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The prevention of neurological disorders associated to latent toxoplasmosis must begin in early ages

Opinion Article

The prevention of neurological disorders associated to latent toxoplasmosis must begin in early ages

  • Luis Fonte 1*
  • María Ginori 2
  • Kirenia Oliva 1
  • Pedro Casanova 1
  • Doris Ginorio 1
  • Yaxsier Rodríguez 3

1* Research Diagnostic and Reference Center, Institute of Tropical Medicine “Pedro Kourí”, Havana 11400, Cuba.

2 Department or Teaching, Polyclinic “Plaza de la Revolución”, Havana 11300, Cuba.

3 Pathology Department, Hospital Center of Institute of Tropical Medicine “Pedro Kourí”, Havana 11400, Cuba.

Citation: Fonte, L., Ginori, M., Oliva, K., Casanova, P., Ginorio, D., & Rodríguez, Y. (2025). The prevention of neurological Disorders associated to latent toxoplasmosis must begin in early ages. Chronicles of Clinical Reviews and Case Reports, The Geek Chronicles, 1, 1-6.

Received: February 17, 2025 | Accepted: March 4, 2025 | Published: April 22, 2025

Abstract

Abstract:

The association between latent toxoplasmosis and the development of neurological disorders constitutes a health problem of unknown dimensions. In the absence of effective drugs against bradyzoites of Toxoplasma gondii and vaccines against the parasite, other actions targeting different phases of its life cycle are in use to prevent and control the transmission. Since the prevalence of latent toxoplasmosis is already high at the end of adolescence, and bearing in mind the possible adverse consequences related to the presence of the silent form of the infection, the implementation of those prevention measures must begin at early ages.

Keywords: Toxoplasma gondii; Latent Toxoplasmosis; Neurological Disorders; Prevention; Early Ages.

Introduction

Toxoplasma gondii and toxoplasmosis. A brief overview

Toxoplasma gondii is an apicomplexan parasite able to replicate in any nucleated cell of a wide range of animals [1]. T. gondii, owing to its high transmissibility and prolonged presence in its host, is regard as one of the most successful microorganisms on the life scale, affecting around 30% of the world’s population (prevalences from 10% to 90% have been documented) [1,2].

The life cycle of T. gondii occurs in two stages and different scenarios: (i) the sexual phase, which takes place in cells of the intestine epithelium of the definitive hosts. In this site, non-sporulated oocysts are generated and then expelled in the stool; (ii) the asexual phase, which commences with the intake of the oocysts by the intermediary hosts (animals wherein the sexual phase cannot progress). The sporozoos arising from the swallowed oocysts invade the intestine epithelial cells and become tachyzoites, which propagate virtually to all organs, with particular tropism towards muscles, the retina and the central nervous system (CNS). Once in those final localizations, they turn into bradyzoites, which are structured into cysts inside several cell types, primarily muscle cells and CNS neurons. The bradyzoites are relatively resistant to immune responses and, in an apparently silent form, survive in their cellular niches until host death [3]. Humans acquire T. gondii infection mainly by three routes: (i) ingestion of sporulated oocysts in contaminated water or food, (ii) intake of tissue cysts in raw or undercooked meat containing them, and (iii) parasite transmission to the fetus [3].

The clinical course of T. gondii infection depends mainly on the immune competence of the host [4,5]. In healthy persons, the primary infection is commonly asymptomatic or shows moderately with general clinical manifestations, included fever, and lymph node inflammation [5]. In immune depressed persons, as those suffering of acquired immune deficiency syndrome, the symptoms and signs of the primary infection are more severe or a reactivation of a latent toxoplasmosis can occur [5].  If the primary infection happens during pregnancy, there will be a high risk of parasite transmission to the fetus, given that it is not immunologically ready to fight back such an attack [5]. This could result in miscarriage, fetal defects (for example, intracranial calcifications, hydrocephalus and microcephaly), and complications in newborns (for instance, chorioretinitis, blindness, deafness and mental retardation) [6]. Depressed.

