Neuroinflammation in autism spectrum disorder: what do current studies show? A narrative review

Belous, Mihaela; Jelaga, Dorin; Caraman, N.; Nastas, Igor

dc.contributor.author	Belous, Mihaela
dc.contributor.author	Jelaga, Dorin
dc.contributor.author	Caraman, N.
dc.contributor.author	Nastas, Igor
dc.date.accessioned	2026-02-10T11:37:15Z
dc.date.available	2026-02-10T11:37:15Z
dc.date.issued	2025
dc.identifier.citation	BELOUS, Mihaela; Dorin JELAGA; N. CARAMAN and Igor NASTAS. Neuroinflammation in autism spectrum disorder: what do current studies show? A narrative review. In: Satellite Conference “New horizons in mental health” organized within the Anniversary Congress “80 Years of Innovation in Health and Medical Education” of Nicolae Testemițanu State University of Medicine and Pharmacy, 20-23 October 2025, Chisinau, Republic of Moldova. Abstract book/ presidents of the scientific committee: Emil Ceban, Jana Chihai. Chișinău: [s. n.], 2025, p. 55. ISBN 978-5-86654-547-6.	en_US
dc.identifier.isbn	978-5-86654-547-6
dc.identifier.uri	https://sanatatemintala.md/images/Abstract%20BOOK%202025.pdf
dc.identifier.uri	https://repository.usmf.md/handle/20.500.12710/32552
dc.description.abstract	Evidence increasingly implicates immune–brain interactions in autism spectrum disorder (ASD). This review synthesizes human and translational findings on neuroinflammation and its relevance to ASD heterogeneity and treatment prospects. Narrative review of post-mortem, cerebrospinal fluid (CSF), blood, neuroimaging, and animal literature examining glial activation, cytokine profiles, blood–brain barrier (BBB) integrity, and peripheral–central immune crosstalk in ASD. Post-mortem studies frequently report microglial and astroglial activation, altered complement signaling, and cytokine dysregulation in cortical and cerebellar regions. CSF and peripheral assays often demonstrate elevated pro-inflammatory mediators (e.g., IL-6, TNF-α), though effect sizes vary and subgroups exist. Positron emission tomography using TSPO ligands shows mixed results, reflecting methodological limits (ligand affinity polymorphisms, age/sex effects) and biological heterogeneity. Genomic and transcriptomic data suggest immune-related pathways in subsets of individuals with ASD, while maternal immune activation models recapitulate ASD-like behaviors and microglial priming, underscoring developmental timing. Emerging work links gut dysbiosis and epithelial permeability to peripheral immune activation and possible BBB effects, but causality remains unresolved. Clinically, immune signatures correlate with symptom severity in some cohorts; however, anti-inflammatory or microglia-modulating interventions (e.g., minocycline, ibudilast, omega-3s) yield inconsistent, small-sample benefits and lack robust biomarkers to guide selection. Overall, convergent evidence supports context-dependent neuroinflammation in ASD—not universal, but salient in biologically defined subtypes. Priorities include longitudinal, multimodal studies (peripheral + CSF + imaging), stratification by age/sex/comorbidity, and development of validated inflammatory endophenotypes to enable targeted trials.	en_US
dc.language.iso	en	en_US
dc.publisher	Universitatea de Stat de Medicină și Farmacie "Nicolae Testemiţanu" din Republica Moldova, Ministerul Sănătăţii al Republicii Moldova	en_US
dc.relation.ispartof	Satellite Conference “New horizons in mental health” organized within the Anniversary Congress “80 Years of Innovation in Health and Medical Education” of Nicolae Testemițanu State University of Medicine and Pharmacy, 20-23 October 2025, Chisinau, Republic of Moldova	en_US
dc.title	Neuroinflammation in autism spectrum disorder: what do current studies show? A narrative review	en_US
dc.type	Other	en_US