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Infant deaths from congenital anomalies: novel use of Child Death Overview Panel data

Title: Infant deaths from congenital anomalies: novel use of Child Death Overview Panel data
Authors: Firth, Catriona; Petherick, Emily; Oddie, Sam J
Publisher Information: BMJ Publishing Group Ltd
Publication Year: 2018
Collection: HighWire Press (Stanford University)
Subject Terms: Original article
Description: Objective We aimed to assess Child Death Overview Panel (CDOP) data validity, and cause of death classification, by comparison with information from a local birth cohort study (Born in Bradford, BiB), and another cause of death coding system (causes of death and associated conditions—CODAC). We then aimed to use CDOP data to calculate ethnic-specific infant mortality rates (IMRs), and compare characteristics of infants who died of congenital anomalies (CA) with those who died from other causes (non-CA). Design Retrospective cohort study. Setting Bradford Metropolitan District. Patients All infant deaths, 2008 to 2013. Main outcome measures Infant mortality rates from CA and non-CA causes. Results 315 infant deaths were included, 56 of whom were BiB recruits. Agreement between CDOP and BiB was moderate to perfect for all characteristics except ethnicity, which showed weak agreement (kappa=0.58). The same deaths (27/56) were classified as CA by CDOP and CODAC. IMRs (per 1000 live births, 2009–2013) were highest in Pakistani infants (all causes 9.8, CA cause 5.5) compared with white British (all causes 4.3, CA cause 1.3) and other infants (all causes 5.1, CA cause 1.4). In multivariate analysis, infants who died of CA cause were more likely to have been born at term (OR 3.18) and to consanguineous parents (OR 3.28) than infants who died of non-CA cause. Conclusions Excess Pakistani mortality appears to be partly explained by an excess of deaths from CA, which in this population appears associated with a greater prevalence of consanguinity.
Document Type: text
File Description: text/html
Language: English
Relation: http://adc.bmj.com/cgi/content/short/103/11/1027; http://dx.doi.org/10.1136/archdischild-2017-314256
DOI: 10.1136/archdischild-2017-314256
Availability: http://adc.bmj.com/cgi/content/short/103/11/1027; https://doi.org/10.1136/archdischild-2017-314256
Rights: Copyright (C) 2018, BMJ Publishing Group Ltd
Accession Number: edsbas.DB69B06F
Database: BASE