The neural pathway represents the main and fastest communication route between the gut and the brain, between the ENS and the VN, as well as in the modulation of neuronal activity by microbial metabolites [15].

As the tenth cranial nerve, the VN supplies intestinal innervation through its celiac and hepatic branches. It transmits afferent signals from the GI tract to the vagal nuclei in the brainstem, modulating both limbic and cortical centers [40]. The branches of the VN have sensory properties in their afferent area, representing 80% of the fibers originating in the nodosum ganglion. In contrast, motor properties in 20% of its fibers originate from the dorsal motor nucleus of the VN [40, 87]. Furthermore, it influences neural pathways that modulate emotions, mood, and cognitive functions [88].

Currently, the VN has been distinguished as a mechanosensor that not only detects mechanical stimuli through ion channels such as ASIC, TRP, and PIEZO, but also differentiates pharmacological and hormonal changes at enteric levels [40, 88]. Additionally, its nerve endings and sensory cells, called “neuropods”, have the capacity to detect metabolites and GM that significantly influence VN actions [88]. The GM has essential functions at the intestinal level, such as maintaining pH, controlling peristalsis, nourishing epithelial cells, providing digestive enzymes and vitamins, and regulating the excitability of nerve endings that affect immune and endocrine pathways related to the CNS [40, 88]. It is worth mentioning that the VN does not have direct contact with the GM. It communicates through epithelial cells that transmit luminal signals, diffusion of compounds, and bacterial metabolites; so neuroendocrine cells are a primary component for the chemosensitivity interface [89].

The immunological pathway actively participates in the intestinal barrier, not only as a static barrier but also as a dynamic one that responds to both internal and external stimuli [90]. It is composed of the intestinal mucosal epithelium, an outer mucosal layer with commensal microbiota, antimicrobial proteins, secretory immunoglobulin A molecules, a middle layer with specialized epithelial cells, and an inner lamina propria where the immune system is located, populated by innate cells such as dendritic cells and macrophages, as well as cells of the adaptive response such as T and B cells [90, 91]. Moreover, dysbiosis causes an exacerbated increase in harmful lipopolysaccharide (LPS)-forming bacteria, and because it directly affects the intestinal barrier, the gut becomes significantly more permeable, facilitating the translocation of pathogens into the bloodstream [15, 40]. This leads to a systemic inflammatory response mediated by the intestines’ lymphoid tissue in relation to GM, integrating neuro-inflammatory processes influenced by inflammatory cytokines such as IL-1β, IL-6, TNF-α and IFN-γ that cross both the intestinal barrier and the BBB, generating damage to resident microglia of the CNS and promoting neuroinflammation by activating TLR4 and the nuclear factor kappa B pathway [88].

The interaction between hormonal pathways and neuronal signals represented by the VN is fundamental for bidirectional communication of the MGBA [73].

Although its nerve endings do not maintain direct contact with the GM or the luminal contents, the VN detects intestinal chemical changes indirectly through enteroendocrine cells (EECs). These cells represent approximately 1% of the intestinal epithelium and function as chemo sensors capable of identifying GM-derived metabolites, particularly SCFAs [21, 74, 89].

Upon activation, EECs release mediators such as cholecystokinin, glucagon-like peptide-1, and 5-HT, whose intestinal synthesis depends on microbial metabolites [21, 89]. Likewise, 5-HT acts on 5-HT3 receptors present on vagal afferent fibers, allowing rapid communication with brain circuits related to autonomic, emotional, and cognitive regulation [89].

Another key group of metabolites that modulate EECs and VN activity is derived from tryptophan metabolism. Reducing circulating tryptophan levels in the GM, it affects serotonergic neurotransmission, which impacts the functioning of both the CNS and the ENS [38, 92].

ASD refers to a group of early-onset difficulties in social communication accompanied by repetitive sensory and motor patterns of behavior, which stem from a substantial genetic contribution along with additional contributing factors [109]. In ASD, GWAS have identified genes involved in synaptic signaling, neuronal development, and intercellular communication [110]. Interestingly, several of these genes, such as CNTNAP2, SHANK3, and NLGN4, also regulate intestinal functions and interaction with the microbiota [111, 112].

