Introduction
The Child Behavior Checklist (CBCL; Achenbach and Rescorla
2000) is a widely used parent-report checklist, which measures a broad range of behavioral and emotional problems. A number of studies have provided evidence of the utility of the CBCL in identifying children with autism spectrum disorders (ASD) at different ages (Biederman et al.
2010; Ooi et al.
2011; So et al.
2012). However, the majority of studies indicate that the CBCL 1½-5 might perform best in Level 1 screening, namely identifying potential cases of ASD in low risk populations, rather than in level 2 screening, among children referred for developmental evaluation. Indeed, the CBCL 1½-5 Pervasive Developmental Problems scale (PDP) and the Withdrawn Syndrome scale have shown a good sensitivity and specificity when children with ASD are compared with children with typical development (TD) (Havdahl et al.
2016; Limberg et al.
2017; Rescorla et al.
2015). However, specificity becomes suboptimal, meaning that there is a risk of over-identifying children with ASD (false positives) when the comparison group is composed of children with other behavioral, emotional, or developmental problems. For example, in Muratori et al. (
2011), where the CBCL 1½-5 was used with three groups of children aged 24–60 months (101 diagnosed with ASD, 95 diagnosed with other psychiatric disorders (OPD), and 117 with TD), when the ASD group was compared with the TD group sensitivity/specificity values were 85%/90% for the DSM-PDP scale and 89%/92% for the Withdrawn scale. On the other hand, when the ASD group was compared with the OPD group, specificity was lower (60% for the DSM-PDP scale and 65% for the Withdrawn scale), indicating that some children in the OPD group had high scores on these scales even though they did not have ASD. It is noteworthy that sensitivity was unchanged (85% and 89%, respectively), indicating that both scales identified most of the children who received a diagnosis of ASD. So far, high sensitivity and specificity have been reported both in comparison with children with TD (n = 47) and children with OPD (n = 47) in only one study with young children with ASD (n = 47; age 18–36 months) (Narzisi et al.
2013). In this study, the comparison between the ASD group and the OPD group yielded a sensitivity of 0.85 and a specificity of 0.83 for the PDP scale and a sensitivity of 0.90 and a specificity of 0.83 for the Withdrawn scale. However, this optimal result was not replicated in the largest ASD screening study using the CBCL 1½-5 (Levy et al.
2019). In this study the DSM -PDP scale showed high sensitivity (80%) for identifying children with ASD (n = 656), whereas specificity varied depending on the comparison group (93% for 827 population controls, 85% for 646 children with developmental delay but no autistic features, and 50% for 284 children with developmental delay and autistic features). Thus, its utility as a level two screener needs to be further studied in order to understand with which clinical/at risk populations its specificity might be higher. Instead, its use as a level one screener has shown satisfactory levels for both sensitivity and specificity, suggesting its utility in routine developmental screening.
Since 2006 the American Academy of Pediatrics has recommended routine developmental screening with both broadband and autism-specific instruments at specified ages (Johnson and Myers
2007). Nevertheless, autism specific instruments are usually preferred. The most widely used autism specific screening tools are subsequent adaptations of the CHAT (Baron-Cohen et al.
2000), such as the Modified Checklist for Autism in Toddlers (M-CHAT; Robins et al.
2001). However, results on the sensitivity and specificity of these tools are not satisfactory. In one of the largest studies using the M-CHAT with a Follow-Up Interview (M-CHAT/F Robins et al.
2014) on a cohort of 25,999 children aged 16–26 months and followed-up through 4 to 8 years (Guthrie et al.
2019), the instrument yielded an overall sensitivity of 38.8%, and a positive predictive value (PPV) of 14.6%. When other developmental concerns were included as outcomes the PPV increased to 72.6%, however the sensitivity dropped to 11.7%, suggesting a limited utility of the M-CHAT/F for screening purposes.
