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Immunopsychiatry: important facts

Published online by Cambridge University Press:  18 April 2017

G. M. Khandaker*
Affiliation:
Department of Psychiatry, University of Cambridge, Cambridge, UK Cambridgeshire and Peterborough NHS Foundation Trust, Cambridge, UK
R. Dantzer
Affiliation:
Department of Symptom Research, University of Texas MD Anderson Cancer Centre, Houston, TX, USA
P. B. Jones
Affiliation:
Department of Psychiatry, University of Cambridge, Cambridge, UK Cambridgeshire and Peterborough NHS Foundation Trust, Cambridge, UK
*
*Address for correspondence: Dr G. M. Khandaker, Department of Psychiatry, University of Cambridge, Box 189, Cambridge Biomedical Campus, Cambridge CB2 0QQ, UK. (Email: [email protected])
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Abstract

Accumulating evidence indicate a role for the immune system particularly inflammation and autoimmunity in the aetiology of major psychiatric disorders such as depression and schizophrenia. In this paper, we discuss some of the key advances in immunopsychiatry in order to highlight to psychiatrists and other health professionals how an increased understanding of this field might enhance our knowledge of illness mechanism and approaches to treatment. We present a brief overview of clinical research that link inflammation and autoimmunity with depression and psychosis, including potential role of inflammation in treatment response, current evidence for the effectiveness of immune-modulating treatment for depression and psychosis, and possible role of inflammation in common physical comorbidities for these disorders such as coronary heart disease and diabetes mellitus. Gaining a better understanding of the role of immune system could be paradigm changing for psychiatry. We need collaborations between clinicians and scientists to deliver high-quality translational research in order to fully realise the clinical potential of this exciting and rapidly expanding field.

Type
Short Teaching Article
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
Copyright
Copyright © Cambridge University Press 2017

Introduction

There are intricate interactions between the immune system and the brain that may offer new mechanistic understanding and insights for novel therapies for psychiatric disorders. In particular, proinflammatory cytokines and circulating autoantibodies can influence the brain leading to changes in mood, cognition and behaviour; so may be relevant for the pathogenesis and treatment of depression, psychosis and other major psychiatric disorders (Raison et al. Reference Raison, Capuron and Miller2006; Dantzer et al. Reference Dantzer, O'Connor, Freund, Johnson and Kelley2008; Khandaker et al. Reference Khandaker, Cousins, Deakin, Lennox, Yolken and Jones2015). In this paper, we present a brief overview of clinical research that link inflammation and autoimmunity with depression and psychosis. We discuss potential role of inflammation in treatment response, current evidence for the effectiveness of immune-modulating treatment for depression and psychosis, and possible role of inflammation in common physical comorbidities for these disorders. Our aim is to inform psychiatrists and other health professionals about a few key advances (see Textbox) in the field of immunopsychiatry that could impact on clinical practice rather than providing a comprehensive literature review regarding the immune system and mental disorders. Unless specified otherwise, in this context inflammation refers to chronic, low-grade systemic inflammation as reflected by increased concentrations of circulating inflammatory markers in peripheral blood such as cytokines and acute phase proteins, rather than inflammation in the classical sense, which is clinically manifest by the so-called cardinal signs.

Evidence for a role of inflammation in depression

Depression is common in people with a chronic inflammatory illness such as rheumatoid arthritis (Dickens & Creed, Reference Dickens and Creed2001). About 30–50% of patients with hepatitis C virus develop depression following treatment with interferon (Bonaccorso et al. Reference Bonaccorso, Marino, Biondi, Grimaldi, Ippoliti and Maes2002), which is a potent inducer of inflammatory cytokines. These clinical observations provide clues that inflammation may play a role in depression. Indeed, inducing inflammation in healthy volunteers in experimental setting with a typhoid vaccine leads to depressive symptoms and reduced cognitive performance, which is mediated by increase in circulating interleukin 6 (IL-6) levels (Harrison et al. Reference Harrison, Brydon, Walker, Gray, Steptoe and Critchley2009), a pleiotropic, proinflammatory cytokine. Furthermore, systematic reviews and meta-analyses of cross-sectional studies have confirmed that the levels of circulating proinflammatory cytokines such as IL-6, IL-1β, tumour necrosis factor alpha (TNF-α) and acute phase proteins such as C-reactive protein (CRP) are elevated in acutely depressed patients, which are largely normalised after recovery (Howren et al. Reference Howren, Lamkin and Suls2009; Haapakoski et al. Reference Haapakoski, Mathieu, Ebmeier, Alenius and Kivimaki2015; Goldsmith et al. Reference Goldsmith, Rapaport and Miller2016). However, a limitation of the cross-sectional studies is that they cannot determine whether increase in inflammatory markers is a cause or consequence of illness (i.e. reverse causality).

