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Long-term survival of children born with congenital anomalies: A systematic review and meta-analysis of population-based studies


Authors: Svetlana V. Glinianaia aff001;  Joan K. Morris aff002;  Kate E. Best aff001;  Michele Santoro aff003;  Alessio Coi aff003;  Annarita Armaroli aff004;  Judith Rankin aff001
Authors place of work: Population Health Sciences Institute, Faculty of Medical Sciences, Newcastle University, Newcastle upon Tyne, United Kingdom aff001;  Population Health Research Institute, St George’s, University of London, London, United Kingdom aff002;  Institute of Clinical Physiology, National Research Council, Pisa, Italy aff003;  Center for Clinical and Epidemiological Research, University of Ferrara, Ferrara, Italy aff004
Published in the journal: Long-term survival of children born with congenital anomalies: A systematic review and meta-analysis of population-based studies. PLoS Med 17(9): e1003356. doi:10.1371/journal.pmed.1003356
Category: Research Article
doi: https://doi.org/10.1371/journal.pmed.1003356

Summary

Background

Following a reduction in global child mortality due to communicable diseases, the relative contribution of congenital anomalies to child mortality is increasing. Although infant survival of children born with congenital anomalies has improved for many anomaly types in recent decades, there is less evidence on survival beyond infancy. We aimed to systematically review, summarise, and quantify the existing population-based data on long-term survival of individuals born with specific major congenital anomalies and examine the factors associated with survival.

Methods and findings

Seven electronic databases (Medline, Embase, Scopus, PsycINFO, CINAHL, ProQuest Natural, and Biological Science Collections), reference lists, and citations of the included articles for studies published 1 January 1995 to 30 April 2020 were searched. Screening for eligibility, data extraction, and quality appraisal were performed in duplicate. We included original population-based studies that reported long-term survival (beyond 1 year of life) of children born with a major congenital anomaly with the follow-up starting from birth that were published in the English language as peer-reviewed papers. Studies on congenital heart defects (CHDs) were excluded because of a recent systematic review of population-based studies of CHD survival. Meta-analysis was performed to pool survival estimates, accounting for trends over time. Of 10,888 identified articles, 55 (n = 367,801 live births) met the inclusion criteria and were summarised narratively, 41 studies (n = 54,676) investigating eight congenital anomaly types (spina bifida [n = 7,422], encephalocele [n = 1,562], oesophageal atresia [n = 6,303], biliary atresia [n = 3,877], diaphragmatic hernia [n = 6,176], gastroschisis [n = 4,845], Down syndrome by presence of CHD [n = 22,317], and trisomy 18 [n = 2,174]) were included in the meta-analysis. These studies covered birth years from 1970 to 2015. Survival for children with spina bifida, oesophageal atresia, biliary atresia, diaphragmatic hernia, gastroschisis, and Down syndrome with an associated CHD has significantly improved over time, with the pooled odds ratios (ORs) of surviving per 10-year increase in birth year being OR = 1.34 (95% confidence interval [95% CI] 1.24–1.46), OR = 1.50 (95% CI 1.38–1.62), OR = 1.62 (95% CI 1.28–2.05), OR = 1.57 (95% CI 1.37–1.81), OR = 1.24 (95% CI 1.02–1.5), and OR = 1.99 (95% CI 1.67–2.37), respectively (p < 0.001 for all, except for gastroschisis [p = 0.029]). There was no observed improvement for children with encephalocele (OR = 0.98, 95% CI 0.95–1.01, p = 0.19) and children with biliary atresia surviving with native liver (OR = 0.96, 95% CI 0.88–1.03, p = 0.26). The presence of additional structural anomalies, low birth weight, and earlier year of birth were the most commonly reported predictors of reduced survival for any congenital anomaly type. The main limitation of the meta-analysis was the small number of studies and the small size of the cohorts, which limited the predictive capabilities of the models resulting in wide confidence intervals.

Conclusions

This systematic review and meta-analysis summarises estimates of long-term survival associated with major congenital anomalies. We report a significant improvement in survival of children with specific congenital anomalies over the last few decades and predict survival estimates up to 20 years of age for those born in 2020. This information is important for the planning and delivery of specialised medical, social, and education services and for counselling affected families. This trial was registered on the PROSPERO database (CRD42017074675).

Keywords:

Metaanalysis – cohort studies – children – Systematic reviews – congenital anomalies – cleft lip and palate – Down syndrome – Spina bifida

Introduction

Globally, mortality in children aged under 5 years has halved since 1990, mainly because of a sharp reduction in deaths from communicable diseases as a result of targeted child health strategies and interventions of the United Nations (UN) Millennium Development Goals [1]. Following this worldwide reduction, the relative contribution of congenital anomalies to child mortality is increasing globally and is therefore outlined as an emerging priority to be addressed by the UN Sustainable Development Goals in the post-2015 child health agenda [2]. Although the contribution of congenital anomalies to infant mortality is well described, in particular for developed countries [35], there is less research focused on survival beyond the first year of life. However, this is of considerable public health importance, as according to evidence from North America and Europe, the mortality rate of individuals born with congenital anomalies significantly exceeds that of the general population after infancy as well [69]. In addition, a large variation in child death rates still exists between countries, even within Europe [10]. In 2012, the child death rates (age 0–14 years) were about 60% higher in the United Kingdom and Belgium compared to Sweden, with an additional 10 Western European countries being 30% higher than Sweden [10]. Currently, a quantitative summary of population-based studies of survival beyond infancy for specific congenital anomalies is lacking. Accurate estimates of long-term survival are important for clinicians counselling parents when a congenital anomaly is diagnosed pre- or postnatally and for public health commissioners to ensure adequate resources are in place to provide high-quality medical and social care for these individuals. Importantly, it is essential that estimates are provided according to type of congenital anomaly, given the diversity in aetiology, treatment, and prognosis.

We performed a systematic review and meta-analysis to summarise and quantify the existing population-based data on long-term survival (beyond infancy) of individuals born with specific major congenital anomalies that manifest in childhood and explore the risk factors associated with survival.

