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3. Higher risk of cerebral palsy, seizures/epilepsy, visual- and hearing impairments, cancer, injury and child abuse in children with congenital anomalies:Data from the EUROlinkCAT study

Author

Urhoj, Stine Kjaer, Morris, Joan, Loane, Maria, Ballardini, Elisa, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Gissler, Mika, Given, Joanne, Heino, Anna, Jordan, Sue, Neville, Amanda, Santoro, Michele, Tan, Joachim, Tucker, David, Wellesley, Diana, Garne, Ester, Damkjaer, Mads, Urhoj, Stine Kjaer, Morris, Joan, Loane, Maria, Ballardini, Elisa, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Gissler, Mika, Given, Joanne, Heino, Anna, Jordan, Sue, Neville, Amanda, Santoro, Michele, Tan, Joachim, Tucker, David, Wellesley, Diana, Garne, Ester, and Damkjaer, Mads

Abstract

AIM: The aim is to examine the risk of cerebral palsy, seizures/epilepsy, visual- and hearing impairments, cancer, injury/poisoning and child abuse in children with and without a congenital anomaly up to age 5 and 10 years.METHODS: This is a population-based data linkage cohort study linking information from the European Surveillance of Congenital Anomalies network (EUROCAT) and birth registries to hospital discharge databases. We included 91 504 live born children with major congenital anomalies born from 1995 to 2014 from nine EUROCAT registries in five countries and 1 960 727 live born children without congenital anomalies (reference children). Prevalence and relative risk (RR) were estimated for each of the co-morbidities using Kaplan-Meier survival estimates.RESULTS: Children with congenital anomalies had higher risks of the co-morbidities than reference children. The prevalences in the reference children were generally very low. The RR was 13.8 (95% CI 12.5-15.1) for cerebral palsy, 2.5 (95% CI 2.4-2.6) for seizures/epilepsy, 40.8 (95% CI 33.2-50.2) for visual impairments, 10.0 (95% CI 9.2-10.9) for hearing loss, 3.6 (95% CI 3.2-4.2) for cancer, 1.5 (95% CI 1.4-1.5) for injuries/poisoning and 2.4 (95% CI 1.7-3.4) for child abuse.CONCLUSION: Children with congenital anomalies were more likely to be diagnosed with the specified co-morbidities compared to reference children.

Published
2024

4. Higher risk of cerebral palsy, seizures/epilepsy, visual‐ and hearing impairments, cancer, injury and child abuse in children with congenital anomalies: Data from the EUROlinkCAT study

Author

Urhoj, Stine Kjaer, primary, Morris, Joan, additional, Loane, Maria, additional, Ballardini, Elisa, additional, Barrachina‐Bonet, Laia, additional, Cavero‐Carbonell, Clara, additional, Coi, Alessio, additional, Gissler, Mika, additional, Given, Joanne, additional, Heino, Anna, additional, Jordan, Sue, additional, Neville, Amanda, additional, Santoro, Michele, additional, Tan, Joachim, additional, Tucker, David, additional, Wellesley, Diana, additional, Garne, Ester, additional, and Damkjaer, Mads, additional

Published
2024
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5. Antiasthmatic prescriptions in children with and without congenital anomalies: a population-based study

Author

Divin, Natalie, primary, Given, Joanne Emma, additional, Tan, Joachim, additional, Astolfi, Gianni, additional, Ballardini, Elisa, additional, Barrachina-Bonet, Laia, additional, Cavero-Carbonell, Clara, additional, Coi, Alessio, additional, Garne, Ester, additional, Gissler, Mika, additional, Heino, Anna, additional, Jordan, Susan, additional, Pierini, Anna, additional, Scanlon, Ieuan, additional, Urhøj, Stine Kjær, additional, Morris, Joan K, additional, and Loane, Maria, additional

Published
2023
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6. Creating a population-based cohort of children born with and without congenital anomalies using birth data matched to hospital discharge databases in 11 European regions: Assessment of linkage success and data quality

Author

Loane, Maria, primary, Given, Joanne E., additional, Tan, Joachim, additional, Barišić, Ingeborg, additional, Barrachina-Bonet, Laia, additional, Cavero-Carbonell, Clara, additional, Coi, Alessio, additional, Densem, James, additional, Garne, Ester, additional, Gissler, Mika, additional, Heino, Anna, additional, Jordan, Sue, additional, Lutke, Renee, additional, Neville, Amanda J., additional, Odak, Ljubica, additional, Puccini, Aurora, additional, Santoro, Michele, additional, Scanlon, Ieuan, additional, Urhoj, Stine K., additional, de Walle, Hermien E. K., additional, Wellesley, Diana, additional, and Morris, Joan K., additional

Published
2023
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7. Prevalencia de la Telangiectasia Hemorrágica Hereditaria: estudio de base poblacional en la Comunitat Valenciana (España)

Author

Palomares, Miriam de la Natividad, Barrachina Bonet, Laia, Guardiola Vilarroig, Sandra, Zurriaga Llorens, Oscar, Cavero Carbonell, Clara, Palomares, Miriam de la Natividad, Barrachina Bonet, Laia, Guardiola Vilarroig, Sandra, Zurriaga Llorens, Oscar, and Cavero Carbonell, Clara