Thus, for this purpose primary care practitioners might use broadband developmental screening tools rather than autism specific screening measures. If broad screeners were shown to be sensitive to autism, they could be used as a first level screen, while narrowband autism-specific screens could be used as a second level screen only for children with an autism risk indicated on the broadband screening (Hardy et al.
2015). In this regard, the broadband tool CBCL 1½-5 has shown high sensitivity and specificity as a first level screening tool, and the items of the PDP scale, revised with the publication of the DSM-5 and renamed ASD scale after removal of 1 item, are consistent with the DSM-5 diagnostic category of ASD (Achenbach
2014; Rescorla, Adams et al.
2019; Rescorla, Ghassabian et al.
2019a). Moreover, confirmatory factor analyses with data from population samples in 24 societies (
N = 19,850) have shown good measurement invariance across societies (Rescorla, Adams et al. 2019). Compared to narrowband autism-specific screening tools the CBCL 1½-5 might offer several advantages as it requires minimal time commitment and cost. In addition it summarizes in a unique profile single behaviors pointed out by parents, identifying a wide range of behavioral and emotional problems, and it compares scores with normative data, limiting possible mistakes in the interpretation of results. Furthermore, as it contains a wide variety of behavioral/emotional problems, a parent’s pre-existing disposition to endorse or deny features of ASD may be less likely to influence ratings than might be the case on an ASD-specific instrument, and the age range covered spans the full period in which ASD is usually diagnosed, unlike many of the ASD-specific screening instruments (Rescorla, Winder-Patel et al.
2019b).
Few studies have tested the CBCL 1½-5 on clinically referred children with ASD as early as 18 months, mainly because families reach medical services when children are older (Ferrante et al.
2015; Garrido et al.
2018). However, improving early screening and diagnosis is fundamental because it means children can have an earlier access to intervention, which has been shown to significantly improve outcomes (Dawson et al.
2010; Wetherby et al.
2014). Consequently, establishing the efficacy of this instrument at a younger age would be of assistance to pediatricians in the early detection of children who need referral for diagnostic evaluation, as well as representing a valid support to clinicians in the diagnostic process.
In the past decade several studies with longitudinal designs have been implemented in order to study the development of ASD, identify specific precocious signs of the disorder and test early screening instruments (Zwaigenbaum et al.
2013,
2015; Costanzo et al.
2015). Many prospective studies have been conducted on children at familial risk for ASD due to an affected older sibling (Jones et al.
2014; Szatmari et al.
2016). Indeed, younger siblings of children with ASD are at a higher risk of developing ASD themselves: approximately 20% receive a diagnosis of ASD (Charman et al.
2016; Ozonoff et al.
2014). However, early diagnosis of ASD in children who may show sub-clinical ASD symptoms due to a familial genetic risk is quite complex. In their study of siblings at familial risk for ASD, Charman et al. (
2016) found that among those who did not have an ASD outcome, around 11% had mild-to-moderate levels of developmental delay and 30% had high scores on the Autism Diagnostic Observation Schedule–2nd edition (ADOS-2; Lord et al.
2012). In these children who did not develop ASD, parents also reported high levels of ASD symptoms on the Autism Diagnostic Interview-Revised (ADI-R; Lord et al.
1994), as well as low adaptive functioning on the Vineland Adaptive Behavior Scales—2nd edition (Vineland-II; Sparrow et al.
2005). These findings on early emerging characteristics are an example of how complex an early diagnosis in infant siblings at familial risk for ASD can be.
As regards the use of the CBCL 1½–5 with younger siblings of children with ASD, Rescorla, Winder-Patel et al. (
2019b) compared 56 2-year-old children at high risk for ASD with 26 low-risk children with an older sibling with TD. Consistently with previous studies, they found that the CBCL 1½–5 PDP scale and the Withdrawn syndrome scale differentiated well between children diagnosed with ASD and those not diagnosed. These data however were not replicated in another study performed by Nilsson Jobs et al.