Recently, longitudinal studies have shown that elevated cytokine levels precede, and so could potentially cause, depressive symptoms. Based on over 4000 participants from the Avon Longitudinal Study of Parents and Children (ALSPAC) birth cohort, we have shown that elevated serum levels of IL-6 in childhood increase risks of developing depressive and psychotic symptoms subsequently in adulthood in a linear, dose–response fashion (Khandaker et al. Reference Khandaker, Pearson, Zammit, Lewis and Jones2014a ). In this study, evidence for an association persisted after taking into account effects of sociodemographic factors, maternal depression and other potential confounders. A longitudinal association between circulating IL-6 and CRP levels and subsequent development and persistence of depressive symptoms have been reported from other cohorts (Gimeno et al. Reference Gimeno, Kivimaki, Brunner, Elovainio, De Vogli, Steptoe, Kumari, Lowe, Rumley, Marmot and Ferrie2009; Zalli et al. Reference Zalli, Jovanova, Hoogendijk, Tiemeier and Carvalho2016). Taken together the current evidence indicates that inflammation is unlikely to be merely a consequence of depression or stress (which can cause immune-activation). Inflammation precedes depression so could be a causal risk factor for the illness.

However, observed association between inflammatory markers and depression could still be due to residual confounding, so more definitive studies, such as Mendelian randomization and randomised controlled trials (RCTs), are needed to establish whether the association between inflammation and depression is causal. Elevated CRP levels are associated with somatic (e.g. fatigue, anorexia, altered sleep) rather than psychological symptoms of depression in general population (Jokela et al. Reference Jokela, Virtanen, Batty and Kivimaki2016) and in cancer patients who develop depressive symptoms after interferon treatment (Capuron et al. Reference Capuron, Gumnick, Musselman, Lawson, Reemsnyder, Nemeroff and Miller2002). Therefore, focusing on specific symptoms/group of symptoms might help to elucidate further the role of inflammation in depression. Animal experimental studies suggest that inflammatory cytokines communicate with the brain using a number of pathways, and affect mood, cognition and behaviour by altering neurotransmitter metabolism, activating the hypothalamic–pituitary–adrenal (HPA) axis, increasing oxidative stress, and reducing synaptic plasticity possibly as a result of activation of microglia (a marker of neuroinflammation) (Raison et al. Reference Raison, Capuron and Miller2006; Dantzer et al. Reference Dantzer, O'Connor, Freund, Johnson and Kelley2008). It remains to be seen whether neuroinflammation corresponds with severity of depression or response to antidepressant treatment in humans.

Evidence for a role of inflammation, atopy and autoimmunity in psychosis

Epidemiological studies indicate a role of infection, inflammation and autoimmunity in schizophrenia (Khandaker et al. Reference Khandaker, Cousins, Deakin, Lennox, Yolken and Jones2015; Khandaker & Dantzer, Reference Khandaker and Dantzer2016). Schizophrenia is associated with increased prevalence of various infections, including neurotropic viruses from the Herpesviridae family, and the intracellular parasite, Toxoplasma gondii. However, it is unclear whether increased infection is a result of poor lifestyle, so more convincing results have come from longitudinal studies. Exposure to a variety of infection during foetal development, including herpes simplex virus type 2 (HSV-2), cytomegalovirus (CMV), influenza, T. gondii, non-specific viral/bacterial infection and elevated maternal inflammatory marker levels, is associated with risk of schizophrenia and related psychotic illness in adult life, though the strength of association for each of these exposures vary; reviewed (Brown & Derkits, Reference Brown and Derkits2010; Khandaker et al. Reference Khandaker, Zimbron, Dalman, Lewis and Jones2012, Reference Khandaker, Zimbron, Lewis and Jones2013). A linear, dose–response relationship has been reported between hospitalisation with a serious infection (CNS or non-CNS) during childhood and risk of adult psychotic disorders (Benros et al. Reference Benros, Nielsen, Nordentoft, Eaton, Dalton and Mortensen2011).

