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The association of kynurenine pathway metabolites with symptom severity and clinical features of bipolar disorder: An overview

Published online by Cambridge University Press:  11 November 2022

Francesco Bartoli
Affiliation:
Department of Medicine and Surgery, University of Milano-Bicocca, Monza, Italy
Riccardo M. Cioni
Affiliation:
Department of Medicine and Surgery, University of Milano-Bicocca, Monza, Italy
Daniele Cavaleri*
Affiliation:
Department of Medicine and Surgery, University of Milano-Bicocca, Monza, Italy
Tommaso Callovini
Affiliation:
Department of Medicine and Surgery, University of Milano-Bicocca, Monza, Italy
Cristina Crocamo
Affiliation:
Department of Medicine and Surgery, University of Milano-Bicocca, Monza, Italy
Błażej Misiak
Affiliation:
Department of Psychiatry, Wrocław Medical University, Wrocław, Poland
Jonathan B. Savitz
Affiliation:
Laureate Institute for Brain Research, Tulsa, Oklahoma, USA Oxley College of Health Sciences, The University of Tulsa, Tulsa, Oklahoma, USA
Giuseppe Carrà
Affiliation:
Department of Medicine and Surgery, University of Milano-Bicocca, Monza, Italy Division of Psychiatry, University College London, London, United Kingdom
*
*Author for correspondence: Daniele Cavaleri, E-mail: [email protected]

Abstract

Background

The balance between neurotoxic and neuroprotective effects of kynurenine pathway (KP) components has been recently proposed as a key element in the pathophysiology of bipolar disorder (BD) and related mood episodes. This comprehensive overview explored the link of KP with symptom severity and other clinical features of BD.

Methods

We searched Medline, Embase, and PsycInfo electronic databases for studies assessing the association of peripheral and/or central concentrations of KP metabolites with putative clinical features, including symptom severity and other clinical domains in BD.

Results

We included the findings of 13 observational studies investigating the possible variations of KP metabolites according to symptom severity, psychotic features, suicidal behaviors, and sleep disturbances in BD. Studies testing the relationship between KP metabolites and depression severity generated mixed and inconsistent findings. No statistically significant correlations with manic symptoms were found. Moreover, heterogeneous variations of the KP across different clinical domains were shown. Few available studies found (a) higher levels of cerebrospinal fluid kynurenic acid and lower of plasma quinolinic acid in BD with psychotic features, (b) lower central and peripheral picolinic acid levels in BD with suicide attempts, and (c) no significant correlations between KP metabolites and BD-related sleep disturbances.

Conclusions

An imbalance of KP metabolism toward the neurotoxic branches is likely to occur in people with BD, though evidence on variations according to specific clinical features of BD is less clear. Additional research is needed to clarify the role of KP in the etiopathogenesis of BD and related clinical features.

Type
Review/Meta-analysis
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, provided the original article is properly cited.
Copyright
© The Author(s), 2022. Published by Cambridge University Press on behalf of the European Psychiatric Association

