Study population

MoBa is a nationwide, prospective, population-based cohort that includes 114 552 children born from 1999 to 2009.^{Reference Magnus, Birke, Vejrup, Haugan, Alsaker and Daltveit8} Mothers were recruited at the ultrasound examination provided free of charge to all pregnant women around gestational week 18. Of the women invited to participate, 41% consented. Fathers were also invited to participate if the mothers had consented first. The parents completed questionnaires during pregnancy, and have continued to receive questionnaires as the children grow older. Children with ASD diagnoses have been identified and ascertained through the Autism Birth Cohort (ABC) Study, a study of ASD nested within MoBa.^{Reference Stoltenberg, Schjolberg, Bresnahan, Hornig, Hirtz and Dahl9}

The 36-month questionnaire was distributed to MoBa participants born in 2001 and later, a total of 100 364 children. Of these, there were 58 520 (58%) whose parents returned the questionnaire. ASD case ascertainment has been conducted until 31 December 2015. By that time, the age range of the children whose parents completed the 36-month questionnaire was 6.5–14.7 years (mean 10.2 years).

The SCQ

The SCQ items are modified questions from the standardised diagnostic interview for ASD, the Autism Diagnostic Interview – Revised (ADI-R).^{Reference Lord, Rutter and Le Couteur10} The items were selected to detect deficits in social interaction and communication, and repetitive and stereotyped behaviours.^{Reference Berument, Rutter, Lord, Pickles and Bailey7} The first SCQ item is used to determine if the child has phrase speech. If so, the other 39 items are scored. A total score of ≥15 is considered screen-positive for ASD. If the child does not have phrase speech, only the 33 non-verbal items are scored.

Previous studies of the SCQ have utilised clinic-based study samples where children have already been diagnosed with ASD or referred for evaluations of ASD. The manual cut-off level of 15 is based on the initial validation study, which included participants from 4 to 32 years of age.^{Reference Berument, Rutter, Lord, Pickles and Bailey7} A subsequent American study showed that the SCQ had lower sensitivity in children under 8 years compared with children who were 8 years or older.^{Reference Corsello, Hus, Pickles, Risi, Cook and Leventhal11} To achieve a sensitivity of 80% in children under 8 years of age, the cut-off had to be lowered to ≥12 for children aged 5–7 years and ≥11 for children under 5 years. More recent studies have also supported the use of 11 as the cut-off level in preschool and elementary-school children.^{Reference Moody, Reyes, Ledbetter, Wiggins, DiGuiseppi and Alexander12,Reference Barnard-Brak, Brewer, Chesnut, Richman and Schaeffer13}

ASD screening in the MoBa cohort

The SCQ was embedded in the questionnaire distributed to MoBa participants at age 36 months. When the MoBa questionnaire was designed, there were no available screening instruments that had been tested in 3-year-olds. The SCQ was chosen because it captures all common symptoms of autism in children, and because the initial validation study indicated that it performed well at age 4 years and older.^{Reference Berument, Rutter, Lord, Pickles and Bailey7} The investigators who initiated the screening procedures in 2004 decided not to use the seven verbal SCQ items for screening, because they assumed that a large proportion of children with ASD would not have developed spoken language by 3 years of age. In order to ensure high sensitivity, it was decided to use a more lenient cut-off level than 15, and screen-positivity for ASD was defined by a score of ≥12 on the 33 non-verbal SCQ items. Screen-positive children were invited to participate in a 1-day diagnostic assessment. A randomly selected group of age-matched controls was also invited. Controls were selected every 2 weeks among MoBa participants who had passed the age of 37.5 months during the 2 preceding weeks.

Even though the seven verbal SCQ items were not used for screening by the ABC Study, the data are still available. In this article, we have included all the SCQ items in the analyses. We have also estimated the sensitivity and specificity of the SCQ at different cut-off levels:

1. (a) the cut-off recommended by the SCQ manual: ≥15 for the 39 scored items.

2. (b) the cut-off recommended by more recent studies: ≥11 for the 39 scored items.

3. (c) the cut-off used in the ABC Study: ≥12 for the 33 non-verbal items.

Other methods of identifying potential individuals with ASD

In addition to screening, the ABC Study used several methods to detect individuals with ASD in the cohort. The following participants were considered to potentially have ASD and invited to the clinical assessments.

1. (a) Children referred from their physicians or parents, if there was reason to suspect ASD. Referrals were elicited through annual newsletters to MoBa participants and information on the website of the Norwegian Institute of Public Health.

