Cryptococcus neoformans Glucuronoxylomannan and Sterylglucoside Are Required for Host Protection in an Animal Vaccination Model

2019 | Colombo, A.C., Rella, A., Normile, T., Joffe, L.S., Tavares, P.M., de S. Araújo, G.R., Frases, S., Orner, E.P., Farnoud, A.M., Fries, B.C., Sheridan, B., Nimrichter, L., Rodrigues, M.L., Del Poeta, M.

open-access mBio, doi:10.1128/mBio.02909-18

Abstract

Cryptococcus neoformans is an encapsulated fungal pathogen that causes meningoencephalitis. There are no prophylactic tools for cryptococcosis. Previously, our group showed that a C. neoformans mutant lacking the gene encoding sterylglucosidase (Δsgl1) induced protection in both immunocompetent and immunocompromised murine models of cryptococcosis. Since sterylglucosidase catalyzes degradation of sterylglucosides (SGs), accumulation of this glycolipid could be responsible for protective immunity. In this study, we analyzed whether the activity of SGs is sufficient for the protective effect induced by the Δsgl1 strain. We observed that the accumulation of SGs impacted several properties of the main polysaccharide that composes the fungal capsule, glucuronoxylomannan (GXM). We therefore used genetic manipulation to delete the SGL1 gene in the acapsular mutant Δcap59 to generate a double mutant (strain Δcap59/Δsgl1) that was shown to be nonpathogenic and cleared from the lung of mice within 7 days post-intranasal infection. The inflammatory immune response triggered by the Δcap59/Δsgl1 mutant in the lung differed from the response seen with the other strains. The double mutant did not induce protection in a vaccination model, suggesting that SG-related protection requires the main capsular polysaccharide. Finally, GXM-containing extracellular vesicles (EVs) enriched in SGs delayed the acute lethality of Galleria mellonella against C. neoformans infection. These studies highlighted a key role for GXM and SGs in inducing protection against a secondary cryptococcal infection, and, since EVs notoriously contain GXM, these results suggest the potential use of Δsgl1 EVs as a vaccination strategy for cryptococcosis.

IMPORTANCE: The number of deaths from cryptococcal meningitis is around 180,000 per year. The disease is the second leading cause of mortality among individuals with AIDS. Antifungal treatment is costly and associated with adverse effects and resistance, evidencing the urgency of development of both therapeutic and prophylactic tools. Here we demonstrate the key roles of polysaccharide- and glycolipid-containing structures in a vaccination model to prevent cryptococcosis.

Cite as

Colombo, A.C., Rella, A., Normile, T., Joffe, L.S., Tavares, P.M., de S. Araújo, G.R., Frases, S., Orner, E.P., Farnoud, A.M., Fries, B.C., Sheridan, B., Nimrichter, L., Rodrigues, M.L., Del Poeta, M., 2019. Cryptococcus neoformans Glucuronoxylomannan and Sterylglucoside Are Required for Host Protection in an Animal Vaccination Model. mBio. https://doi.org/10.1128/mbio.02909-18

Citations

Influence of aversive stimulation on haloperidol-induced catalepsy in rats

2019 | Barroca, N.C.B., Guarda, M.D., da Silva, N.T., Colombo, A.C., Reimer, A.E., Brandão, M.L., de Oliveira, A.R.

Behavioural Pharmacology, doi:10.1097/FBP.0000000000000462

Abstract

Catalepsy – an immobile state in which individuals fail to change imposed postures – can be induced by haloperidol. In rats, the pattern of haloperidol-induced catalepsy is very similar to that observed in Parkinson’s disease (PD). As some PD symptoms seem to depend on the patient’s emotional state, and as anxiety disorders are common in PD, it is possible that the central mechanisms regulating emotional and cataleptic states interplay. Previously, we showed that haloperidol impaired contextual-induced alarm calls in rats, without affecting footshock-evoked calls. Here, we evaluated the influence of distinct aversive stimulations on the haloperidol-induced catalepsy. First, male Wistar rats were subjected to catalepsy tests to establish a baseline state after haloperidol or saline administration. Next, distinct cohorts were exposed to open-field; elevated plus-maze; open-arm confinement; inescapable footshocks; contextual conditioned fear; or corticosterone administration. Subsequently, catalepsy tests were performed again. Haloperidol-induced catalepsy was verified in all drug-treated animals. Exposure to open-field, elevated plus-maze, open-arm confinement, footshocks, or administration of corticosterone had no significant effect on haloperidol-induced catalepsy. Contextual conditioned fear, which is supposed to promote a more intense fear, increased catalepsy over time. Our findings suggest that only specific defensive circuitries modulate the nigrostriatal system mediating the haloperidol-induced cataleptic state.

