has been challenged by reports claiming that pure HSPs are not innate ligands; it is only the bacterial molecules trapped by the HSPs that can signal the innate immune system. In this review, we discuss data suggesting that both views, in essence, are correct; pure HSPs are indeed innate immunostimulators, but HSPs can also function as transducers of pathogen signals. In other words, HSPs perform diverse functions in two alternative modes of inflammation: sterile inflammation, which results from endogenous stimuli and is necessary for body maintenance, and septic inflammation, which protects us from environmental pathogens. Endogenous HSPs are key players in the modulation of these two modes of inflammation, and as such, they are potential targets for new and more efficient therapies for cancer, infections, and autoimmunity.

	Introduction

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

 
Heat shock proteins (HSPs)³ were originally identified as a group of proteins inducible by heat shock, but it was soon discovered that HSPs could also be induced by other stimuli such as growth factors, inflammation, and infection (1). HSPs span a broad distribution of molecular masses (10–170 kDa) and intracellular locations and are involved in an ever-growing list of physiological processes (2). Nevertheless, a unifying theme of HSPs is their chaperone activity, which contributes to cell survival under stress by facilitating the proper folding of denatured proteins (2).

The high homology existing between human and microbial HSPs initially suggested that they could trigger autoimmune disorders through immune cross-reactivity. Indeed, HSP-specific immune responses have been implicated in the pathogenesis of type 1 diabetes mellitus (T1DM) (3, 4, 5), arthritis (6, 7, 8, 9), Behçet’s disease (10), and systemic lupus erythematosus (11). However, HSPs can also inhibit autoimmune diseases such as arthritis (12, 13, 14, 15, 16, 17) and T1DM (18, 19); these regulatory activities of HSP60 are beginning to be exploited for the treatment of human T1DM. The p277 peptide from human HSP60 (aa 437–460) has been reported to halt cell destruction in newly diagnosed T1DM patients, leading to lower requirements for exogenous insulin (20).

The role of HSPs in immunity got a new twist when HSPs were found to activate the immune system through nonclonal receptors such as TLRs. Srivastava and colleagues (21, 22) demonstrated that HSPs are endogenous adjuvants that could be used to induce strong tumor- or pathogen-specific immunity. These experiments paved the way to the discovery of the effects that HSPs have on macrophages (23, 24), dendritic cells (DCs) (23, 24), T cells (25, 26, 27, 28), B cells (29, 30), and NK cells via different receptors; some of these effects and the receptors involved are listed in Table I. However, the immunostimulatory activity of HSPs has been challenged recently by reports that assign the stimulus to bacterial contaminants in the HSP preparations and not to the HSPs themselves (31, 32, 33). These reports are compatible with the teaching that TLRs only recognize foreign molecules, contributing to discrimination between self and non-self (34). Therefore, we are left to wonder whether HSPs have any innate immune effects not due to bacterial contaminants. Moreover, does the copurification of HSPs with bacterial contaminants add anything to our knowledge of the roles of HSPs in vivo?

	Do pure HSPs have any effect on innate immunity?

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

Mammalian HSP70 and gp96 purified from murine livers and kidneys were shown to activate macrophages and DCs (41). Based on the mammalian origin of these HSP preparations and their purification by a pyrogen-free method, the effects of HSP70 and gp96 on macrophages and DCs cannot be easily assigned to bacterial contaminants. We have used human HSP60 and HSP70 produced in an eukaryotic cell-free system, and therefore free of bacterial contaminants, to demonstrate that pure HSP60 or HSP70 can activate primary macrophages and the macrophage-like cell line RAW (Nussbaum et al., manuscript in preparation). Moreover, mammalian cells induced to display HSP70 on their surface can activate macrophages by way of TLR2 and TLR4 signaling (42).

The effects of pure HSPs have also been studied on non-APC cell types. Highly purified HSP60 can stimulate T cells (25, 26, 27, 43). Moreover, synthetic peptides of human HSP70 (44) can activate NK cells, and a peptide of human HSP60 (25) as well as whole HSP60 can modify T cell behavior via TLR2 (25, 26, 27).

All in all, these results indicate that mammalian HSPs can activate innate immunity in the absence of bacterial contaminants. Although some of these effects seem to be mediated by TLRs, their participation in each one of the observed effects should be carefully analyzed. Whether microbial HSPs are also endowed with immuno-stimulatory activities is still open to speculation; however, the high degree of sequence conservation in HSPs throughout evolution suggests that HSPs from different organisms may share immuno-stimulatory properties.

