Principal pathogenetic components and biological endophenotypes in autism spectrum disorders

Sacco, Roberto; Curatolo, Paolo; Manzi, Barbara; Militerni, Roberto; Bravaccio, Carmela; Frolli, Alessandro; Lenti, C; Saccani, Monica; Elia, Maurizio; Reichelt, Karl L.; Pascucci, Tiziana; Puglisi-Allegra, Stefano; Persico, Antonio M.

doi:10.1002/aur.151

Cited by 89 publications

(105 citation statements)

References 47 publications

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“…Finally, neuroinflammation is also a frequent finding in postmortem brains of autistic individuals [64,65]. It may represent a nonspecific consequence of insufficient neurite pruning and abnormal wiring of neural networks, resulting in elevated oxidative stress (possibly a common feature shared by several neurodevelopmental disorders) [66], but it could also stem from a broader immune dysfunction which, together with gastrointestinal disturbances and recurrent infections, collectively qualifies ASD as a systemic disorder [67][68][69][70][71].…”

Section: Autism Spectrum Disorder: Clinical Traits Neuropsychologicamentioning

confidence: 99%

Endocannabinoid Signaling in Autism

et al. 2015

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Autism spectrum disorder (ASD) is a complex behavioral condition with onset during early childhood and a lifelong course in the vast majority of cases. To date, no behavioral, genetic, brain imaging, or electrophysiological test can specifically validate a clinical diagnosis of ASD. However, these medical procedures are often implemented in order to screen for syndromic forms of the disorder (i.e., autism comorbid with known medical conditions). In the last 25 years a good deal of information has been accumulated on the main components of the Bendocannabinoid (eCB) system^, a rather complex ensemble of lipid signals (Bendocannabinoids^), their target receptors, purported transporters, and metabolic enzymes. It has been clearly documented that eCB signaling plays a key role in many human health and disease conditions of the central nervous system, thus opening the avenue to the therapeutic exploitation of eCB-oriented drugs for the treatment of psychiatric, neurodegenerative, and neuroinflammatory disorders. Here we present a modern view of the eCB system, and alterations of its main components in human patients and animal models relevant to ASD. This review will thus provide a critical perspective necessary to explore the potential exploitation of distinct elements of eCB system as targets of innovative therapeutics against ASD.Key Words Autism spectrum disorder . endocannabinoid system . fragile X syndrome . metabolic regulation . reward system The Endocannabinoid SystemTwenty-five years after the cloning and expression of a complementary DNA that encoded a G protein-coupled receptor, named type-1 cannabinoid (CB 1 ) receptor [1], there is a good deal of information on the main components of the so-called Bendocannabinoid (eCB) system^, as well as on its role in controlling cannabinergic signaling in human health and disease [2][3][4]. Anandamide (AEA) and 2-arachidonoylglycerol (2-AG) are the most active eCBs as yet identified, although this family of bioactive lipids includes other arachidonic acid (AA) derivatives with cannabimimetic properties (i.e., noladin ether, virodhamine, N-arachidonoyldopamine, to name but a few). The classical dogma that eCBs are synthesized and released Bon demand^upon (patho)physiological stimuli has been recently revisited on the basis of unexpected evidence for intracellular reservoirs and transporters of eCBs. These new entities have been shown to drive intracellular trafficking of eCBs, adding a new dimension to the regulation of their biological activity [5]. To date, several metabolic routes have B. Chakrabarti, A. Persico and N. Battista are equal first authors.

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Section: Autism Spectrum Disorder: Clinical Traits Neuropsychologicamentioning

confidence: 99%

Endocannabinoid Signaling in Autism

et al. 2015

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“…Diagnostic screening procedures used to exclude syndromic forms have been previously described (Sacco et al, 2010). Briefly, patients fulfilling Diagnostic and Statistical Manual IV (DSM-IV) diagnostic criteria for Autistic Disorder, Asperger Disorder or PDDNOS were screened for nonsyndromic autism using MRI, EEG, audiometry, urinary aminoacid and organic acid measurements, cytogenetic and fragile-X testing.…”

Section: Patient Samplementioning

confidence: 99%

Urinaryp-cresol is elevated in young French children with autism spectrum disorder: a replication study

et al. 2014

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The aromatic compound p-cresol (4-methylphenol) has been found elevated in the urines of Italian autistic children up to 8 years of age. The present study aims at replicating these initial findings in an ethnically distinct sample and at extending them by measuring also the three components of urinary p-cresol, namely p-cresylsulfate, p-cresylglucuronate and free p-cresol. Total urinary p-cresol, p-cresylsulfate and p-cresylglucuronate were significantly elevated in 33 French autism spectrum disorder (ASD) cases compared with 33 sex-and age-matched controls (p50.05). This increase was limited to ASD children aged 8 years (p50.01), and not older (p ¼ 0.17). Urinary levels of p-cresol and p-cresylsulfate were associated with stereotypic, compulsive/repetitive behaviors (p50.05), although not with overall autism severity. These results confirm the elevation of urinary p-cresol in a sizable set of small autistic children and spur interest into biomarker roles for p-cresol and p-cresylsulfate in autism.

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“…In fact, macrocephaly (i.e., head circumference >97th percentile) has been consistently described in approximately 20% of autistic children [55,58,59], serotonin blood levels are elevated in 20%50% of autistic subjects [47], and increased urinary excretion rates of oligopeptides and multiple solutes is found in 20-60% of autistic patients, with significant interethnic differences [50,60,61]. The implementation of these endophenotypes in our studies is detailed in the following section.…”

Section: Endophenotypes In Autism Genetic Researchmentioning

confidence: 92%

“…We aim at refining our morphometric analysis in the future, by collecting photographs of each patient in frontal and lateral view by web-cam, and applying one of several available automated morphometric analysis methods to the face and the head [56,57,66,67]. Finally, we have designed a simple ad hoc questionnaire currently including 36 patient-and family-history variables [60], exploring the following areas:…”

Section: Our Roadmap: Methodological Issues and Strategiesmentioning

confidence: 99%

“…In another study we searched for basic mechanisms underlying ASD by analyzing the clinical variables present in our ad hoc questionnaire on data collected from 245 Italian patients [60]. We identified at least four principal components that could play a relevant role in the pathogenesis of this disease: (i) "sensory dysfunction and abnormalities in the sleep-wake rhythm", (ii) "immune system abnormality" also including medical complications during pregnancy and repeated spontaneous abortions; (iii) "cognitive/motor developmental delay", and (iv) "repetitive behaviour".…”

Section: Our Roadmap: Methodological Issues and Strategiesmentioning

confidence: 99%

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