Abstract

BACKGROUND // The Hereditary Haemorrhagic Telangiectasia (HHT) is a low prevalence disease which presents heterogeneous signs and symptoms and just few population-based epidemiological studies are available. The aims of this paper were to describe the sociodemographic characteristics of people affected by HHT in the Valencian Region (VR), to determine its prevalence and mortality rate, and to analyse the sources of recruitment and verification tests used by the Rare Diseases Information System of the VR (SIER-CV). METHODS // Cross-sectional observational epidemiological study of HHT prevalent cases between 2010-2019 in SIER-CV was performed. The distribution of sociodemographic and clinical characteristics were determined, the prevalence and mortality rates, and the sources of recruitment and verification tests used by SIER-CV were analysed. Statistical analysis was performed using Stata (version 16.1) and Microsoft Excel Office. RESULTS // During 2010-2019, two hundred cases were identified, 55.5% were female. The mean ages were: 56.8 years at recruitment and 50.9 years at diagnosis. 48.4% of cases were diagnosed between thirty-six/sixty-four years of age. 25.5% died, with a mean age of 76.6 years, identifying statistically significant differences above the age of 64. The prevalence was 39.6/1,000,000 inhabitants and the crude mortality rate was 10.1/1,000,000 inhabitants. 95.5% of cases were recruited from the Hospital discharges database and the most frequent verification test was the clinical basis (45.7%). CONCLUSIONS // The increasing trend in prevalence coincides with a better knowledge of HHT, which favours its detection, and also with dying at older ages. To describe the situation of HHT in the VR facilitates its health management and contributes to the establishment of the relevant health policies for the HHT. The need to promote genetic diagnosis and to incorporate the Primary Care Clinical History as a source of recruitment in the population-based regist, FUNDAMENTOS // La Telangiectasia Hemorrágica Hereditaria (THH) es una enfermedad de baja prevalencia, que se presenta con signos y síntomas muy heterogéneos y de la que apenas se dispone de estudios epidemiológicos de base poblacional. Los objetivos de este estudio fueron describir las características sociodemográficas de las personas afectadas por THH en la Comunitat Valenciana (CV), determinar su prevalencia y mortalidad, y analizar las fuentes de captación y pruebas de verificación utilizadas por el Sistema de Información de Enfermedades Raras de la CV (SIER-CV). MÉTODOS // Se realizó un estudio epidemiológico observacional transversal de casos prevalentes de THH durante 2010-2019 en el SIER-CV. Se determinó la distribución de las características sociodemográficas y clínicas, la prevalencia y mortalidad, y se analizaron las fuentes de captación y pruebas de verificación utilizadas por SIER-CV. El análisis estadístico de los datos se realizó mediante el programa Stata (versión 16.1) y Microsoft Excel Office. RESULTADOS // Durante 2010-2019 se identificaron doscientos casos, de los que el 55,5% eran mujeres. Las edades medias fueron: de captación 56,8 años, y de diagnóstico 50,9 años. El 48,4% fueron diagnosticados entre los treinta y seis, y los sesenta y cuatro años. Fallecieron el 25,5%, con 76,6 años de edad media, identificándose diferencias estadísticamente significativas en mayores de sesenta y cuatro años. La prevalencia fue 39,6 por cada millón de habitantes y la tasa cruda de mortalidad de 10,1 por cada millón de habitantes. El 95,5% se captaron por el Conjunto Mínimo Básico de Datos y la prueba de verificación más frecuente fue la base clínica (45,7%). CONCLUSIONES // La tendencia ascendente de la prevalencia coincide con un mejor conocimiento de la THH, que facilita la detección de casos, y también con fallecimientos en edades avanzadas. Describir la situación de la THH en la CV facilita su manejo sanitario y contribuye al establecimiento de las polític

Published
2023

8. Antiasthmatic prescriptions in children with and without congenital anomalies:a population-based study

Author

Divin, Natalie, Given, Joanne Emma, Tan, Joachim, Astolfi, Gianni, Ballardini, Elisa, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Garne, Ester, Gissler, Mika, Heino, Anna, Jordan, Susan, Pierini, Anna, Scanlon, Ieuan, Urhøj, Stine Kjær, Morris, Joan K, Loane, Maria, Divin, Natalie, Given, Joanne Emma, Tan, Joachim, Astolfi, Gianni, Ballardini, Elisa, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Garne, Ester, Gissler, Mika, Heino, Anna, Jordan, Susan, Pierini, Anna, Scanlon, Ieuan, Urhøj, Stine Kjær, Morris, Joan K, and Loane, Maria

Abstract

OBJECTIVES: To explore the risk of being prescribed/dispensed medications for respiratory symptoms and breathing difficulties in children with and without congenital anomalies.DESIGN: A EUROlinkCAT population-based data linkage cohort study. Data on children with and without congenital anomalies were linked to prescription databases to identify children who did/did not receive antiasthmatic prescriptions. Data were analysed by age, European region, class of antiasthmatic, anomaly, sex, gestational age and birth cohort.SETTING: Children born 2000-2014 in six regions within five European countries.PARTICIPANTS: 60 662 children with congenital anomalies and 1 722 912 reference children up to age 10 years.PRIMARY OUTCOME MEASURE: Relative risks (RR) of >1 antiasthmatic prescription in a year, identified using Anatomical Therapeutic Chemical classification codes beginning with R03.RESULTS: There were significant differences in the prescribing of antiasthmatics in the six regions. Children with congenital anomalies had a significantly higher risk of being prescribed antiasthmatics (RR 1.41, 95% CI 1.35 to 1.48) compared with reference children. The increased risk was consistent across all regions and all age groups. Children with congenital anomalies were more likely to be prescribed beta-2 agonists (RR 1.71, 95% CI 1.60 to 1.83) and inhaled corticosteroids (RR 1.74, 95% CI 1.61 to 1.87). Children with oesophageal atresia, genetic syndromes and chromosomal anomalies had over twice the risk of being prescribed antiasthmatics compared with reference children. Children with congenital anomalies born <32 weeks gestational age were over twice as likely to be prescribed antiasthmatics than those born at term (RR 2.20, 95% CI 2.10 to 2.30).CONCLUSION: This study documents the additional burden of respiratory symptoms and breathing difficulties for children with congenital anomalies, particularly those born preterm, compared with

Published
2023

9. Creating a population-based cohort of children born with and without congenital anomalies using birth data matched to hospital discharge databases in 11 European regions:Assessment of linkage success and data quality

Author

Loane, Maria, Given, Joanne E, Tan, Joachim, Barišić, Ingeborg, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Densem, James, Garne, Ester, Gissler, Mika, Heino, Anna, Jordan, Sue, Lutke, Renee, Neville, Amanda J, Odak, Ljubica, Puccini, Aurora, Santoro, Michele, Scanlon, Ieuan, Urhoj, Stine K, de Walle, Hermien E K, Wellesley, Diana, Morris, Joan K, Loane, Maria, Given, Joanne E, Tan, Joachim, Barišić, Ingeborg, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Densem, James, Garne, Ester, Gissler, Mika, Heino, Anna, Jordan, Sue, Lutke, Renee, Neville, Amanda J, Odak, Ljubica, Puccini, Aurora, Santoro, Michele, Scanlon, Ieuan, Urhoj, Stine K, de Walle, Hermien E K, Wellesley, Diana, and Morris, Joan K