It is well known that patients diagnosed with ASD have alterations in their GM, characterized by dysbiosis, reduced microbial diversity, and elevated markers such as calprotectin and lactoferrin. These findings suggest the presence of persistent intestinal inflammation and altered immune pathways that simultaneously impact the GI system and neurodevelopment [18, 19]. Several systematic reviews and meta-analyses have evaluated the association between IBD and ASD, finding a higher prevalence of Crohn’s disease and ulcerative colitis in people with ASD, reinforcing the possibility of shared immunogenetic susceptibility [113, 114].

Previous data have served as the basis for establishing a bidirectional relationship between the microbiome and ASD, which has enabled the development of subsequent studies using Mendelian randomization (MR) to investigate genetic causality. These analyses have highlighted the role of intestinal permeability and interaction with immune genes, positioning dysbiosis as a modulator of genetic pathways relevant to neurodevelopment in ASD [115]. Along these lines, Yang et al. (2025) [116] combined GWAS and MR analyses, identifying a genetic overlap between loci associated with microbiota and immunity and loci at risk for ASD, demonstrating a shared genetic-microbial architecture. Complementarily, Hetta et al. (2025) [115] reviewed evidence of the GBA by integrating genetic data from ASD, highlighting genes linked to immunity, metabolism, and intestinal barrier function, suggesting common mediating mechanisms. This approach has been corroborated by Li et al. (2023) [117], who, using single nucleotide polymorphisms (SNPs) derived from GWAS consortia in MR analyses, demonstrated a bidirectional relationship between microbiota and ASD.

Epilepsy is characterized as a chronic neurological disorder that affects more than 70 million people worldwide. Its pathophysiology is complex, and 60% of cases are idiopathic [118]. Moreover, it has been demonstrated that patients diagnosed with epilepsy have GI symptoms, and patients with IBD are more susceptible to developing epilepsy, indicating a relationship between epilepsy and the gut. Ding et al. (2021) [119] reported that patients with epilepsy have an altered microbiota composition that promotes neuroimmunity and neuroinflammation.

A GWAS meta-analysis conducted by the International League Against Epilepsy reported that 26 risk loci for the development of epilepsy were found. The results of the analysis revealed that the most relevant variants are located in genes involved in neuronal synapses, and enriched genes expressed in inhibitory and excitatory neurons were found. The study, therefore, highlighted that the CACNA2D2 gene, which encodes the calcium channel subunit, is related to the risk of presenting epilepsy [106]. Likewise, a systematic review conducted by Jacobs et al. (2025) [120] aimed at identifying risk variants for epilepsy reported that 79 SNPs located in 64 genes were found to be associated with epilepsy. The most associated genes were SCN1A, which encodes the sodium channel subunit in neurons, which is essential for action potential. Other variants observed in the Asian population were rs2292096 and rs149212747, which were associated with epileptic status and focal epilepsy [120]. Moreover, Zhang et al. (2024) [121] identified genes that are related to the risk of developing epilepsy and reported 1,506 genes, classifying them according to their potential association with the development of the disease, highlighting SCN1A. Another associated gene is STXBP1, which is even related to encephalopathy, and the BCOR and APC2 genes [121]. Another gene associated with the development of focal epilepsy is PROX1, which encodes transcription factors and plays a role in nerve cell maturation [122]. Finally, a study conducted by Thakran demonstrated 30 variants in seven loci associated with the risk of developing epilepsy. The related loci were rs17031055/4q31.3 (DCHS2), rs9322462/6q25.2 (CNKSR3), rs73182224/3q27.2 (DGKG), rs2938010/10q26.13 (CTBP2), rs11652575/17p11.2 (SLC5A10), and rs75328617/8q24.23 (RNU1-35P) [123, 124].

SCZ is a psychiatric syndrome marked by psychotic features like hallucinations, delirium, and deorganized speech, as well as cognitive impairments affecting executive function, memory, and processing speed, which are common in this pathology [125]. Heritable factors could explain almost 80% of the risk of SCZ in the population; however, only a small part of this component has been demonstrated to be attributable to common disease-associated single-nucleotide variants [126].