Introduction

Bipolar disorder (BD) is a severe and chronic mental illness [Reference Carvalho, Firth and Vieta1] with an estimated lifetime prevalence of about 2% [Reference Merikangas, Jin, He, Kessler, Lee and Sampson2]. BD is typically characterized by disabling mood fluctuations as well as, in its current conception, by an array of symptoms including sleep disturbances, psychotic features, and suicidal behaviors [Reference Carvalho, Firth and Vieta1]. Pharmacological treatments of BD rely on many different agents, including mood stabilizers, antipsychotics, and antidepressants [Reference Yatham, Kennedy, Parikh, Schaffer, Bond and Frey3]. Nonetheless, the neurobiology of BD is still far from clear. The kynurenine pathway (KP), key to the metabolism of the essential amino acid L-tryptophan (TRP), is among the most studied enzymatic pathways because of its potential involvement in a range of neuroinflammatory disorders, including BD [Reference Savitz4]. TRP is the substrate of various bioactive compounds that have many physiological roles, notably neural transmission and signaling [Reference Platten, Nollen, Röhrig, Fallarino and Opitz5, Reference Cervenka, Agudelo and Ruas6]. Although serotonin is its best-known metabolite, owing to its role in the pathophysiology of mood disorders [Reference Coppen7], more than 95% of TRP is not converted into serotonin but rather metabolized along the KP [Reference Savitz4, Reference Cervenka, Agudelo and Ruas6]. The KP has been investigated since the early twentieth century [Reference Schwarcz and Stone8] but its importance was long thought to be linked primarily to the de novo synthesis of nicotinamide and, consequently, nicotinamide adenine dinucleotide, a coenzyme involved in several biological processes such as redox reactions required for mitochondrial function [Reference Savitz4, Reference Platten, Nollen, Röhrig, Fallarino and Opitz5, Reference Schwarcz and Stone8, Reference Schwarcz, Bruno, Muchowski and Wu9]. Instead, no intrinsic neurobiological activity was demonstrated for the metabolites of the pathway until the late 1970s [Reference Schwarcz and Stone8, Reference Lapin10]. Since then, interest in the KP has grown gradually [Reference Schwarcz and Stone8], and research has led to the discovery that many of the metabolites generated along the pathway—collectively known also as “kynurenines (KYNs)” or “TRP catabolites”—are physiologically active and involved in inflammation, immunoregulation, and brain function [Reference Savitz4, Reference Cervenka, Agudelo and Ruas6, Reference Schwarcz and Stone8]. Thus, the KP has attracted the attention of disparate disciplines [Reference Schwarcz and Stone8], including psychiatry, because of its potential role in the etiopathogenesis of a number of diseases [Reference Savitz4, Reference Cervenka, Agudelo and Ruas6].

An overview of the KP is reported in Figure 1. In brief, the enzyme indoleamine 2,3-dioxygenase (IDO), with its two isoforms (IDO1 and IDO2), transforms TRP into KYN in the immune system and the brain, while tryptophan dioxygenase is responsible for the same reaction in the liver. The KYN/TRP ratio in the blood thus describes the activity of IDO and can be used as a proxy for the conversion of TRP into KYN. KYN is in turn catabolized into different molecules including kynurenic acid (KYNA), anthranilic acid (AA), 3-hydroxykynurenine (3HK), xanthurenic acid (XA), 3-hydroxyanthranilic acid (3HAA), quinolinic acid (QA), and picolinic acid (PA) [Reference Myint11]. The main branch of the cascade leads to 3HK, 3HAA, and QA (the so-called “QA branch”), whereas KYNA and XA are formed in competing branches of the pathway [Reference Savitz4]. Kynurenine 3-mono-oxygenase catabolizes KYN into 3HK leading it down the QA branch, hence its inhibition leads to the accumulation of KYN and increases its catabolism toward the production of KYNA via the KYN aminotransferase (KAT) isozymes (KAT-2 in the brain) whose activity is mirrored by the KYNA/KYN ratio [Reference Liu, Ding, Zhang, Mellor, Wu and Zhao12, Reference Yoshida, Fujigaki, Kato, Yamazaki, Fujigaki and Kunisawa13].

Figure 1. Schematic representation of the kynurenine pathway and related blood variations in bipolar disorder. –, decrease in bipolar disorder (red); ±, no variations in bipolar disorder (blue); ?, unclear variations in bipolar disorder (gray). Abbreviations: IDO, indoleamine 2,3-dioxygenase; KAT, kynurenine aminotransferase; KMO, kynurenine 3-monooxygenase; KYNU, kynureninase; NAD+, nicotinamide adenine dinucleotide; TDO, tryptophan 2,3-dioxygenase.

KP metabolites are putatively neuroactive, theoretically modulating neuroplasticity and influencing NMDA receptor signaling and glutamatergic neurotransmission [Reference Savitz4]. For example, KYNA seems to have a neuroprotective role by antagonizing the excitotoxic effect of QA and competitively inhibiting ionotropic glutamate receptors in order to attenuate activity at the glycine co-agonist site of the NMDA receptor [Reference Savitz4, Reference Schwarcz and Stone8]. Other potentially neuroprotective components of the pathway include XA [Reference Fazio, Lionetto, Curto, Iacovelli, Cavallari and Zappulla14], AA [Reference Schwarcz and Stone8], and PA [Reference Beninger, Colton, Ingles, Jhamandas and Boegman15]. Conversely, QA has been proven to be neurotoxic through a variety of mechanisms that include NMDA agonism with associated oxidative stress, lipid peroxidation, and interference with glutamatergic transmission [Reference Guillemin16].