Methods

Search strategy

This study is reported as per the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guideline (S1 PRISMA Checklist). A protocol for this systematic review was registered on the International Prospective Register of Systematic Reviews (PROSPERO) database (CRD42017074675) (S1 Text). We conducted comprehensive literature searches using a combination of the following sources of information:

  • Electronic bibliographical databases: MEDLINE, EMBASE, Scopus, PsycINFO, CINAHL, ProQuest Natural, and Biological Science Collections and also the databases of the systematic reviews, i.e., PROSPERO, the JBI Database of Systematic Reviews and Implementation Reports. We used key words and subject headings (dependent on the database) combining the keywords for the population (birth, pregnancy, delivery), exposure (congenital anomaly, including specific anomaly groups), outcome (long-term survival, mortality), and study design (population-based studies), incorporating elements of the PICOS (Population/Patient, Intervention/Exposure, Comparator group, Outcome, Study design) framework into our systematic search strategy [11] (S1 Table). The final search results were limited to English papers and to humans, whereas the initial searches had no language limitations to examine whether there were any relevant studies we could have missed. We have identified 66 papers published in non-English language (79% from Europe) based on Medline search, but no papers met our inclusion criteria.

  • Manual searching of the reference lists of the included full papers and of the relevant previous literature reviews, including systematic, was performed.

  • Citation searching for studies that had referenced the included studies was performed via the Google Scholar citation function.

  • Keyword searches in key journals, including Birth Defects Research, Archives of Disease in Childhood, Pediatrics, The Journal of Pediatrics, and Journal of Pediatric Surgery, were also undertaken.

  • Authors were contacted if there was insufficient information to decide whether the study met the inclusion criteria or if additional information for the inclusion in the meta-analysis was needed.

  • Reference lists and citations of any new articles identified were further searched for any additional studies in the iterative process until no new studies were identified. Database searches were completed in March 2019 and updated in May 2020.

SVG conducted all searches and screened the titles and abstracts of all the identified records according to the inclusion criteria, and three other authors (MS, AC, JR) independently screened a random 10% sample of the records using the Rayyan software for systematic reviews [12]. Any discrepancies (n = 4) in the included studies were discussed amongst all authors and agreement reached.

Definitions and classification of congenital anomalies

Major congenital anomalies in the included studies were classified according to the International Classification of Disease (ICD) revision 8 (ICD-8) [8], ICD-9 (majority of papers), ICD-10 [1315], and British Paediatric Association (BPA-ICD-9) diagnosis coding [1620] or surgical codes [21]. Some papers that included a long birth year period used more than one ICD version for the corresponding time periods [9,2225]. The included studies reported the survival estimates for all congenital anomalies combined (e.g., ICD-9 codes 740.0–759.9) and/or by congenital anomaly group (the system affected, e.g., urinary system, ICD-9 753.0–753.9) and/or subtype (the individual disorder, e.g., spina bifida, ICD-9 741). Some European studies [14,15,17] classified major congenital anomalies according to European Surveillance of Congenital Anomalies (EUROCAT) guidelines [26,27]. We have presented the congenital anomaly subtypes within the major congenital anomaly groups according to the EUROCAT classification [26].

Eligibility criteria

Studies meeting the following criteria were included: (1) being an original population-based peer-reviewed study that reported long-term (beyond 1 year of life) survival of children born with a major congenital anomaly that manifests in childhood; (2) reporting survival probability (or the number of patients born and the number or proportion alive at age >1 year) for these children that were followed up from birth; (3) being published from 1 January 1995 to 30 April 2020 to increase comparability of included birth cohorts in relation to medical care and treatment availability/policies; (4) involving humans only and published in the English language.

Studies were excluded if (1) they reported survival during the first year of life only; (2) patients were not followed up from birth, because this may have under-ascertained deaths occurring prior to follow-up (e.g., if follow-up began after surgical correction); (3) they were not population-based, as other study designs are more likely to incur ascertainment bias (e.g., hospital-based studies may capture more severe phenotypes); (4) they focused on individuals born with congenital heart defect (CHD), because there was a recently published systematic review covering these population-based studies [28]; (5) they followed up a restricted subgroup of patients (e.g., preterm births only or extracorporeal membrane oxygenation [ECMO] patients only). No exclusions were made based on the birth year of studied cohorts.

Data extraction

Information on the following study characteristics was extracted: study location, birth year period, duration of follow-up/years of survival, congenital anomaly type and if isolated/non-isolated, sources of case ascertainment (e.g., congenital anomaly register) and sources of death identification (e.g., linkage with a mortality database), number of cases and deaths, Kaplan-Meier survival estimates reported, or the survival estimates calculated by the reviewers. Authors were contacted if survival estimates were reported for subgroups of patients only (e.g., by sex or age at operation), if it was not possible to calculate 95% confidence intervals (95% CIs) or extract survival estimates from the Kaplan-Meier curves, or if further information was required or clarification needed (n = 18). If the authors did not respond after two reminders or if the study was closed and access to the data was not possible, we calculated the lower and upper limits of the 95% CI according to the efficient-score method (corrected for continuity) described by Newcombe, 1998 [29], based on the procedure outlined by Wilson, 1927 [30] (http://www.vassarstats.net/survival.html). If survival estimates were not reported in the text or tables of the included paper, they were extracted from Kaplan-Meier survival curves, where available, using PlotDigitizer software [31]. If none of the above was possible, the study was excluded.

Data extraction and quality appraisal of the included studies were performed in duplicate, i.e., all by SVG and a subset of studies by each coauthor. Data were entered into piloted data extraction forms (S2 Table).