2. (b) Children whose parents reported autism, Asperger syndrome or autistic traits in the MoBa questionnaires at ages 5 and 7 years.

3. (c) Children diagnosed with ASD by specialist health services. Data from all hospitals and out-patient clinics are reported to the Norwegian Patient Register (NPR), beginning in 2008.^{Reference Suren, Bakken, Aase, Chin, Gunnes and Lie14} Reporting is linked to the government reimbursement system. We conducted annual linkages between MoBa and the NPR from 2008 to 2015 to identify MoBa participants with ASD diagnoses. Until all MoBa children reached 36 months of age in 2012, children with ASD diagnoses in the NPR were invited to the clinical assessments. After that, the diagnoses have been confirmed through medical record reviews, as described below.

ASD case ascertainment

The clinical assessment of the ABC Study included the ADI-R and the Autism Diagnostic Observation Schedule.^{Reference Lord, Risi, Lambrecht, Cook, Leventhal and DiLavore15} Diagnoses were based on the DSM-IV-TR.¹⁶ The ASD case definition included codes 299.00 (autistic disorder), 299.80 (Asperger disorder) and 299.80 (pervasive developmental disorder not otherwise specified).

After 2012, case ascertainment has been conducted through medical record reviews at the clinics where the diagnoses were recorded. In Norwegian specialist health services, diagnoses are coded according to the ICD-10.¹⁷ The ASD case definition of our reviews included codes F84.0 (childhood autism), F84.1 (atypical autism), F84.5 (Asperger syndrome), F84.8 (other pervasive developmental disorder) and F84.9 (pervasive developmental disorder, unspecified).

Other factors affecting sensitivity, specificity and screening participation

To examine whether sensitivity and specificity were affected by other types of developmental delay, we stratified the individuals with ASD by the presence or absence of phrase speech (reported on the first SCQ item) and cognitive delay (IQ below 70 at cognitive testing). We examined whether screening participation and screening performance were associated with sociodemographic characteristics of the families: parental education, parental age, maternal parity and maternal living status. We also examined whether these sociodemographic characteristics were associated with children's risk of ASD.

Statistical analyses

First, we evaluated how well the individual SCQ items differentiated between individuals with and without ASD. These abilities were evaluated by likelihood ratios (LRs).^{Reference Hunink, Glasziou, Siegel, Weeks, Pliskin and Elstein18} An LR is the ratio between the probability of a positive score in the presence of a condition (true positivity) and the probability of a positive score in the absence of the condition (false positivity). A high LR value indicates a high precision of a screening item, whereas an LR value close to one indicates that a screening item does not discriminate between individuals with and without the condition. The ability of a test to distinguish between ‘cases’ and ‘non-cases’ is generally considered to be poor when LR values are lower than 2.^{Reference Soreide, Korner and Soreide19}

We then determined sensitivity, specificity and positive and negative predictive values of the SCQ at the different cut-off levels described previously. We also explored the screening performance of the SCQ through receiver operating characteristic (ROC) curves. ROC curves were created for the SCQ total (manual) score and for each of the three SCQ domains, i.e. communication, social interaction and repetitive behaviours. In an ROC curve, sensitivity (the true-positive proportion) is plotted on the y-axis, whereas 1 – specificity (the false-positive proportion) is plotted on the x-axis.^{Reference Hunink, Glasziou, Siegel, Weeks, Pliskin and Elstein18} The area under the ROC curve (AUC) is a measure of the overall ability to differentiate between cases and non-cases, and can be interpreted as the probability that a randomly chosen pair of one case and one non-case will be correctly categorised.^{Reference Hunink, Glasziou, Siegel, Weeks, Pliskin and Elstein18} An AUC value of 0.9–1 is considered excellent, while 0.80–0.89 is good and 0.70–0.79 is fair.^{Reference Carter, Pan, Rai and Galandiuk20} Values below 0.70 are poor, and tests with values close to 0.50 are of no value.^{Reference Carter, Pan, Rai and Galandiuk20} Associations between screening participation, sociodemographic characteristics and ASD diagnoses were assessed by Pearson's χ² tests.

Ethics

The authors assert that all procedures contributing to this work comply with the ethical standards of the relevant national and institutional committees on human experimentation and with the Helsinki Declaration of 1975, as revised in 2008. MoBa is regulated under the Norwegian Health Registry Act. Written informed consent was obtained from mothers and fathers who participate. The consent covers linkages to health registries and reviews of medical records. The ABC Study has approval from the Regional Committee for Medical and Health Research Ethics for South-East Norway. Participation in the clinical assessments of the ABC Study was based on an additional written informed consent.