This study included 77 Japanese children with Autistic disorder (AD) and 57 TD children (91 boys and 43 girls, aged 38–98 months). Participants were recruited from Kanazawa University and affiliated hospitals. We confirmed that no TD child had a history of neurological, neuropsychiatric, or neurodevelopmental disorders. The diagnosis of AD was established according to the Diagnostic and Statistical Manual of Mental Disorders (4th edition) [29] using the Diagnostic Interview for Social and Communication Disorders [30] or the Autism Diagnostic Observation Schedule-Generic [31] or the Autism Diagnostic Observation Schedule 2 [32], details of which are given in the S1 and S2 Tables. We excluded participants with blindness, deafness, and other neuropsychiatric disorders, including epilepsy and ongoing medication. Intelligence is also an important factor in ASD, and high- and low-functioning autism are often distinguished based on intelligence quotient (IQ) scores [33]. “High functioning autism” is a term used for individuals with ASD who have an intelligence of 70 or above, especially indicating individuals without moderate to severe intellectual disability. ASDs with lower intelligence and those with higher intelligence are potentially different in terms of their cognitive profiles and genetic etiology. For example, Szatmari et al. (1998) reported that different genetic factors may account for the higher and lower functioning forms of autism [34]. Thus, we excluded 10 participants with an IQ <70. IQ was assessed using the mental processing composite scale of the Kaufman Assessment Battery for Children (K-ABC). Overall, we analyzed 67 children with AD (49 boys, 18 girls, aged 38–98 months) and 57 TD children (34 boys, 23 girls, aged 53–90 months). These are also part of an ongoing project (Bambi plan, http://bambiplan.w3.kanazawa-u.ac.jp/pdf/jusen_english.pdf). We are continually recruiting participants as part of a large epidemiological study, and some participants overlapped with those in our earlier study [35]. However, their results did not overlap. Additionally, the emphases of the earlier study differed from those of this study. The study was approved by the institutional review board of Kanazawa University Hospital and conducted per tenets of the Declaration of Helsinki [36]. Written informed consent was obtained from all participants’ guardians.

Buccal mucosa cells were obtained from all participants by gently scraping the mucosa with a cotton swab. DNA was extracted from the cells, followed by whole genome amplification using the PicoPLEX WGA kit (Takara Bio, Mountain View, CA, USA). DNA concentrations were measured using a Qubit4 fluorometer (Thermo Fisher Scientific, Waltham, MA, USA). Genotyping of rs2710102 was performed by real-time PCR (ViiA 7, Applied Biosystems, Foster City, CA, USA) using the rhAmp SNP Genotyping system (assay name: CD.GT.TKKG0518.1: Integrated DNA Technologies, Coralville, IA, USA). The following RNA-DNA hybrid primers were used: 5′-TTGGTTAACATTTACTCTGAGACC[T/C]GAGAA-3′, and 5′-GCTGGAGTGAACCTGTTTGATTATTGCTGAT-3′ as locus-specific primers (https://sg.idtdna.com/pages/products/qpcr-and-pcr/genotyping/rhamp-snp-genotyping).

The Social Responsiveness Scale (SRS) [37] was used to assess the participants’ social reciprocity: A 65-item rating scale that measures sociality and autistic mannerisms as a quantitative trait in TD children and children with ASD [38–40]. It measures subscales of social awareness, social cognition, social communication, social motivation, and autistic mannerisms to generate a single measure. We used gender-normed social responsiveness scale T scores (SRS-T) of each subscale [41]. Higher scores indicated greater difficulties in social reciprocity. The SRS has been one of the most frequently used quantitative measures of ASD symptoms, with very strong measurement properties in healthy volunteers and clinical cases of ASD [42]. In this context, this questionnaire is suitable for measuring sub-threshold autistic traits.

The participants’ parents filled out this questionnaire indicating how strongly they agreed with each question by checking one of the following: “never true,” “sometimes true,” “often true,” or “always true,” that were further scored as one, two, three, and four points, respectively [43]. Consequently, T-scores of SRS reflect the children’s social reciprocity in their natural social contexts [37]. It can describe moderate deficiencies in reciprocal social behavior that are “clinically significant” in ASD as well as in the general population [3].