The balance between neurotoxic and neuroprotective effects of KP metabolites has led to several different, and not always consistent, hypotheses concerning their role in the pathophysiology of BD. In particular, a few systematic reviews and meta-analyses have been recently published, highlighting significant variations of the KP in BD and related mood episodes, involving blood TRP, KYN, KYNA, and XA [Reference Bartoli, Cioni, Callovini, Cavaleri, Crocamo and Carrà17Reference Marx, McGuinness, Rocks, Ruusunen, Cleminson and Walker20] (Figure 1). Notwithstanding this body of evidence, whether specific clinical features of BD might be linked to the peripheral and central levels of KP metabolites remains unknown. This work is thus aimed at providing a comprehensive overview synthesizing available evidence on the association between variations of the KP and BD clinical features.

Methods

We performed an overview of research exploring the possible link between the KP and BD-related symptom severity and other clinical features, following standard methods set to report nonquantitative and narrative syntheses [Reference Baethge, Goldbeck-Wood and Mertens21, Reference Green, Johnson and Adams22]. Medline, Embase, and PsycInfo electronic databases (via Ovid) were systematically searched for articles published up to August 2022. The following search phrase was used: “(tryptophan OR kynurenine OR kynurenic OR anthranilic OR quinolinic OR picolinic OR xanthurenic) AND (bipolar OR mania OR manic)” as multiple purpose search in title, abstract, heading words, and keywords. We also explored the reference list of our recent systematic review and meta-analysis in this field [Reference Bartoli, Misiak, Callovini, Cavaleri, Cioni and Crocamo18]. No language or publication date restrictions were applied. We included studies that explored the association of peripheral and/or central concentrations of KP metabolites (TRP, KYN, KYNA, AA, 3HK, XA, 3HAA, QA, and PA), or their ratios, with clinical features of BD. To improve the consistency and comparability of data, we excluded studies that provide mixed data for subjects with BD and individuals with other psychiatric diagnoses. Moreover, we excluded “gray” literature, conference abstracts, dissertations, and all publications not having undergone a peer-review process. After a preliminary screening based on titles and abstracts, full texts were retrieved to evaluate eligibility. Articles were independently screened and read in full text by three authors (R.M.C., D.C., and T.C.). Any disagreement was resolved by discussion with the other authors.

Results

Our search generated 1,808 articles (483 from Medline, 963 from Embase, and 362 from PsycInfo) and, after removing duplicates, 1,144 studies were screened. Despite the wide variability in terms of study design, single hypotheses tested, and characteristics of included samples, we included in this overview 13 observational studies [Reference Savitz, Dantzer, Wurfel, Victor, Ford and Bodurka23Reference Fellendorf, Gostner, Lenger, Platzer, Birner and Maget35]. Clinical features of BD assessed in this body of evidence were symptoms (depression and mania) severity [Reference Savitz, Dantzer, Wurfel, Victor, Ford and Bodurka23Reference Benevenuto, Saxena, Fries, Valvassori, Kahlon and Saxena28, Reference Myint, Kim, Verkerk, Park, Scharpé and Steinbusch30], suicidal behaviors [Reference Trepci, Sellgren, Pålsson, Brundin, Khanlarkhani and Schwieler29, Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31, Reference Brundin, Sellgren, Lim, Grit, Pålsson and Landén34], psychotic features [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24, Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31Reference Sellgren, Kegel, Bergen, Ekman, Olsson and Larsson33], and sleep disturbances [Reference Mukherjee, Krishnamurthy, Millett, Reider, Can and Groer26, Reference Fellendorf, Gostner, Lenger, Platzer, Birner and Maget35]. The characteristics of the studies included in this overview are reported in Table 1.

Table 1. Characteristics of included studies.