GWAS and gene expression profiling have identified multiple genes that implicate immune-related pathways, inflammatory processes, cytoskeletal development, and synaptic function; a few of them have also been reported in IBD, particularly in regions that encode genes of the major histocompatibility complex and modulators of the intestinal immune response [127].

Thanks to large-scale GWAS studies, it has been possible to identify more than 270 loci associated with SCZ, including GRIN2A, DRD2, and MHC genes. These findings have served as the basis for identifying overlaps with GI disorders [93, 128]. Key findings include genes related to neurodevelopment and immune regulation, with common SNPs highlighting immune functions associated with GI disorders [129].

Nikolova et al. (2021) [19] reviewed the evidence on microbiota alterations in psychiatric disorders, including SCZ, noting that microbial changes may influence immune pathways and intestinal permeability linked to genetic risk factors.

There is currently evidence of a shared genetic etiology, mediated by immune mechanisms, between GI diseases and SCZ. This has been demonstrated through cross-GWAS and MR analyses, identifying overlaps of SNPs in the major histocompatibility complex, IL23R, and Th17 pathways [45]. For their part, Xie et al. (2024) [20] performed integrated GWAS analyses showing that SCZ shares multiple loci with GI disorders, identifying immune and dopaminergic genes that link GI and psychiatric phenotypes. Shared transcriptional mechanisms between inflammation and neuropsychiatric vulnerability have also been proposed. This was demonstrated by TWAS by the Uellendahl-Werth et al. (2022) [130] group, who identified genes such as PTPN22, ATG16L1, and HLA-DQA1, expressed in both the intestines and the brain. Similarly, Wang et al. (2024) [127] showed through genetic cross-analysis that SCZ and IBD share loci such as IL23R, STAT3, and TNFSF15, suggesting pleiotropy and possible bidirectional causal effects. This bidirectional causality between IBD and SCZ was also demonstrated by Qian et al. (2022) [131], who identified the involvement of IL23/Th17 and MHC genes through MR, proposing that immune dysregulation may affect both systems [131] (Table 1).

Although this section summarizes evidence linking alterations in the gut microbiome with GI disorders and psychiatric phenotypes, these associations should be interpreted with caution. The reported relationships are primarily correlational and do not necessarily indicate direct causal mechanisms, as they may be influenced by multiple confounding factors, including dietary patterns, medication exposure, disease chronicity, psychosocial context, and population heterogeneity across the studied cohorts.

Moreover, GWAS and MR analyses offer valuable insights into potential causal pathways; however, they are subject to important limitations, such as the risk of horizontal pleiotropy and the limited generalizability of findings, given that a substantial proportion of studies have been conducted in predominantly European or Asian populations. Consequently, these results should be regarded as hypothesis-generating rather than conclusive evidence, underscoring the need for replication in more diverse populations and for longitudinal study designs to better elucidate the complexity of these interactions.

Over the past few years, multiple studies have demonstrated reproducible alterations in the composition of the GM in patients with ASD compared to neurotypical subjects. In a systematic review, Ding et al. (2017) [135] reported that most studies agree on a reduction of microorganisms such as Bifidobacterium and Prevotella, but an increase in Clostridium spp., Desulfovibrio, and Bacteroides in children with ASD. This suggests a pattern of intestinal dysbiosis and the activation of low-grade inflammatory processes, mechanisms that may contribute to alterations in the GBA. It was also noted that SCFAs, particularly propionic acid, play a key role in modulating neuronal gene expression [135].

In a study conducted by Wang et al. (2012) [136], 23 children with ASD were compared with 31 controls. Total fecal SCFA levels were significantly higher in ASD patients (136.6 ± 8.7 mmol/kg) than in controls (111.1 ± 6.6 mmol/kg; p < 0.05). Furthermore, propionic acid has been shown to modulate the expression of the tyrosine hydroxylase gene via the transcription factor CREB, suggesting an epigenetic mechanism through which SCFAs may influence monoaminergic neurotransmitter pathways such as dopamine (DA) and 5-HT [136].

