Elevated protein concentrations in newborn blood and the risks of autism spectrum disorder, and of social impairment, at age 10 years among infants born before the 28th week of gestation

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作者
Steven J. Korzeniewski
Elizabeth N. Allred
T. Michael O’Shea
Alan Leviton
Karl C. K. Kuban
机构
[1] Wayne State University School of Medicine,Department of Obstetrics and Gynecology
[2] Boston Children’s Hospital,Departments of Neurology
[3] and Harvard Medical School,Department of Pediatrics
[4] University of North Carolina,Departments of Pediatrics
[5] Boston Medical Center and Boston University,undefined
[6] Children’s Hospital,undefined
[7] Baystate Medical Center,undefined
[8] Beth Israel Deaconess Medical Center,undefined
[9] Brigham and Women’s Hospital,undefined
[10] Massachusetts General Hospital,undefined
[11] Floating Hospital for Children at Tufts Medical Center,undefined
[12] UMass Memorial Health Care,undefined
[13] Yale University School of Medicine,undefined
[14] Wake Forest University Baptist Medical Center and Forsyth Medical Center,undefined
[15] University Health Systems of Eastern Carolina,undefined
[16] North Carolina Children’s Hospital,undefined
[17] Helen DeVos Children’s Hospital,undefined
[18] Sparrow Hospital,undefined
[19] Michigan State University,undefined
[20] University of Chicago Medical Center,undefined
[21] William Beaumont Hospital,undefined
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Among the 1 of 10 children who are born preterm annually in the United States, 6% are born before the third trimester. Among children who survive birth before the 28th week of gestation, the risks of autism spectrum disorder (ASD) and non-autistic social impairment are severalfold higher than in the general population. We examined the relationship between top quartile inflammation-related protein concentrations among children born extremely preterm and ASD or, separately, a high score on the Social Responsiveness Scale (SRS total score ≥65) among those who did not meet ASD criteria, using information only from the subset of children whose DAS-II verbal or non-verbal IQ was ≥70, who were assessed for ASD, and who had proteins measured in blood collected on ≥2 days (N = 763). ASD (N = 36) assessed at age 10 years is associated with recurrent top quartile concentrations of inflammation-related proteins during the first post-natal month (e.g., SAA odds ratio (OR); 95% confidence interval (CI): 2.5; 1.2–5.3) and IL-6 (OR; 95% CI: 2.6; 1.03–6.4)). Top quartile concentrations of neurotrophic proteins appear to moderate the increased risk of ASD associated with repeated top quartile concentrations of inflammation-related proteins. High (top quartile) concentrations of SAA are associated with elevated risk of ASD (2.8; 1.2–6.7) when Ang-1 concentrations are below the top quartile, but not when Ang-1 concentrations are high (1.3; 0.3–5.8). Similarly, high concentrations of TNF-α are associated with heightened risk of SRS-defined social impairment (N = 130) (2.0; 1.1–3.8) when ANG-1 concentrations are not high, but not when ANG-1 concentrations are elevated (0.5; 0.1–4.2).
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