Abbreviations: 3HAA, 3-hydroxyanthranilic acid; 3HK, 3-hydroxikynurenine; CSF, cerebrospinal fluid; KYN, kynurenine; KYNA, kynurenic acid; PA, picolinic acid; QA, quinolinic acid; TRP, tryptophan.

a Tested in 204 subjects.

b Median.

Kynurenine pathway and depressive symptoms severity

Observational studies testing the relationship between peripheral KP metabolites and depression severity generated mixed findings [Reference Savitz, Dantzer, Wurfel, Victor, Ford and Bodurka23Reference Benevenuto, Saxena, Fries, Valvassori, Kahlon and Saxena28]. In the majority of studies, no significant correlations between most KP metabolites and depressive symptoms were found. Savitz et al. [Reference Savitz, Dantzer, Wurfel, Victor, Ford and Bodurka23] found that 3HK (but not other KP metabolites) was correlated with depression severity among 63 individuals with BD. In addition, van den Ameele et al. [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24] reported a negative—albeit weak—correlation between peripheral KYNA concentrations and depression severity in a sample of 67 individuals with BD. No statistically significant correlations with depression severity were found for TRP, KYN, 3HK, and QA. Maget et al. [Reference Maget, Platzer, Bengesser, Fellendorf, Birner and Queissner25] showed a negative correlation between Hamilton Depression Rating Scale (HDRS) scores and KYNA/KYN ratio (as a proxy of KAT activity) among 156 subjects with BD. Moreover, Mukherjee et al. [Reference Mukherjee, Krishnamurthy, Millett, Reider, Can and Groer26] found that depressive symptom severity was significantly associated with both KYN and TRP in a sample of 21 individuals with BD, when total sleep time and BMI were accounted for. Conversely, among 66 participants with bipolar depression, Comai et al. [Reference Comai, Melloni, Lorenzi, Bollettini, Vai and Zanardi27] showed a negative correlation of HDRS scores with TRP. In addition, data on 49 children and adolescents with BD [Reference Benevenuto, Saxena, Fries, Valvassori, Kahlon and Saxena28] showed that depressive symptoms were negatively correlated with KYN and the KYN/TRP ratio, and positively correlated with the KYNA/KYN ratio. Finally, the only study testing CSF in 101 individuals with BD did not find any statistically significant association of different KP metabolites with depressive symptoms [Reference Trepci, Sellgren, Pålsson, Brundin, Khanlarkhani and Schwieler29].

Kynurenine pathway and manic symptom severity

Data on the relationship between peripheral KP metabolites and manic symptom severity were available from five studies [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24Reference Mukherjee, Krishnamurthy, Millett, Reider, Can and Groer26, Reference Benevenuto, Saxena, Fries, Valvassori, Kahlon and Saxena28, Reference Myint, Kim, Verkerk, Park, Scharpé and Steinbusch30], including one on children and adolescents [Reference Benevenuto, Saxena, Fries, Valvassori, Kahlon and Saxena28] and four on adults with BD [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24Reference Mukherjee, Krishnamurthy, Millett, Reider, Can and Groer26, Reference Myint, Kim, Verkerk, Park, Scharpé and Steinbusch30]. None of these studies could show any statistically significant correlation between manic symptoms, as measured by the Young Mania Rating Scale [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24, Reference Maget, Platzer, Bengesser, Fellendorf, Birner and Queissner25, Reference Benevenuto, Saxena, Fries, Valvassori, Kahlon and Saxena28, Reference Myint, Kim, Verkerk, Park, Scharpé and Steinbusch30] or the Clinician-Administered Rating Scale for Mania [Reference Mukherjee, Krishnamurthy, Millett, Reider, Can and Groer26], and different KP metabolites. Similarly, the only study testing central levels of KP metabolites did not show any relevant correlation with manic symptoms [Reference Trepci, Sellgren, Pålsson, Brundin, Khanlarkhani and Schwieler29].