Statistical analysis

Where three or more articles reported survival with the number of births (or where the numbers of births could be estimated from the 95% CIs provided) for a specific congenital anomaly, a meta-analysis was performed to estimate pooled survival at ages 1, 5, 10, and 20 (and 25, where available) years. The Stata program “gllamm” was used to fit univariate multilevel meta-analysis of longitudinal data to allow for the correlations in survival over several time periods within studies [32,33]. Survival according to age (0–25 years) was modelled using the logistic regression options within the gllamm program: family(binomial) and link(logit). The outcome of interest was the number of deaths occurring out of the total number of live births. The number of deaths at each time point, if not provided, was estimated from the published proportions surviving and the number of live births by assuming there was no loss to follow-up. Calculating the number of deaths in this way will be unbiased (as the proportion surviving is unbiased) but will result in slightly too narrow confidence intervals. To confirm that this is valid, an alternative method using the arcsine square root transformation [34] of the published survival estimate was applied and the estimated standard error was calculated, and a model was fitted in gllamm using the weighted regression options instead of the logistic regression above. Both methods reported consistent results, and hence, the results of the logistic regression models are reported here, as they enable the interpretation of the odds of increasing survival over time. Studies were treated as a random effect and cohort of birth and age at survival as fixed effects nested within the studies. Age was modelled as a continuous variable using a linear term or, where significant (according to a likelihood ratio test), a quadratic term. Cohort of birth was modelled as a continuous variable. Most included studies reported survival across distinct periods (e.g., between 2000 and 2009), so the mean year of birth was used (e.g., 2005). For studies that reported survival estimates for multiple cohorts (e.g., 2000–2004, 2005–2009), survival for both cohorts were entered into the model, again with average year of birth for each cohort (e.g., 2002 and 2007). Using the models, survival at ages 1, 5, 10, 20, and 25 years was estimated for patients born in 2000 and 2020. Models were fitted separately for each type of congenital anomaly. Odds ratios (ORs) representing the increase/decrease in survival per 10-year increase in time were extracted from the models. Where fewer than three studies reported survival for a specific congenital anomaly, the survival estimates were discussed narratively. The ages for which more than three studies reported a survival rate were plotted separately; often, the reports were at 5 or 10 years of age. This allows the reader to evaluate the changes that have occurred over time in the survival of the children up to 5 years of age and separately up to 10 years of age. All modelled survival curves, although plotted on two separate figures, are derived from the one model fitted on all the data.

Analysis was performed in Stata 15 (StataCorp), and p < 0.05 was considered statistically significant.

Quality appraisal

The Newcastle-Ottawa Quality Assessment Scale (NOS) for cohort studies [35] was used to assess the quality of the included studies. The scale assesses information bias, selection bias, and confounding (S2 Table). Although a traditional cohort study can be awarded a maximum of nine stars, for survival population-based studies a comparison group is not a mandatory component of the study design; therefore, a maximum of six stars can be allocated to the majority of the included studies (S3 Table).

Results

Search results

A total of 10,888 records identified from the electronic database searches and other sources were available for screening titles and abstracts (Fig 1). After excluding 10,660 records, 228 were eligible for full text review. After further exclusion of 173 articles, 55 met the inclusion criteria, covering a total population of 367,801 live births with various types of major congenital anomalies. Earlier follow-up studies based on the same population were replaced by more recent ones if they also reported survival at a younger age (n = 2 [36,37]). However, if survival at a more advanced age only was reported in the later article [38], the earlier article was also included (n = 1 [39]).

Fig. 1. PRISMA flowchart of searches, screening, and study selection.
PRISMA flowchart of searches, screening, and study selection.
PRISMA, Preferred Reporting Items for Systematic Reviews and Meta-Analyses.

Characteristics of included studies

Table 1 provides the description of 55 studies included in this review. Further detail on the sources of case ascertainment and death identification and the description of the comparison group, if any, are given in S4 Table. Nine studies analysed long-term survival of all congenital anomalies combined: seven with [6,8,15,17,4042] and two without [7,43] stratification by congenital anomaly group/subtype (Table 1). Other studies (n = 46) focused on specific groups or subtypes of congenital anomalies: the central nervous system (n = 5 [4449]), including spina bifida [4446,48,49] and encephaloсele [44,47]; orofacial clefts (n = 1 [16]); anomalies of the digestive system (n = 22), including oesophageal atresia [9,50,51], anorectal malformations [52], congenital diaphragmatic hernia (CDH) [18,23,51,53,54], biliary atresia [3639,5564], and Hirschsprung disease [24]; abdominal wall defects (n = 1 [21]); chromosomal anomalies (n = 12), including trisomy 21 [14,19,22,6569,70,71], trisomy 13 [25,72], and trisomy 18 [25,72]; skeletal dysplasias (n = 2 [13,20]); and Prader-Willi syndrome (PWS) (n = 1 [73]). The included studies were conducted in Europe (n = 29 [8,9,1315,17,2124,3639,44,45,5054,5658,60,61,64,65,68]), the United States of America (n = 12 [7,1820,40,41,43,4648,70,72]), Australia (n = 7 [16,42,59,66,67,69,73]), Canada (n = 3 [6,25,63]), Japan (n = 1 [62]), Brazil (n = 1 [55]), and Hong Kong (n = 1 [71]). One international study reported survival of children with spina bifida from a number of registries from Europe and the USA [49]. As all included studies were population-based, sources of case ascertainment for most studies (n = 39) were congenital anomaly registers or surveillance programmes that either included all types of major congenital anomalies or were anomaly-specific. The majority of these studies linked their congenital anomaly data with death registration data to ascertain data on age at death (S4 Table).

Tab. 1. Description of included studies.
Description of included studies.

As our literature search was restricted to years between January 1995 and April 2020, the publication years ranged between 1997 [68] and 2020 [71], whereas patients were mostly born between 1970 and 2010, with the earliest birth year in 1950 [73] and the latest ending in June 2016 [58]. Table 1 also describes the duration of follow-up, the survival age analysed, and whether survival was reported in the papers (with or without 95% CI) or estimated by our reviewers. Table 1 also gives the NOS scores that range between 5 and 8 respective of the use of the comparison group that is not mandatory for the survival studies (see S3 Table for detailed scoring). According to NOS, all studies were of low risk of bias.

Survival of children with different congenital anomalies

Table 2 shows survival estimates overall and by birth cohort, where reported, for individuals up to 25 years of age for studies estimating survival for all congenital anomalies combined and by different group/type. S5 Table presents more detail for studies reporting survival estimates by other risk factors (e.g., ethnicity or presence of additional anomalies). Most studies reported 1- and 5-year survival estimates only. Survival varied considerably according to anomaly; therefore, survival estimates are presented by different groups and subtypes (Table 2). The 5-year survival for all anomalies combined varied from 85% to 95%, owing to different inclusion and exclusion criteria. It was not considered appropriate to pool survival estimates for all congenital anomalies combined, because of the diversity of the contributing congenital anomaly groups.