Gao and Tsan’s experiments, in summary, do not invalidate the conclusion that mammalian HSPs may themselves function as endogenous adjuvants, but they rightly call our attention to the physiological role played by complexes of HSPs with other molecules, self and non-self. The nature of these complexes and their possible physiological significance should be considered.

	HSPs as carriers of self-molecules

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

 
HSPs can bind a broad array of peptides (23), including those that result from cell metabolism. Although the lifespan of such peptides within the cell is very short (45, 46), a fraction of them are likely to interact with endogenous HSPs, forming HSP-peptide complexes that reflect the intracellular environment and the state of the cell in which they were formed. These HSP-peptide complexes contribute to the fine-tuning of specific immune responses but can also play a role in immune-mediated disorders.

HSP-peptide complexes derived from cancer cells include tumor-associated Ags. Based on the immunostimulatory adjuvant properties of HSPs, these HSP-peptide complexes are likely to activate tumor-specific immunity and could therefore contribute to the immunosurveillance of tumors. Moreover, HSP-peptide complexes purified from tumors can also be used in cancer immunotherapy as a tool to induce strong antitumor immune responses in mice (47) and humans (48).

The same mechanism that facilitates the induction of effective antitumor immunity also might favor the development, under different circumstances, of pathologic autoimmunity. Brain samples taken from multiple sclerosis (MS) patients or from a rodent model of MS contain complexes of HSP70 with myelin basic protein or proteolipid protein (49), Ags that are well-known targets in MS (50). These HSP-peptide complexes facilitate peptide up-take and presentation, increasing the activation of the Ag-specific T cells that drive the disease (49, 51). Similar observations have been made in the synovial fluid of rheumatoid arthritis patients, where HSP70 complexed with self-proteins might contribute to Ag spreading and the perpetuation of the inflammatory process in the joint (52).

Surprisingly, HSP-peptide complexes can also shut down Ag-specific immunity (53). Although the mechanisms involved in this Ag-specific immunomodulation are not completely understood, HSP-peptide complexes have already been used with success to down-regulate CNS and cell-specific, T cell-mediated autoimmunity (50, 54).

In summary, HSP-peptide complexes are sources of information that can influence the immune response, manifesting both pro- and anti-inflammatory activities. They can contribute to the perpetuation of certain autoimmune disorders, but they might also provide new tools for the immunotherapy of cancer and pathologic autoimmunity.

	HSPs as carriers of foreign molecules

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

 
In the event of an infection, the ability of HSPs to interact with a broad array of peptides allows them to bind microbial peptides and enhance their immunogenicity (21, 55, 56). However, endogenous HSPs can also interact with microbial molecules other than peptides to facilitate their detection by the immune system; this is exemplified by the interaction of bacterial DNA and LPS with HSPs.

Bacterial DNA harbors unmethylated CpG motifs that stimulate innate immunity via TLR9 (57). HSP90 binds unmethylated CpG-motifs and might directly interact with TLR9 (58). Moreover, intracellular HSP90 seems to be involved in the signal transduction triggered by CpG motifs, which can be blocked with the HSP90-specific inhibitor geldanamycin (59). In this way, HSP90 can play two roles in the immune detection of bacterial DNA: it facilitates the interaction of CpG-containing DNA with TLR9, while it also mediates the resulting intracellular signaling.

HSPs are also involved in the amplification of the immune response to LPS. Triantafilou et al. (60) have shown recently that the LPS receptor complex includes HSP70 and HSP90 in addition to the MD2 and TLR4 molecules. Indeed, HSP70, HSP90, and gp96 can bind LPS directly (60, 61, 62). Upon binding LPS, HSP70 and HSP90 are targeted to the Golgi apparatus together with TLR4, suggesting that HSP70 and HSP90 are not only involved in the transfer of LPS to the TLR4-MD2 complex but are also involved in LPS-triggered signal transduction (63). Indeed, a blocker of HSP90 activity could inhibit the activation of NF-B triggered by LPS (59).

Thus, during the course of an infection, self-HSPs interact with microbial molecules such as peptides, DNA, or LPS to facilitate their immune detection. Moreover, some HSPs are directly involved in signal-transduction pathways triggered by microbial molecules. These observations underscore the importance of the experiments that called attention to the bacterial contaminants in recombinant HSP preparations (31, 32, 33); these contaminants might simply reflect the ability of HSPs to interact with different microbial molecules and augment their immunostimulatory activities in vivo. This seems to be the case for HSP70/LPS complexes, which are more immunostimulatory than their isolated components (64).