2019, in which CBCL 1½–5 ratings by parents and preschool staff were compared in a sample of 46 3-year-old children at high risk for ASD and 14 low-risk TD controls. In their study, parent ratings were able to discriminate between groups that differed substantially in terms of symptoms (high-risk versus low-risk group), while they were less able to detect (or report) more subtle differences between affected and unaffected high-risk siblings. In contrast, preschool staff ratings were more accurate than parent ratings at differentiating children with and without ASD, and more closely associated with clinician-rated symptoms. In their discussion of the results, the authors hypothesized that parents’ reduced opportunity to observe different children’s behavior (compared to preschool staff) and the experience of an older child with ASD could bias parents’ ratings of the younger child.
Research on the CBCL 1½–5 as a tool to identify children with ASD among younger siblings of children with a diagnosis of ASD, is still quite limited. To this end, we evaluated the capacity of the CBCL 1½–5 to discriminate between children who were developing autism and their peers with typical development at 18 months of age.
In Study 1, we investigated the ability of the CBCL 1½–5 to discriminate children clinically referred for ASD at 18 months of age, who at 30 months received a confirmatory diagnosis of ASD, from children with TD matched for age and sex (cognitive level was controlled for). In Study 2, we investigated the ability of the CBCL 1½–5 to discriminate the following three groups: siblings of children with ASD at 18 months of age, who at 30 months received a diagnosis of ASD; siblings of children with ASD at 18 months of age, who at 30 months did not receive a diagnosis of ASD; and children with TD at 18 months. As in Study 1, the groups were matched for age, sex, and the effect of cognitive level was controlled for. In both studies further analyses were performed to assess correlation between parent ratings and clinicians’ observations, and ROC analyses were performed to evaluate the discriminative capacity of CBCL 1½-5-ASD related scales.
To our knowledge this is the first study to evaluate the capacity of the CBCL 1½-5 to discriminate children with ASD as early as 18 months. The inclusion of a group of children at familiar risk for ASD will contribute to the existing literature on sibling cohorts, where autism symptomatology can be expressed differently compared to clinically referred children who do not have familiarity for the disorder.
Discussion
This study aimed to explore whether the CBCL 1½-5 could provide useful information for identifying children at risk for ASD as early as 18 months. Our results (Study 1) show that the CBCL 1½-5 Withdrawn and PDP scales can differentiate children with ASD from children with TD at this early age. Furthermore, group membership (ASD vs. NonASD) was predicted by the Withdrawn and PDP scale
T scores, but not by the level of cognitive ability. We also found that higher scores on these scales correlated positively with the clinician’s assessment of autism with the ADOS-2 semi-structured observation. These results confirm findings from previous studies on older children with ASD. Indeed, both the DSM-PDP scale and the Withdrawn Syndrome scale have shown an ability to differentiate children with ASD from children with TD at 24 months (Rescorla, Winder-Patel et al.
2019b), between 18 and 36 months (Narzisi et al.
2013), and between 24 and 60 months (Muratori et al.
2011). These results are not surprising as the two scales have five overlapping items. However, the DSM -PDP scale includes more specific ASD-like behaviors than the Withdrawn scale (i.e. 63. Repeatedly rocks head or body, 80. Strange behavior) and has been reported to have higher sensitivity compared to the Withdrawn scale (Levy et al.
2019).
Although screening at 18 months vs. 24 months or later ages has the potential to significantly accelerate the diagnostic process, there is a risk that some children with milder traits may be screened negative at this young age. Indeed, in their sample of 120 children with ASD, Zwaigenbaum et al.
2016 found that only 16% were diagnosed correctly at 18 months, 46% received their diagnosis at 24 months, and another 38% at 36 months, with children with more advanced language and adaptive skills and milder ASD symptoms being diagnosed later. If accuracy is a priority for Level 2 screening, this is not the case with Level 1 screening, which seeks to maximize sensitivity in order to avoid missing potential cases (few false negatives), accepting that some children will be false positives (they may have other behavioral/emotional problems that need attention).