Tab. 2. Survival estimates by congenital anomaly type at age 1–25 years, overall and by birth cohort.
Survival estimates by congenital anomaly type at age 1–25 years, overall and by birth cohort.

Congenital anomalies of the nervous system

Survival in live births with anencephaly analysed by four studies was extremely low and varied from 0% [15,42] to 7.3% [40] by year 1 (Table 2).

Seven studies of survival in children born with spina bifida [6,15,4042,45,48] including 7,422 live births were summarised in a meta-analysis, with pooled survival estimates of 92%, 91%, 89%, and 88% at ages 5, 10, 20, and 25 years predicted for children born in 2020 (Table 3). Survival has improved significantly over time, with an increased OR per 10-year increase in birth year 1.34 (95% CI 1.24–1.46, p < 0.001) (Table 3 and Fig 2).

Fig. 2. Survival estimates (with 95% confidence intervals) of children with spina bifida at 1 (a), 5 (b), and 10 (c) years of age over time (10 birth cohorts from 7 studies).
Survival estimates (with 95% confidence intervals) of children with spina bifida at 1 (a), 5 (b), and 10 (c) years of age over time (10 birth cohorts from 7 studies).
The numbers at survival points indicate the included study, which may appear more than once if survival was reported for more than one birth cohort: 1 –Agha, 2006, Canada; 2 –Borgstedt-Bakke, 2017, western Denmark; 3 –Wong, 2001, Atlanta, USA; 4 –Tennant, 2010, Northern England; 5 –Wang, 2011; USA, 6 –Wang, 2015, USA; 7 –Schneuer, 2019, New South Wales, Australia.
Tab. 3. Predicted survival estimates for children born with selected congenital anomalies in 2000 and 2020 (results of the meta-analysis).
Predicted survival estimates for children born with selected congenital anomalies in 2000 and 2020 (results of the meta-analysis).

Four studies [15,40,41,47] reported survival of 1,562 encephalocele live births, with pooled survival estimates of 72%, 72%, 71%, and 71% at ages 5, 10, 20, and 25 years predicted for infants born in 2020 (Table 3). A small decrease in survival was observed over time, which was not statistically significant (p = 0.19) but was included in the model predictions to be consistent with the models for other congenital anomalies and acknowledging that the power from analysing only 4 studies is very low (Table 3 and S1 Fig).

Survival in individuals with hydrocephalus was reported in four studies, with the three more recent studies reporting very similar survival rates at age 5 years [15,40,42] and at 15 years in two studies with longer follow-up. The earlier study (1967–1979) reported lower survival of 50.8% for male individuals by age 18 years [8] (Table 2). Comparison of survival between these studies is difficult owing to differences in the inclusion criteria.

Orofacial clefts

Seven studies providing survival estimates for children born with orofacial clefts [6,1517,4042] included 32,492 live births. There was insufficient number of studies reporting data by specific cleft type that met criteria for a meta-analysis; therefore, the survival data are presented in Table 2. Generally, 1-year and long-term survival of children with isolated cleft lip is over 99% [15,16], about 96%–97% for isolated cleft palate [15,16] and much lower for non-isolated orofacial cleft types [40,41].

Anomalies of the digestive system

Seven studies reporting survival in children with oesophageal atresia (n = 6,303) were summarised in a meta-analysis [9,15,4042,50,51]. There was a statistically significant improvement in survival over time, with an increased OR of 1.50 (95% CI 1.38–1.62, p < 0.001) per 10-year increase in birth year. The pooled survival estimates predicted for infants born in 2020 were 93%, 93%, 92%, and 92% at ages 5, 10, 20, and 25 years, respectively (Table 3 and Fig 3).

Fig. 3. Survival estimates (with 95% confidence intervals) of children with oesophageal atresia at 1 (a) and 5 (b) years of age over time (7 studies).
Survival estimates (with 95% confidence intervals) of children with oesophageal atresia at 1 (a) and 5 (b) years of age over time (7 studies).
The numbers at survival points indicate the included study: 1 –Cassina, 2016, Northeast Italy; 2 –Garne, 2002, Funen, Denmark; 3 –Oddsberg, 2012, Sweden; 4 –Tennant, 2010, Northern England; 5 –Wang, 2011 USA; 6 –Wang, 2015, USA; 7 –Schneuer, 2019, New South Wales, Australia.

The survival estimates for children with anorectal malformations and for those with Hirschsprung disease were reported in four [15,40,41,52] and three studies [15,24,42] with survival ranging between 86% and 97% and between 93% and 98%, respectively (Table 2).

Fourteen studies (n = 3,877 live births) reporting overall (after Kasai hepatoportoenterostomy [KP]) and/or liver transplantation) and/or survival with native liver (NLS, without liver transplantation) in children born with biliary atresia [15,3638,5564] were included in the meta-analysis. Pooled overall survival for biliary atresia at ages 5, 10, and 20 years were estimated to be 94%, 92%, and 88% for infants born in 2020 (Table 3). Fig 4 and Table 3 show a significant linear increasing trend in the overall survival and ORs for improvement in survival over time with OR = 1.62 (95% CI 1.28–2.05, p < 0.001). A small decrease in survival was observed over time in NLS, which was not statistically significant (p = 0.26) but was included in the model predictions to be consistent with the models for other congenital anomalies (Table 3). The predicted 5-year survival estimate was 41% (95% CI 33–49) for infants born in 2020 (the survival curve is shown in S2 Fig).

Fig. 4. Survival estimates (with 95% confidence intervals) of children with biliary atresia at 5 (a) and 10 (b) years of age over time (11 birth cohorts from 9 studies).
Survival estimates (with 95% confidence intervals) of children with biliary atresia at 5 (a) and 10 (b) years of age over time (11 birth cohorts from 9 studies).
The numbers at survival points indicate the included study which may appear more than once if survival was reported for more than one birth cohort: 1 –McKiernan, 2000, UK and Ireland; 3 –Nio, 2003, Japan; 6 –Tennant, 2010, Northern England; 8 –Wildhaber, 2008, Switzerland; 9 –Davenport, 2011, England and Wales, 10 –Chardot, 2013, France; 11 –Pakarinen, 2018, Nordic countries; 13 –Grizelj, 2010, Croatia; 15 –Tu, 2015, South Australia.

