Childhood infections and autism spectrum disorders and/or intellectual disability: a register-based cohort study

Childhood infections and autism spectrum disorders and/or intellectual disability: a register-based cohort study

To explore the associations between childhood infections and subsequent diagnoses of autism spectrum disorder (ASD), intellectual disability (ID), and their co-occurrence. The association between specialized care for any infection, defined by ICD-codes, and later ASD or ID was investigated in a regi...

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Bibliographic Details
Published in:Journal of neurodevelopmental disorders Vol. 14; no. 1; p. 12
Main Authors: Karlsson, Håkan, Sjöqvist, Hugo, Brynge, Martin, Gardner, Renee, Dalman, Christina
Format: Journal Article
Language:English
Published: England BioMed Central Ltd 13-02-2022
BioMed Central
BMC
Subjects:
Analysis
Autism
Autism spectrum disorders
Care and treatment
Cesarean section
Childhood
Children
Children & youth
Cohort analysis
Diagnosis
Diseases
Families & family life
Family income
Gestational age
Infection
Infections
Intellectual disabilities
Intellectual disability
Medical research
Medicin och hälsovetenskap
Medicine, Experimental
Mental disorders
Obstetrics
Regression analysis
Risk
Sensitivity analysis
Siblings
Socioeconomic factors
Survival analysis
Autism spectrum disorders
Infection
Risk
Intellectual disability
Childhood
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Summary:To explore the associations between childhood infections and subsequent diagnoses of autism spectrum disorder (ASD), intellectual disability (ID), and their co-occurrence. The association between specialized care for any infection, defined by ICD-codes, and later ASD or ID was investigated in a register-based cohort of 556,732 individuals born 1987-2010, resident in Stockholm County, followed from birth to their 18th birthday or December 31, 2016. We considered as potential confounders children's characteristics, family socioeconomic factors, obstetric complications, and parental histories of treatment for infection and psychiatric disorders in survival analyses with extended Cox regression models. Residual confounding by shared familial factors was addressed in sibling analyses using within-strata estimation in Cox regression models. Sensitivity analyses with the exclusion of congenital causes of ASD/ID and documented risk for infections were also performed. Crude estimates indicated that infections during childhood were associated with later ASD and ID with the largest risks observed for diagnoses involving ID. Inclusion of covariates, exclusion of congenital causes of ASD/ID from the population, and sibling comparisons highlighted the potential for confounding by both heritable and non-heritable factors, though risks remained in all adjusted models. In adjusted sibling comparisons, excluding congenital causes, infections were associated with later "ASD without ID" (HR 1.24, 95%CI 1.15-1.33), "ASD with ID" (1.57, 1.35-1.82), and "ID without ASD" (2.01, 1.76-2.28). Risks associated with infections varied by age at exposure and by age at diagnosis of ASD/ID. Infections during childhood may contribute to a later diagnosis of ID and ASD.
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ISSN:1866-1947
1866-1955
1866-1955
DOI:10.1186/s11689-022-09422-4