The Japanese version of the K-ABC [44], based on neuropsychological and information-processing theories, was used to assess the intelligence of all participants, with a distinction between problem-solving and knowledge of facts. The former was interpreted as intelligence, whereas the latter was defined as an achievement. Problem-solving abilities were measured using two mental processing scales [45], the sequential processing scale, which requires the child to solve problems in serial or temporal order, and the simultaneous processing scale, which requires the child to integrate multiple stimuli simultaneously to solve problems. The mental processing composite scale is a unification of the sequential and simultaneous processing scales, intended to measure total general intelligence. The achievement scale measures the degree of knowledge and skills that children acquire from the environment. These scores are provided as age-adjusted standardized scores normalized to a mean of 100 and a standard deviation of 15.

One of the goals of developing K-ABC was to separate intelligence from other factors, including achievement. Notably, although the achievement scale was reported to be well-correlated with language skills, the association of language skills with the two mental processing scales was reported to be weak. For example, Wiebe et al. reported that the correlation coefficient between the achievement scale and verbal IQ measured by Wechsler Intelligence Scale for Children-Revised was 0.77. In the same study, the correlation coefficient between sequential processing scale or simultaneous processing and verbal IQ were 0.54 and 0.63, respectively [46]. Since our objective was to examine the effect of rs2710102 on intelligence rather than on language skills, we focused on two mental processing scales in this study.

Statistical analyses were performed using Stata software (ver. 16.1; Stata Corp., College Station, TX, USA). First, we checked the differences in age and scores in SRS-T and K-ABC between children with AD and TD using Student’s t-tests. Sex differences were tested using the chi-square test. Further, we employed a chi-square test to compare the group (AD or TD) and rs2710102 genotypes. Based on these results, we assumed a proper genetic model and evaluated the risk allele for AD. Based on the genetic model, we investigated the association between social reciprocity and the participants’ genotypic status after controlling for the disease group. In particular, we applied linear regression models to predict SRS total T-scores based on the participants’ group, genotype, and the interaction between group and genotype. If a significant interaction was observed or when appropriate, we investigated the association between genetic status and SRS-T score in each group. In addition to SRS total T-scores, as an exploratory analysis, we examined the correlation between each subscale of SRS and the genotype. In those models, we used each subscale of SRS (i.e., social awareness subscale, social cognitive subscale, social communication subscale, social motivation subscale, and autistic mannerisms sub-scale) as dependent variables instead of total SRS-T scores.

We also applied linear regression models to predict the K-ABC two mental processing scales (simultaneous processing scale and sequential processing scale) based on the participants’ group, genotype, and interaction with the group and adopted the same model for the achievement scale. A p-value <0.05 indicated statistical significance. If a significant interaction effect was observed or when appropriate, we applied post-hoc analysis to elucidate the association between the genotype and K-ABC scores in each group. In the post-hoc analyses, we predicted the sequential processing scale or simultaneous processing scale based on the participants’ group, genotype, and interaction with the group.

As an exploratory analysis, to control possible effects of SRS total T-scores on the scores in K-ABC or vice-versa, we analyzed the effect of genotype on SRS total T-scores controlling on the effect of intelligence. We further examined the effect of genotype on intelligence controlling for the effect of SRS total T-scores. Specifically, we applied linear regression models in each participant’s group (i.e., AD or TD) to predict (i) SRS total T-scores based on the genotype and simultaneous processing scale in K-ABC, (ii) SRS total T-scores based on the genotype and sequential processing scale in K-ABC, (iii) simultaneous processing scale in K-ABC based on the genotype and SRS total T-scores, and (iv) sequential processing scale in K-ABC based on the genotype and SRS total T-scores.

Before applying linear regression, we verified that our data met the assumptions for the regression analysis. Specifically, we used standard methods to verify linearity, normality, homogeneity of variance, model specifications, influence, and collinearity. However, the assumption of homogeneity was violated in some regression models. Therefore, we used heteroskedasticity-robust standard errors [47].

The distribution of CNTNAP2 rs2710102 (A/G) genotypes among the 124 sampled subjects were as follows: Twenty-eight participants were homozygous AA genotype, 67 participants carried the heterozygous AG, and 29 were homozygous GG. Tests for the Hardy-Weinberg equilibrium exhibited no deviations from the expected genotype distribution (p > 0.05). The SRS total T-score was significantly higher in children with AD compared to that in TD children [t(120) = -12.23, p < 0.001]. The mental processing composite scale score was significantly lower in children with AD than in TD children [t(120) = 3.05, p = 0.0027]. This observation was consistent across sequential and simultaneous processing scales. The sequential processing scale and simultaneous processing scale scores were significantly lower in children with AD than in TD children [t(120) = 3.46, p = 0.0007; and t(120) = 2.40, p = 0.0177, respectively]. However, we observed no significant differences in achievement scale scores. The participant characteristics are presented in Table 1. There was no significant difference in age or sex between the groups.