Similarly, Kang et al. (2017) [137] conducted a clinical trial involving 18 children with ASD who received FMT for eight weeks, followed by an additional eight-week follow-up period. Using 16S rRNA sequencing, a reduced microbial diversity was initially observed in ASD patients compared to neurotypical children. The results revealed an abundance of Desulfovibrio and Sutterella and a significant decrease in Bifidobacterium. However, after FMT intervention, normalization of the microbial profile was reported, with an increase in Bifidobacterium and Prevotella, and a reduction in Desulfovibrio and Sutterella. Moreover, microbial changes correlated with significant clinical improvements in GI symptoms, including a reduction in constipation, diarrhea, and abdominal pain. These modifications were also associated with improvements in ASD behavioral scales, specifically the Childhood Autism Rating Scale and the Social Responsiveness Scale, both of which decreased by approximately 10% at the end of treatment. This suggests that changes in the GM occurred concomitantly with reductions in behavioral symptoms [137].

In the same line, Lewandowska-Pietruszka et al. (2023) [138] analyzed 44 studies on the composition and function of the GM in children with ASD. Specifically, Adams et al. (2011) [139], De Angelis et al. (2013) [140], Wang et al. (2012) [40], Liu et al. (2019) [141], and He et al. (2023) [142] reported an increase in Firmicutes ranging from approximately 36–81%, as well as Pseudomonadota around 78%, and a decrease in Bacteroidetes to about 56%. Consequently, the Bacteroidetes:Firmicutes (B:F) ratio tends to be around 56% compared with controls [40, 138–142]. These findings were associated with GI symptoms and more severe behavioral scores in several studies [138]. Moreover, the review highlighted that up to 70% of children with ASD reported GI symptoms, supporting a close clinical interaction between dysbiosis and somatic manifestations of the disorder. Additionally, the review presents heterogeneous but consistent evidence regarding alterations in microbial metabolites relevant to the GBA. Several primary studies, including Kang et al. (2018) [143], De Angelis et al. (2013) [140], and He et al. (2023) [142], showed changes in SCFAs profiles and tryptophan metabolites, with reported variations in propionate, butyrate, and acetate that correlated with behavioral parameters in some cohorts.

Collectively, these studies support that ASD is associated with a reproducible intestinal dysbiosis characterized by an increase in Firmicutes, particularly Clostridium spp., Desulfovibrio, and Sutterella, along with a decrease in Bacteroidetes, Bifidobacterium, and Prevotella [135, 138, 141–142]. These microbial shifts correlate with alterations in microbial metabolites, particularly propionate and butyrate, that modulate epigenetic and neurotransmitter pathways such as DA and 5-HT, in addition to influencing intestinal inflammation and epithelial permeability [136, 138, 143, 144]. In summary, the evidence supports a functional role of the GM in the GBA of ASD, although longitudinal studies are required to confirm causality and therapeutic potential [137, 138].

Unlike predominantly psychiatric disorders such as ASD, epilepsy is a neurological condition in which alterations of the GM have gained increasing relevance due to their potential influence on neuronal excitability and therapeutic response [49]. In recent years, interest in understanding this interaction has grown in both pediatric and adult populations [102]. Key lines of research include the role of the microbiota in drug-resistant epilepsy (DRE) and the microbial changes induced by the ketogenic diet (KD), which are considered potential mediators because of their anticonvulsant effects [102].

Although intestinal dysbiosis has been proposed to contribute to the pathophysiology of epilepsy through mechanisms of the GBA, the exact processes remain incompletely understood [49, 102, 145]. This microbial ecosystem plays an active role in immune modulation and inflammatory processes and produces multiple neurotransmitters involved in bidirectional communication with the CNS [21, 22]. These functions suggest that alterations in bacterial composition may influence neuronal excitability and, consequently, seizure threshold.