Nevertheless, in our study, the ability of the CBCL 1½-5 to differentiate between children who are developing ASD and their peers with TD appeared specific to the clinically referred group. In the other at-risk group (Study 2), composed of children at familial risk for developing ASD due to an older affected brother/sister, the CBCL 1½-5 had difficulty in differentiating correctly between siblings who were developing ASD and the control group of children with TD. When the effect of cognitive level was removed, and the groups were matched on cognitive level, by using the standardized residuals of the
T scores with cognitive level as predictor, no significant differences appeared between groups. The SIB-ASD CBCL 1½-5T scores were below clinical cut-offs and quite similar to the control group of children with TD as well as to the SIB-NonASD group (see the
T scores on the CBCL 1½-5 scales of the three groups SIB-ASD, SIB-NonASD, and TD in Table
3).
Our results on the use of the CBCL 1½-5 in siblings differ from findings in a previous study by Rescorla, Winder-Patel et al. (
2019b), who in a similar small group of 13 SIB-ASD children found higher scores on the Withdrawn and DSM-PDP scales in siblings diagnosed with ASD compared both to low risk children and to siblings without a diagnosis. As their study was conducted on older children (24 months of age) than our toddlers, it is possible that by the time the children had reached their second birthday atypical behaviors may have become more evident for parents who filled in the CBCL 1½-5. Furthermore, Rescorla does not quantify the ADOS-2 scores of the children in her sample, so we were not able to compare our data with hers regarding the severity of autistic profiles.
Conversely, the characteristics of our SIB-ASD sample do not appear particularly different from other descriptions of siblings with ASD of the same age. In Chawarska’s study on predictors of later outcomes in younger siblings of children with ASD, the mean ADOS-2 severity score index of 69 SIB-ASD children who were correctly identified at 18 months was 6 and increased to 7 at 36 months (Chawarska et al.
2014). Our severity score index of 6.7 indicates that the symptomatology of our SIB-ASD sample was not particularly low and was recognized quite clearly by clinicians at the ADOS-2 semi-structured observation. Cognitive and adaptive functioning were significantly lower in our SIB-ASD group than in the SIB-NonASD group, although on average they did not reveal a clinical delay (mean scores were above 70 on all subscales). These profiles are similar to those presented in other studies on siblings’ developmental trajectories which show a slower developmental rate in SIB-ASD children (Landa and Garrett-Mayer
2006; Sacrey et al.
2019).
Our results regarding the difficulties of the CBCL 1½-5 to clearly identify autistic symptoms in the siblings were partially unexpected. Firstly, because this instrument proved useful in clinically referred children of the same age (Study 1) and secondly, because parents of autistic children have generally been shown to be sensitive to their younger children’s development (Herlihy et al.
2015; Richards et al.
2016; Sacrey et al.
2015). The different discriminative capacity of the CBCL 1½-5 in our two studies might be explained by differences in the ascertainment method of the two groups. Indeed, children who are recruited in prospective longitudinal studies are more likely to display fewer and less severe symptoms than those recruited on the basis of clinical referral or with a provisional diagnosis (Sacrey et al.
2017). Thus, it is possible that with individuals of this kind, screening instruments whose properties include greater variance in the distribution of features are more informative (Pasco et al.
2019).
Furthermore, although it has been shown that parents of children subsequently diagnosed with ASD are more likely to report concerns about their child’s development than parents of children with TD and children with other developmental difficulties, their concerns tend to be more about broad behavioral issues rather than about social communication and interaction (Pasco et al.