Similar to depression, antipsychotic naïve first episode psychosis and acute psychotic relapse are associated with increased serum levels of proinflammatory cytokines, such as IL-1β, IL-6, TNF-α and decreased serum levels of the anti-inflammatory cytokine, IL-10, which tend to normalise after remission of symptoms with antipsychotic treatment (Miller et al. Reference Miller, Buckley, Seabolt, Mellor and Kirkpatrick2011; Upthegrove et al. Reference Upthegrove, Manzanares-Teson and Barnes2014; Goldsmith et al. Reference Goldsmith, Rapaport and Miller2016). Serum cytokine levels, including IL-6 are associated with illness severity, duration and anti-psychotic treatment (Maes et al. Reference Maes, Meltzer and Bosmans1994; Miller et al. Reference Miller, Buckley, Seabolt, Mellor and Kirkpatrick2011). IL-1β and IL-6 levels have been reported to be elevated in the cerebrospinal fluid (CSF) of schizophrenia patients (Garver et al. Reference Garver, Tamas and Holcomb2003). However, it is not clear to what extent peripheral inflammation is related to inflammatory activity in the CNS, so further studies are needed. Recently population-based longitudinal studies have shown that elevated IL-6 and CRP levels in childhood or adolescence are associated with increased risk of developing psychotic symptoms (Khandaker et al. Reference Khandaker, Pearson, Zammit, Lewis and Jones2014a ) and schizophrenia (Metcalf et al. Reference Metcalf, Jones, Nordstrom, Timonen, Maki, Miettunen, Jaaskelainen, Jarvelin, Stochl, Murray, Veijola and Khandaker2017) subsequently in adulthood. As with depression, the longitudinal studies indicate that inflammation could be a causal risk factor for psychosis. Adverse experiences in early-life could be a source of low-grade systemic inflammation in healthy people, as levels of circulating inflammatory markers in adults are associated with childhood adversity/maltreatment (Baumeister et al. Reference Baumeister, Akhtar, Ciufolini, Pariante and Mondelli2016) and sub-optimal foetal environment as indexed by low birth weight (Tzoulaki et al. Reference Tzoulaki, Jarvelin, Hartikainen, Leinonen, Pouta, Paldanius, Ruokonen, Canoy, Sovio, Saikku and Elliott2008). Therefore, whether low-grade systemic inflammation mediates the relationship between early-life adversity and adult depression or psychosis is a hypothesis that needs testing.