Kynurenine pathway and psychotic features

Four studies [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24, Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31Reference Sellgren, Kegel, Bergen, Ekman, Olsson and Larsson33] explored the relationship of psychotic features with peripheral and/or central KP metabolites in BD. In the study by Sellgren et al. [Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31], KYNA was found to be increased in CSF—but not in plasma—in individuals with BD and a history of psychotic features. Results confirmed findings from BD subjects belonging to the same cohort [Reference Olsson, Sellgren, Engberg, Landen and Erhardt32, Reference Sellgren, Kegel, Bergen, Ekman, Olsson and Larsson33], showing a significant association between a history of psychosis and CSF levels of KYNA during euthymia. Finally, van den Ameele et al. [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24], assessing 67 subjects with BD, found decreased plasma QA in a subgroup of participants with lifetime psychotic features, although no KP metabolites were significantly correlated with Positive and Negative Syndrome Scale.

Kynurenine pathway and suicidal behaviors

The possible link between the KP and suicidality in BD has been addressed in three studies so far [Reference Trepci, Sellgren, Pålsson, Brundin, Khanlarkhani and Schwieler29, Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31, Reference Brundin, Sellgren, Lim, Grit, Pålsson and Landén34]. Brundin et al. [Reference Brundin, Sellgren, Lim, Grit, Pålsson and Landén34] reported that plasma levels of PA in 21 subjects with BD who attempted suicide were lower than in 29 healthy individuals, whereas no differences in QA concentrations were found. In a later study, Sellgren et al. [Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31] explored the peripheral and central concentrations of KYNA in relationship to lifetime suicide attempt or self-harm in individuals with BD: neither blood nor CSF KYNA levels differed from those of BD subjects without such a history. Nonetheless, higher CSF KYNA in subjects with suicide attempts, when compared with healthy controls, was found. Finally, in a study from the same research group [Reference Trepci, Sellgren, Pålsson, Brundin, Khanlarkhani and Schwieler29], TRP levels were found to be higher in participants with a history of suicidal behavior compared to subjects without a similar history, whereas PA levels and the KYN/TRP ratio were found to be lower. No significant differences were found as for the other biomarkers addressed (KYN, KYNA, QA, and the PA/QA ratio) between the two groups.

Kynurenine pathway and sleep disturbances

Two studies provided data on the relationship between KP metabolites and sleep [Reference Mukherjee, Krishnamurthy, Millett, Reider, Can and Groer26, Reference Fellendorf, Gostner, Lenger, Platzer, Birner and Maget35]. One study tested the relationship between KP and sleep [Reference Mukherjee, Krishnamurthy, Millett, Reider, Can and Groer26], measuring TRP, KYN, and the KYN/TRP ratio in 21 subjects with BD. No associations between TRP, KYN, or the KYN/TRP ratio and total sleep time were found in any of the two groups. Consistently, Fellendorf et al. [Reference Fellendorf, Gostner, Lenger, Platzer, Birner and Maget35] did not find any correlation between TRP and the insomnia HDRS items in subjects with BD, even though a negative association of both KYN and the KYN/TRP ratio with difficulties falling asleep was found.

Discussion

Summary and interpretation of findings

In recent years, several studies have explored the potential role of KP metabolites as possible measurable biomarkers of BD, analyzing their links with relevant clinical features of the disorder. Nonetheless, evidence in this field generated mixed findings, not allowing us to draw firm and consistent conclusions. In particular, none of the studies included in our overview could find any statistically significant correlations between KP metabolites and manic symptoms, and studies correlating depression symptom severity and the KP showed heterogeneous findings involving different KP metabolites in adults and youths with BD. In particular, results pointed toward correlations in different directions between depressive symptom severity and blood TRP, KYN, and KYN/KYNA. Inconsistent evidence, based on a limited number of studies, was also reported about the relationship between alterations in KP metabolism and different clinical domains such as psychotic features, suicidal behavior, and sleep disturbances. First, evidence regarding the association between the KP and psychotic features in BD shows a selective increase of KYNA in CSF—but not in plasma—and a possible decrease in plasma QA. However, these findings are at best to be replicated, considering that they were derived from similar samples by the same research group [Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31Reference Sellgren, Kegel, Bergen, Ekman, Olsson and Larsson33], and only one study tested the relationship between other KP metabolites and psychotic features [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24]. Second, few and small studies testing the possible relationship between the KP and suicidality in BD highlighted that a history of suicidal behavior might be associated with an imbalance of KP metabolites. In particular, higher TRP and KYNA levels, lower PA concentrations, and the KYN/TRP ratio in CSF [Reference Trepci, Sellgren, Pålsson, Brundin, Khanlarkhani and Schwieler29, Reference Sellgren, Gracias, Jungholm, Perlis, Engberg and Schwieler31], as well as lower blood levels of PA, compared with healthy controls [Reference Brundin, Sellgren, Lim, Grit, Pålsson and Landén34] were found. Finally, few data are available on sleep disturbances, a common occurrence in BD. Sleep may alleviate neuroinflammation, promoting the cellular clearance of brain metabolic toxins [Reference Xie, Kang, Xu, Chen, Liao and Thiyagarajan36]. Consistently, sleep deprivation might activate the enzymatic degradation of TRP and a subsequent increase of neurotoxic metabolites including KYNA [Reference Bhat, Pires, Tan, Babu Chidambaram and Guillemin37]. However, available studies do not show consistent correlations between total sleep time and KP metabolites, even though KYN and the KYN/TRP ratio might be associated with some sleep-related subdomains [Reference Fellendorf, Gostner, Lenger, Platzer, Birner and Maget35].