Using the serologic detection of anti-T. gondii antibodies as a diagnostic tool, numerous studies have demonstrated that the proportion of infected persons increases with age [7-11]. In addition, those surveys also found that the proportion of individuals with antibodies against the parasite is already high from early ages. For instances, studies to estimate the seroprevalence of anti-T. gondii antibodies in Iran, Cuba and Bosnia and Herzegovina found 25.6%, 20.3% and 10.9%, respectively, in individuals under 20 years, and 33%, 29.7% and 30.9%, respectively, in general population (7,8,9).

Latent toxoplasmosis affects neurological functions of intermediary hosts

During many years, chronic infection by T. gondii has been considered clinically silent [3].  In general, two arguments have been used to support that assumption: (i) the absence of clinical manifestations in almost all the individuals who were seropositive for T. gondii, and (ii) the primary demonstration of the quiescent character of the bradyzoites present in the CNS of chronically infected individuals. However, in the course of the last three decades, a growing number of studies in rodents, which -like humans- act as intermediary hosts of T. gondii, have evidenced that chronic infection by this protozoan can alter important neurological functions of those animals: memory, learning, locomotion and, very significantly, behavioral [6,12-14].

In relation with those studies, the most captivating are some works showing conduct variations of chronically infected rodents. For instance, the expansion of moving spaces; the more confident movements around open areas; and more surprisingly, the development of a potential attraction to cat urine [15-17]. According to the hypothesis advanced by Lefèvre et al. in 2009 [18], those behavioral changes constitute a refined evolutive gain that allows the immature parasite (T. gondii bradyzoite) to live in an intermediary host (rodent) that subsequently will be ingested by the definitive host (cat). As a result, the parasite completes its life cycle and perpetuates its existence. The human is not the best intermediary host for T. gondii because our species does not have a natural predator. Nevertheless, and in line with that hypothesis, a relatively recent study on chimpanzee, a living primate still predated by a feline species, showed that T. gondii infection decreases the animal phobia for leopard urine [19].

Numerous studies in humans, using different designs and anti-T. gondii antibody detection tests, have shown an association between latent  and a decline of cognitive functions (working and verbal memory impairments [6,20], reduced sensitivity towards motivational effects of rewards [21], and damaged of executive functioning [6], mood variations (major depression disorder [5] and bipolar disorder [5,22,23]), behavioral changes (higher frequency of suicidal attempts [24,25], traffic accidents [26] and promiscuity [6]), psychiatric diseases (schizophrenia [6,25], obsessive-compulsive disorders [6,27]) and degenerative diseases (Alzheimer disease [6,28], multiple sclerosis [29,30] and Huntington disease [31]).

From a more holistic perspective, the results of a very recent systematic review and meta-analysis offer generic support for the existence of the aforementioned associations. Of 49 studies containing 21,093 participants and conducted in 18 countries, the global pooled seroprevalence of T. gondii IgG antibody was 38.27% among neuropsychiatric patients and 25.31% in healthy controls [5]. Interestingly, and apart from that review, some works have found a direct relationship between the length of T. gondii infection, measured by the decrease in serum antibody titers against the parasite, and the depth of several personality changes [32].

Several mechanisms, or combinations of them, have been alluded to explain the association of T. gondii chronic infection and neurological disorders: alterations of neuron morphology and functions induced by the parasite (e.g., mental maladies like schizophrenia, bipolar and obsessive-compulsive disorders are associated with a lowering of spines density and dendritic functions induced by the infection [33-34]), neurotransmission impairments caused by the chronic infection (e.g., it has been reported higher levels of dopamine and lower levels of serotonin and norepinephrine in the brain of mice chronically infected [35]), hormonal changes within the context of the infection (e.g., in persons with bipolar disorder have been shown lesser levels of corticosterone production [5]), and inflammation caused by the immune response to T. gondii (e.g., some studies in mice show that the immune response control the replication of bradyzoites inside the cysts creating an adjacent proinflammatory environment [5,36]).