Further support for a role of the immune system in schizophrenia comes from studies pointing to links with atopy and autoimmunity (Benros et al. Reference Benros, Nielsen, Nordentoft, Eaton, Dalton and Mortensen2011). There is some evidence that childhood atopic disorders such as asthma, eczema are associated with increased risk of psychotic symptoms in adolescence (Khandaker et al. Reference Khandaker, Zammit, Lewis and Jones2014b ) and schizophrenia in adulthood (Pedersen et al. Reference Pedersen, Benros, Agerbo, Borglum and Mortensen2012). The prevalence of autoimmune conditions is increased in people with schizophrenia and their unaffected first-degree relatives (Eaton et al. Reference Eaton, Byrne, Ewald, Mors, Chen, Agerbo and Mortensen2006). Schizophrenia is associated with serum antibodies against dietary antigens, such as gliadin and casein (Lachance & McKenzie, Reference Lachance and McKenzie2014). Increased autoantibodies against neuronal cell surface targets, such as N-methyl-D-aspartate receptor (NMDAR) and components of the voltage-gated potassium channel complex, have been reported in some cases of psychosis in some (Zandi et al. Reference Zandi, Irani, Lang, Waters, Jones, McKenna, Coles, Vincent and Lennox2011; Steiner et al. Reference Steiner, Walter, Glanz, Sarnyai, Bernstein, Vielhaber, Kastner, Skalej, Jordan, Schiltz, Klingbeil, Wandinger, Bogerts and Stoecker2013), but not all studies (de Witte et al. Reference de Witte, Hoffmann, van Mierlo, Titulaer, Kahn and Martinez-Martinez2015); reviewed (Pollak et al. Reference Pollak, McCormack, Peakman, Nicholson and David2014). Anti-NMDAR antibodies have been typically associated with the eponymous encephalitis, which is often associated with psychotic symptoms. Not all anti-NMADR antibody positive cases of psychosis have classic features of encephalitis, suggesting these antibodies might be a cause of psychosis in some people. Similarly, elimination of autoantibodies by plasmapheresis improves psychotic symptoms in some cases of first episode psychosis (Zandi et al. Reference Zandi, Irani, Lang, Waters, Jones, McKenna, Coles, Vincent and Lennox2011, Reference Zandi, Deakin, Morris, Buckley, Jacobson, Scoriels, Cox, Coles, Jones, Vincent and Lennox2014). However, anti-NMDAR antibodies are also increased in depression and bipolar disorder (Pearlman & Najjar, Reference Pearlman and Najjar2014). It remains to be established whether antibody positive patients differ from antibody-negative patients in terms of underlying pathology and response to antipsychotic treatment, and whether immunomodulatory treatments are effective in alleviating psychotic symptoms in this group using RCT. There is limited data on the relationships between neuronal autoantibodies and other aspects of immunity such as cytokines and microglial activation. Nevertheless, given these antibodies are present in about 5% of patients with first episode psychosis (Zandi et al. Reference Zandi, Irani, Lang, Waters, Jones, McKenna, Coles, Vincent and Lennox2011), some psychiatric services in the UK now screen for these antibodies in new onset cases.

Neuroimaging and genome wide association studies (GWAS) support a role for the immune system in schizophrenia. Neuroimaging studies using PET provide evidence for neuroinflammation in patients with schizophrenia and in persons with subclinical symptoms, who are at high risk of psychosis and are related to at-risk symptom severity (Bloomfield et al. Reference Bloomfield, Selvaraj, Veronese, Rizzo, Bertoldo, Owen, Bloomfield, Bonoldi, Kalk, Turkheimer, McGuire, de Paola and Howes2016). Evidence of microglial activation in the entire grey matter and hippocampus indicates that neuroinflammation might contribute to grey matter volume loss and cognitive deterioration in schizophrenia (Doorduin et al. Reference Doorduin, de Vries, Willemsen, de Groot, Dierckx and Klein2009). The largest GWAS of schizophrenia to date has shown that in addition to genes expressed in the brain, schizophrenia is associated with genes involved in adaptive immunity (CD19 and CD 20 B-lymphocytes) and the major histocompatibility complex (MHC) region on chromosome six (Schizophrenia Working Group of the Psychiatric Genomics, 2014). The association between schizophrenia and the MHC locus arises in part from variations of the complement component 4 (C4) genes. C4 is a critical component of the classical complement cascade, an innate immune system pathway that recognizes and eliminates pathogens and cellular debris. The brain expression of C4A is increased in schizophrenia (Sekar et al. Reference Sekar, Bialas, de Rivera, Davis, Hammond, Kamitaki, Tooley, Presumey, Baum, Van Doren, Genovese, Rose, Handsaker, Daly, Carroll, Stevens and McCarroll2016). In mice, C4 tags synapses to be eliminated by microglial cells (synaptic pruning) that express C4 receptors during postnatal development. Excessive complement activity could lead to altered neurodevelopment as a result of excessive synaptic pruning.