Abstract

Linking routinely collected healthcare administrative data is a valuable method for conducting research on morbidity outcomes, but linkage quality and accuracy needs to be assessed for bias as the data were not collected for research. The aim of this study was to describe the rates of linking data on children with and without congenital anomalies to regional or national hospital discharge databases and to evaluate the quality of the matched data. Eleven population-based EUROCAT registries participated in a EUROlinkCAT study linking data on children with a congenital anomaly and children without congenital anomalies (reference children) born between 1995 and 2014 to administrative databases including hospital discharge records. Odds ratios (OR), adjusted by region, were estimated to assess the association of maternal and child characteristics on the likelihood of being matched. Data on 102,654 children with congenital anomalies were extracted from 11 EUROCAT registries and 2,199,379 reference children from birth registers in seven regions. Overall, 97% of children with congenital anomalies and 95% of reference children were successfully matched to administrative databases. Information on maternal age, multiple birth status, sex, gestational age and birthweight were >95% complete in the linked datasets for most regions. Compared with children born at term, those born at ≤27 weeks and 28-31 weeks were less likely to be matched (adjusted OR 0.23, 95% CI 0.21-0.25 and adjusted OR 0.75, 95% CI 0.70-0.81 respectively). For children born 32-36 weeks, those with congenital anomalies were less likely to be matched (adjusted OR 0.78, 95% CI 0.71-0.85) while reference children were more likely to be matched (adjusted OR 1.28, 95% CI 1.24-1.32). Children born to teenage mothers and mothers ≥35 years were less likely to be matched compared with mothers aged 20-34 years (adjusted ORs 0.92, 95% CI 0.88-0.96; and 0.87, 95% CI 0.86-0.89 respectively). The accuracy of linkage an

Published
2023

10. Prescriptions for insulin and insulin analogues in children with and without major congenital anomalies:a data linkage cohort study across six European regions

Author

Given, Joanne, Morris, Joan K, Garne, Ester, Ballardini, Elisa, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Gissler, Mika, Gorini, Francesca, Heino, Anna, Jordan, Sue, Neville, Amanda J, Pierini, Anna, Scanlon, Ieuan, Tan, Joachim, Urhoj, Stine K, Loane, Maria, Given, Joanne, Morris, Joan K, Garne, Ester, Ballardini, Elisa, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Gissler, Mika, Gorini, Francesca, Heino, Anna, Jordan, Sue, Neville, Amanda J, Pierini, Anna, Scanlon, Ieuan, Tan, Joachim, Urhoj, Stine K, and Loane, Maria

Abstract

UNLABELLED: Are children with major congenital anomalies more likely to develop diabetes requiring insulin therapy, as indicated by prescriptions for insulin, than children without congenital anomalies? The aim of this study is to evaluate prescription rates of insulin/insulin analogues in children aged 0-9 years with and without major congenital anomalies. A EUROlinkCAT data linkage cohort study, involving six population-based congenital anomaly registries in five countries. Data on children with major congenital anomalies (60,662) and children without congenital anomalies (1,722,912), the reference group, were linked to prescription records. Birth cohort and gestational age were examined. The mean follow-up for all children was 6.2 years. In children with congenital anomalies aged 0-3 years, 0.04 per 100 child-years (95% CIs 0.01-0.07) had > 1 prescription for insulin/insulin analogues compared with 0.03 (95% CIs 0.01-0.06) in reference children, increasing ten-fold by age 8-9 years. The risk of > 1 prescription for insulin/insulin analogues aged 0-9 years in children with non-chromosomal anomalies (RR 0.92, 95% CI 0.84-1.00) was similar to that of reference children. However, children with chromosomal anomalies (RR 2.37, 95% CI 1.91-2.96), and specifically children with Down syndrome (RR 3.44, 95% CIs 2.70-4.37), Down syndrome with congenital heart defects (RR 3.86, 95% CIs 2.88-5.16) and Down syndrome without congenital heart defects (RR 2.78, 95% CIs 1.82-4.27), had a significantly increased risk of > 1 prescription for insulin/insulin analogues aged 0-9 years compared to reference children. Female children had a reduced risk of > 1 prescription aged 0-9 years compared with male children (RR 0.76, 95% CI 0.64-0.90 for children with congenital anomalies and RR 0.90, 95% CI 0.87-0.93 for reference children). Children without congenital anomalies born preterm (< 37 weeks) were more likely to have > 1 insulin/insulin analogue prescription compa

Published
2023

12. Wilson's disease in Spain: validation of sources of information used by the Rare Diseases Registries

Author

Moreno-Marro, Sandra, Barrachina-Bonet, Laia, Páramo-Rodríguez, Lucía, Alonso-Ferreira, Veronica, Guardiola-Vilarroig, Sandra, Vicente, Esther, García-López, María, Palomar-Rodríguez, Joaquín, Zoni, Ana Clara, Zurriaga, Óscar, Cavero-Carbonell, Clara, Grupo de trabajo Wilson-RAER, Fundació Per Amor a l’Art, Universidad Pública de Navarra. Departamento de Ciencias de la Salud, and Nafarroako Unibertsitate Publikoa. Osasun Zientziak Saila

Subjects
Adult, Male, medicine.medical_specialty, Health information systems, Epidemiology, Population, Enfermedad de Wilson, Primary care, Sistemas de información en salud, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Hepatolenticular Degeneration, Clinical history, Prevalence, medicine, Epidemiología, Humans, Registries, 030212 general & internal medicine, Fuentes de datos, education, Wilson disease, Gynecology, education.field_of_study, 030505 public health, Enfermedades raras, business.industry, Public Health, Environmental and Occupational Health, Hospital discharge database, Data sources, Atencion primaria, Predictive value, Rare diseases, Cross-Sectional Studies, Spain, Female, Public aspects of medicine, RA1-1270, Prevalencia, 0305 other medical science, business
Abstract