Nine studies of children born with CDH (n = 6,176) were summarised in a meta-analysis [15,18,23,4042,51,53,54]; pooled survival estimates of 83% at ages 5, 10, 20, and 25 years respectively predicted for infants born in 2020 were reported in Table 3. The studies demonstrated that the majority of deaths occurred within the first year of life, with survival plateauing after that. Survival has improved significantly over time, with an increased OR per 10-year increase in birth year of 1.57 (95% CI 1.37–1.81, p < 0.001) (Table 3 and Fig 5).

Fig. 5. Survival estimates (with 95% confidence intervals) of children with congenital diaphragmatic hernia at 1 (a) and 5 (b) years of age over time (5 studies).
Survival estimates (with 95% confidence intervals) of children with congenital diaphragmatic hernia at 1 (a) and 5 (b) years of age over time (5 studies).
The numbers at survival points indicate the included study: 2 –Garne, 2002, Denmark; 6 –Tennant, 2010, Northern England; 7 –Wang, 2011, USA; 8 –Wang, 2015, USA; 9 –Schneuer, 2019, New South Wales, Australia.

Abdominal wall defects

Five studies (n = 4,845) reporting survival of children born with gastroschisis were summarised in a meta-analysis [15,21,4042]. There was a statistically significant improvement in survival over time, with an increased OR of 1.24 (95% CI 1.02–1.50, p = 0.029) per 10-year increase in birth year. Similar to studies on CDH, the majority of deaths occurred within the first year of life, with survival plateauing after that. The pooled survival estimates predicted for children born in 2020 were 94%, 93%, and 92% at ages 5, 10, and 20 years, respectively (Table 3 and Fig 6). Survival was consistently higher for gastroschisis than omphalocele in the three register-based studies reporting survival for both conditions [15,40,41] (Table 2).

Fig. 6. Survival estimates (with 95% confidence intervals) of children with gastroschisis at 1 (a) and 5 (b) years of age over time (5 studies).
Survival estimates (with 95% confidence intervals) of children with gastroschisis at 1 (a) and 5 (b) years of age over time (5 studies).
The numbers at survival points indicate the included study: 1—Risby, 2017, southern Denmark; 2—Schneuer, 2019, New South Wales, Australia; 3—Tennant, 2010, Northern England; 4—Wang, 2011, USA; 5—Wang, 2015, USA.

Chromosomal anomalies: Trisomies 21, 13, and 18

Survival of children born with Down syndrome (trisomy 21) reported by the presence of CHD in 10 studies (22,317 live births) [14,19,22,42,6570] was summarised in the meta-analysis. We found significantly increasing survival trends over time for children with Down syndrome associated with CHD (OR = 1.99, 95% CI 1.67–2.37, p < 0.001) per 10-year increase in birth year; Table 3 and Fig 7). Children with Down syndrome without CHD had relatively high survival for live births in 2000 with no statistically significant improvement over time predicted for those born in 2020 (OR = 1.17, 95% CI 0.91–1.5, p = 0.23) (Table 3 and Fig 8). As there was a significant improvement in children with Down syndrome with CHD, the estimated improvement in children without CHD (although not statistically significant) was also modelled. For children born in 2020, pooled survival for Down syndrome at ages 5, 10, and 20 years were estimated to be 97%, 97%, and 96% for those both with and without CHD.

Fig. 7. Survival estimates (with 95% confidence intervals) of children with Down syndrome associated with congenital heart defect at 1 (a), 5 (b), and 10 (c) years of age over time (11 birth cohorts from 10 studies).
Survival estimates (with 95% confidence intervals) of children with Down syndrome associated with congenital heart defect at 1 (a), 5 (b), and 10 (c) years of age over time (11 birth cohorts from 10 studies).
The numbers at survival points indicate the included study, which may appear more than once if survival was reported for more than one birth cohort: 1 –Glasson, 2016, Western Australia; 2 –Hayes, 1997, Ireland; 3 –Kucik, 2013, USA; 4 –Leonard, 2000, Western Australia; 5 –Rankin, 2012, Northern England; 6 –Rasmussen, 2006, Atlanta, USA; 10 –Brodwall, 2018, Norway; 11 –Frid, 1999, northern Sweden; 12 –Halliday, 2009, Victoria, Australia, 13 –Schneuer, 2019, New South Wales, Australia.
Fig. 8. Survival estimates (with 95% confidence intervals) of children with Down syndrome without congenital heart defect at 1 (a), 5 (b), and 10 (c) years of age over time (11 birth cohorts from 10 studies).
Survival estimates (with 95% confidence intervals) of children with Down syndrome without congenital heart defect at 1 (a), 5 (b), and 10 (c) years of age over time (11 birth cohorts from 10 studies).
The numbers at survival points indicate the included study, which may appear more than once if survival was reported for more than one birth cohort: 1 –Glasson, 2016, Western Australia; 2 –Hayes, 1997, Ireland; 3 –Kucik, 2013, USA; 4 –Leonard, 2000, Western Australia; 5 –Rankin, 2012, Northern England; 6 –Rasmussen, 2006, Atlanta, USA; 10 –Brodwall, 2018, Norway; 11 –Frid, 1999, northern Sweden; 12 –Halliday, 2009, Victoria, Australia, 13 –Schneuer, 2019, New South Wales, Australia.

Studies analysing long-term survival in children with trisomies 13 (n = 4) and 18 (n = 5) reported consistently low 1-year survival ranging from 12% [72] to 21% [40] for trisomy 13 and from 2% [15] to 20.6% [42] for trisomy 18 (Table 2). However, large studies from the USA and Canada have shown that the majority of those individuals who survived to 1 year were alive at 5 [72], 10 [25], and 15 [40] years. A Canadian study reported that 76% and 65% of 1-year survivors with trisomy 13 were alive at 5 and 10 years, respectively; the corresponding figures for trisomy 18 were 90% and 77% [25]. In a USA study, conditional 5-year survival (for those who survived the first year of life) was over 80% for both trisomies 13 and 18 [72]. Four studies (n = 2,174) reporting survival of children born with trisomy 18 were summarised in a meta-analysis [25,40,42,72]. The pooled survival estimates predicted for children born in 2020 were 14% and 13% at ages 5 and 10 years, respectively (Table 3 and S3 Fig). The time trends were not tested, owing to a very small size of the most recent study reporting higher survival.

