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Interagency Autism Coordinating Committee (IACC)
Autism Research Database
Project Element Element Description

Project Title

Project Title

Immune regulation and neurodevelopmental disorders

Principal Investigator

Principal Investigator

Ashwood, Paul

Description

Description

Autism Spectrum Disorders (ASD) are behaviorally defined by deficits incommunication, social reciprocity, and repetitive stereotypic behaviors. While genetic and environmentalfactors are likely contributors to these disorders, little is known about the pathophysiology in ASD. Many in vitrostudies, post-mortem brain studies and proteomic studies in plasma and cerebral spinal fluid have describedthe presence of increased immune activation in ASD, whilst clinical and epidemiological studies suggest thatthere is an increase in immune mediated conditions such as allergies, asthma and autoimmunity. Activation ofthese immune responses is more prominent in individuals with exacerbated behavioral impairments in ASD.We hypothesize that an underlying mechanism common to this diverse array of findings is the lack of immunecontrol or regulation that can lead to immune activation and inflammation. Our published data and preliminaryfindings suggest a lack of production of immune regulatory cytokines such as transforming growth factor beta 1(TGFβ1) and interleukin (IL)-10. Decreases in these factors were associated with worse behavioral outcomesand more co-morbidities in ASD. In animal models with face and construct validity to ASD decreases inCD4+FoxP3+ regulatory T cells (Tregs) were observed. However, no studies have yet to address the functionalcellular mechanisms of Tregs in ASD or their role in animal models of ASD. We will test the innovativehypothesis that a lack of cellular immune regulation by Tregs is a predictive risk factor for ASD diagnosis, andthat targeting immune control mechanisms can alleviate behavioral abnormalities. Parallel clinical andpreclinical experiments will be performed. The proposed studies will determine the Tregs cellular mechanisms ofimmune control in cord blood samples from children that later receive a diagnosis of ASD, and compare this tochildren with typical development (Aim #1). This proposal will directly assess specific cellular mechanisms forwhich there are novel therapeutic potential. One of these therapeutic approaches, adoptive transfer of Tregs, willbe utilized to rescue the behavioral impairments present in a preclinical mouse model that exhibits manyfeatures with relevance to ASD (Aim #2). The proposal will directly assess the relationship of immunedysregulation in ASD and behavior abnormalities. If successful, this research will validate thetransformative concept that ASD is, for some, a disorder due to defects in immune regulation and control byTregs, and will validate a novel mechanism for one of the most visible public health concerns of our time.

Funder

Funder

National Institutes of Health

Funding Country

Funding Country

United States

Fiscal Year Funding

Fiscal Year Funding

235500

Current Award Period

Current Award Period

2016-2018

Strategic Plan Question

Strategic Plan Question

Question 2: What is the Biology Underlying ASD?

Funder’s Project Link

Funder’s Project Link

NIH RePORTER Project Page Go to website disclaimer

Institution

Institution

University of California, Davis

Institute Location

Institute Location

United States

Project Number

Project Number

1R21HD086669-01A1

Government or Private

Government or Private

Government

History/Related Projects

History/Related Projects

N/A

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