Inflammation and response to psychotropic treatments

Inflammation is associated with poor response to antidepressant and antipsychotic treatments. About a third of depressed patients have elevated circulating CRP levels (Wium-Andersen et al. Reference Wium-Andersen, Orsted, Nielsen and Nordestgaard2013) while a third of patients are antidepressant resistant (Nemeroff, Reference Nemeroff2007) – this may not be a coincidence. Indeed, activation of the inflammatory system as reflected by elevated serum concentrations of IL-6 and other cytokines predicts poor response to antidepressants (O'Brien et al. Reference O'Brien, Scully, Fitzgerald, Scott and Dinan2007; Carvalho et al. Reference Carvalho, Torre, Papadopoulos, Poon, Juruena, Markopoulou, Cleare and Pariante2013). Patients who do not respond to selective serotonin reuptake inhibitors and other antidepressants continue to show elevated levels of IL-6, CRP and other inflammatory markers (Maes et al. Reference Maes, Bosmans, De Jongh, Kenis, Vandoolaeghe and Neels1997). Findings from patients with psychosis are similar. Patients with first episode psychosis who do not respond to antipsychotic drugs have elevated levels of IL-6 and INF-γ at the start of treatment compared with responders (Mondelli et al. Reference Mondelli, Ciufolini, Belvederi Murri, Bonaccorso, Di Forti, Giordano, Marques, Zunszain, Morgan, Murray, Pariante and Dazzan2015). Furthermore, non-responders continue to show elevated levels of these inflammatory markers after 3 months of antipsychotic treatment compared with responders (Mondelli et al. Reference Mondelli, Ciufolini, Belvederi Murri, Bonaccorso, Di Forti, Giordano, Marques, Zunszain, Morgan, Murray, Pariante and Dazzan2015). While these findings are illuminating, longitudinal studies of inflammation and treatment response based on incident cases are limited. Inflammatory marker levels can be influenced by psychological stress, body mass, life style (e.g. smoking, alcohol use) and some psychotropic drugs. So further research is needed to understand whether and how measuring inflammation in clinical setting could be useful for predicting response to antidepressant/antipsychotic treatment, and for identifying patients who are likely to benefit from immunomodulatory treatments.

It is thought that depressed patients with elevated inflammatory markers display resistance to antidepressants because these drugs do not rectify inflammation-related pathologies such as activation of the kynurenine pathway (Christmas et al. Reference Christmas, Potokar and Davies2011). Inflammatory cytokines such as IFN and IL-6 activate indoleamine 2,3-dioxygenase (IDO), an enzyme that shifts metabolism of tryptophan towards kynurenine (Haroon et al. Reference Haroon, Raison and Miller2012). Further metabolism of kynurenine in the brain leads to increased production of neurotoxic and potentially depressogenic metabolites such as 3-hydroxykynurenine (3-HK) and quinolinic acid. In mice, lipopolysaccharide-induced systemic inflammation leads to depression-like behaviour through activation of IDO (O'Connor et al. Reference O'Connor, Lawson, Andre, Moreau, Lestage, Castanon, Kelley and Dantzer2009). Blocking inflammation with minocycline (a broad spectrum antibiotic) (O'Connor et al. Reference O'Connor, Lawson, Andre, Moreau, Lestage, Castanon, Kelley and Dantzer2009) or an anti-IL-6 monoclonal antibody (Hodes et al. Reference Hodes, Pfau, Leboeuf, Golden, Christoffel, Bregman, Rebusi, Heshmati, Aleyasin, Warren, Lebonte, Horn, Lapidus, Stelzhammer, Wong, Bahn, Krishnan, Bolanos-Guzman, Murrough, Merad and Russo2014) prevents development of depression-like behaviour. Pertinent to psychosis, kynurenic acid is the only naturally occurring NMDAR antagonist in the human CNS (Schwarcz & Pellicciari, Reference Schwarcz and Pellicciari2002). NMDAR antagonism and glutamatergic hypofunction have long been proposed to underlie psychotic symptoms and cognitive dysfunction in schizophrenia (Carlsson & Carlsson, Reference Carlsson and Carlsson1990). Indeed, there is evidence that levels of kynurenine and kynurenic acid are elevated in the CSF and brain tissue of schizophrenia patients compared with healthy controls (Erhardt et al. Reference Erhardt, Blennow, Nordin, Skogh, Lindstrom and Engberg2001; Schwarcz et al. Reference Schwarcz, Rassoulpour, Wu, Medoff, Tamminga and Roberts2001). In future, examination of markers of inflammation and IDO activation in peripheral blood and in CSF in different stages of illness, their relationship with treatment response would be helpful to understand fully the implications of these findings for depression and psychosis.