Other congenital anomalies

Fewer studies analysing survival in children born with limb anomalies, renal anomalies, and skeletal dysplasias and syndromes met our inclusion criteria, with four being register-based studies that analysed a range of main anomaly groups/subtypes [15,4042] (Table 2).

Survival of children born with upper or lower-limb defects was similar at about 87%–89% at 5 and 8 years of age in both USA register-based studies that included isolated anomalies and those with additional anomalies [40,41], whereas survival for upper-limb defects was higher at 99% than that for lower-limb defects at 93%% after 1 year of age in an English register-based study that included only isolated anomalies [15]. However, the latter study was much smaller, with ≤3 deaths for these anomalies.

Survival of children with urinary-system anomalies is not comparable between the studies, because of the differences in inclusion criteria (isolated versus non-isolated) and different birth year periods (Table 2).

Four studies reporting survival/mortality for children with skeletal dysplasia beyond 1 year of age were quite heterogeneous in terms of subtypes included, which may have caused differences in survival between a recent Australian study [42] and three other studies [13,15,20].

Two studies reported survival in patients with PWS, but the sample size was very low (n = 10, with one death) in one [15]. According to an Australian study using data from the PWS register, 10-year survival (97%) was similar to 1-year survival (98.6%); however, by age 25 it reduced to 89% [73].

Factors associated with survival of children with congenital anomalies

Table 4 shows that overall, long-term survival in children born with congenital anomalies was much lower than in the reference populations, with the risks of death varying from 6.7 to 12.9 times greater than in the general population in the three studies reporting this [68]. In the USA study, the hazard ratio (HR) of death at age 7 years was only slightly reduced (from 7.2 to 6.9) when adjusted for child’s sex and mother’s race, age, and education [7] (Table 4). Table 4 also shows risks of death associated with some specific congenital anomalies compared to the reference population.

Tab. 4. Risk of death in children born with a congenital anomaly (CA) compared to the reference population.
Risk of death in children born with a congenital anomaly (CA) compared to the reference population.

Studies analysing survival predictors reported the presence of additional major anomalies as a universal risk factor of reduced survival [9,14,19,22,36,37,40,44,46,47,50,52,65,66,68,69,71,72] (Table 5), even after adjustment for such factors as birth cohort, birth weight, and/or gestational age at delivery [9,14,19,40,44,50,69,72] (Table 5). Other common risk factors associated with survival in children with congenital anomalies had a low birth weight (LBW) [9,14,19,40,47,48,50,52,66,69,71] or preterm birth [14,40,42,72] and earlier birth year period, after adjustment for covariates [9,14,19,40,50,66,69,71] (Table 5). Ethnicity was inconsistently associated with survival of children with some anomalies in USA studies. Hispanic ethnicity was associated with reduced survival by age 8 years in children with spina bifida weighing at birth between 1,500 and 2,499 g, but not in those with lower (<1,500 g) or higher (≥2,500 g) birth weight [46]. In another multistate USA study [41], there was no significant association of spina bifida survival at ≤8 years with any ethnic group when adjusted for covariates (Table 5, S6 Table). However, the latter study reported a significantly increased adjusted HR for reduced survival in Black and Hispanic children for both orofacial clefts and those with oesophageal atresia after adjustment for essential covariates and significantly increased adjusted HR for Down syndrome and CDH in Black children only [41] (S6 Table). Black ethnicity, however, was associated with a lower risk of death at 5 years for trisomy 18 [72]. In New York state, maternal nativity (‘Others’ versus ‘US born’) was significantly associated with a higher risk of death up to 25 years for all congenital anomalies and for anomalies of the central nervous system when adjusted for other factors including ethnicity [40]. Being aboriginal had a significant independent effect on reduced 10-year survival of children with Down syndrome in an earlier Australian study after adjustment for presence of CHD, birth weight, and birth cohort [69], but not in a more recent study [66] (Table 5).

Tab. 5. Predictors of survival/mortality in the included studies that explored factors associated with long-term survival at different age points beyond 1 year of life.
Predictors of survival/mortality in the included studies that explored factors associated with long-term survival at different age points beyond 1 year of life.

Because of the rarity of biliary atresia and dependence of outcome on successful and timely KP, the survival factors most commonly explored in these children were annual centre caseload [36,38,39,58,61] and age at KP [36,37,55,56,58,63,64]. The higher centre caseload—i.e., care centralisation associated with centralisation of surgical and medical resources and better surgical staff experience—and earlier age at KP were considered as positive factors for survival. Earlier KP was associated with better NLS at age 4 years [55,63,64] and 5 years [58]. The 20-year NLS was also higher for children operated at a younger age compared to >90 days in a French study [36] and to >75 days in a Dutch study [56]. However, 10-year NLS was not associated with age at KP in a UK study [37]. Centre caseload (<5 versus >5) was the only significant factor for both 5-year overall survival and NLS in an earlier UK study after adjustment for confounders [39], but at 13 years it remained a significant factor for NLS only [38]. Centre caseload (<3 versus >3) was also a significant predictor of 5-year NLS in a collaborative Scandinavian study [58], and in Finland centralisation of care for patients with biliary atresia significantly increased both overall and NLS to age 4 years [60] (Table 5). In a French study, lower centre caseload was significantly associated with both reduced overall survival and NLS in the earlier period (1986–1996) but not in the later (1992–2002 and 2003–2009) periods [36] (Table 5).