Cite as

Barroca, N.C.B., Guarda, M.D., da Silva, N.T., Colombo, A.C., Reimer, A.E., Brandão, M.L., de Oliveira, A.R., 2019. Influence of aversive stimulation on haloperidol-induced catalepsy in rats. Behavioural Pharmacology. https://doi.org/10.1097/fbp.0000000000000462

Citations

The putative flippase Apt1 is required for intracellular membrane architecture and biosynthesis of polysaccharide and lipids in Cryptococcus neoformans

2018 | Rizzo, J., Colombo, A.C., Zamith-Miranda, D., Silva, V.K.A., Allegood, J.C., Casadevall, A., Del Poeta, M., Nosanchuk, J.D., Kronstad, J.W., Rodrigues, M.L.

Biochimica et Biophysica Acta (BBA) - Molecular Cell Research, doi:10.1016/j.bbamcr.2017.12.007

Abstract

Flippases are responsible for the asymmetric distribution of phospholipids in biological membranes. In the encapsulated fungal pathogen Cryptococcus neoformans, the putative flippase Apt1 is an important regulator of polysaccharide secretion and pathogenesis in mice by unknown mechanisms. In this study, we analyzed the role of C. neoformans Apt1 in intracellular membrane architecture and synthesis of polysaccharide and lipids. Analysis of wild type (WT), apt1Δ (mutant) and apt1Δ::APT1 (complemented) strains by transmission electron microscopy revealed that deletion of APT1 resulted in the formation of irregular vacuoles. Disorganization of vacuolar membranes in apt1Δ cells was accompanied by a significant increase in the amounts of intra-vacuolar and pigment-containing vesicles. Quantitative immunogold labeling of C. neoformans cells with a monoclonal antibody raised to a major capsular component suggested impaired polysaccharide synthesis. APT1 deletion also affected synthesis of phosphatidylserine, phosphatidylethanolamine, inositolphosphoryl ceramide, glucosylceramide and ergosterylglycoside. These results reveal novel functions of Apt1 and are in agreement with the notion that this putative flippase plays an important role in the physiology of C. neoformans.

Cite as

Rizzo, J., Colombo, A.C., Zamith-Miranda, D., Silva, V.K.A., Allegood, J.C., Casadevall, A., Del Poeta, M., Nosanchuk, J.D., Kronstad, J.W., Rodrigues, M.L., 2018. The putative flippase Apt1 is required for intracellular membrane architecture and biosynthesis of polysaccharide and lipids in Cryptococcus neoformans. Biochimica et Biophysica Acta (BBA) - Molecular Cell Research. https://doi.org/10.1016/j.bbamcr.2017.12.007

Citations

Dual role of dopamine D2 -like receptors in the mediation of conditioned and unconditioned fear

2015 | Brandão, M.L., de Oliveira, A.R., Muthuraju, S., Colombo, A.C., Saito, V.M., Talbot, T.

FEBS Letters, doi:10.1016/j.febslet.2015.02.036

Abstract

A reduction of dopamine release or D2 receptor blockade in the terminal fields of the mesolimbic system, particularly the amygdala, clearly reduces conditioned fear. Similar D2 receptor antagonism in the neural substrates of fear in the midbrain tectum attenuates the processing of unconditioned aversive information. However, the implications of the interplay between opposing actions of dopamine in the rostral and caudal segments of the dopaminergic system are still unclear. Previous studies from this laboratory have reported the effects of dopaminergic drugs on behavior in rats in the elevated plus maze, auditory-evoked potentials (AEPs) recorded from the midbrain tectum, fear-potentiated startle, and conditioned freezing. These findings led to an interesting framework on the functional roles of dopamine in both anxiety and fear states. Dopamine D2 receptor inhibition in the terminal fields of the mesolimbic dopamine system generally causes anxiolytic-like effects, whereas the activity of midbrain substrates of unconditioned fear are enhanced by D2 receptor antagonists, suggesting that D2 receptor-mediated mechanisms play opposing roles in fear/anxiety processes, depending on the brain region under study. Dopamine appears to mediate conditioned fear by acting at rostral levels of the brain and regulate unconditioned fear at the midbrain level, likely by reducing the sensorimotor gating of aversive events.