On the other hand, it is necessary to remark that most of the studies mentioned earlier have been of association type. Thus, the development of drugs capable of acting on T. gondii bradyzoites or the obtaining of vaccines against the protozoan are necessary. Both approaches would allow, with the elimination of the cause, the disappearance or attenuation of the neurological disorders.

At present, the most effective therapeutic option for T. gondii infection involves the combined use of pyrimethamine and sulfadiazine [37]. However, in addition to increased T. gondii resistance [38], it has been proven that this combination is effective against tachyzoites and practically ineffective against tissue-encysted bradyzoites [39]. Consequently, vaccination seems to be the most promising alternative to control latent T. gondii infections [40,41]. Nevertheless, Toxovax™, the only

commercially available vaccine against T. gondii, has lonely been authorized to prevent abortion caused by the parasite in sheep [40,41]. In this scenario, and taking into consideration the associations mentioned above, the development of new drugs and effective vaccines against toxoplasmosis is a pressing need.

The prevention of toxoplasmosis, including its latent form, must be faced from a One Health approach that incorporates diverse types of measures that target different phases of the life cycle of T. gondii. Among them, it should be mentioned the implementation of education programs for evading contact with infectious stages of the parasite; the execution of actions to ensure food and water safety; the securing of drugs for the treatment of active infections; the promotion of procedures for preventing livestock infection; and the development of vaccines both to prevent shedding of oocysts by definitive hosts and to prevent infection of humans [39].

Generally, the application of that set of measures, or part of them, requires considerable resources and is often not sustainable. This is a difficulty that other parasite control programs have gone through, for example, soil-transmitted helminthes [42]. One of the most effective ways to achieve this sustainability is the prioritized implementation of prevention and control actions on those population groups at greater risk of being infected by the parasite and in which it could have its deleterious effects for a longer period [43].Taking into account that the prevalence of T. gondii infection is already high from early ages, as the surveys mentioned above demonstrated, the prevention of latent toxoplasmosis must begin in children and adolescents in order to avoid possible subtle alterations at those ages, when the mental disorders and illnesses that usually appear in older people have not developed.

Conclusions

The relatively recent demonstration of association between latent toxoplasmosis and the development of neurological disorders evidences a health problem of unknown dimensions: a third part of the planet’s population is at risk of developing incapacitating neurological conditions, with all that they mean in terms of human suffering and social burden. In the absence of effective drugs against bradyzoites of T. gondii and vaccines against the parasite, other actions targeting different phases of its life cycle are in use to prevent the transmission. Since the prevalence of latent toxoplasmosis is already high at the end of adolescence, and bearing in mind the possible adverse consequences related with the presence of the silent form of the infection, the implementation of those prevention measures must begin at early ages.

Ethics approval and consent to participate

Not applicable

Consent for publication

Not applicable

Funding

No fund

Acknowledgements

Not applicable

Author contributions:

All authors listed have made a substantial, direct and intellectual contribution to the work, and approved it for publication.

Conflict of Interest:

The authors declare that the preparation of the manuscript was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

