Abstract Background Toxoplasma gondii (T. gondii) is a protozoan parasite present in around a third of the human population. Infected individuals are commonly asymptomatic, though recent reports have suggested that infection might influence aspects of the host’s behavior. In particular, Toxoplasma infection has been linked to schizophrenia, suicide attempt, differences in aspects of personality and poorer neurocognitive performance. However, these studies are often conducted in clinical samples or convenience samples. Methods/Results In a population-representative birth-cohort of individuals tested for presence of antibodies to T. gondii (N = 837) we investigated the association between infection and four facets of human behavior: neuropsychiatric disorder (schizophrenia and major depression), poor impulse control (suicidal behavior and criminality), personality, and neurocognitive performance. Suicide attempt was marginally more frequent among individuals with T. gondii seropositivity (p = .06). Seropositive individuals also performed worse on one out of 14 measures of neuropsychological function. Conclusion On the whole, there was little evidence that T. gondii was related to increased risk of psychiatric disorder, poor impulse control, personality aberrations or neurocognitive impairment.

Citation: Sugden K, Moffitt TE, Pinto L, Poulton R, Williams BS, Caspi A (2016) Is Toxoplasma Gondii Infection Related to Brain and Behavior Impairments in Humans? Evidence from a Population-Representative Birth Cohort. PLoS ONE 11(2): e0148435. https://doi.org/10.1371/journal.pone.0148435 Editor: Herbert B. Tanowitz, Albert Einstein College of Medicine, UNITED STATES Received: June 17, 2015; Accepted: January 18, 2016; Published: February 17, 2016 Copyright: © 2016 Sugden et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Data Availability: Due to restrictions set by the University of Otago IRB, data are available upon request. Requests for the data may be made to the corresponding author (karen.sugden@duke.edu). Funding: The Dunedin Multidisciplinary Health and Development Research Unit is supported by the New Zealand Health Research Council (http://www.hrc.govt.nz/; RP). This research received support from US National Institute on Aging (NIA: https://www.nia.nih.gov/) grants AG032282, AG048895 (AC and TEM), and UK Medical Research Council (http://www.mrc.ac.uk/) grant MR/K00381X (AC and TEM). Additional support was provided by the Jacobs Foundation (http://jacobsfoundation.org/) Jacobs Prize 2010 (AC and TEM). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Competing interests: The authors have declared that no competing interests exist.