Based on the functions performed by HSPs, alone and in complex with other molecules, we can briefly consider some of the physiological roles of HSPs in the regulation of the immune response and inflammation generally (Fig. 1).

View larger version (33K): [in this window] [in a new window]   FIGURE 1. Sterile and septic inflammation.

	HSP physiology in the absence of infection

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

Endogenous HSPs help to keep autoimmunity under control through direct and indirect mechanisms. Human HSP60 can directly inhibit chemotaxis and activate anti-inflammatory activities in human T cells, via TLR2 and suppressor of cytokine signaling 3 (25, 27). Remarkably, naive T cells are more sensitive to the effects of HSP60 than memory T cells, suggesting that this form of regulation might be of importance during the induction of primary immune responses.

HSP60 signaling via innate receptors can also influence T cell cytokine polarization. Human T cells activated by mitogen in the presence of HSP60 show a decreased secretion of IFN- and an increased secretion of IL-10, associated with down-regulation of T-bet, NFATp, and NF-B, and a concomitant up-regulation of GATA-3 (26). In other words, soluble HSP60, acting via TLRs, can inhibit the proinflammatory activities of T cells.

HSPs can also regulate autoimmunity, indirectly, by activating regulatory T cells that control pathogenic T cells specific for self-Ags other than HSPs. These HSP-specific regulatory T cells can be activated and expanded by several regimes of vaccination. We have used DNA constructs coding for human HSP60, HSP70, or HSP90 to boost regulatory T cell responses capable of halting the progression of autoimmune diabetes (19) or arthritis (12, 13, 14). Other investigators have used purified mammalian gp96 to activate regulatory T cells that inhibit CNS or cell-specific autoimmunity (54). The immunomodulatory mechanisms used by these HSP-specific regulatory T cells are diverse; however, one mechanism of particular interest might be the recognition by anti-ergotypic T regulators of up-regulated HSPs on activated pathogenic T cells; such anti-ergotypic T regulators have been reviewed recently (65).

Promotion of inflammation.

Heart surgery and stroke have been shown to trigger the release of HSPs to the circulation (66, 67). Moreover, disorders associated with pathogenic inflammation, such as T1DM (3) and atherosclerosis (68), show a positive correlation with increased levels of serum HSPs. It is likely that different signaling pathways might lead to the secretion of HSPs in different contexts (42, 69); but the origin of the circulating HSPs associated with inflammation might be necrotic tissue. Basu et al. (36) demonstrated that necrotic but not apoptotic cell death triggers the release of HSP70, gp96, and HSP90. The secreted HSPs were purified and shown to activate macrophages and DCs via the NF-B pathway (36). When the effect of LPS was studied on the same cells, the kinetics of NF-B activation triggered by LPS were shown to be faster than those following stimulation by HSP, pointing out uncharacterized differences in the signaling pathways involved.

Purified HSPs have been shown to activate APCs in vitro, but what is the role of HSPs in immunity and autoimmunity in vivo? To study the relationship between APC activation by self-HSPs and autoimmunity, Liu et al. (70) generated transgenic mice expressing gp96 on the surface of several cell types. The expression of the transgene did not alter B cell or T cell development. However, the transgene triggered a lupus-like syndrome characterized by proliferative nephritis, hypergammaglobulemia, and Abs to the nucleus and to ds- and ssDNA. This autoimmune disorder seems to be triggered by the hyperstimulation of DCs by membrane-bound gp96, which finally results in the activation of self-reactive T and B cells. Interestingly, the hyperstimulation of DCs and the systemic lupus erythematosus-like syndrome was mediated by the adaptor molecule MyD88, involved in several TLR signal transduction pathways (71).

Millar et al. (72) used a different approach to study the effect of DC activation by endogenous HSPs in autoimmunity. They used double-transgenic mice that express the lymphocytic choriomeningitis virus glycoprotein (GP) in pancreatic cells, along with transgenic GP-specific TCRs in the majority of their mature CD8⁺ T cells. In these mice, the administration of the GP epitope (gp33) recognized by the transgenic TCR or HSP70 alone did not trigger disease. However, overt diabetes was induced when HSP70 and gp33 were administered simultaneously (72). Notably, a physical interaction between gp33 and HSP70 was not needed to trigger the diabetes. The authors suggested that the induction of overt diabetes was due to a combination of Ag-specific activation triggered by gp33 with the adjuvant effects of HSP70.