Various gut bacteria are capable of synthesizing neurotransmitters relevant to brain activity [21, 22, 102, 119]. Certain Bacillus species produce DA and norepinephrine (NE); Bifidobacterium generates GABA; Enterococcus and Streptococcus synthesize 5-HT; and Escherichia coli can produce both NE and 5-HT [49]. Given that epilepsy is characterized by an imbalance between GABAergic inhibition and glutamatergic excitation, these bacterial metabolites may play a key modulatory role in its pathophysiology [102].

De Caro et al. (2019) [146] explored the relationship between intestinal inflammation and epilepsy in a murine model. The authors induced colitis using dextran sodium sulfate in CD1 mice and observed that GI inflammation increased susceptibility to picrotoxin-induced seizures and reduced the anticonvulsant efficacy of drugs such as phenobarbital, valproate, carbamazepine, and phenytoin. Anti-inflammatory treatment partially reversed these effects, suggesting that intestinal inflammation enhances neuronal excitability and alters the response to antiepileptic drugs, reinforcing the functional link between GM and epilepsy [146].

Reproducible differences in the composition of the GM of patients with epilepsy have been described when compared with healthy controls [119]. Likewise, variations have been reported between the microbiota of pediatric and adult patients, as well as between those with DRE, leading to the proposal of differentiated dietary strategies [147]. In children with DRE, Xie et al. (2017) [148] reported reduced microbial diversity and a predominance of Firmicutes and Actinobacteria, along with a decrease in Bacteroidetes and Proteobacteria, suggesting a characteristic dysbiotic profile associated with the disease.

Several studies have identified alterations in the GM in epilepsy, generally characterized by reduced microbial diversity and dysbiosis compared with healthy controls [119, 149, 150]. Both studies reported decreased alpha diversity in patients with epilepsy, as well as increases in Actinobacteria and shifts in genera such as Blautia, Subdoligranulum, and Bifidobacterium, particularly associated with DRE [149, 150]. However, heterogeneous results were observed in other taxonomic variations: Gong et al. (2020) [150] reported an increase in Verrucomicrobia and a reduction in Proteobacteria, whereas Cui et al. (2022) [149] found higher abundance of Proteobacteria and Escherichia-Shigella in patients. Although these findings do not define a unique microbial signature, they collectively support the presence of an altered microbiota profile associated with epilepsy, particularly in DRE.

Conventional therapy for epilepsy relies on the use of antiepileptic drugs; however, around 30% of patients do not achieve adequate seizure control, a condition known as DRE [49, 50]. In these cases, it becomes essential to explore alternative or complementary treatments that may improve therapeutic response. Several studies suggest that DRE may be associated with alterations in the GM. Peng et al. (2018) [51] observed that patients with DRE who experienced four or fewer seizures per year showed a greater abundance of Bifidobacterium and Lactobacillus compared with those with more frequent seizures, suggesting that dysbiosis may contribute to the maintenance of neuronal hyperexcitability and pharmacoresistance.

Among the most promising non-pharmacological approaches is the KD, characterized by a high proportion of lipids, low carbohydrate content, and adequate protein intake [151–153]. This diet induces a state of ketosis with low glucose levels and elevated fatty acids and ketone bodies, which have been linked to antiepileptic and neuroprotective effects by enhancing neuronal energy efficiency and modulating inhibitory neurotransmission [152, 153]. Traditionally, the KD has been used in pediatric patients with refractory epilepsy, where it has shown significant clinical benefits. Martin-McGill et al. (2020) [151] reported that children treated with the KD exhibited up to three times less epileptic activity and were six times more likely to achieve ≥ 50% seizure reduction compared with those on conventional diets.

The therapeutic effect of the KD may be mediated, at least in part, by changes in the GM. Xie et al. (2017) [148] demonstrated that after one week of KD intervention, there was a relative increase in Bacteroides, Prevotella, and Bifidobacterium, along with a decrease in Firmicutes and partial normalization of the B:F ratio. These changes correlated with a ≥ 50% reduction in seizure frequency in 64% of patients [148].