Effectiveness of immunomodulatory treatment in depression and psychosis

Anti-inflammatory drugs may be helpful for patients with depression and psychosis. A meta-analysis of RCTs of non-steroidal anti-inflammatory drugs (NSAIDs), administered as sole treatment or as adjunct to antidepressants, indicates that they are more effective than placebo in treating depression (Kohler et al. Reference Kohler, Benros, Nordentoft, Farkouh, Iyengar, Mors and Krogh2014). The effect size for Celecoxib (a selective cyclooxygenase 2 inhibitor) based on 10 RCTs was SMD = −0.29 (95% CI −0.49 to −0.08). However, cyclooxygenase-2 inhibitors increase risk of cardiovascular disease (Mukherjee et al. Reference Mukherjee, Nissen and Topol2001), a known comorbidity for depression, so their use in this patient group may be problematic. Besides, it unclear whether improvements in mood is due to improvements in physical illness or due to the effect of NSAIDs on pathways other than inflammation such as glucocorticoid receptor (Nikkheslat et al. Reference Nikkheslat, Zunszain, Horowitz, Barbosa, Parker, Myint, Schwarz, Tylee, Carvalho and Pariante2015).

More recently studies have examined the effectiveness of cytokine modulators (e.g. anti-cytokine monoclonal antibodies and cytokine inhibitors) for depression. We have conducted a systematic review and meta-analysis of secondary outcome data on depressive symptoms from clinical trials of cytokine modulators in patients with chronic inflammatory illnesses. Based on seven RCTs, we have found that cytokine modulators have a significant antidepressant effect; effect size, SMD = 0.40 (95% CI 0.22–0.59) (Kappelmann et al. Reference Kappelmann, Lewis, Dantzer, Jones and Khandaker2016). Crucially, improvements in depressive symptoms are independent of improvements in physical illness, suggesting mood improvement is not merely a by-product of physical improvement; cytokines may indeed be causally related to depressive symptoms. Only one RCT to date has investigated the effectiveness of a monoclonal antibody using depression as a primary outcome (Raison et al. Reference Raison, Rutherford, Woolwine, Shuo, Schettler, Drake, Haroon and Miller2013). Although overall no benefit of infliximab (anti-TNF monoclonal antibody) was observed, the study found that the higher the level of inflammation at the start of trial the greater the improvement in depressive symptoms by the end of trial (Raison et al. Reference Raison, Rutherford, Woolwine, Shuo, Schettler, Drake, Haroon and Miller2013). Together, these findings indicate that cytokine modulating drugs could be useful for depressed patients, particularly those with evidence of inflammation, but further work is needed to establish their efficacy, safety and cost-benefit for treating depression.

In schizophrenia, a meta-analysis of RCTs of NSAIDs as adjuncts to antipsychotics has shown promising results especially for aspirin and non-acetyl cysteine (Sommer et al. Reference Sommer, van Westrhenen, Begemann, de Witte, Leucht and Kahn2014). Dopaminergic drugs, which include all anti-psychotics currently in use, are effective in controlling positive symptoms, but cognitive dysfunction and negative symptoms rarely respond to these drugs. This may indicate fundamental differences in the mechanism underlying different types of symptoms. Preclinical studies of peripheral immune-to-brain communication lend support for a role of inflammation in the pathogenesis of these difficult-to-treat symptoms (Khandaker et al. Reference Khandaker, Cousins, Deakin, Lennox, Yolken and Jones2015; Khandaker & Dantzer, Reference Khandaker and Dantzer2016). In future, targeting these symptoms with immunological treatment could be a clinically fruitful strategy. Indeed, minocycline, a centrally acting tetracyclic anti-inflammatory agent, improves negative symptoms and cognitive function in schizophrenia (Chaudhry et al. Reference Chaudhry, Hallak, Husain, Minhas, Stirling, Richardson, Dursun, Dunn and Deakin2012). Celecoxib may improve cognitive function in early stages of schizophrenia (Muller et al. Reference Muller, Riedel, Scheppach, Brandstatter, Sokullu, Krampe, Ulmschneider, Engel, Moller and Schwarz2002). Recently, a small, proof-of-concept, open-label study of tocilizumab (anti-IL-6 receptor monoclonal antibody) as adjunct to antipsychotic treatment showed improvements in cognitive function in schizophrenia (Miller et al. Reference Miller, Dias, Lemos and Buckley2016), but more definitive trials are needed. A subgroup of patients with depression (Wium-Andersen et al. Reference Wium-Andersen, Orsted, Nielsen and Nordestgaard2013) and psychosis (Mondelli et al. Reference Mondelli, Ciufolini, Belvederi Murri, Bonaccorso, Di Forti, Giordano, Marques, Zunszain, Morgan, Murray, Pariante and Dazzan2015) show evidence of inflammation, so RCTs of anti-inflammatory drugs based on ‘inflamed’ rather than all patients of depression/psychosis are likely to be useful.

