155 results on '"Subbarao, Padmaja"'
Search Results
2. Early prediction of pediatric asthma in the Canadian Healthy Infant Longitudinal Development (CHILD) birth cohort using machine learning
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He, Ping, Moraes, Theo J., Dai, Darlene, Reyna-Vargas, Myrtha E., Dai, Ruixue, Mandhane, Piush, Simons, Elinor, Azad, Meghan B., Hoskinson, Courtney, Petersen, Charisse, Del Bel, Kate L., Turvey, Stuart E., Subbarao, Padmaja, Goldenberg, Anna, and Erdman, Lauren
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- 2024
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3. Pre-labor and post-labor cesarean delivery and early childhood adiposity in the Canadian Healthy Infant Longitudinal Development (CHILD) Cohort Study
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Bridgman, Sarah L., Penfold, Suzanne, Field, Catherine J., Haqq, Andrea M., Mandhane, Piushkumar J., Moraes, Theo J., Turvey, Stuart E., Simons, Elinor, Subbarao, Padmaja, and Kozyrskyj, Anita L.
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- 2024
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4. Comprehensive whole-genome sequence analyses provide insights into the genomic architecture of cerebral palsy
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Fehlings, Darcy L., Zarrei, Mehdi, Engchuan, Worrawat, Sondheimer, Neal, Thiruvahindrapuram, Bhooma, MacDonald, Jeffrey R., Higginbotham, Edward J., Thapa, Ritesh, Behlim, Tarannum, Aimola, Sabrina, Switzer, Lauren, Ng, Pamela, Wei, John, Danthi, Prakroothi S., Pellecchia, Giovanna, Lamoureux, Sylvia, Ho, Karen, Pereira, Sergio L., de Rijke, Jill, Sung, Wilson W. L., Mowjoodi, Alireza, Howe, Jennifer L., Nalpathamkalam, Thomas, Manshaei, Roozbeh, Ghaffari, Siavash, Whitney, Joseph, Patel, Rohan V., Hamdan, Omar, Shaath, Rulan, Trost, Brett, Knights, Shannon, Samdup, Dawa, McCormick, Anna, Hunt, Carolyn, Kirton, Adam, Kawamura, Anne, Mesterman, Ronit, Gorter, Jan Willem, Dlamini, Nomazulu, Merico, Daniele, Hilali, Murto, Hirschfeld, Kyle, Grover, Kritika, Bautista, Nelson X., Han, Kara, Marshall, Christian R., Yuen, Ryan K. C., Subbarao, Padmaja, Azad, Meghan B., Turvey, Stuart E., Mandhane, Piush, Moraes, Theo J., Simons, Elinor, Maxwell, George, Shevell, Michael, Costain, Gregory, Michaud, Jacques L., Hamdan, Fadi F., Gauthier, Julie, Uguen, Kevin, Stavropoulos, Dimitri J., Wintle, Richard F., Oskoui, Maryam, and Scherer, Stephen W.
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- 2024
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5. Antibiotics taken within the first year of life are linked to infant gut microbiome disruption and elevated atopic dermatitis risk
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Hoskinson, Courtney, Medeleanu, Maria V., Reyna, Myrtha E., Dai, Darlene L.Y., Chowdhury, Biswajit, Moraes, Theo J., Mandhane, Piushkumar J., Simons, Elinor, Kozyrskyj, Anita L., Azad, Meghan B., Petersen, Charisse, Turvey, Stuart E., and Subbarao, Padmaja
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- 2024
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6. Association between gas stove use and childhood asthma in the Canadian CHILD Cohort Study
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Bédard, Marc-Antoine, Reyna, Myrtha E., Moraes, Theo J., Simons, Elinor, Turvey, Stuart E., Mandhane, Piush, Brook, Jeffrey R., and Subbarao, Padmaja
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- 2023
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7. Delayed gut microbiota maturation in the first year of life is a hallmark of pediatric allergic disease
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Hoskinson, Courtney, Dai, Darlene L. Y., Del Bel, Kate L., Becker, Allan B., Moraes, Theo J., Mandhane, Piushkumar J., Finlay, B. Brett, Simons, Elinor, Kozyrskyj, Anita L., Azad, Meghan B., Subbarao, Padmaja, Petersen, Charisse, and Turvey, Stuart E.