Taken together, current evidence indicates that epilepsy, particularly DRE, is associated with gut dysbiosis characterized by reduced bacterial diversity and a B:F imbalance, which may contribute to both epileptogenesis and pharmacoresistance [102, 119, 146, 148]. This imbalance promotes a pro-inflammatory state and alterations in neurotransmitters such as GABA and 5-HT, fostering neuronal hyperexcitability [21, 22]. In this context, the KD has shown beneficial effects by remodeling the microbiota, increasing Bacteroides, Prevotella, and Bifidobacterium, and normalizing the B:F ratio, changes associated with significant seizure reduction [148, 151]. These findings strengthen the role of the GBA as a key component in the pathophysiology and management of epilepsy and DRE.

Analogous to ASD and epilepsy, SCZ has emerged as another neuropsychiatric condition in which the GM plays a relevant modulatory role. Over the past few years, metagenomic and metabolomic studies have demonstrated consistent alterations in the bacterial composition and microbial diversity of patients with SCZ, including a reduction of butyrate-producing bacteria and an increase in pro-inflammatory genera, suggesting a functionally active dysbiosis within the GBA [154].

In this context, a recent meta-analysis by Murray et al. (2023) [155] examined 10 studies including more than 1,200 participants and found that patients with SCZ exhibited a significant reduction in microbial alpha diversity (p < 0.001) and an altered B:F ratio, together with an increase in the phyla Proteobacteria and Actinobacteria. These changes reflect a pro-inflammatory and metabolically dysfunctional microbial state. The study highlighted the decrease of microbial metabolic pathways associated with butyrate synthesis, along with an increase in pathways producing propionic acid and succinate. At the genus level, Lactobacillus, Prevotella, Akkermansia, Clostridium, and Bacteroides were increased, while Faecalibacterium, Roseburia, and Coprococcus (butyrate-producing bacteria) were markedly decreased [155].

Complementarily, in a metagenomic study including 171 individuals (90 unmedicated patients and 81 controls), Zhu et al. (2020) [156] identified a significant increase in Akkermansia muciniphila, Bacteroides plebeius, and Clostridium symbiosum (p < 0.01) in SCZ patients. These species, which are involved in intestinal mucin degradation, were associated with increased epithelial permeability and LPS translocation-processes capable of activating microglia and inducing neuroinflammation. Moreover, the authors reported a reduction of Faecalibacterium prausnitzii, negatively correlated with plasma IL-6 levels, supporting the link between loss of butyrate-producing bacteria and systemic inflammation [156].

In another study, Li et al. (2020) [157] analyzed the GM of 90 patients with SCZ and 69 controls using 16S rRNA sequencing. They observed an increase of Prevotella copri and Lactobacillus fermentum in individuals with greater clinical severity according to the Positive and Negative Syndrome Scale. Correlations between these genera and negative and cognitive symptoms were r = 0.42 and r = 0.39, respectively (p < 0.05). The authors concluded that Prevotella, through the production of succinate and other intermediates of the tricarboxylic acid cycle, may contribute to neuronal mitochondrial dysfunction and altered cerebral energy metabolism described in SCZ [157].

Consistently, Deng et al. (2022) [23] in a cohort of 92 patients and 81 controls, confirmed a significant decrease of Faecalibacterium and Roseburia (p < 0.001), along with elevated Escherichia-Shigella and Ruminococcus gnavus. The loss of butyrate-producing bacteria was associated with higher levels of C-reactive protein and IL-6, and showed a negative correlation with total Negative Syndrome Scale score (r = −0.41, p < 0.001). This pattern supports the hypothesis that intestinal dysbiosis contributes to systemic inflammation and neuroimmune dysfunction in SCZ [23].

Similarly, Li et al. (2024) [24] integrated metagenomic and metabolomic analyses in 53 patients with SCZ and 57 controls, identifying an increase in Bacteroides and Alistipes (propionate-producing species) and a reduction in Coprococcus and Ruminococcus bromii (butyrate-producing species). Fecal levels of butyrate and isobutyrate were 35% lower in patients (p < 0.001), correlating with greater clinical severity (r = −0.46) and higher plasma IL-1β levels [24].