Cite as

Brandão, M.L., de Oliveira, A.R., Muthuraju, S., Colombo, A.C., Saito, V.M., Talbot, T., 2015. Dual role of dopamine D2 -like receptors in the mediation of conditioned and unconditioned fear. FEBS Letters. https://doi.org/10.1016/j.febslet.2015.02.036

Citations

Fungal colonization of the brain: anatomopathological aspects of neurological cryptococcosis

2015 | COLOMBO, A.C., RODRIGUES, M.L.

open-access Anais da Academia Brasileira de Ciências, doi:10.1590/0001-3765201520140704

Abstract

Brain infection by the fungus Cryptococcus neoformans results in an estimated 500,000 human deaths per annum. Colonization of the central nervous system (CNS) by C. neoformans causes different clinical syndromes that involve interaction of a number of fungal components with distinct brain cells. In this manuscript, our literature review confirmed the notion that the Cryptococcus field is expanding rapidly, but also suggested that studies on neuropathogenesis still represent a small fraction of basic research activity in the field. We therefore discussed anatomical and physiological aspects of the brain during infection by C. neoformans, in addition to mechanisms by which brain resident cells interact with the fungus. This review suggests that multiple efforts are necessary to improve the knowledge on how C. neoformans affects brain cells, in order to enable the generation of new therapeutic tools in a near future.

Cite as

COLOMBO, A.C., RODRIGUES, M.L., 2015. Fungal colonization of the brain: anatomopathological aspects of neurological cryptococcosis. An. Acad. Bras. Ciênc. https://doi.org/10.1590/0001-3765201520140704

Citations

Dopamine D2-Like Receptors Modulate Unconditioned Fear: Role of the Inferior Colliculus

2014 | de Oliveira, A.R., Colombo, A.C., Muthuraju, S., Almada, R.C., Brandão, M.L.

open-access PLoS ONE, doi:10.1371/journal.pone.0104228

Abstract

Background A reduction of dopamine release or D2 receptor blockade in the terminal fields of the mesolimbic system clearly reduces conditioned fear. Injections of haloperidol, a preferential D2 receptor antagonist, into the inferior colliculus (IC) enhance the processing of unconditioned aversive information. However, a clear characterization of the interplay of D2 receptors in the mediation of unconditioned and conditioned fear is still lacking. Methods The present study investigated the effects of intra-IC injections of the D2 receptor-selective antagonist sulpiride on behavior in the elevated plus maze (EPM), auditory-evoked potentials (AEPs) to loud sounds recorded from the IC, fear-potentiated startle (FPS), and conditioned freezing. Results Intra-IC injections of sulpiride caused clear proaversive effects in the EPM and enhanced AEPs induced by loud auditory stimuli. Intra-IC sulpiride administration did not affect FPS or conditioned freezing. Conclusions Dopamine D2-like receptors of the inferior colliculus play a role in the modulation of unconditioned aversive information but not in the fear-potentiated startle response.

Cite as

de Oliveira, A.R., Colombo, A.C., Muthuraju, S., Almada, R.C., Brandão, M.L., 2014. Dopamine D2-Like Receptors Modulate Unconditioned Fear: Role of the Inferior Colliculus. PLoS ONE. https://doi.org/10.1371/journal.pone.0104228

Citations

Dopaminergic mechanisms underlying catalepsy, fear and anxiety: Do they interact?

2013 | Colombo, A.C., de Oliveira, A.R., Reimer, A.E., Brandão, M.L.

Behavioural Brain Research, doi:10.1371/journal.pone.0104228

Abstract

Haloperidol is a dopamine D2 receptor antagonist that induces catalepsy when systemically administered to rodents. The haloperidol-induced catalepsy is a state of akinesia and rigidity very similar to that seen in Parkinson's disease. There exists great interest in knowing whether or not some degree of emotionality underlies catalepsy. If so, what kind of emotional distress would permeate such motor disturbance? This study is an attempt to shed some light on this issue through an analysis of ultrasound vocalizations (USVs) of 22 kHz, open-field test, and contextual conditioned fear in rats with some degree of catalepsy induced by haloperidol. Systemic administration of haloperidol caused catalepsy and decreased exploratory activity in the open-field. There was no difference in the emission of USVs between groups during the catalepsy or the exploratory behavior in the open-field test. In the contextual conditioned fear, when administered before training session, haloperidol did not change the emission of USVs or the freezing response. When administered before testing session, haloperidol enhanced the freezing response and decreased the emission of USVs on the test day. These findings suggest that the involvement of dopaminergic mechanisms in threatening situations depends on the nature of the aversive stimulus. Activation of D2 receptors occurs in the setting up of adaptive responses to conditioned fear stimuli so that these mechanisms seem to be important for the emission of 22 kHz USVs during the testing phase of the contextual conditioned fear, but not during the training session or the open-field test (unconditioned fear stimuli). Catalepsy, on the other hand, is the result of the blockage of D2 receptors in neural circuits associated to motor behavior that appears to be dissociated from those directly linked to dopamine-mediated neural mechanisms associated to fear.

Cite as

Colombo, A.C., de Oliveira, A.R., Reimer, A.E., Brandão, M.L., 2013. Dopaminergic mechanisms underlying catalepsy, fear and anxiety: Do they interact? Behavioural Brain Research. https://doi.org/10.1016/j.bbr.2013.10.002

Citations