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- 2023
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8. Early sex-dependent differences in metabolic profiles of overweight and adiposity in young children: a cross-sectional analysis
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Azab, Sandi M, Shanmuganathan, Meera, de Souza, Russell J, Kroezen, Zachary, Desai, Dipika, Williams, Natalie C, Morrison, Katherine M, Atkinson, Stephanie A, Teo, Koon K, Azad, Meghan B, Simons, Elinor, Moraes, Theo J, Mandhane, Piush J, Turvey, Stuart E, Subbarao, Padmaja, Britz-McKibbin, Philip, and Anand, Sonia S
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- 2023
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9. Genome-wide enhancer-associated tandem repeats are expanded in cardiomyopathy
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Mitina, Aleksandra, Khan, Mahreen, Lesurf, Robert, Yin, Yue, Engchuan, Worrawat, Hamdan, Omar, Pellecchia, Giovanna, Trost, Brett, Backstrom, Ian, Guo, Keyi, Pallotto, Linda M., Lam Doong, Phoenix Hoi, Wang, Zhuozhi, Nalpathamkalam, Thomas, Thiruvahindrapuram, Bhooma, Papaz, Tanya, Pearson, Christopher E., Ragoussis, Jiannis, Subbarao, Padmaja, Azad, Meghan B., Turvey, Stuart E., Mandhane, Piushkumar, Moraes, Theo J., Simons, Elinor, Scherer, Stephen W., Lougheed, Jane, Mondal, Tapas, Smythe, John, Altamirano-Diaz, Luis, Oechslin, Erwin, Mital, Seema, and Yuen, Ryan K.C.
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- 2024
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10. Semiautomated Segmentation and Analysis of Airway Lumen in Pediatric Patients Using Ultra Short Echo Time MRI
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Genkin, Daniel, Zanette, Brandon, Grzela, Patrick, Benkert, Thomas, Subbarao, Padmaja, Moraes, Theo J., Katz, Sherri, Ratjen, Felix, Santyr, Giles, and Kirby, Miranda
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- 2024
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11. Organophosphate ester flame retardants and plasticizers in house dust and mental health outcomes among Canadian mothers: A nested prospective cohort study in CHILD
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Foster, Stephanie A., Kile, Molly L., Hystad, Perry, Diamond, Miriam L., Jantunen, Liisa M., Mandhane, Piush J., Moraes, Theo J., Navaranjan, Garthika, Scott, James A., Simons, Elinor, Subbarao, Padmaja, Takaro, Tim K., Turvey, Stuart E., and Brook, Jeffrey R.
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- 2024
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12. Early-immune development in asthma: A review of the literature
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Medeleanu, Maria V., Qian, Yu Chen, Moraes, Theo J., and Subbarao, Padmaja
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- 2023
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13. Breastfeeding enrichment of B. longum subsp. infantis mitigates the effect of antibiotics on the microbiota and childhood asthma risk
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Dai, Darlene L.Y., Petersen, Charisse, Hoskinson, Courtney, Del Bel, Kate L., Becker, Allan B., Moraes, Theo J., Mandhane, Piushkumar J., Finlay, B. Brett, Simons, Elinor, Kozyrskyj, Anita L., Patrick, David M., Subbarao, Padmaja, Bode, Lars, Azad, Meghan B., and Turvey, Stuart E.
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- 2023
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14. Childhood body mass index and associations with infant gut metabolites and secretory IgA: findings from a prospective cohort study
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Bridgman, Sarah L., Malmuthuge, Nilusha, Mandal, Rupasri, Field, Catherine J., Haqq, Andrea M., Mandhane, Piushkumar J., Moraes, Theo J., Turvey, Stuart E., Simons, Elinor, Subbarao, Padmaja, Scott, James A., Wishart, David S., and Kozyrskyj, Anita L.
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- 2022
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15. Longitudinal body mass index trajectories at preschool age: children with rapid growth have differential composition of the gut microbiota in the first year of life
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Reyna, Myrtha E., Petersen, Charisse, Dai, Darlene L. Y., Dai, Ruixue, Becker, Allan B., Azad, Meghan B., Miliku, Kozeta, Lefebvre, Diana L., Moraes, Theo J., Mandhane, Piushkumar J., Boutin, Rozlyn C. T., Finlay, B. Brett, Simons, Elinor, Kozyrskyj, Anita L., Lou, Wendy, Turvey, Stuart E., and Subbarao, Padmaja
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- 2022
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16. Development of a predictive algorithm to identify pre-school children at risk for behavior changes associated with sleep-related breathing disorders
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Ezeugwu, Victor E., Adamko, Darryl, van Eeden, Charmaine, Dubeau, Aimee, Turvey, Stuart E., Moraes, Theo J., Simons, Elinor, Subbarao, Padmaja, Wishart, David S., and Mandhane, Piushkumar J.