[ES] Objetivo: Evaluar las fuentes de información empleadas por los Registros Autonómicos de Enfermedades Raras (RAER) para la captación de la enfermedad de Wilson en España, calcular su prevalencia y mortalidad, y describir las características sociodemográficas de las personas afectadas. Método: Estudio epidemiológico transversal, periodo 2010-2015. Se captaron los posibles casos mediante los códigos 275.1 (CIE-9-MC), E83.0 (CIE-10) y 905 ORPHA en 15 RAER y el Registro de Pacientes de Enfermedades Raras del Instituto de Salud Carlos III. Los diagnósticos fueron validados revisando la documentación clínica. Se calcularon el valor predictivo positivo (VPP) de las fuentes de información, la prevalencia, la mortalidad y la distribución de las características sociodemográficas. Resultados: El Conjunto Mínimo Básico de Datos (CMBD) fue la fuente de información más utilizada por los RAER (VPP = 39,4%), seguida del Registro de Medicamentos Huérfanos (RMH) (VPP = 81,9%). La Historia Clínica de Atención Primaria (HCAP) obtuvo un VPP del 55,9%. Las combinaciones con mayor VPP fueron las del RMH con el CMBD (VPP = 95,8%) y del RMH con la HCAP (VPP = 92,9%). Se confirmaron 514 casos, el 57,2% eran hombres, cuya edad mediana de diagnóstico fue de 21,3 años. La prevalencia fue de 1,64/100.000 habitantes en 2015 y la mortalidad del 3,0%, siendo ambas superiores en los hombres. Conclusión: Se recomienda la incorporación en los RAER del RMH y de la HCAP, ya que su combinación y la del RMH con el CMBD podrían utilizarse como criterio de validación automática para la enfermedad de Wilson. La prevalencia obtenida fue similar a la de otros países próximos a España. [EN] Objective: To evaluate the sources of information used by the Regional Population-based Registries of Rare Diseases (RRD) for Wilson's Disease identification in Spain; to calculate its prevalence and mortality; and to describe the sociodemographic characteristics of those affected. Method: Cross-sectional epidemiological study, period 2010-2015. Possible cases were identified by codes 275.1 (ICD-9-CM), E83.0 (ICD-10) and 905 (ORPHAcode) in: 15 participating RRD and the Rare Disease Patients Registry of the Carlos III Health Institute. The diagnoses were confirmed through a clinical documentation review. The positive predictive value (PPV) of the sources of information used by RRD and their combinations were obtained. The prevalence, mortality and the distribution of sociodemographic characteristics were calculated. Results: The Hospital Discharge Database (HDD) was the most used source by the RRD (PPV=39.4%), followed by the Orphan Drugs Registry (ODR) (PPV=81.9%). The Clinical History of Primary Care (PC) obtains PPV=55.9%. The combinations with highest PPV were the ODR with HDD (PPV=95.8%) and the ODR with PC (PPV=92.9%). 514 cases were confirmed, 57.2% men, with a median age of diagnosis of 21.3 years. The prevalence was 1.64/100,000 inhabitants in 2015 and mortality rate was 3.0%, being both higher in men. Conclusions: Incorporation of ODR and PC into the RRD is recommended, as its combination and ODR with HDD could be used as an automatic validation criterion for Wilson's disease. The prevalence obtained was similar to that of countries close to Spain. Este proyecto ha sido posible gracias a los fondos recibidos por la Fundació Per Amor a l’Art (Convenio CPRESC00043). Sí

Published
2021
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13. Prescriptions for insulin and insulin analogues in children with and without major congenital anomalies: A data linkage cohort study across six European regions

Author

Given, Joanne, primary, Morris, Joan K., additional, Garne, Ester, additional, Ballardini, Elisa, additional, Barrachina-Bonet, Laia, additional, Cavero-Carbonell, Clara, additional, Gissler, Mika, additional, Gorini, Francesca, additional, Heino, Anna, additional, Jordan, Sue, additional, Neville, Amanda J., additional, Pierini, Anna, additional, Scanlon, Ieuan, additional, Tan, Joachim, additional, Urhoj, Stine K., additional, and Loane, Maria, additional

Published
2022
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14. From Inception to ConcePTION: Genesis of a Network to Support Better Monitoring and Communication of Medication Safety During Pregnancy and Breastfeeding

Author

Thurin, Nicolas H, Pajouheshnia, Romin, Roberto, Giuseppe, Dodd, Caitlin, Hyeraci, Giulia, Bartolini, Claudia, Paoletti, Olga, Nordeng, Hedvig, Wallach-Kildemoes, Helle, Ehrenstein, Vera, Dudukina, Elena, MacDonald, Thomas, De Paoli, Giorgia, Loane, Maria, Damase-Michel, Christine, Beau, Anna-Belle, Droz-Perroteau, Cécile, Lassalle, Régis, Bergman, Jorieke, Swart, Karin, Schink, Tania, Cavero-Carbonell, Clara, Barrachina-Bonet, Laia, Gomez-Lumbreras, Ainhoa, Giner-Soriano, Maria, Aragón, María, Neville, Amanda J, Puccini, Aurora, Pierini, Anna, Ientile, Valentina, Trifirò, Gianluca, Rissmann, Anke, Leinonen, Maarit K, Martikainen, Visa, Jordan, Sue, Thayer, Daniel, Scanlon, Ieuan, Georgiou, Mary E, Cunnington, Marianne, Swertz, Morris, Sturkenboom, Miriam, Gini, Rosa, Thurin, Nicolas H, Pajouheshnia, Romin, Roberto, Giuseppe, Dodd, Caitlin, Hyeraci, Giulia, Bartolini, Claudia, Paoletti, Olga, Nordeng, Hedvig, Wallach-Kildemoes, Helle, Ehrenstein, Vera, Dudukina, Elena, MacDonald, Thomas, De Paoli, Giorgia, Loane, Maria, Damase-Michel, Christine, Beau, Anna-Belle, Droz-Perroteau, Cécile, Lassalle, Régis, Bergman, Jorieke, Swart, Karin, Schink, Tania, Cavero-Carbonell, Clara, Barrachina-Bonet, Laia, Gomez-Lumbreras, Ainhoa, Giner-Soriano, Maria, Aragón, María, Neville, Amanda J, Puccini, Aurora, Pierini, Anna, Ientile, Valentina, Trifirò, Gianluca, Rissmann, Anke, Leinonen, Maarit K, Martikainen, Visa, Jordan, Sue, Thayer, Daniel, Scanlon, Ieuan, Georgiou, Mary E, Cunnington, Marianne, Swertz, Morris, Sturkenboom, Miriam, and Gini, Rosa

Abstract

In 2019, the Innovative Medicines Initiative (IMI) funded the ConcePTION project-Building an ecosystem for better monitoring and communicating safety of medicines use in pregnancy and breastfeeding: validated and regulatory endorsed workflows for fast, optimised evidence generation-with the vision that there is a societal obligation to rapidly reduce uncertainty about the safety of medication use in pregnancy and breastfeeding. The present paper introduces the set of concepts used to describe the European data sources involved in the ConcePTION project and illustrates the ConcePTION Common Data Model (CDM), which serves as the keystone of the federated ConcePTION network. Based on data availability and content analysis of 21 European data sources, the ConcePTION CDM has been structured with six tables designed to capture data from routine healthcare, three tables for data from public health surveillance activities, three curated tables for derived data on population (e.g., observation time and mother-child linkage), plus four metadata tables. By its first anniversary, the ConcePTION CDM has enabled 13 data sources to run common scripts to contribute to major European projects, demonstrating its capacity to facilitate effective and transparent deployment of distributed analytics, and its potential to address questions about utilization, effectiveness, and safety of medicines in special populations, including during pregnancy and breastfeeding, and, more broadly, in the general population.