An important point to address, considering the paucity of data on drug-free or drug-naïve individuals, is the possible confounding role of pharmacological treatment on the relationship between the KP and different clinical features of BD. Indeed, studies addressing changes in KP metabolites suggest that psychoactive drugs may influence KP metabolism. For example, lithium, a highly pleiotropic agent, interacting with several different molecular targets, may counteract TRP catabolism by inhibiting the inflammation-induced TRP breakdown [Reference Göttert, Fidzinski, Kraus, Schneider, Holtkamp and Endres38]. Consistently, a recent study estimated an association of poorer response to lithium with higher levels of KYN, the KYN/TRP ratio, and QA, which could indicate a pro-inflammatory state with a higher degradation of TRP toward the neurotoxic branch [Reference Fellendorf, Manchia, Squassina, Pisanu, Dall’Acqua and Sut39]. In addition, other mood stabilizers, such as valproate [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24] and lamotrigine [Reference Trepci, Sellgren, Pålsson, Brundin, Khanlarkhani and Schwieler29], might influence peripheral and central levels of KP metabolites in BD. Another key issue making even more complex the relationship between KP metabolites and clinical features seems the reciprocal influence of inflammation and the KP. Indeed, a heterogeneous pathogenesis of BD has been suggested, with inflammatory abnormalities and a potential response to drugs with anti-inflammatory properties [Reference Bartoli, Cavaleri, Bachi, Moretti, Riboldi and Crocamo40], possibly occurring in specific subsets of patients [Reference Jones, Daskalakis, Carvalho, Strawbridge, Young and Mulsant41, Reference Schlaaff, Dobrowolny, Frodl, Mawrin, Gos and Steiner42]. Preclinical evidence has shown that inflammation can significantly shunt TRP metabolism toward the KP through the upregulation of the expression and activity of key enzymes of the cascade [Reference Schwarcz and Stone8]. In clinical studies on BD, significant correlations between the KYN/TRP ratio—a proxy measure of IDO activity—and TNF [Reference Van den Ameele, van Nuijs, Lai, Schuermans, Verkerk and van Diermen24], C-reactive protein [Reference Wurfel, Drevets, Bliss, McMillin, Suzuki and Ford43], and body mass index [Reference Reininghaus, McIntyre, Reininghaus, Geisler, Bengesser and Lackner44] have been shown. For instance, body mass index is an important factor influencing KP metabolites [Reference Favennec, Hennart, Caiazzo, Leloire, Yengo and Verbanck45], and obese people with BD might represent a distinct immune-metabolic population [Reference Reininghaus, McIntyre, Reininghaus, Geisler, Bengesser and Lackner44]. Thus, the potential role of immune-metabolic abnormalities should be considered in the interpretation of findings on BD clinical features and the KP. In addition, also structural brain changes involving white matter (WM) in people with BD [Reference Pezzoli, Emsell, Yip, Dima, Giannakopoulos and Zarei46] might be correlated with the KP. Neuroimaging research has shown that higher levels of KYNA, which putatively protects from glutamate excitotoxicity, could exert a neuroprotective effect on WM microstructure [Reference Poletti, Myint, Schüetze, Bollettini, Mazza and Grillitsch47]. Similarly, the neuroprotective KYNA/3HK ratio seems associated with hippocampal and amygdalar volumes in BD [Reference Savitz, Dantzer, Wurfel, Victor, Ford and Bodurka23], and the KYN/TRP ratio negatively with corpus callosum microstructure integrity, amygdala volume, and cortical thickness in the frontoparietal regions [Reference Poletti, Melloni, Aggio, Colombo, Valtorta and Benedetti48]. Additional studies should thus address if specific neurostructural and neurofunctional alterations might correlate with KP metabolites. Finally, an additional consideration is needed about the complex relationship between central and peripheral levels of KP metabolites in BD [Reference Skorobogatov, De Picker, Verkerk, Coppens, Leboyer and Müller49]: the poor concordance between them outlines the need for additional research to determine the validity of blood assessment as a proxy marker for CNS processes. This could at least partially explain the inconsistency generated by evidence in this field so far.