In summary, recent evidence confirms that SCZ is associated with intestinal dysbiosis characterized by reduced microbial diversity and a marked decrease in butyrate-producing bacteria such as Faecalibacterium, Roseburia, and Coprococcus [154, 155]. These alterations are accompanied by an increase in pro-inflammatory genera such as Prevotella, Lactobacillus, and Akkermansia, promoting a systemic inflammatory and metabolically dysfunctional state []. This state is reflected in elevated IL-6 and IL-1β levels, correlating with greater clinical severity and negative or cognitive symptoms [24, 157]. Finally, the decrease in SCFAs, especially butyrate, contributes to the dysfunction of the GBA and the neuroimmune impairment observed in this disorder [154, 155] (Table 2).

During childhood and adolescence, microbial alterations appear to exert a more profound impact on intestinal permeability, immune activation, and the production of neuroactive metabolites (such as SCFAs) [158, 159]. Pediatric patients with ASD or epilepsy exhibit a more unstable microbiota due to reduced bacterial diversity. In contrast, in SCZ, MGBA alterations appear to be influenced predominantly by chronic inflammation, metabolic status, lifestyle factors, and disease duration [160].

Sex-related differences have been demonstrated and are mediated by sex hormones, which modulate Th1, Th2, and Th17 lymphocyte expression as well as the composition of the GM. These effects alter intestinal permeability, SCFA production, and systemic inflammatory signaling toward the CNS [158, 161].

Low fiber intake and diets high in saturated fats or ultra-processed foods are associated with reduced microbial diversity, decreased abundance of butyrate-producing bacteria, and a pro-inflammatory state. In contrast, fiber-rich diets promote SCFA production, which has been associated with neuroprotective effects [162, 163].

Sustained activation of the HPA axis alters intestinal permeability through cortisol-mediated mechanisms, reinforcing a bidirectional cycle between dysbiosis, inflammation, and symptom exacerbation [158].

Psychotropic medications act as direct modulators of the MGBA by altering the composition and function of the GM. Antipsychotics, antiepileptics, and antidepressants reduce alpha diversity, decrease butyrate-producing bacteria, and promote the expansion of pro-inflammatory taxa (e.g., Proteobacteria) [160, 164, 165].

We concluded that MGBA alterations in ASD, epilepsy, and SCZ do not represent static or uniform biological states, but rather dynamic phenomena profoundly modulated by age, sex, diet, stress, comorbidities, genetic burden, pharmacological exposure, and the clinical course of the disease. This heterogeneity likely explains the variability observed in clinical presentation, therapeutic response, and prognosis across these disorders.

Probiotics are defined as live microorganisms that have a beneficial impact on the host. They are mainly composed of Bifidobacterium and lactic acid-producing bacteria. The metabolites synthesised by probiotics are key mediators in diet-induced host-microbe interactions, and can exert anti-oxidant and anti-inflammatory effects [16]. Prebiotics are termed as nonviable food components that can also regulate GM as an alternative to probiotic supplementation. They are mainly composed of oligosaccharides and fermented fibers, and have also shown positive effects on certain neurological disorders [53]. The stimulation of probiotic bacteria by prebiotics increases the production of can reverse the effects of dysbiosis and chronic stress; thus, they may be an effective treatment for neurological conditions [166].

Psychobiotics, defined as live microorganisms that, when administered in adequate amounts, confer mental health benefits through modulation of the GBA, have demonstrated potential in preclinical and early clinical studies in ASD and SCZ. These agents may influence neurotransmitter synthesis, immune signaling, and regulation of the HPA axis, with reported effects on clinical symptoms and inflammatory markers in these populations [58, 59, 167]. In ASD, psychobiotic interventions have been associated with favorable shifts in GM composition and increased production of neuroactive metabolites, including SCFAs and serotonin, both of which play key roles in neurodevelopmental processes. In addition, patients with ASD have been associated with altered levels of Bacteroides, Firmicutes, Prevoltella and Clostridium. These alterations can all be managed with the administration of psychobiotics [59, 60, 168]. In SCZ, psychobiotics and related probiotic formulations have shown potential to mitigate neuroinflammation and cognitive dysfunction; however, the clinical evidence remains constrained by small sample sizes and substantial methodological heterogeneity [169].