Published
2022

15. From Inception to ConcePTION: Genesis of a Network to Support Better Monitoring and Communication of Medication Safety During Pregnancy and Breastfeeding

Author

Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, Thurin, Nicolas H, Pajouheshnia, Romin, Roberto, Giuseppe, Dodd, Caitlin, Hyeraci, Giulia, Bartolini, Claudia, Paoletti, Olga, Nordeng, Hedvig, Wallach-Kildemoes, Helle, Ehrenstein, Vera, Dudukina, Elena, MacDonald, Thomas, De Paoli, Giorgia, Loane, Maria, Damase-Michel, Christine, Beau, Anna-Belle, Droz-Perroteau, Cécile, Lassalle, Régis, Bergman, Jorieke, Swart, Karin, Schink, Tania, Cavero-Carbonell, Clara, Barrachina-Bonet, Laia, Gomez-Lumbreras, Ainhoa, Giner-Soriano, Maria, Aragón, María, Neville, Amanda J, Puccini, Aurora, Pierini, Anna, Ientile, Valentina, Trifirò, Gianluca, Rissmann, Anke, Leinonen, Maarit K, Martikainen, Visa, Jordan, Sue, Thayer, Daniel, Scanlon, Ieuan, Georgiou, Mary E, Cunnington, Marianne, Swertz, Morris, Sturkenboom, Miriam, Gini, Rosa, Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, Thurin, Nicolas H, Pajouheshnia, Romin, Roberto, Giuseppe, Dodd, Caitlin, Hyeraci, Giulia, Bartolini, Claudia, Paoletti, Olga, Nordeng, Hedvig, Wallach-Kildemoes, Helle, Ehrenstein, Vera, Dudukina, Elena, MacDonald, Thomas, De Paoli, Giorgia, Loane, Maria, Damase-Michel, Christine, Beau, Anna-Belle, Droz-Perroteau, Cécile, Lassalle, Régis, Bergman, Jorieke, Swart, Karin, Schink, Tania, Cavero-Carbonell, Clara, Barrachina-Bonet, Laia, Gomez-Lumbreras, Ainhoa, Giner-Soriano, Maria, Aragón, María, Neville, Amanda J, Puccini, Aurora, Pierini, Anna, Ientile, Valentina, Trifirò, Gianluca, Rissmann, Anke, Leinonen, Maarit K, Martikainen, Visa, Jordan, Sue, Thayer, Daniel, Scanlon, Ieuan, Georgiou, Mary E, Cunnington, Marianne, Swertz, Morris, Sturkenboom, Miriam, and Gini, Rosa

Published
2022

16. Prescription of cardiovascular medication in children with congenital heart defects across six European Regions from 2000 to 2014:data from the EUROlinkCAT population-based cohort study

Author

Damkjaer, Mads, Urhøj, Stine Kjær, Tan, Joachim, Briggs, Gillian, Loane, Maria, Given, Joanne Emma, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Neville, Amanda J, Heino, Anna, Kiuru-Kuhlefelt, Sonja, Jordan, Susan, Scanlon, Ieuan, Pierini, Anna, Puccini, Aurora, Garne, Ester, Morris, Joan K, Damkjaer, Mads, Urhøj, Stine Kjær, Tan, Joachim, Briggs, Gillian, Loane, Maria, Given, Joanne Emma, Barrachina-Bonet, Laia, Cavero-Carbonell, Clara, Coi, Alessio, Neville, Amanda J, Heino, Anna, Kiuru-Kuhlefelt, Sonja, Jordan, Susan, Scanlon, Ieuan, Pierini, Anna, Puccini, Aurora, Garne, Ester, and Morris, Joan K

Abstract

OBJECTIVES: Advances in surgical management strategies have substantially reduced fatality from congenital heart defects (CHD). Decreased infant mortality might be expected, consequentially to result in greater morbidity in older children due to complications later in childhood and adolescence. This study aims to evaluate the use of cardiovascular medication (CVM) as an indicator of disease burden in children born with CHD in the first 10 years of life.DESIGN: Population-based cohort study.SETTING: Six population-based registries from the European Surveillance of Congenital Anomalies (EUROCAT) network participated. Data from live born children with major congenital anomalies (CA) born from 2000 to 2014 were linked to prescription databases. Four groups of children were analysed: CA, CHD, severe CHD (sCHD) and ventricular septal defect (VSD) without sCHD. Live born children without CA were included as reference group.PARTICIPANTS: We obtained data on 61 038 children born with a CA, including 19 678 with CHD, 3392 with sCHD, 12 728 children with VSD without sCHD, and 1 725 496 reference children.RESULTS: Children born with sCHD were the most likely to receive a CVM prescription (42.9%, 95% CI, 26.3 to 58.5) in the first year of life compared with 13.3% (6.7 to 22.0) of children with any CHD, 5.9% (3.7 to 8.7) of children with any CA and 0.1% (0.0 to 0.1) of reference children. Medication was less likely to be prescribed after the first year of life for sCHD; 18.8% (14.8 to 23.1) for children 1-4 years and 15.8% (12.0 to 20.1) 5-9 years. Children with sCHD were most likely to receive a diuretic (36.4%, 18.6 to 54.5), an antihypertensive (6.9%, 3.7 to 11.3) or a beta-blocker (5.5%, 2.9 to9.2).CONCLUSION: Almost half of all children with sCHD were prescribed CVM in their first year of life. For all four groups of children with anomalies, the proportion of children with a CVM prescription decreased with age.

Published
2022

17. From Inception to ConcePTION: Genesis of a Network to Support Better Monitoring and Communication of Medication Safety During Pregnancy and Breastfeeding