Introduction Toxoplasma gondii (T. gondii) is an obligate protozoan parasite of all warm-blooded mammals including humans, where infection has been linked to schizophrenia, suicide attempt, differences in aspects of personality and poorer neurocognitive performance. In humans, the primary source of infection is through contact with the feces of infected animals, especially domestic cats, the definitive host in which the T. gondii protozoan completes its life cycle. Alternate sources of infection occur through contact and ingestion of infected meat (especially pork), maternal-fetal transmission and exposure to soil and water contaminated with oocytes. T. gondii is geographically omnipresent, and it is estimated that age-adjusted country-level seroprevalence ranges from around 3% in South Korea to 76% in Costa Rica [1]. In rare cases, Toxoplasmosis can present with severe pathological symptoms, including retinochoroiditis, myocarditis and meningoencephalitis, potentially leading to death [2]. However, most infected humans are asymptomatic, exhibiting few or no physiological symptoms. Because of this asymptomatic nature, it was long thought that latent T. gondii infection was of little public health significance except in cases of concurrent immunosuppression, such as HIV infection. However, recent reports have suggested that infection with T. gondii might have previously unrecognized consequences in humans. One such consequence concerns host behavioral manipulation. In terms of the relationship between the intermediate and the definitive host, modifying normal interactions between the two would be advantageous to the parasites’ transmission and reproduction. In other words, modification of a rodent’s normal aversive reaction to felines would be advantageous to the parasite, since it would generate a higher chance of it being consumed by the cat, the organism in which the parasite’s life cycle is completed [3]. Indeed, evidence exists that infection of mice by T. gondii predicts innate loss of fear of cat urine [4] and impaired working memory [5]. These observations have led to the hypothesis that such manipulations might not be unique to rodent hosts. As such, extrapolations of these phenomena to correlates of human behavior are gaining attention. In line with observed effects of infection on rodents’ behavior, most human research has focused on behavioral domains involving psychiatric illness, impulsivity and aberrant neurocognitive processes. The most heavily researched correlate of T. gondii infection is schizophrenia. Interestingly, some acute cases of T. gondii infection result in hallucinations, a key feature of schizophrenia, and reports of inflated numbers of T. gondii positive individuals in samples of psychiatric inpatients were made as early as the 1950’s [6]. The culmination of these findings is a recent meta-analysis of 38 studies, which suggests that T. gondii infection increases the odds of developing schizophrenia 2.7 times (OR, 2.71, 95%CI 1.93–3.80) [7]. In addition, links with T. gondii have also been suggested with major depressive disorder; however, these suggestions have been more hyperbolic. One case report demonstrated alleviation of depressive symptoms upon successful T. gondii treatment [8], whilst another reported a correlation between cat bites and depression in women [9]. However, association studies of T. gondii infection with depression have been inconsistent [10, 11]. Poor impulse regulation, including violent and risk-taking behavior, is another potential consequence of infection. Latent T. gondii infection has been associated with increased human trait aggression in females and increased impulsivity in males [12]. Other studies have reported links between T. gondii antibody titer and suicide attempt [13–15]. Complementing these individual-level studies, cross-national comparisons have documented that national seroprevalence rates of T. gondii antibodies titers are positively correlated with higher nation-wide rates of both suicide and homicide [1, 16, 17]. Yet another study has reported higher incidence in seropositivity amongst prison inmates compared to controls [18]. Further reports show that T. gondii seropositivity is related to both fatal and non-fatal traffic road accidents [19, 20], presumably reflecting poor impulse regulation. Finally, there is some evidence that neurocognitive and personality differences exist between seropositive and seronegative individuals. In particular, slower reaction times [21, 22] and poor attention [23] appear to be associated with T. gondii seropositivity, along with lower scores of Novelty Seeking [24]. This study tested the hypothesis that T. gondii infection is related to impairment in brain and behavior, as measured by a range of phenotypes encompassing neuropsychiatric disorders, poor impulse control, personality and neurocognitive deficits. We tested the hypothesis in a population-representative birth cohort of adults enrolled in the Dunedin Longitudinal Study. We drew on data derived from psychiatric interviews, neuropsychological testing, and a search of administrative records to conduct, to our knowledge, the most comprehensive evaluation to date of the link between T. Gondii infection and the full panoply of presumptive impairments.

Materials and Methods Participants Participants are members of the Dunedin Multidisciplinary Health and Development Study, a longitudinal investigation of health and behavior in a population-representative birth cohort [25]. Study members (N = 1,037; 91% of eligible births; 52% male, 48% female) were all individuals born between April 1972 and March 1973 in Dunedin, New Zealand, who were eligible for the longitudinal study based on residence in the province at age 3 and who participated in the first follow-up assessment at age 3. The cohort represents the full range of socioeconomic status in the general population of New Zealand’s South Island and matches the NZ National Health and Nutrition Survey on adult health indicators (e.g. BMI, smoking, GP visits)[26]. The majority of cohort members are White. Assessments were carried out at ages 3, 5, 7, 9, 11, 13, 15, 18, 21, 26, 32, and most recently, 38 years, when we assessed 95% of the 1,007 study members who were still alive. At each assessment wave, Study members (including emigrants and prisoners) were brought to the Dunedin Multidisciplinary Health and Development Research Unit for a full day of interviews and examinations. These data are supplemented by searches of official records, and by questionnaires that were mailed to informants nominated by the Study members themselves. Written informed consent was obtained from all Study members. The University of Otago Ethics Committee approved each phase of the Study and the consent procedure. Blood collection and processing Venous blood samples were collected from Study members at age 38 by a trained phlebotomist using standard blood collection apparatus. Blood was collected into 10ml K 2 EDTA Vacutainer tubes (BD, Franklin Lakes, NJ). After the necessary initial inversion, tubes were processed by centrifugation at 2,000g for 10 minutes (K 2 EDTA) and the plasma fraction was transferred into 2ml cryovials. All plasma was stored at -80°C until analysis. T. gondii IgG level measurement Levels of IgG antibodies to T. gondii were determined using a Toxoplasma IgG Immunosimplicity EIA kit (Diamedix, FL., USA). Briefly, plasma was diluted 1 in 100 in sample diluent prior to assaying, and 100μL of diluted samples, standards (0 IU/ml, 50 IU/ml and 250IU/ml), controls (high positive, low positive and negative) and blank (sample diluent only) were placed in the reaction plate. Reactions were performed following the manufacturer’s instructions. All EIA reactions were performed in duplicate. Upon completion of the reactions, OD readings at 450nm (correcting for background at 600nm) were read using a Spectramax-384 spectrophotometer (Molecular Devices, Sunnydale, CA) and data acquired using SoftMax Pro software (Molecular Devices). Raw OD units were transformed by subtracting the mean OD value of the sample blank, and a standard curve was calculated using a point-point curve fit of the standards. The resulting equation was used to extrapolate sample OD values into IU/ml units. These values were multiplied by the initial dilution factor (1 in 100) to derive an estimate of plasma IU/ml. Duplicate values were then averaged to derive a mean IU/ml per sample. The manufacturer-recommended cut-off value for seropositivity for anti-Toxoplasma IgG using this EIA assay was 50 IU/ml, based on the WHO 3rd International Standard for Anti-Toxoplasma; Values above 50 IU/ml were designated positive for anti-Toxoplasma IgG; all other values were designated negative. The mean within-assay coefficient of variation (%CV) was 11.3%. Outcome measures The measures used as outcome variables in this study are described in Table 1. Briefly, we assessed four facets of human behavior: neuropsychiatric disorder (DSM diagnosis of schizophrenia and depression), indicators of poor impulse control (non-suicidal self-injury, attempted suicide, criminal convictions, and accident claims), Big-five personality traits (Openness to Experience, Conscientiousness, Extraversion, Agreeableness, and Neuroticism), and neurocognitive performance (e.g., general intelligence, executive functions, memory, and processing speed). PPT PowerPoint slide