Transdiagnostic effect of inflammation and the common cause hypothesis

The association between inflammation and psychiatric disorders transcends traditional diagnostic boundaries. In addition to depression and psychosis, evidence for a link with inflammation exists for a number of disorders, including anxiety (Rossi et al. Reference Rossi, Sacchetti, Napolitano, De Chiara, Motta, Studer, Musella, Barbieri, Bari, Bernardi, Maccarrone, Usiello and Centonze2012; Khandaker et al. Reference Khandaker, Zammit, Lewis and Jones2016), post-traumatic stress disorder (Eraly et al. Reference Eraly, Nievergelt, Maihofer, Barkauskas, Biswas, Agorastos, O'Connor and Baker2014), autism (Brown et al. Reference Brown, Sourander, Hinkka-Yli-Salomaki, McKeague, Sundvall and Surcel2014) and dementias (Schmidt et al. Reference Schmidt, Schmidt, Curb, Masaki, White and Launer2002). Inflammation is likely to be relevant for some, not all, cases of depression/psychosis, because, as with most chronic illnesses, no risk factor alone is necessary or sufficient for causing an illness. Inflammation is no different in this regard; evidence for inflammation is seen in a sup-group of patients with depression and psychosis (Wium-Andersen et al. Reference Wium-Andersen, Orsted, Nielsen and Nordestgaard2013; Mondelli et al. Reference Mondelli, Ciufolini, Belvederi Murri, Bonaccorso, Di Forti, Giordano, Marques, Zunszain, Morgan, Murray, Pariante and Dazzan2015). One explanation for the transdiagnostic effect could be that inflammation contributes to features common to different psychiatric syndromes such as fatigue, anhedonia and cognitive difficulties. Furthermore, this lack of specificity is not unique to inflammation. It is well known that there is overlap in the genetic risk for depression, schizophrenia and bipolar disorder. Psychological stress is a common risk factor for many physical and psychiatric illnesses.

Taking a broader perspective on causal models for illness, the idea of specificity of association between a risk factor and a disease fits well causal models for some illnesses (e.g. Koch's postulates and Tuberculosis), but might be problematic in the case of chronic illnesses. Smoking is associated with numerous illnesses, including cancers and cardiovascular diseases. Similarly, inflammation might be a common underlying mechanism for a number of chronic illnesses of adult life such as depression, schizophrenia, coronary heart disease and diabetes mellitus that are highly comorbid with each other. All of these illnesses are associated with inflammation (Pradhan et al. Reference Pradhan, Manson, Rifai, Buring and Ridker2001; Danesh et al. Reference Danesh, Wheeler, Hirschfield, Eda, Eiriksdottir, Rumley, Lowe, Pepys and Gudnason2004; Khandaker et al. Reference Khandaker, Pearson, Zammit, Lewis and Jones2014a ; Metcalf et al. Reference Metcalf, Jones, Nordstrom, Timonen, Maki, Miettunen, Jaaskelainen, Jarvelin, Stochl, Murray, Veijola and Khandaker2017), which could be linked with early-life factors influencing inflammatory regulation, such as impaired foetal development or childhood maltreatment. This idea is consistent with the common-cause or developmental programming hypothesis by David Barker (Barker et al. Reference Barker, Gluckman, Godfrey, Harding, Owens and Robinson1993a ). Developmental programming refers to permanent alteration in physiological system(s) following exposure to adversity during a specific ‘developmental window’. The resulting physiological alterations, in combination with genetic and/or other environmental factors, can increase risks of several diseases in adulthood. Empirical evidence from longitudinal studies supports the developmental programming hypothesis. Low birth weight (a marker of suboptimal foetal development) and childhood maltreatment are associated with increased circulating CRP levels (Tzoulaki et al. Reference Tzoulaki, Jarvelin, Hartikainen, Leinonen, Pouta, Paldanius, Ruokonen, Canoy, Sovio, Saikku and Elliott2008) as well as risks of heart disease, diabetes mellitus, depression and schizophrenia (Barker et al. Reference Barker, Hales, Fall, Osmond, Phipps and Clark1993b ; Abel et al. Reference Abel, Wicks, Susser, Dalman, Pedersen, Mortensen and Webb2010). Indeed, there is evidence that inflammation moderates the association between childhood maltreatment and risk of depression in adulthood (Danese et al. Reference Danese, Moffitt, Pariante, Ambler, Poulton and Caspi2008). In future, population-based epidemiological, clinical and experimental studies are needed to understand whether and how inflammation contributes to the comorbidity between chronic cardio-metabolic and psychiatric illnesses of adult life. Experimental studies would be particularly useful to understand how early-life adversity might ‘programme’ the immune system.