Synbiotics, combinations of probiotics and prebiotics, have been specifically studied in ASD. In vitro data suggest that synbiotics containing Limosilactobacillus fermentum K73 can shift the GM toward increased abundance of beneficial genera and enhance production of butyric acid and microbial serotonin, while reducing propionic acid, changes considered favorable in ASD pathophysiology [60]. These findings support the rationale for symbiotic interventions as adjunctive strategies in ASD and SCZ. However, the current evidence on the use of synbiotics is inconsistent, given that the formulations of the administered compound, the dosages, the lengths of treatment, the evaluation tools, and the method of administration are variable [170]. More research is warranted to fully uncover the benefits of this therapeutic option in all neuropsychiatric conditions.

Postbiotics, non-viable microbial products or metabolites, are emerging as a safer and more stable alternative to live probiotics, with anti-inflammatory and antioxidant properties. In SCZ, postbiotics such as SCFAs have been proposed to modulate neuroinflammation and BBB integrity, but clinical data are preliminary and largely extrapolated from mechanistic studies [59, 169].

Paraprobiotics, inactivated microbial cells, are not specifically addressed in the current medical literature relevant to ASD, epilepsy, or SCZ, and their role remains speculative.

Bacteriocins, antimicrobial peptides produced by bacteria, are not recognized as established therapeutic agents for GBA modulation in ASD, epilepsy, or SCZ in the current literature. Their mention in this context is not supported by clinical or translational studies in the referenced sources [59, 169].

For epilepsy, the reviewed medical literature does not provide direct evidence regarding the use of psychobiotics, postbiotics, synbiotics, paraprobiotics, or bacteriocins for GBA modulation or symptom management. In summary, psychobiotics and synbiotics have the most evidence for potential benefit in ASD and SCZ, primarily through modulation of GM, neuroactive metabolites, and immune signaling [58–60, 167–169]. Postbiotics represent a promising area for future research, particularly in SCZ. Paraprobiotics and bacteriocins are not established interventions for these indications. Across all categories, the field is limited by small sample sizes, inconsistent methodologies, and a lack of large-scale, long term clinical trials, highlighting the need for further research to clarify efficacy, safety, and mechanistic pathways [58, 59, 169, 171].

FMT is defined as a procedure involving the transfer of minimally handled fecal material from healthy donors to the gut of a recipient, and can be administered by a colonoscope, as an enema, as a nasogastric or nasoduodenal tube [172]. Also, for preoperative preparation, patients generally receive high-volume bowel cleansing regardless of the administration route. Moreover, some protocols additionally administer GI motility inhibitors to improve the retention of fecal microbiota in the receptor [173]. This process is intended to correct microbiota-related imbalances and associated diseases [174]. In today’s medicine, FMT has been investigated as a therapeutic approach for a range of communicable and noncommunicable diseases, with growing interest in recent years in its potential application to neurological and psychiatric disorders such as SCZ, epilepsy and ASD [61–63].

As it has been previously mentioned, VN is the main neural pathway of the MGBA. Its endings can detect gut microorganisms and their metabolites, subsequently conveying this information to the CNS [88]. For decades, vagal activity has been linked to complex behaviors such as attention, motion, emotion, and communication due to its connection to the prefrontal cortex and amygdala [64]. Vagus nerve stimulation (VNS) is a technique that uses electrical impulses to stimulate the VN, it requires surgical implantation of a bipolar electrode around the left cervical nerve and a pulse generator under the skin of the left chest. In this context, Steenbergen et al. (2021) [64] reported that VNS, applied via a mild electrical stimulus to the auricular branch of the VN, improved the recognition of specific emotions. These results strengthen the notion that VNS may serve as a therapeutic strategy to enhance social functioning in neurological disorders [64]. Its main side effects include surgical complications, dyspnea, paresthesias, headache, pharyngitis, pain, cough, or hoarseness [181].