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larger image TIFF original image Download: Table 1. Brief description of neuropsychiatric, impulse control, personality and neurocognitive outcome measures used in the study. https://doi.org/10.1371/journal.pone.0148435.t001 Statistical analysis The association between T. gondii infection status and the various phenotypes were tested using SPSS version 22 (IBM, New York, NY) and SAS (SAS Institute Inc., Cary, NC). We tested associations between T. gondii infection and outcomes in a regression of the form: A = a + b1(T. gondii) + b2(sex) + e, where A is one of the 27 outcome measures. The form of regression varied depending on whether the outcome under consideration represented binary or continuous data.

Results Plasma samples were available for 837 individuals at age 38 (423 male, 50.4%). Of these individuals, 236 (28.2%) had T. gondii IgG antibodies above 50 UI/ml, indicating a positive T. gondii infection status. This is similar to seroprevalence rates in other developed Western countries [1]. Males (32.6%) were significantly more likely to test positive for T. gondii than females (23.7%) (χ2(df) = 8.28(1), p < 0.01). All subsequent inferential tests included a statistical control for sex. T. gondii infection status was not related to socioeconomic status (SES); proportions of individuals testing positive for T. gondii IgG in low, medium and high SES groups were 32.2%, 29.4% and 23.4%, respectively (χ2(df) = 4.41(1), p = 0.11). We compared people with missing (N = 200) versus non-missing (N = 837) T. gondii seroprevalence data at age 38. Seroprevalence data were missing because a) for cultural reasons, Maori-ancestry cohort members’ blood was not studied (7% of cohort), b) Study members either did not consent to phlebotomy (2%), did not take part at age-38 assessment (5%), or died before age 38 (3%), or c) immunoassay data did not pass quality control (2%). Across all 27 outcome variables tested in our analysis, we found only three differences: Study members with missing T. gondii data were more likely to meet a diagnosis of schizophrenia (N = 13, 10.7%; OR (95% CI) = 4.07 (2.01–8.24), p < .01), a diagnosis of major depression (N = 28, 24.1%; OR (95% CI) = 1.77 (1.11–2.83), p = .02), and were more likely to have an adult criminal conviction (N = 54, 39.1%; OR (95% CI) = 1.60 (1.04–2.46), p = .03). 1. Is T. gondii infection status related to neuropsychiatric conditions? We tested whether T. gondii seropositivity was associated with increased prevalence of two neuropsychiatric disorders; schizophrenia and major depression. T. gondii seropositivity was not significantly associated to either of these conditions (Table 2). PPT PowerPoint slide

