ASD is a complex neurodevelopmental disorder with multifactorial etiology, characterized by the impairment of two main functional areas: (1) continuous communication and social interaction deficits, and (2) restrictive and repetitive behaviors and interests. The incidence among sexes is a male/female rate of 3:1 [1,2].

ASD diagnostic criteria are available in the Diagnostic and Statistical Manual of Mental Disorders-5 [3], describing persistent deficits in social communication and social interaction across multiple contexts, such as deficits in social–emotional reciprocity; nonverbal communicative behaviors; and developing, maintaining and understanding relationships. Moreover, ASD children present behavior restricted and repetitive patterns of interests or activities, as manifested by at least two of the following: (a) repetitive or stereotyped motor movements, use of objects or speech; (b) insistence on sameness, inflexible adherence to routines or ritualized patterns of verbal or nonverbal behavior; (c) fixated and restricted interests that are abnormal in intensity or focus; and (d) hyper- or hypo-reactivity to sensory input or unusual interest in sensory aspects of the environment. Such symptoms must be present in the early period of development, be generally evident at the age of 3 and cause significant clinical impairment of global functioning. In 2014 in the United States, the Centers for Disease Control (CDC) estimated 1 case out of 68 children of the age of 8 [4], and in 2018, the CDC reported an ASD prevalence rate of 1 in 44 or an incidence rate of 2.3% [5].

Considering the great geographical variability and the methodologic differences employed in prevalence studies, the actual prevalence of ASD is estimated to be higher than 2.5% in the United States and 1.5% in Denmark, Finland and Sweden. In Italy, the prevalence of children diagnosed with ASD is estimated to be 1 out of 77 among children between 9 and 17 years old, with a higher risk for the male sex; the number of male patients is four times higher than the number of female patients.

The disease is now defined as a complex disorder with multifactorial etiopathology because it seems to be determined by the contribution of many risk factors, such as genetics, epigenetics and environmental factors.

Much evidence supports genetic factors as the predominant cause of ASD. Emphasis on the genetic component from epidemiological data derives from familiarity and the high incidence of the autistic behavioral phenotype in the context of genetic diseases with well-known etiology. The amount of ASD cases with a genetic base represents 10–20% of the overall number of autistic patients. Concordance studies on twins have shown very suggestive data; the concordance among monozygotic twins has been shown to be variable from 70% to 90%, whereas that between dizygotic twins is between 0–10% [6]. Moreover, ASD incidence is estimated to be 2% among siblings, with a 100 times higher risk than the normal population (0.02%). Furthermore, the recurrence risk is significantly higher in families with a first diagnosis of ASD than it is in the normal population. In particular, families with a first child diagnosed with ASD have greater probabilities of having an autistic second child depending on the child’s sex, as follows: 15–25% if the child is male, and 5–15% if the child is female. Last, the presence of many first-grade relatives diagnosed with ASD testifies to the importance of the genetic hypothesis [7,8]. There are ASD forms that are similar to genetic syndromes, and these forms represent 10% of all ASD diagnoses. Beyond the findings of specific alterations that cause specific syndromes, genetic anomalies implied in ASD can be caused by mutations in one gene or in the total number of copy variations (CNVs). Besides specific genetic alterations that cause well-known clinical pictures, there are uncommon genetic variants (with a documented presence of less than 1% of the general population). These mutation sites are in correspondence with genes of great importance in the process of neurodevelopment, and the most documented are CNVs, such as microdeletion or microduplication; nonsense mutation with the insertion of a stop codon; and missense mutation with the creation of aberrant products, such as inactive proteins or proteins with reduced biological activity [9].

Some relevant examples include genes that code for synaptic transmembrane proteins, such us neuroligine 3 and 4 and neurexine 1 and 3, which are crucial for synaptic function; others are SHANK family genes (SHANK 1, 2, 3) that codify for proteins involved in synapsis formation and dendritic spine maturation. In detail, SHANK 3 is involved in dendritic development and in a pathway with reelin, a protein that is essential for the stabilization and the laminar organization of the cerebral cortex [10]. Even if the scientific community well accepts the role of genetic anomalies, many studies have shown similar associations with environmental risk factors.

A plethora of environmental risk factors have been taken into consideration, and most of them refer to the pre/peri-natal period because the maximum development of the central nervous system (CNS) is in this period. Risk factors that influence neurodevelopment and provoke long-term alterations in the brain’s physiology include pre-natal exposition to viral infections (e.g., Cytomegalovirus and Rubivirus); environmental toxic substances, such as pesticides, phthalates, solvents, environmental pollutants, and heavy metals; stress; alcohol intake; and diet [11]. An association between maternal conditions and ASD risk has been demonstrated.

The most common predisposing factors of ASD are neurodevelopment anomalies during the first and the second trimester of pre-natal life [12]. Other causes are less frequent but not completely negligible. Among these, cerebellar damage has been identified in the peri-natal period, which increases the risk of developing autism by 30 times. Neuropathology post-mortem studies on histological samples of CNS taken from autistic patients have shown the presence of cytoarchitectonic anomalies, which can involve various brain regions. Among these, reduced apoptosis and/or enhanced cellular proliferation (particularly evident in macrocephalic patients), neuronal migration alteration or anomalies in the process of cellular maturation and differentiation have been described [13]. From a functional point of view, neuropathological anomalies bring the formation of an atypical neural network characterized by reduced long-distance connectivity and exceeding local connectivity [14].

A bidirectional interaction between the gastrointestinal (GI) tract, gut microenvironment and CNS, called the ‘microbiota–gut–brain axis’, regulates intestinal and neurological homeostasis. An impairment of this complex system can promote, in the presence of other contributing factors, the pathogenesis of nervous-system-related diseases, such as ASD.

Enteric symptoms (including constipation, diarrhea, recurrent abdominal pain/bloating and gastroesophageal reflux) are frequent among ASD patients, who often present alterations in intestinal motility and dysfunction of the epithelial barrier.

2. Intestinal Permeability in ASD

3. Microbiota–Gut–Brain Axis Involvement in ASD