A chi-square test revealed a significant difference between the genotypes and groups (χ²(2) = 6.56, p = 0.038). Allele and genotype frequencies are presented in Table 2. The genetic model was determined based on these results. According to the selected genetic model [48], we transformed the three genotypes (AA, AG, and GG) into two variables. In particular, considering our results and the findings of previous studies [21], we assumed the co-dominant model: Carriers of the A-allele (AA + AG) versus G-allele homozygotes. This indicates that allele A increases autistic traits. Additionally, we employed a chi-square test to investigate the difference between carriers of the A-allele and the groups. However, this difference was not significant (χ²(2) = 1.29, p = 0.256).

We applied linear regression models to predict the SRS total T-score based on the participants’ group (AD or TD), genotype (carriers of the A-allele or G-allele homozygotes), and interaction between group and genotype. Table 3 and Fig 1 summarize results of regression models. In this model, carriers of the A-allele and the group were significantly affected [t(120) = 2.11, p = 0.036] and [t(120) = 8.82, p < 0.001], respectively, details of which are given in the S1 Fig.

Additionally, the F statistic was significant [F(3, 120) = 65.63, p < 0.001]. However, the interaction was not significant [t(120) = -1.24, p = 0.216]. For this particular model, the assumption of normality was violated. According to the histogram, this was caused by different patterns of association in AD or TD. Hence, we applied linear regression to predict the SRS total T-score based on genotypes in each group. As a result, a significant main effect of genotype was observed for TD [t(55) = 2.11, p = 0.039]. However, this association was not significant in children with AD.

As an exploratory analysis, to further investigate the association between the genotype and social reciprocity, we examined the correlation between each subscale of SRS and the genotype. Aside from the main effect of the participants’ group, we observed a significant effect only for the model predicting social awareness subscale. Specifically, we observed a main effect of the genotype to be significant [t(120) = 1.99, p = 0.049] for the model, indicating that carriers of the A-allele had a higher social awareness subscale of SRS. Post-hoc analysis demonstrated that this effect was larger in the TD group, although it did not reach statistical significance [t(55) = 1.98, p = 0.52]. The results are presented in S3 Table.

For the model predicting the mental processing composite scale based on the participants’ group (AD or TD), genotype (carriers of the A-allele or G-allele homozygotes), and interaction with the group, only the main effect of the group was observed to be significant [t(120) = -2.74, p = 0.007]. No other factors were observed to be statistically significant. For the model predicting the simultaneous processing scale, the main effect of genotype was observed to be significant [t(120) = -2.19, p = 0.030], and the group [t(120) = -3.43, p < 0.001] was also observed to be significant. The interaction effect was also significant [t(120) = 2.55, p = 0.011]. Hence, we applied a post-hoc analysis to predict the simultaneous processing scale based on the genotypes in each group, and a significant main effect of genotype was observed only for TD [t(55) = -2.19, p = 0.033], scatter plot of which are provided in the S2 Fig. Table 4 summarizes the results of the models predicting the simultaneous processing scale. For the model predicting the sequential processing scale, no factor was observed to be significant.

This study has several limitations. First, the sample size was too small to investigate behavioral characteristics. Larger samples are thus needed to clarify characteristics of autistic traits in TD children. Second, we did not use multiple tests in the current study. Most genetic studies with relatively few polymorphisms are not sufficiently powered to derive definitive conclusions when adjusting the results for multiple testing [61]. Further, adjusting for multiple tests may increase the chance of type II errors owing to the conservative nature of the Bonferroni adjustment [62]. Third, we need to confirm the association between these results and neural substrates. The ongoing study may assist in providing more evidence on genetic-behavior-brain interactions using neuroimaging methods. Fourth, we could not prove a cause-and-effect association between the genetic changes and behavioral characteristics. Further studies are thus required to elucidate the underlying biological mechanisms. Moreover, all our participants were children, and we did not include any adolescents or adults. These results should not be generalized unless validated in older individuals. Fifth, although the K-ABC second edition (K-ABC II, [63]) was released in 2004, we used the original version of K-ABC [64]. Similarly, we used the original version of SRS rather than SRS-2 [41], which is available from 2017. This was because the Japanese version of neither the K-ABC second edition nor SRS second edition had been verified at the time we started this study. However, in any case, this did not align with the current best practice standards. Sixth, all the TD children were native Japanese with no previous or existing developmental, learning, or behavioral problems according to information obtained from questionnaires completed by their parents. Consequently, it might be possible that some children we classified as TD had AD. This should be especially considered for those who had higher SRS total T-scores.