2019). If, on the one hand, parents who have older children with ASD are inevitably better informed about the emerging signs of autism than most parents of young children, it is possible that when comparing their younger offspring with the older child with autism rather than to “typical development” they may tend to under-report autistic-like behavioral symptoms, especially when they differ from the older sibling’s behavioral profile. Indeed, in our sibling group the SIB-ASD group showed unexpectedly low scores on the CBCL 1½-5 and SIB-NonASD children scored even lower. Inconsistencies between parent reports of autistic traits and observations by other informants such as teachers or clinicians are quite common and should not be considered as contradictory but as complementary, as each informant provides unique information based on their specific experiences or situational specificity (Möricke et al.
2016). Indeed, Nilsson Jobs et al. (
2019), who tested the efficacy of the CBCL 1½-5 in siblings at heightened risk of developing ASD, found that teachers’ reports of autistic symptoms increased the likelihood of correctly differentiating between siblings with and without ASD. In the light of these observations it is possible that in sibling populations clinicians may benefit by asking multiple informants to fill in the CBCL 1½-5.
When interpreting the results of the present study important limitations should be taken into account. The main limitation of this work is the small group size of the SIB-ASD group. However, this is a fairly common limitation in sibling studies and our group size is similar to the ones in the two previous studies on the use of the CBCL 1½-5 in sibling populations (n.13 Rescorla, Winder-Patel et al.
2019b; n.10 Nilsson Jobs et al.
2019). Despite the limited sample size, we believe that the inclusion of this group of children is important. Indeed, it provides complementary information, not limited to clinically referred toddlers whose parents are already aware of the reasons for concern, on the use of the CBCL 1½-5 in toddlers who are at risk for autism. Nevertheless, generalizability of the findings from Study 2 should be addressed with caution as non-significant results could be the result of the small sample size and less powerful statistics. The wide variability of ASD traits within children at familial risk and the young age of the children could also have contributed to this result. Indeed, in their study on high-risk siblings Rescorla, Winder-Patel et al. (
2019b) suggest that a lower DSM-PDP cut-off point might be preferable when screening for ASD at a young age, when symptoms may be more subtle or less severe. Another possible limitation regarding our non-significant findings for study 2, may be related to the fact that the computation of the
T score of the PDP scale also included an item recently excluded (item 3,
afraid to try new things) as it did not meet the threshold for inclusion in the DSM-5 version of the scale. Indeed in our sample of siblings who received a clinical diagnosis of ASD, only 20% of parents reported some kind of problem on item 3. However this error was evenly distributed across children (e.g. also in study 1, where the CBCL correctly identified children with autism, only 45% of children obtained a higher score than 0 on item 3). Another limitation is the fact that no follow-up data is available from the TD group in order to ascertain developmental outcome. However, at the moment of recruitment there were no clinical concerns regarding these children’s development. Furthermore, a measure of cognitive ability was not available for all the children in the TD group, so we selected a reduced number of children with TD (n.27) for Study 2 and we were only able to control for the effect of cognitive level in a sub-group of children in Study 1. In the future, it would be useful to include also a group of children with developmental delay (DD), in order to better evaluate the effects of cognitive level on ASD screening. In previous studies a higher rate of false positives has been reported in DD groups (Rescorla et al.
2015; Havdahl et al.
2016). However, Levy et al.
2019 found that the CBCL 1½-5 screening capacity was higher among DD children who did not share ASD features than among DD children who had ASD features (44% of their DD sample), indicating the importance of considering phenotypical differences among DD children.
In conclusion, our findings suggest that when parents raise concerns for ASD by presenting high scores on the Withdrawn and PDP scales, an evaluation for ASD is highly recommended as there is a strong likelihood that the child may have the disorder. We believe our preliminary study lays the foundation for a future population study, which could better verify the discriminative capacity of this instrument at the 18-month well-child visits.
However, when looking at families who already have a child with ASD, we found low agreement between parent ratings on the CBCL 1½-5 and the diagnostic assessment performed by the clinician. Thus, we strongly recommend that younger siblings of children with ASD be followed in longitudinal surveillance programs. Moreover, multiple sources of information should be collected in order to gain a more exhaustive picture of the child’s communication and social development.
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