In summary, similar to what we have described for HSP-autoantigen complexes, endogenous HSPs can either up-regulate or down-regulate autoimmune diseases depending, among other factors, on the type of immune cell targeted and the mix of HSP and other self- and foreign molecules at the site.

	HSP physiology during infection

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

 
Augmentation of the adaptive immune response.

CpG motifs present in bacterial DNA have been shown to trigger the release of HSP70 from macrophages (73). Some of the secreted HSP70 molecules were found to be loaded with peptides; these HSP70-peptide complexes were taken up by DCs and could activate peptide-specific T cells. Infection, LPS, and cytokines are also known to up-regulate HSP levels (74, 75). Thus, the up-regulation and secretion of self-HSPs triggered by infection, together with the adjuvant function of microbial HSPs and their role as immunodominant Ags, might facilitate the induction of an efficient immune response against invading pathogens.

Regulation of the innate immune response.

The up-regulation of HSPs and their release to the circulation as a consequence of infection adds another level of complexity to the host/pathogen interaction. HSP60, HSP70, and bacterial LPS signal cells via TLR2/TLR4 mechanisms (76). The signaling pathways triggered by different TLRs are known to interfere with each other (77, 78, 79, 80, 81, 82). Thus, the cross-talk between different signaling pathways activated by self- and/or foreign immunostimulators might represent a regulatory mechanism that fine tunes and controls potentially harmful immune responses. Indeed, repetitive activation of macrophages with self-HSP60 renders them nonresponsive to LPS, and LPS stimulation can abrogate the subsequent response to HSP60 (83, 84). This observation also suggests that, by triggering different TLRs, the environment can alter homeostatic responses mediated by endogenous adjuvants such as HSPs. These interactions might constitute the molecular basis for the hygiene hypothesis, which links exposure to environmental microbes to a lower prevalence of immune-mediated disorders (85).

Nevertheless, HSPs might also participate in positive feedback loops that perpetuate inflammation. Infection triggers HSP up-regulation and release. However, these newly released HSPs can bind microbial products and increase their proinflammatory activities, leading to the release of more proinflammatory factors, that prompt the induction and release of more HSPs. Positive feedback loops can lead to chaos. The study of the interactions of HSPs with microbial molecules and the modulation of their inflammatory activities should open new horizons in our understanding of the complex mechanisms that connect autoimmune disorders with environmental stimuli.

	Sterile and septic inflammation

Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

 
How can we connect the different roles played by HSPs in physiology (Table II)? We might begin by considering the concept of inflammation. Inflammation is "a process which begins following a sublethal injury and ends with complete healing" (86). From this point of view, inflammation that is needed for healing is essential for body maintenance (87). Indeed, inflammation is involved in processes as diverse as angiogenesis, wound healing, tissue remodeling and regeneration, connective tissue formation (88), and the recovery of function following trauma to the CNS (89). However, in addition to maintenance, inflammation must also keep foreign pathogens under tight control. Inflammation, then, performs two types of services: maintenance and defense.

Given the danger that an uncontrolled inflammatory response might represent for the individual, several regulatory mechanisms have been selected through evolution. The immune system has to determine the exact location, kinetics, and intensity of the inflammatory response needed to perform each biological process. By being involved in both forms of inflammation, HSPs are key elements in fine-tuning the inflammatory response (87). The central position of HSPs in immunoregulation and in the healthy immune repertoire (90) could be used strategically in our quest to develop better therapies for cancer, infections, and autoimmune disorders. Nature has learned to use HSPs; so might we.

	Footnotes

 
The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked advertisement in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

¹ This work is supported in part by grants from the Center for the Study of Emerging Diseases and by the European Union.

² Address correspondence and reprint requests to Dr. Irun R. Cohen, Department of Immunology, Weizmann Institute of Science, Rehovot 76100, Israel. E-mail address: irun.cohen{at}weizmann.ac.il

³ Abbreviations used in this paper: HSP, heat shock protein; T1DM, type 1 diabetes mellitus; Ms, multiple sclerosis; GP, glycoprotein.

Received for publication April 26, 2005. Accepted for publication June 6, 2005.

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Top Abstract Introduction Do pure HSPs have... HSPs as carriers of... HSPs as carriers of... HSP physiology in the... HSP physiology during infection Sterile and septic inflammation References

 

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