Limitations

The interpretation of findings synthesized in this overview requires caution considering some important limitations. First, based on the available literature, our review included a heterogeneous body of evidence not allowing us to perform any quantitative synthesis of the available data. Second, despite running a rigorous search aiming at providing a thorough overview of the topic, the narrative nature of our synthesis precluded stronger evidence-based inferences [Reference Collins and Fauser50]. Third, several metabolites of the KP—namely XA, AA, 3HAA, and PA—have been poorly studied in people with BD so far, limiting the comprehensiveness of our overview. Finally, the eligible studies did not assess differences between participants in terms of other important clinical characteristics of BD, including different stages of the disease, specific features such as anxiety and mixed states [Reference Bartoli, Crocamo and Carrà51], and psychiatric and substance-related comorbid conditions, which are highly prevalent in BD [Reference Bartoli, Crocamo and Carrà52Reference Hunt, Malhi, Cleary, Lai and Sitharthan54] and might be correlated with KP abnormalities [Reference Morales-Puerto, Giménez-Gómez, Pérez-Hernández, Abuin-Martínez, Gil de Biedma-Elduayen and Vidal55].

Conclusions

Although an imbalance of KP metabolism toward the neurotoxic branches in BD has been previously suggested, the evidence on variations of KP metabolites according to depressive and manic symptom severity as well as other clinical features is limited so far. Additional research, focusing on both blood and CSF concentrations of KP metabolites and taking into account also the BD-related immune-inflammatory and brain integrity burden, is needed. This would be helpful to address if variations of the KP, standing at the crossroads of monoaminergic, glutamatergic, and immune mechanisms of affective disorders, may represent a novel approach to understand etiopathogenesis and illness burden of BD.

Data Availability Statement

The data that support the findings of this study are available from the corresponding author upon reasonable request.

Acknowledgements

None.

Author Contributions

Conceptualization: F.B.; Data curation: R.M.C., D.C., T.C., B.M., J.B.S.; Investigation: F.B., R.M.C., D.C., T.C.; Methodology: F.B., C.C.; Project administration: F.B., G.C.; Supervision: B.M., J.B.S., G.C.; Visualization: R.M.C., D.C.; Writing—original draft: F.B., R.M.C., D.C., T.C.; Writing—review and editing: C.C., B.M., J.B.S., G.C.

Financial Support

This research received no specific grant from any funding agency, commercial or not-for-profit sectors.

Conflict of Interest

The authors declare none.

Footnotes

F.B. and R.M.C. share joint first authorship.

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Figure 0

Figure 1. Schematic representation of the kynurenine pathway and related blood variations in bipolar disorder. –, decrease in bipolar disorder (red); ±, no variations in bipolar disorder (blue); ?, unclear variations in bipolar disorder (gray). Abbreviations: IDO, indoleamine 2,3-dioxygenase; KAT, kynurenine aminotransferase; KMO, kynurenine 3-monooxygenase; KYNU, kynureninase; NAD+, nicotinamide adenine dinucleotide; TDO, tryptophan 2,3-dioxygenase.

Figure 1

Table 1. Characteristics of included studies.

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