References

  1. Torgerson, P.R.; Mastroiacovo, P. The global burden of congenital toxoplasmosis: a systematic review. Bull. World. Health. Organ. 2013, 91, 501‐508.
    Publisher | Google Scholor
  2. Safarpour, H.; Cevik, M.; Zarean, M. Global status of Toxoplasma gondii infection and associated risk factors in people living with HIV. AIDS 2020, 34, 469‐474.
    Publisher | Google Scholor
  3. Dubey, JP. History of the discovery of the life cycle of Toxoplasma gondii. Int. J. Parasitol, 2009, 39, 877-882.
    Publisher | Google Scholor
  4. Schlüter, D.; Barragan, A. Advances and challenges in understanding cerebral toxoplasmosis. Front. Immunol, 2019, 10.
    Publisher | Google Scholor
  5. Bisetegn, H.; Debash, H.; Ebrahim, H. Global seroprevalence of Toxoplasma gondii infection among patients with mental and neurological disorders: a systematic review and meta‐analysis. Health. Sci. Rep. 2023, 6, e1319.
    Publisher | Google Scholor
  6. Flegr, J. Toxoplasma Infection. In Encyclopedia of Sexual Psychology and Behavior; Shackelford, T.K., Eds.; Springer, Germany, 2024.
    Publisher | Google Scholor
  7. Hamidi, F.; Rostami, A.; Hosseini, S.A.; Calero-Bernal, R.; Hajavi, J.; Ahmadi, R.; et al. Anti-Toxoplasma gondii IgG seroprevalence in the general population in Iran: A systematic review and meta-analysis, 2000–2023. PLoS ONE 2024, 19, e0307941.
    Publisher | Google Scholor
  8. Machín, R.; Martínez, R.; Fachado, A.; Pividal, J.; Bravo, J. Encuesta Nacional de Toxoplasma. Prevalencia por sexo y edades. Cuba. Rev. Cubana. Med. Trop. 1993, 45, 146-51. [Accessed 02/03/2024], available in:
    Publisher | Google Scholor
  9. Šušak, B.; Martinović, K.; Jakovac, S.; Arapović, J. Seroprevalence of Toxoplasma gondii among general population in Bosnia and Herzegovina: 10-Years single center experience. Clin. Epidemiol. Glob. Health. 2023, 22, 101336.
    Publisher | Google Scholor
  10. van den Berg, O.E.; Stanoeva, K.R.; Zonneveld, R.; Hoek-van Deursen, D.; van der Klis, F.R.; van de Kassteele, J.; et al. Seroprevalence of Toxoplasma gondii and associated risk factors for infection in the Netherlands: third cross-sectional national study. Epidemiol. Infect. 2023, 151, 1-8
    Publisher | Google Scholor
  11. Giese, L.; Seeber. F.; Aebischer, A.; Kuhnert, R.; Schlaud, M.; Stark, S. Toxoplasma gondii Infections and associated factors in female Children and adolescents, Germany. Emerg. Infect. Dis. 2024, 30, 995-999.
    Publisher | Google Scholor
  12. Parlog. A.; Schluter, D.; Dunay, I.R. Toxoplasma gondii –induced neuronal alterations. Parasite Immunol. 2015, 37, 159-170.
    Publisher | Google Scholor
  13. Tedford, E.; McConkey, G. Neurophysiological changes induced by chronic Toxoplasma gondii infection. Pathogens 2017, 6, 2.
    Publisher | Google Scholor
  14. Mahmoudvand, H.; Ziaali, N.; Aghaei, I.; Sheibani, V.; Keshavarz, H.; Shabani, M. The possible association between Toxoplasma gondii infection and risk of anxiety and cognitive disorders in BALB/c mice. Pathogens Global Health 2016, 10, 1-8.
    Publisher | Google Scholor
  15. Berdoy, M.; Webster, J.P; Macdonald, D.W. Fatal attraction in rats infected with Toxoplasma gondii. Proc. R. Soc. Lond. B. 2000, 267, 1591-4.
    Publisher | Google Scholor