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larger image TIFF original image Download: Table 2. The association between T. gondii infection status and the range of neuropsychiatric disorders, indicators of poor impulse control and personality. https://doi.org/10.1371/journal.pone.0148435.t002 2. Is T. gondii infection status related to poor impulse control? We tested whether T. gondii seropositivity was associated with poor impulse control, as reflected in four phenotypes: non-suicidal self-injury, suicide attempt, criminal convictions, and traffic-related offences and accidents. T. gondii was not significantly associated with non-suicidal self-injury, but there was a suggestive link between latent infection and suicide attempt (Table 2). In regards to criminal behavior, there was no significant association between T. gondii seropositivity and criminal convictions, as reflected in official conviction records (Table 2). We further probed this non-significant association by testing whether T. gondii seropositivity was linked to certain types of criminal offenses (e.g., violence, driving) that have been previously examined in studies of T. gondii infection. T. gondii seropositivity was not significantly associated with increased risk of any type of criminal offending (Table 2). 3. Is T. gondii infection status related to personality differences? In order to summarize the possible psychological differences that are associated with infection by T. gondii, we examined the personality profiles of individuals who tested positive versus negative for T. gondii antibodies. To do this, we measured the Five-Factor Model of personality. The past two decades have led to a consensus among psychologists that personality differences can be organized along five broad dimensions: Openness to Experience, Conscientiousness, Extraversion, Agreeableness, and Neuroticism [34]. Table 2 describes the mean scores across all traits for seropositive and seronegative individuals. The personality profiles of individuals who tested positive for T. gondii antibodies were indistinguishable from the personality profiles of individuals who tested negative. 4. Is T. gondii infection status related to poorer neurocognitive performance? Lastly, we assessed the relationship between T. gondii seropositivity and a comprehensive range of neurocognitive functions at age 38 (Table 3). We tested whether performance on the WAIS-IV test of general intelligence at age 38 was associated with T. gondii seropositivity. There were no significant IQ differences between seropositive versus seronegative individuals. We then tested whether T. gondii seropositivity was associated with poorer performance on a range of functions encompassing verbal comprehension, perceptual reasoning, working memory, processing speed, executive functioning, motor functions and memory. T. gondii infection status was associated with poorer memory performance on the Rey Auditory Verbal Learning test. Associations between T. gondii infection status and all other tests of neurocognitive functions were not significant. PPT PowerPoint slide

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larger image TIFF original image Download: Table 3. The association between T. gondii infection status and neurocognitive function. https://doi.org/10.1371/journal.pone.0148435.t003