Conclusions

Pathophysiologic explanations and pharmacotherapy for major psychiatric disorders such as depression and schizophrenia are predicated on monoamine neurotransmitters. However, heterogeneity in clinical presentation, illness course and treatment response suggest other mechanisms are involved. A better understanding of the role of immune system could be paradigm changing for psychiatry by providing novel mechanisms and treatments for these disorders, which are among leading causes of disability worldwide. The field now needs studies to investigate causality of association and RCTs of novel immunotherapies for depression and psychosis. In future, immunotherapeutic strategies could include immune-phenotyping of patients to predict treatment response and anti-inflammatory treatment for patients with evidence of inflammation. Shifting the focus of research from syndrome to symptom (or constellation of symptoms) may help to fully elucidate the role of immune system in the aetiology of psychiatric disorders. Accumulating evidence from preclinical studies suggests inflammation is a key mechanism underlying cognition and behaviour, which needs to be translated into human studies of affective and cognitive neuroscience. A clearer understanding of the immunological aspects of psychiatric disorders may lead to novel approaches to diagnosis and treatment but would require close collaborations between clinicians and researchers to deliver high-quality translational research.

Immunopsychiatry: Key facts

  • Depression is common in people with a chronic inflammatory illness, and immuno-activation leads to depressive symptoms in patients and healthy volunteers

  • Schizophrenia and related psychotic disorders are associated with prenatal and childhood infections, atopic disorders and autoimmunity

  • Elevated circulating inflammatory markers increase future risk of depression and psychosis in healthy people suggesting inflammation might cause these disorders

  • Circulating inflammatory markers are elevated in acute depression and psychosis, which tend to normalise after recovery, but continue to be elevated in treatment resistant cases

  • There is evidence of neuroinflammation in schizophrenia as demonstrated by activation of microglia in patients as well as those who are at risk of developing the illness

  • Anti-NMDA receptor and anti-VGKC antibodies may be responsible for about 5% of all cases of psychosis

  • Elevated circulating inflammatory markers are associated with poor response to antidepressant and antipsychotic treatment

  • Measuring circulating inflammatory markers may aid treatment decisions

  • Emerging evidence indicates anti-inflammatory agents may be effective treatments for patients with depression and psychosis particularly those with evidence of inflammation

  • Inflammation might be a common mechanism underlying the comorbidities between depression, schizophrenia, coronary heart disease and diabetes mellitus

Acknowledgements

GMK is supported by an Intermediate Clinical Fellowship from the Wellcome Trust (201486/Z/16/Z) and a Clinical Lecturer Starter Grant from the Academy of Medical Sciences, UK (grant no. 80354). PBJ acknowledges grant support from the Wellcome Trust (095844/Z/11/Z & 088869/Z/09/Z) and NIHR (RP-PG-0606–1335, Cambridge Biomedical Research Centre and CLAHRC East of England). RD has received grants from the National Institute of Neurological Diseases and Stroke of the National Institutes of Health (grants R01 NS073939; R01 NS074999), the National Cancer Institute (R01CA193522) and the National Institute of Mental Health (R21MH104694).

Declaration of Interest

The authors have no competing financial interests in relation to the work described. PBJ received an honorarium that he donated to his department, from Roche (UK) for taking part in an advisory board to advise on education about schizophrenia for psychiatrists.

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