Author

Data Science & Biostatistiek, Thurin, Nicolas H, Pajouheshnia, Romin, Roberto, Giuseppe, Dodd, Caitlin, Hyeraci, Giulia, Bartolini, Claudia, Paoletti, Olga, Nordeng, Hedvig, Wallach-Kildemoes, Helle, Ehrenstein, Vera, Dudukina, Elena, MacDonald, Thomas, De Paoli, Giorgia, Loane, Maria, Damase-Michel, Christine, Beau, Anna-Belle, Droz-Perroteau, Cécile, Lassalle, Régis, Bergman, Jorieke, Swart, Karin, Schink, Tania, Cavero-Carbonell, Clara, Barrachina-Bonet, Laia, Gomez-Lumbreras, Ainhoa, Giner-Soriano, Maria, Aragón, María, Neville, Amanda J, Puccini, Aurora, Pierini, Anna, Ientile, Valentina, Trifirò, Gianluca, Rissmann, Anke, Leinonen, Maarit K, Martikainen, Visa, Jordan, Sue, Thayer, Daniel, Scanlon, Ieuan, Georgiou, Mary E, Cunnington, Marianne, Swertz, Morris, Sturkenboom, Miriam, Gini, Rosa, Data Science & Biostatistiek, Thurin, Nicolas H, Pajouheshnia, Romin, Roberto, Giuseppe, Dodd, Caitlin, Hyeraci, Giulia, Bartolini, Claudia, Paoletti, Olga, Nordeng, Hedvig, Wallach-Kildemoes, Helle, Ehrenstein, Vera, Dudukina, Elena, MacDonald, Thomas, De Paoli, Giorgia, Loane, Maria, Damase-Michel, Christine, Beau, Anna-Belle, Droz-Perroteau, Cécile, Lassalle, Régis, Bergman, Jorieke, Swart, Karin, Schink, Tania, Cavero-Carbonell, Clara, Barrachina-Bonet, Laia, Gomez-Lumbreras, Ainhoa, Giner-Soriano, Maria, Aragón, María, Neville, Amanda J, Puccini, Aurora, Pierini, Anna, Ientile, Valentina, Trifirò, Gianluca, Rissmann, Anke, Leinonen, Maarit K, Martikainen, Visa, Jordan, Sue, Thayer, Daniel, Scanlon, Ieuan, Georgiou, Mary E, Cunnington, Marianne, Swertz, Morris, Sturkenboom, Miriam, and Gini, Rosa

Published
2022

18. Prescription of cardiovascular medication in children with congenital heart defects across six European Regions from 2000 to 2014: data from the EUROlinkCAT population-based cohort study

Author

Damkjaer, Mads, primary, Urhoj, Stine Kjaer, additional, Tan, Joachim, additional, Briggs, Gillian, additional, Loane, Maria, additional, Given, Joanne Emma, additional, Barrachina-Bonet, Laia, additional, Cavero-Carbonell, Clara, additional, Coi, Alessio, additional, Neville, Amanda J, additional, Heino, Anna, additional, Kiuru-Kuhlefelt, Sonja, additional, Jordan, Susan, additional, Scanlon, Ieuan, additional, Pierini, Anna, additional, Puccini, Aurora, additional, Garne, Ester, additional, and Morris, Joan K, additional

Published
2022
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19. From Inception to ConcePTION: Genesis of a Network to Support Better Monitoring and Communication of Medication Safety During Pregnancy and Breastfeeding

Author

Thurin, Nicolas H., primary, Pajouheshnia, Romin, additional, Roberto, Giuseppe, additional, Dodd, Caitlin, additional, Hyeraci, Giulia, additional, Bartolini, Claudia, additional, Paoletti, Olga, additional, Nordeng, Hedvig, additional, Wallach‐Kildemoes, Helle, additional, Ehrenstein, Vera, additional, Dudukina, Elena, additional, MacDonald, Thomas, additional, De Paoli, Giorgia, additional, Loane, Maria, additional, Damase‐Michel, Christine, additional, Beau, Anna‐Belle, additional, Droz‐Perroteau, Cécile, additional, Lassalle, Régis, additional, Bergman, Jorieke, additional, Swart, Karin, additional, Schink, Tania, additional, Cavero‐Carbonell, Clara, additional, Barrachina‐Bonet, Laia, additional, Gomez‐Lumbreras, Ainhoa, additional, Giner‐Soriano, Maria, additional, Aragón, María, additional, Neville, Amanda J., additional, Puccini, Aurora, additional, Pierini, Anna, additional, Ientile, Valentina, additional, Trifirò, Gianluca, additional, Rissmann, Anke, additional, Leinonen, Maarit K., additional, Martikainen, Visa, additional, Jordan, Sue, additional, Thayer, Daniel, additional, Scanlon, Ieuan, additional, Georgiou, Mary E., additional, Cunnington, Marianne, additional, Swertz, Morris, additional, Sturkenboom, Miriam, additional, and Gini, Rosa, additional

Published
2021
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20. Inception to ConcePTION: A conceptual framework for characterizing pharmacoepidemiologic data sources. A study from the ConcePTION project

Author

Pajouheshnia, Romin, Thurin, Nicolas H., Roberto, Giuseppe, Dodd, Caitlin, Hyeraci, Giulia, Bartolini, Claudia, Paoletti, Olga, Nordeng, Hedvig, Wallach-Kildemoes, Helle, Ehrenstein, Vera, Dudukina, Elena, Macdonald, Thomas, Paoli, Giorgia, Loane, Maria, Damase-Michel, Christine, Beau, Anna-Belle, Droz-Perroteau, Cecile, Lassalle, Regis, Swart-Polinder, Karin, Schink, Tania, Cavero-Carbonell, Clara, Barrachina-Bonet, Laia, Gomez-Lumbreras, Ainhoa, Giner-Soriano, Maria, Aragon, Maria, Neville, Amanda J., Armaroli, Annarita, Puccini, Aurora, Pierini, Anna, Ientile, Valentina, Trifiro, Gianluca, Gatt, Miriam, Rissmann, Anke, Leinonen, Maarit K., Martikainen, Visa, Jordan, Sue, Georgiou, Mary E., Cunnington, Marianne, Sturkenboom, Miriam, and Rosa Gini

Published
2021

21. Vigilancia epidemiológica de las anomalías congénitas cardíacas: La Tetralogía de Fallot en la Comunitat Valenciana, 2007-2017

Author

Cavero Carbonell, Clara, García Villodre, Laura, Barrachina Bonet, Laia, Moreno Marro, Sandra, Páramo Rodríguez, Lucía, Guardiola Vilarroig, Sandra, Zurriaga Llorens, Oscar, Cavero Carbonell, Clara, García Villodre, Laura, Barrachina Bonet, Laia, Moreno Marro, Sandra, Páramo Rodríguez, Lucía, Guardiola Vilarroig, Sandra, and Zurriaga Llorens, Oscar