Discussion Our results suggest that a positive test for T. gondii antibodies does not result in increased susceptibility to neuropsychiatric disorders, poor impulse control or impaired neurocognitive ability. Moreover, we found no association between seropositivity and aberrant personality functions. Some traits which have been linked previously to T. gondii seropositivity were marginally associated in our cohort. For example, we found that recently-attempted suicide was more common in seropositive individuals. This trend is consistent with previous studies, where history of suicide attempt, but not completion, has been related to both antibody titer [13] and seropositivity [15]. Similarly, our seropositive individuals performed more poorly on one test of verbal learning and memory (the Rey Auditory Verbal Learning Test), but this finding was the only significant difference among 14 tests and may have emerged by chance, since it was not evident on other tests of memory (the CANTAB visual paired associates and the Wechsler Memory Scale Paired Associates). In contrast to previous studies, we did not observe a significant association between T. gondii seropositivity and schizophrenia. Approximately 40 reports have now been published showing links between schizophrenia and/or psychotic symptoms and infection status, leading to the suggestion that psychosis-spectrum conditions are a consequence of infection. Biological pathways have been proposed and pursued, centering on the schizophrenia-linked candidate neurotransmitter dopamine; in rodents, infection with T. gondii leads to aberrant dopamine signaling [35] and reduced expression of genes within the dopamine pathway, such as DRD1, DRD5 and MAOA [36]. However, we found no link to schizophrenia or its associated neuropsychological deficits in our cohort. One explanation is that our failure to detect statistically significant associations between T. gondii infection and brain and behavior impairments represents a false negative in an accumulating evidence base. False negative findings arise for a number of reasons, including low statistical power to detect associations due to small sample sizes (especially in relation to schizophrenia). In our case, the possibility of false negatives needs to be evaluated against several strengths of our study design. First, this is, to our knowledge, the most comprehensive assessment of the possible link between T. gondii infection and a variety of impairments in a single cohort. Previous positive associations have been reported across different studies, often in selected or clinical samples; for example, one study will examine the link to violence, another the link to schizophrenia, and yet another the link to self-injury, and so forth. Given that many of these impairments are correlated in the population and are characterized by comorbid presentation, it would be expected that they should be detectable through deep and comprehensive phenotyping of the same individuals drawn from a single birth cohort. Second, although our cohort is of only modest size, it is adequately powered to detect small effect sizes (r = 0.1). Moreover, we have previously published positive findings in this cohort using these same brain and behavior phenotypes [27, 28, 37, 38]. Third, our phenotypic assessment encompasses multiple sources including administrative records, reliable clinical interviews, well-established personality measures and standardized neurocognitive assessments, and failure to detect associations cannot be attributable to unreliable or idiosyncratic measurement practices. Fourth, we have minimized unwanted heterogeneity by studying participants who are the same chronological age. It is generally accepted that rates of infection increase as individuals age, probably due to cumulative increases in exposure opportunities [39]. By testing our hypotheses in a cohort of same-aged individuals, we were able to reduce the chance of spurious associations deriving from age-related exposure differences. We do note two disadvantages of our study. First, T. gondii antibody status was assessed at age 38 only. We were unable to correlate the timing of acquisition of infection with subsequent changes in behavior. This is a limitation of all studies restricted to analysis of behavioral correlates post-infection, the current study included. Since infection might have influences on brain development (e.g. [40, 41]) there might developmentally-sensitive periods where effects of infection are magnified. It would be of great interest to conduct a similar investigation in a cohort of younger individuals who can be tracked longitudinally in order to determine cause and effect of the infection-behavior relationship. Disproportionate sample attrition can be a confounder in association studies, although often study design limits the ability to test and document missingness. We found evidence of selective missing data for three of our 27 outcome variables; although this observation would be expected by chance, it is still a consideration. A further consideration for all studies of T. gondii and behavioral outcomes, the present study included, is variation of both the parasite and host and the relationship to pathogenicity. There are a number of different T. gondii strains which differ in both virulence and prevalence across populations [1]. Human genetic variation, especially within the major histocompatibility complex, appears to be involved in pathogenicity of T. gondii [42]. Given these observations, some potentially interesting future directions for studies of T. gondii infection correlates are inclusion of measures of T. gondii strain and host response to infection (for example, magnitude of response to parasite antigens). This addition is necessary in order to determine whether discrepancies between reports can be ascribed to population-specific human and/or T. gondii variation. A second explanation of our null findings is that earlier reports of links between T. gondii infection and behavioral impairments are exaggerated. Interest in the role of external organisms influencing human psychiatric and cognitive health is currently high. This is, in part, due to an increasing recognition of the role that inflammatory processes play in brain integrity [43–45], and in part due to the frustrating scientific search for biological causes with large effects in common mental disorders and processes (e.g. [46, 47]). Interest in T. gondii in particular has not only captured the imagination of researchers, but also the lay public. T. gondii is a microorganism whose source of transmission is common and relatable, as evidenced by numerous recent popular opinion pieces (e.g., “How Your Cat Is Making You Crazy”, [48]). It has been observed that the ‘hotter’ the topic and as more studies are reported and accumulate, replication becomes more difficult [49]. If we accept that the findings reported in the present article represent scenario two, then views of the link between T. gondii and aberrant behavior may need to be tempered accordingly. In conclusion, our data do not support the hypothesis that infection by T. gondii is related to negative behavioral outcomes in a population-representative cohort of early middle-aged individuals. In the presence of conflicting reports, better research designs are needed to fully establish the extent to which T. gondii influences impairments in brain and behavior phenotypes.

Acknowledgments We thank the Dunedin Study members, Dunedin Unit research staff, and Study founder Phil Silva.

Author Contributions Conceived and designed the experiments: KS TEM AC. Performed the experiments: KS LP BSW. Analyzed the data: KS. Contributed reagents/materials/analysis tools: TEM RP AC. Wrote the paper: KS AC.