Discussion

This systematic review and meta-analysis summarise long-term survival for individuals born with a range of congenital anomalies from population-based studies, covering a total population of 367,801 live births with congenital anomalies. This work is part of the ‘EUROlinkCAT: Establishing a linked European Cohort of Children with Congenital Anomalies’, a collaborative project investigating survival, morbidity, and educational outcomes in children born with congenital anomalies using population-based data from multiple EUROCAT registries linked to a number of health and education datasets (https://www.eurolinkcat.eu/). A total of 55 studies were included in the narrative synthesis, with 41 studies included in meta-analyses. Our meta-analyses showed predicted 20-year survival for children born in 2020 as 89% for spina bifida (n = 7 studies), 71% for encephalocele (n = 4), 92% for oesophageal atresia (n = 7), 88% for biliary atresia (n = 14), 83% for CDH (n = 9), 92% for gastroschisis (n = 5), and 96% for Down syndrome both with and without CHD (n = 10). As expected, the first year of life was critical for survival of children with a congenital anomaly, but there remained a gradual decline in survival beyond infancy that exceeded that of the general population. Our meta-analyses showed statistically significant improvement in survival over time in those with spina bifida, oesophageal atresia, biliary atresia, CDH, gastroschisis, and Down syndrome in those with CHD, but not in those with encephalocele, biliary atresia with a native liver, or Down syndrome without CHD. The evidence from individual studies showed that improvement in survival was not equal for all patient groups, being more pronounced, for example, for a group with non-isolated anomalies [50] or differing by ethnic group [18]. The commonest significant independent predictors of reduced survival for any congenital anomaly type were presence of additional structural anomalies, LBW, and earlier birth year period.

Advances in prenatal diagnosis, neonatal care (including intensive care, standard use of antenatal steroids, and surfactant therapy for prevention of neonatal mortality and morbidity in preterm births), early surgical interventions, ECMO, care centralisation, and liver transplantation (for biliary atresia patients) were likely to improve survival in these children. One of the factors that may have contributed to the improvement in survival of live births with spina bifida over the last 30 years, reported by individual studies [45,46] and revealed by our meta-analysis, is the increasing use and accuracy of prenatal diagnosis and the consequent increase in terminations of pregnancy for fetal anomaly (TOPFAs) for most severe anomaly types. One of the included studies found an independent association of annual TOPFA rate with increase in survival [15]. Indeed, there is evidence of an association between the increased TOPFA rates and reduced live-birth prevalence of congenital anomalies and consequent reduction in infant mortality [74,75]. Periconceptional folic acid intake or fortification is likely to be another factor of improving survival by reducing the number of severe types of spina bifida [76]. Advances in neonatal and surgical care, including early neonatal or elective fetal surgery for spina bifida repair [77,78], may have also contributed to increased long-term survival of these patients.

In addition to the above listed general advances in prenatal diagnosis and neonatal care contributing to improvement in survival of children with various types of congenital anomalies, there are specific principles in care of CDH patients that affect survival of these patients. These are early intubation with avoidance of bag mask ventilation; prevention and treatment of pulmonary hypertension and lung hypoplasia, the primary causes of neonatal mortality in CDH patients, by minimising lung damage using gentle lung ventilation (e.g., high-frequency oscillatory ventilation); gastric decompression, ensuring adequate blood pressure; ECMO, if indicated; and delayed surgical repair after stabilisation of pulmonary and haemodynamic status [79].

Studies of survival of children with biliary atresia, a rare life-limiting progressive disorder of bile ducts, which is fatal without early surgery (KP) and eventually requires liver transplantation, were mostly limited to 4–5 years of follow-up, with two European studies reporting survival at age 20 years [36,56]. Despite a number of existing reviews on biliary atresia, including a systematic review published in 2013 [80], this condition was included in our review, as we aimed to update the existing evidence on a population base and pool data in a meta-analysis. The 4-year NLS was as low as 23.5% before centralisation of care (1987–2005) in Finland, increasing to 76% after centralisation [60]. In addition to centralised care, earlier age at KP was a predictor of better NLS in these patients in some studies [36,55,56,58,63,64], which was in agreement with an earlier systematic review [80]. However, in the UK centre, caseload was the only significant factor associated with better NLS at age 5, 10, or 14 years [3739]. Care centralisation and liver transplantation are crucial factors in the care of these patients, increasing the overall 10-year patient survival to 79.7% in France [36] and 87%, 89%, and 91.5% in the Scandinavian countries [58], UK [37], and Switzerland [64], respectively.

A significant association between birth year and increase in survival of individuals with Down syndrome was reported in some reviewed studies [14,19,66,69]. Recent advances in intensive care of preterm and very LBW babies are likely to account for prevention of infant death in many children with Down syndrome who are at a 2-fold higher risk of infant death compared to very LBW babies without a congenital anomaly, owing to higher risk of infection and lung disease such as bronchopulmonary dysplasia [81]. Improved access to early cardiac surgery in infants with septal defects may have also contributed to their increased long-term survival by prevention of development of pulmonary arterial hypertension and Eisenmenger syndrome, the conditions of high-risk mortality [66,82,83]. Our meta-analysis has shown that survival estimates significantly increased over time for children with CHD, but the improvement for those without CHD was not statistically significant.

Until recently, trisomies 13 and 18 were regarded as lethal conditions, with the majority of prenatally diagnosed cases being electively terminated and those resulting in live births (about 19% and 14% for trisomies 13 and 18, respectively [84]) commonly receiving palliative care only. Two recent studies that analysed survival of children with trisomy 13 or 18 beyond 1 year [25,72] demonstrated that although cumulative survival was low, children who were alive at their first birthday had around an 80% chance of survival to their fifth birthday, and 86% of those who survived to age 5 were likely to live to age 10 years [25]. Despite the emerging evidence that intensive care and surgical interventions improve the survival in these children [85], the debate in the medical community in relation to the interventions to be offered to infants with these trisomies is ongoing [8587] because of severe cognitive impairment in the survivors and considerations in relation to family and societal burden [87]. Current medical experts’ view is that medical care of children with trisomies 13 and 18 should be evidence-based [85], and more consideration should be given to personalised care of these children, providing more information to parents and taking into account their hopes and wishes [86].

The commonest significant independent predictors of reduced survival at and beyond 1 year of life for any congenital anomaly type were presence of additional structural anomalies, LBW, and earlier birth year period. The association with ethnicity was inconsistent in the USA studies across different anomaly types and aboriginality was significantly associated with reduced survival in children with Down syndrome in an earlier study [69] but not in a more recent one [66]. Ethnicity may be a proxy indicator of deprivation, which is associated with increased neonatal and infant mortality across all major causes of death including congenital anomalies [8891]; however, the associations with other deprivation measures were not analysed in the included studies.