Abstract

Background: Tetralogy of Fallot is characterized by the presence of four congenital heart defects. Objective: to describe the temporal trend and distribution of Tetralogy of Fallot, in children under one year in the Valencian Region. Methods: Cases with Tetralogy of Fallot (code Q21.3 from the ICD10-British Paediatric Association) were selected from the Congenital Anomalies Population-based Registry between 2007-2017. Prevalence per 10,000 births with 95%CI was calculated, and a descriptive analysis of sociodemographic and clinical variables was made. Results: 165 cases were identified (43.6% male, 30.9% female and 25.5% unknown). The overall prevalence was 3.1/10,000 births (95%CI:2.6–3.6), being 2015 and 2017 the years with the highest (4.3/10,000 births and 4.7/10,000 births respectively) and 2011 with the lowest (1.8/10,000 births). 72.1% were live births, 24.8% Termination of Pregnancy for Fetal Anomaly (TOPFA) and 3.0% stillbirths. The prevalence in live births was 2.2/10,000 births (95%CI:1.8-2.7) and in TOPFA it was 0.8/10,000 births (95%CI:0.5-1.0), identifying an increasing trend along the period in the last one. 10.1% of live births died during the first year of life and 55.8% were diagnosed prenatally. Mothers younger than 20 years had the highest prevalence (4.8/10,000 births). Conclusions: The prevalence obtained in the Valencian Region was slightly lower than EUROCAT’s but coincides with that of the registries that are closer geographically, and in all of them it is noted that their increasing trend specifically affects cases ending in TOPFA., Fundamentos: La Tetralogía de Fallot está caracterizada por la presencia de cuatro anomalías congénitas cardíacas. El objetivo de este trabajo fue describir la tendencia temporal y distribución de la Tetralogía de Fallot en menores de un año en la Comunitat Valenciana. Métodos: Se seleccionaron los casos con Tetralogía de Fallot (código Q21.3 de la CIE10 de la Asociación Pediátrica Británica) nacidos entre 2007-2017 del Registro Poblacional de anomalías congénitas de la Comunitat Valenciana. Se calculó la prevalencia por 10.000 nacimientos con IC95% y se realizó un análisis descriptivo de las variables sociodemográficas y clínicas. Resultados: Se identificaron 165 casos (43,6% niños, 30,9% niñas y 25,5% de sexo desconocido). La prevalencia global fue 3,1/10.000 nacimientos (IC95%:2,6– 3,6), siendo los años de mayor prevalencia 2015 y 2017 (4,3/10.000 nacimientos y 4,7/10.000 nacimientos respectivamente) y 2011 el de menor (1,8/10.000 nacimientos). El 72,1% fueron nacidos vivos, el 24,8% Interrupciones Voluntarias del Embarazo y el 3,0% nacidos muertos. La prevalencia en nacidos vivos fue 2,2/10.000 nacimientos (IC95%:1,8-2,7) y en Interrupciones Voluntarias del Embarazo fue 0,8/10.000 nacimientos (IC95%:0,5-1,0), identificándose en la segunda una tendencia en aumento a lo largo del periodo. El 10,1% de nacidos vivos fallecieron durante el primer año de vida y el 55,8% se diagnosticaron prenatalmente. El grupo con mayor prevalencia fueron las embarazadas menores de 20 años (4,8/10.000 nacimientos). Conclusiones: La prevalencia obtenida en la Comunitat Valenciana fue ligeramente inferior a la de EUROCAT pero coincide con la de registros próximos geográficamente, y en todos ellos destaca que su tendencia creciente afecta específicamente a casos que finalizan en Interrupciones Voluntarias del Embarazo.

Published
2021

22. Prevention of Neural Tube Defects in Europe: A Public Health Failure

Author

Morris, Joan K., primary, Addor, Marie-Claude, additional, Ballardini, Elisa, additional, Barisic, Ingeborg, additional, Barrachina-Bonet, Laia, additional, Braz, Paula, additional, Cavero-Carbonell, Clara, additional, Den Hond, Elly, additional, Garne, Ester, additional, Gatt, Miriam, additional, Haeusler, Martin, additional, Khoshnood, Babak, additional, Lelong, Nathalie, additional, Kinsner-Ovaskainen, Agnieszka, additional, Kiuru-Kuhlefelt, Sonja, additional, Klungsoyr, Kari, additional, Latos-Bielenska, Anna, additional, Limb, Elizabeth, additional, O'Mahony, Mary T, additional, Perthus, Isabelle, additional, Pierini, Anna, additional, Rankin, Judith, additional, Rissmann, Anke, additional, Rouget, Florence, additional, Sayers, Gerardine, additional, Sipek, Antonin, additional, Stevens, Sarah, additional, Tucker, David, additional, Verellen-Dumoulin, Christine, additional, de Walle, Hermien E. K., additional, Wellesley, Diana, additional, Wertelecki, Wladimir, additional, and Bermejo-Sanchez, Eva, additional

Published
2021
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23. Epidemiological surveillance of congenital heart defects: the Tetralogy of Fallot in the Valencian Region, 2007-2017

Author

Cavero-Carbonell, Clara, Laura Garcia Villodre, Barrachina-Bonet, Laia, Moreno-Marro, Sandra, Paramo-Rodriguez, Lucia, Guardiola-Vilarroig, Sandra, and Zurriaga-Llorens, Oscar

Subjects
Congenital anomalies, Population registry, Epidemiology, Tetralogy of Fallot, Prevalence
Abstract

Background: Tetralogy of Fallot is characterized by the presence of four congenital heart defects. Objective: to describe the temporal trend and distribution of Tetralogy of Fallot. in children under one year in the Valencian Region. Methods: Cases with Tetralogy of Fallot (code Q21.3 from the ICD10-British Paediatric Association) were selected from the Congenital Anomalies Population-based Registry between 2007-2017. Prevalence per 10,000 births with 95%CI was calculated, and a descriptive analysis of sociodemographic and clinical variables was made. Results: 165 cases were identified (43.6% male. 30.9% female and 25.5% unknown). The overall prevalence was 3.1/10,000 births (95%CI:2.6 3.6), being 2015 and 2017 the years with the highest (4.3/10.000 births and 4.7/10,000 births respectively) and 2011 with the lowest (1.8/10,000 births). 72.1% were live births, 24.8% Termination of Pregnancy for Fetal Anomaly (TOPFA) and 3.0% stillbirths. The prevalence in live births was 2.2/10.000 births (95%CI:1.8-2.7) and in TOPFA it was 0.810,000 births (95%CI:0.5-1.0). identifying an increasing trend along the period in the last one. 10.1% of live births died during the first year of life and 55.8% were diagnosed prenatally. Mothers younger than 20 years had the highest prevalence (4.8/10,000 births). Conclusions: The prevalence obtained in the Valencian Region was slightly lower than EUROCAT's but coincides with that of the registries that are closer geographically, and in all of them it is noted that their increasing trend specifically affects cases ending in TOPFA.

24. [Prevalencia de la Telangiectasia Hemorrágica Hereditaria: estudio de base poblacional en la Comunitat Valenciana (España).]