  16. House, K.; Vyas, A.; Sapolsky, R. Predator cat odors activate sexual arousal pathways in brains of Toxoplasma gondii infected rats. PLoS One 2011, 6, e23277.
    Publisher | Google Scholor
  17. Tan, D.; Vyas, A. Toxoplasma gondii infection and testosterone congruently increase tolerance of male rats for risk of reward forfeiture. Horm. Behav. 2016, 79, 37-44.
    Publisher | Google Scholor
  18. Lefèvre, T.; Lebarbenchon. C.; Gauthier-Clerc, M.; Missé, D.; Poulin, R.; Thomas, F. The ecological significance of manipulative parasites. Trends Ecol Evol 2009, 24, 41-48.
    Publisher | Google Scholor
  19. Poirotte, C.; Kappeler, P.M.; Ngoubangoye, B.; Bourgeois, S.; Moussodji, M.; Charpentier, M.J. Morbid attraction to leopard urine in Toxoplasma-infected chimpazees. Curr Biol 2016, 26, 98-99.
    Publisher | Google Scholor
  20. Gajewski, P.D; Falkenstein, M.; Hengstler, J.G.; Golka, K. Toxoplasma gondii impairs memory in infected seniors. Brain. Behav. Immun. 2014, 36, 193-199.
    Publisher | Google Scholor
  21. Stock, A.K.; Dajkic, D.; Kohling, H.L.; von Heinegg, E.H.; Fiedler, M.; Beste, C. Humans with latent toxoplasmosis display altered reward modulation of cognitive control. Sci. Rep. 2017, 7, 10170.
    Publisher | Google Scholor
  22. Sutterland, AL.; Fond, G.; Kuin, A.; Koeter, M.W.J.; Szoke, A.; Leboyer, M.; et al. Beyond the association. Toxoplasma gondii in schizophrenia, bipolar disorder, and addiction: systematic review and meta-analysis. Acta Psychiatr. Scand. 2015, 132, 161-169.
    Publisher | Google Scholor
  23. Hamdani, N.; Daban-Huard, C.; Lajnef, M. Relationship between Toxoplasma gondii infection and bipolar disorder in a French sample. J. Affect. Disord. 2013, 148, 444-448.
    Publisher | Google Scholor
  24. Yagmur, F.; Yazar, S.; Temel, H.O.; Cavusoglu, M. May Toxoplasma gondii increase suicide attempt-preliminary results in Turkish subjects? Forensic. Sci. Int. 2010, 199, 15-17.
    Publisher | Google Scholor
  25. Sutterland, A.L.; Kuin, A.; Kuiper, B.; van Gool, T.; Leboyer, M.; de Haan L. Driving us mad: the association of Toxoplasma gondii with suicide attempts and traffic accidents – a systematic review and meta-analysis. Psychol. Med. 2019, 23, 1-16.
    Publisher | Google Scholor
  26. Kocazeybek, B.; Oner, Y.A.; Turksoy, R. Higher prevalence of toxoplasmosis in victims of traffic accidents suggest increased risk of traffic accident in Toxoplasma-infected inhabitants of Istanbul and its suburbs. Forensic. Sci. Int. 2009, 187, 103-108.
    Publisher | Google Scholor
  27. Miman, O.; Mutlu, E.A.; Ozcan, O.; Atambay, M.; Karlidag, R.; Unal, S. Is there any role of Toxoplasma gondii in the etiology of obsessive-compulsive disorder? Psychiatry. Res. 2010, 177, 263-265.
    Publisher | Google Scholor
  28. Kusbeci, O.Y.; Miman, O.; Yaman, M.; Aktepe, OC.; Yazar, S.; Could Toxoplasma gondii have any role in Alzheimer Disease? Alzheimer Dis. Assoc. Disord. 2011, 25, 1-3.
    Publisher | Google Scholor
  29. Estato, V.; Stipursky, J.; Gomes, F.; Mergener, T.; Allodi, S.; Adesse, D. The Neurotropic parasite Toxoplasma gondii induces sustained neuroinflammation with microvascular dysfunction in infected mice. Am. J. Pathol. 2018, 118, 2674-2678.
    Publisher | Google Scholor