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- 2022
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17. Assessing secondhand and thirdhand tobacco smoke exposure in Canadian infants using questionnaires, biomarkers, and machine learning
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Parks, Jaclyn, McLean, Kathleen E., McCandless, Lawrence, de Souza, Russell J., Brook, Jeffrey R., Scott, James, Turvey, Stuart E., Mandhane, Piush J., Becker, Allan B., Azad, Meghan B., Moraes, Theo J., Lefebvre, Diana L., Sears, Malcolm R., Subbarao, Padmaja, and Takaro, Tim K.
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- 2022
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18. Adenotonsillectomy, bronchoscopy and bronchoalveolar lavage in the management of preschool children with severe asthma: pilot study
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Campisi, Emma S., Reyna, Myrtha E., Brydges, May, Dubeau, Aimee, Moraes, Theo J., Campisi, Paolo, and Subbarao, Padmaja
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- 2022
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19. DNA methylation changes in cord blood and the developmental origins of health and disease – a systematic review and replication study
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Akhabir, Loubna, Stringer, Randa, Desai, Dipika, Mandhane, Piush J, Azad, Meghan B, Moraes, Theo J, Subbarao, Padmaja, Turvey, Stuart E, Paré, Guillaume, and Anand, Sonia S.
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- 2022
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20. Maternal smoking DNA methylation risk score associated with health outcomes in offspring of European and South Asian ancestry.
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Deng, Wei Q., Cawte, Nathan, Campbell, Natalie, Azab, Sandi M., de Souza, Russell J., Lamri, Amel, Morrison, Katherine M., Atkinson, Stephanie A., Subbarao, Padmaja, Turvey, Stuart E., Moraes, Theo J., Teo, Koon K., Mandhane, Piush J., Azad, Meghan B., Simons, Elinor, Paré, Guillaume, and Anand, Sonia S.
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- 2024
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21. Correction: Gestational age at birth and body size from infancy through adolescence: An individual participant data meta-analysis on 253,810 singletons in 16 birth cohort studies
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Vinther, Johan L., Cadman, Tim, Avraam, Demetris, Ekstrøm, Claus T., Sørensen, Thorkild I. A., Elhakeem, Ahmed, Santos, Ana C., de Moira, Angela Pinot, Heude, Barbara, Iñiguez, Carmen, Pizzi, Costanza, Simons, Elinor, Voerman, Ellis, Corpeleijn, Eva, Zariouh, Faryal, Santorelli, Gilian, Inskip, Hazel M., Barros, Henrique, Carson, Jennie, Harris, Jennifer R., Nader, Johanna L., Ronkainen, Justiina, Strandberg-Larsen, Katrine, Santa-Marina, Loreto, Calas, Lucinda, Cederkvist, Luise, Popovic, Maja, Charles, Marie-Aline, Welten, Marieke, Vrijheid, Martine, Azad, Meghan, Subbarao, Padmaja, Burton, Paul, Mandhane, Puishkumar J., Huang, Rae-Chi, Wilson, Rebecca C., Haakma, Sido, Fernández-Barrés, Sílvia, Turvey, Stuart, Santos, Susana, Tough, Suzanne C., Sebert, Sylvain, Moraes, Theo J., Salika, Theodosia, Jaddoe, Vincent W. V., Lawlor, Deborah A., and Nybo Andersen, Anne-Marie
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Biological sciences - Abstract
Author(s): Johan L. Vinther, Tim Cadman, Demetris Avraam, Claus T. Ekstrøm, Thorkild I. A. Sørensen, Ahmed Elhakeem, Ana C. Santos, Angela Pinot de Moira, Barbara Heude, Carmen Iñiguez, Costanza Pizzi, [...]