This systematic review and meta-analysis is strengthened by a rigorous search strategy and comprehensive literature searches using a combination of multiple sources of information to identify relevant papers. Our systematic search strategy was informed by the research protocol registered in the PROSPERO database and developed according to clear inclusion criteria based on elements of the PICOS framework. To ensure that the search strategy was appropriately inclusive, it was piloted using Medline, refined, and retested. Additionally, we manually searched the reference lists of all included papers, citations of the included papers repeating that process for newly identified papers, and also key journals in the field. This approach is recognised to increase the identification of relevant papers [92]. A 10% sample of titles and abstracts of records was screened by coauthors to enable consistency in study inclusion following predefined eligibility criteria. All data were extracted in duplicate by two independent reviewers to ensure accuracy in the reported results and to minimise subjectivity. Authors were contacted where more information was required during data extraction. We also used an established quality-assessment tool as part of the critical appraisal process.

We restricted the start year for our literature searches to 1995 to make the birth cohorts used in the studies more comparable in relation to antenatal and neonatal care and treatment availability/policies and to avoid subsequent differences. In addition, restricting our review to population-based studies with follow-up from birth reduces bias in death ascertainment.

We used multilevel meta-analytic models to allow for studies reporting the survival of different cohorts of births over several time periods. Importantly, we estimated survival for infants born in 2020, which will be useful for counselling parents when a congenital anomaly is diagnosed and for health and social care planning. The gllamm model allows the correlation of survival over time within a study to be modelled whilst allowing for the random effects from different studies. As the included studies used differing birth cohorts with their effect on survival that increased over time, we felt that it would be inappropriate to present I2 heterogeneity results that is a standard measure of variation between studies, usually clinical trials. We also did not test for publication bias, as survival studies profoundly differ by their nature from clinical trials where publication bias can be expected due to a higher likelihood of publication of positive results, which is not the case for survival studies. Moreover, as a number of register-based studies included in the meta-analysis estimated survival of many different anomaly groups and types, publication bias for a specific anomaly is unlikely. Owing to the lack of data in terms of the small number of studies, formal tests for publication bias lack power, and funnel plots were not informative. The paucity of data limits the predictive capabilities of the models, as shown by the wide confidence intervals on some estimates. A further limitation is the assumption that improvements in survival in the past will continue to be maintained in the future. This is a particular issue with Down syndrome children with CHD. There have been recent dramatic improvements in their survival, but such improvements are unlikely to continue, and it is likely that their survival will always be slightly lower than that of children with Down syndrome without CHD. Yet the two models predicted very similar survival for such children born in 2020.

Meta-analysis was not possible for all studies included in this systematic review, as either there was an insufficient number of studies reporting survival for the same anomaly subtype or the studies did not report 95% CI or the number of cases. Moreover, not all studies included in the meta-analysis of some structural anomalies (e.g., spina bifida, CDH) were consistent in their exclusion of non-isolated anomalies, which may have accounted for the variability in the survival estimates. All but one of the included studies were conducted in high-income countries, which limited generalisability of the results to low-income countries. Lack of relevant studies from 66 papers identified from our Medline search not restricted to English language, most of which were from Europe, suggests that population-based studies with long-term follow-up of children with congenital anomalies or linkage studies to identify deaths beyond infancy are rare in low-income countries.

The papers analysing survival predictors were not systematically searched for; only studies eligible for this review that also explored predictors were included. We acknowledge that summarised data on survival predictors reported in the reviewed studies are supplementary and enrich the interpretation of the results but are not a comprehensive review of predictors of congenital anomaly–related survival. Therefore, the association of survival with some important risk factors such as maternal deprivation, shown to be linked to lower infant and child survival [89,93], including children born with congenital anomalies [94], could have been underinvestigated in this review.

This systematic review and meta-analysis summarised the existing international evidence from population-based studies to provide information on long-term survival of children with selected congenital anomalies and temporal changes in survival. Our findings reveal a wide variation in survival by congenital anomaly subtype and suggest reduced survival associated with many anomaly subtypes compared with the reference population. The meta-analysis has demonstrated that survival has significantly improved over time for a number of specific congenital anomalies. We have also provided predicted survival estimates for children born in 2020. This information has important implications for the planning and delivery of public health services, specialised medical care, and educational services and is valuable for clinicians, public health professionals, healthcare providers, and parents. We identified a lack of good-quality, reasonably sized studies for many congenital anomaly subtypes that prevented estimation of their pooled survival and analysis of trends over time. Future survival studies should endeavour to use multicentre case data from different parts of the world linked to reliable mortality data with follow-up from birth to avoid selection bias and underascertainment of deaths.

Supporting information

S1 Fig [tif]
Survival estimates (with 95% CI) of children with encephalocele at 1 year of age over time (4 studies).

S2 Fig [tif]
Survival with native liver (with 95% CI) of children with biliary atresia at 5 (a) and 10 (b) years of age over time (11 birth cohorts from 9 studies).

S3 Fig [tif]
Survival estimates (with 95% CI) of children with trisomy 18 (4 studies).

S1 Table [docx]
Search terms and search results in electronic databases Medline, Embase, and PsycInfo.

S2 Table [docx]
Data extraction form and Newcastle-Ottawa Quality Assessment Scale for cohort studies.

S3 Table [docx]
Quality-assessment scores of the included studies using the Newcastle-Ottawa Quality Assessment Scale for cohort studies.

S4 Table [docx]
Details of sources of case ascertainment and death identification of included studies and description of a comparison group.

S5 Table [docx]
Survival estimates by congenital anomaly type at age 1–25 years, overall and by risk factor.

S6 Table [docx]
Predictors of survival/mortality in the included studies that explored risk factors associated with survival at different age points, including infancy ( = 35), by congenital anomaly group/subtype.

S1 PRISMA Checklist [docx]
PRISMA, Preferred Reporting Items for Systematic Reviews and Meta-Analyses.

S1 Text [docx]
Protocol for PROSPERO registration.


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