  30. D'Haeseleer, M.; Hostenbach, S.; Peeters, I. Cerebral hypoperfusion: a new pathophysiologic concept in multiple sclerosis? J. Cereb. Blood Flow Metab. 2015, 35, 1406-1410.
    Publisher | Google Scholor
  31. Donley, D.W.; Olson, A.R.; Raisbeck, M.R.; Fox, J.H.; Gigley, J.P. Huntingtons Disease mice infected with Toxoplasma gondii demonstrate early Kynurenine pathway activation, altered CD8+ T-Cell responses, and premature mortality. PLoS ONE 2016. 11, e0162404.
    Publisher | Google Scholor
  32. Flegr, J. Influence of latent Toxoplasma infection on human personality, physiology and morphology: Pros and cons of the Toxoplasma–human model in studying the manipulation hypothesis. J. Exp. Biol. 2013, 216, 127-133.
    Publisher | Google Scholor
  33. Parlog, A.; Harsan, L.; Zagrebelsky, M. Chronic murine toxoplasmosis is defined by subtle changes in neuronal connectivity. Dis. Model. Mech. 2014, 7, 459-469.
    Publisher | Google Scholor
  34. Penzes, P.; Cahill, M.; Jones, K.; Van Leeuwen, J.; Woolfrey, K.M. Dendritic spine pathology in neuropsychiatric disorders. Nat. Neurosci. 2011, 14, 285-293.
    Publisher | Google Scholor
  35. Stibbs, H. Changes in brain concentrations of catecholamines and indoleamines in Toxoplasma gondii infected mice. Ann. Trop. Med. Parasitol. 1985, 79, 153-157.
    Publisher | Google Scholor
  36. Blanchard, N.; Dunay, I.R.; Schlüter, D. Persistence of Toxoplasma gondii in the central nervous system: a fine-tuned balance between the parasite, the brain and the immune system. Parasite Immunol. 2015, 37, 150-158.
    Publisher | Google Scholor
  37. Dunay, I.R.; Gajurel, K.; Dhakal, R.; Liesenfeld, O.; Montoya, J.G. Treatment of Toxoplasmosis: Historical Perspective, Animal Models, and Current Clinical Practice. Clin. Microbiol. Rev. 2018, 31.
    Publisher | Google Scholor
  38. Montazeri, M.; Mehrzadi, S.; Sharif, M.; Sarvi, S.; Tanzifi, A.; Aghayan, S.A. Drug Resistance in Toxoplasma gondii. Front. Microbiol. 2018, 9, 2587.
    Publisher | Google Scholor
  39. Smith, N.C.; Goulart, C.; Hayward, J.A.; Kupz, A.; Miller, C.; van Dooren, G.G. Control of human toxoplasmosis. Intern. J. Parasitol. 2021, 51, 95-121.
    Publisher | Google Scholor
  40. Karakavuk, M, H.; Gül, A.; Dö¸skaya, A.D.; Alak, S.E.; Ün, C.; Gürüz, A.Y. DNA vaccine formulations protect against chronic toxoplasmosis. Microb. Pathog. 2021, 158, 105016.
    Publisher | Google Scholor
  41. Wang, J.; Zhang, NZ.; Li, T.T.; He, J.J.; Elsheikha, H.M.; Zhu, X.Q. Advances in the Development of Anti-Toxoplasma gondii Vaccines: Challenges, Opportunities, and Perspectives. Trends Parasitol. 2019; 35; 239-253.
    Publisher | Google Scholor
  42. Humphries, D.; Nguyen, S.; Boakyec, D.; Wilson, M.; Cappello, M. The promise and pitfalls of mass drug administration to control intestinal helminth infections. Curr. Opin. Infect. Dis. 2012, 25, 584-589.
    Publisher | Google Scholor
  43. Gyorkos, T.W.; Maheu-Giroux, M.; Blouin, B.; Casapia, M. Impact of health education on soil-transmitted helminth infections in schoolchildren of the Peruvian amazon: a cluster-randomized controlled trial. PLoS Negl. Trop. Dis. 2013, 7, e2397.
    Publisher | Google Scholor

Copyright: © 2025 Luis Fonte 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.