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The perinatal androgen to estrogen ratio and autistic-like traits in the general population: a longitudinal pregnancy cohort study.

While previous studies have found a link between testosterone levels in amniotic fluid and autistic-like traits, a similar relationship has not been found...

Authors:
Jamnadass ES, Keelan JA, Hollier LP, Hickey M, Maybery MT, Whitehouse AJ.

Authors notes:
J Neurodev Disord. 2015;7(1):17.

Keywords:
Androgens, Autism-Spectrum Quotient, Autistic-like traits, Cord blood, Estrogens, Perinatal, Sex steroids

Abstract:
BACKGROUND: Prenatal androgen exposure has been hypothesized to be linked to autism spectrum disorder (ASD).

While previous studies have found a link between testosterone levels in amniotic fluid and autistic-like traits, a similar relationship has not been found for testosterone in umbilical cord blood.

However, it may be the net biological activity of multiple androgens and estrogens that influences postnatal effects of prenatal sex steroids.

Accordingly, composite levels of androgens (A) and estrogens (E) were investigated, along with their ratio, in relation to autistic-like traits in young adulthood.

METHODS: Sex steroid data in umbilical cord blood were available from 860 individuals at delivery.

Samples were analyzed for androgens (testosterone, androstenedione, and dehydroepiandrosterone) and estrogens (estrone, estradiol, estriol, and estetrol).

Levels of bioavailable testosterone, estradiol, and estrone were measured and used to calculate A and E composites and the A to E ratio.

Participants were approached in early adulthood to complete the autism-spectrum quotient (AQ) as a self-report measure of autistic-like traits, with 183 males (M = 20.10 years, SD = 0.65 years) and 189 females (M =19.92 years, SD = 0.68 years) providing data.

RESULTS: Males exhibited significantly higher androgen composites and A to E composite ratios than females.

Males also scored significantly higher on the details/patterns subscale of the AQ.

Subsequent categorical and continuous analyses, which accounted for covariates, revealed no substantial relationships between the A/E composites or the A to E ratio and the AQ total or subscale scores.

CONCLUSIONS: The current study found no link between the A/E composites or the A to E ratio in cord blood and autistic-like traits in the population as measured by the AQ.

These outcomes do not exclude the possibility that these sex steroid variables may predict other neurodevelopmental traits in early development.