Author

de la Natividad Palomares M, Barrachina-Bonet L, García-Villodre L, Guardiola-Vilarroig S, Zurriaga Llorens Ó, and Cavero-Carbonell C

Subjects
Humans, Female, Aged, Middle Aged, Male, Cross-Sectional Studies, Spain, Death, Prevalence, Telangiectasia, Hereditary Hemorrhagic epidemiology, Telangiectasia, Hereditary Hemorrhagic diagnosis, Telangiectasia, Hereditary Hemorrhagic genetics
Abstract

Objective: The Hereditary Haemorrhagic Telangiectasia (HHT) is a low prevalence disease which presents heterogeneous signs and symptoms and just few population-based epidemiological studies are available. The aims of this paper were to describe the sociodemographic characteristics of people affected by HHT in the Valencian Region (VR), to determine its prevalence and mortality rate, and to analyse the sources of recruitment and verification tests used by the Rare Diseases Information System of the VR (SIER-CV)., Methods: Cross-sectional observational epidemiological study of HHT prevalent cases between 2010-2019 in SIER-CV was performed. The distribution of sociodemographic and clinical characteristics were determined, the prevalence and mortality rates, and the sources of recruitment and verification tests used by SIER-CV were analysed. Statistical analysis was performed using Stata (version 16.1) and Microsoft Excel Office., Results: During 2010-2019, two hundred cases were identified, 55.5% were female. The mean ages were: 56.8 years at recruitment and 50.9 years at diagnosis. 48.4% of cases were diagnosed between thirty-six/sixty-four years of age. 25.5% died, with a mean age of 76.6 years, identifying statistically significant differences above the age of 64. The prevalence was 39.6/1,000,000 inhabitants and the crude mortality rate was 10.1/1,000,000 inhabitants. 95.5% of cases were recruited from the Hospital discharges database and the most frequent verification test was the clinical basis (45.7%)., Conclusions: The increasing trend in prevalence coincides with a better knowledge of HHT, which favours its detection, and also with dying at older ages. To describe the situation of HHT in the VR facilitates its health management and contributes to the establishment of the relevant health policies for the HHT. The need to promote genetic diagnosis and to incorporate the Primary Care Clinical History as a source of recruitment in the population-based registries has been shown.

Published
2023

25. From Inception to ConcePTION: Genesis of a Network to Support Better Monitoring and Communication of Medication Safety During Pregnancy and Breastfeeding.

Author

Thurin NH, Pajouheshnia R, Roberto G, Dodd C, Hyeraci G, Bartolini C, Paoletti O, Nordeng H, Wallach-Kildemoes H, Ehrenstein V, Dudukina E, MacDonald T, De Paoli G, Loane M, Damase-Michel C, Beau AB, Droz-Perroteau C, Lassalle R, Bergman J, Swart K, Schink T, Cavero-Carbonell C, Barrachina-Bonet L, Gomez-Lumbreras A, Giner-Soriano M, Aragón M, Neville AJ, Puccini A, Pierini A, Ientile V, Trifirò G, Rissmann A, Leinonen MK, Martikainen V, Jordan S, Thayer D, Scanlon I, Georgiou ME, Cunnington M, Swertz M, Sturkenboom M, and Gini R

Subjects
Breast Feeding, Communication, Drug Information Services standards, Europe, Female, Humans, Information Storage and Retrieval, Pregnancy, Databases as Topic organization & administration, Drug-Related Side Effects and Adverse Reactions, Health Information Exchange
Abstract

In 2019, the Innovative Medicines Initiative (IMI) funded the ConcePTION project-Building an ecosystem for better monitoring and communicating safety of medicines use in pregnancy and breastfeeding: validated and regulatory endorsed workflows for fast, optimised evidence generation-with the vision that there is a societal obligation to rapidly reduce uncertainty about the safety of medication use in pregnancy and breastfeeding. The present paper introduces the set of concepts used to describe the European data sources involved in the ConcePTION project and illustrates the ConcePTION Common Data Model (CDM), which serves as the keystone of the federated ConcePTION network. Based on data availability and content analysis of 21 European data sources, the ConcePTION CDM has been structured with six tables designed to capture data from routine healthcare, three tables for data from public health surveillance activities, three curated tables for derived data on population (e.g., observation time and mother-child linkage), plus four metadata tables. By its first anniversary, the ConcePTION CDM has enabled 13 data sources to run common scripts to contribute to major European projects, demonstrating its capacity to facilitate effective and transparent deployment of distributed analytics, and its potential to address questions about utilization, effectiveness, and safety of medicines in special populations, including during pregnancy and breastfeeding, and, more broadly, in the general population., (© 2021 The Authors. Clinical Pharmacology & Therapeutics published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published
2022
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26. [Epidemiological surveillance of congenital heart defects: the Tetralogy of Fallot in the Valencian Region, 2007-2017.]

Author

Cavero-Carbonell C, García-Villodre L, Barrachina-Bonet L, Moreno-Marro S, Páramo-Rodríguez L, Guardiola-Vilarroig S, and Zurriaga-Llorens Ó

Subjects
Female, Humans, Infant, Infant, Newborn, Male, Prevalence, Registries, Spain epidemiology, Epidemiological Monitoring, Heart Defects, Congenital epidemiology, Tetralogy of Fallot epidemiology
Abstract

Objective: Tetralogy of Fallot is characterized by the presence of four congenital heart defects. Objective: to describe the temporal trend and distribution of Tetralogy of Fallot, in children under one year in the Valencian Region., Methods: Cases with Tetralogy of Fallot (code Q21.3 from the ICD10-British Paediatric Association) were selected from the Congenital Anomalies Population-based Registry between 2007-2017. Prevalence per 10,000 births with 95%CI was calculated, and a descriptive analysis of sociodemographic and clinical variables was made., Results: 165 cases were identified (43.6% male, 30.9% female and 25.5% unknown). The overall prevalence was 3.1/10,000 births (95%CI:2.6-3.6), being 2015 and 2017 the years with the highest (4.3/10,000 births and 4.7/10,000 births respectively) and 2011 with the lowest (1.8/10,000 births). 72.1% were live births, 24.8% Termination of Pregnancy for Fetal Anomaly (TOPFA) and 3.0% stillbirths. The prevalence in live births was 2.2/10,000 births (95%CI:1.8-2.7) and in TOPFA it was 0.8/10,000 births (95%CI:0.5-1.0), identifying an increasing trend along the period in the last one. 10.1% of live births died during the first year of life and 55.8% were diagnosed prenatally. Mothers younger than 20 years had the highest prevalence (4.8/10,000 births)., Conclusions: The prevalence obtained in the Valencian Region was slightly lower than EUROCAT's but coincides with that of the registries that are closer geographically, and in all of them it is noted that their increasing trend specifically affects cases ending in TOPFA., Competing Interests: Disclosure The authors report no conflicts of interest in this work.

Published
2021

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