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- 2023
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22. Gestational age at birth and body size from infancy through adolescence: An individual participant data meta-analysis on 253,810 singletons in 16 birth cohort studies
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Vinther, Johan L., Cadman, Tim, Avraam, Demetris, Ekstrøm, Claus T., I. A. Sørensen, Thorkild, Elhakeem, Ahmed, Santos, Ana C., Pinot de Moira, Angela, Heude, Barbara, Iñiguez, Carmen, Pizzi, Costanza, Simons, Elinor, Voerman, Ellis, Corpeleijn, Eva, Zariouh, Faryal, Santorelli, Gilian, Inskip, Hazel M., Barros, Henrique, Carson, Jennie, Harris, Jennifer R., Nader, Johanna L., Ronkainen, Justiina, Strandberg-Larsen, Katrine, Santa-Marina, Loreto, Calas, Lucinda, Cederkvist, Luise, Popovic, Maja, Charles, Marie-Aline, Welten, Marieke, Vrijheid, Martine, Azad, Meghan, Subbarao, Padmaja, Burton, Paul, Mandhane, Puishkumar J., Huang, Rae-Chi, Wilson, Rebecca C., Haakma, Sido, Fernández-Barrés, Sílvia, Turvey, Stuart, Santos, Susana, Tough, Suzanne C., Sebert, Sylvain, Moraes, Theo J., Salika, Theodosia, Jaddoe, Vincent W. V., Lawlor, Deborah A., and Nybo Andersen, Anne-Marie
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Gestational age -- Influence ,Infants (Premature) -- Growth ,Company growth ,Biological sciences - Abstract
Background Preterm birth is the leading cause of perinatal morbidity and mortality and is associated with adverse developmental and long-term health outcomes, including several cardiometabolic risk factors and outcomes. However, evidence about the association of preterm birth with later body size derives mainly from studies using birth weight as a proxy of prematurity rather than an actual length of gestation. We investigated the association of gestational age (GA) at birth with body size from infancy through adolescence. Methods and findings We conducted a two-stage individual participant data (IPD) meta-analysis using data from 253,810 mother-child dyads from 16 general population-based cohort studies in Europe (Denmark, Finland, France, Italy, Norway, Portugal, Spain, the Netherlands, United Kingdom), North America (Canada), and Australasia (Australia) to estimate the association of GA with body mass index (BMI) and overweight (including obesity) adjusted for the following maternal characteristics as potential confounders: education, height, prepregnancy BMI, ethnic background, parity, smoking during pregnancy, age at child's birth, gestational diabetes and hypertension, and preeclampsia. Pregnancy and birth cohort studies from the LifeCycle and the EUCAN-Connect projects were invited and were eligible for inclusion if they had information on GA and minimum one measurement of BMI between infancy and adolescence. Using a federated analytical tool (DataSHIELD), we fitted linear and logistic regression models in each cohort separately with a complete-case approach and combined the regression estimates and standard errors through random-effects study-level meta-analysis providing an overall effect estimate at early infancy (>0.0 to 0.5 years), late infancy (>0.5 to 2.0 years), early childhood (>2.0 to 5.0 years), mid-childhood (>5.0 to 9.0 years), late childhood (>9.0 to 14.0 years), and adolescence (>14.0 to 19.0 years). GA was positively associated with BMI in the first decade of life, with the greatest increase in mean BMI z-score during early infancy (0.02, 95% confidence interval (CI): 0.00; 0.05, p < 0.05) per week of increase in GA, while in adolescence, preterm individuals reached similar levels of BMI (0.00, 95% CI: -0.01; 0.01, p 0.9) as term counterparts. The association between GA and overweight revealed a similar pattern of association with an increase in odds ratio (OR) of overweight from late infancy through mid-childhood (OR 1.01 to 1.02) per week increase in GA. By adolescence, however, GA was slightly negatively associated with the risk of overweight (OR 0.98 [95% CI: 0.97; 1.00], p 0.1) per week of increase in GA. Although based on only four cohorts (n = 32,089) that reached the age of adolescence, data suggest that individuals born very preterm may be at increased odds of overweight (OR 1.46 [95% CI: 1.03; 2.08], p < 0.05) compared with term counterparts. Findings were consistent across cohorts and sensitivity analyses despite considerable heterogeneity in cohort characteristics. However, residual confounding may be a limitation in this study, while findings may be less generalisable to settings in low- and middle-income countries. Conclusions This study based on data from infancy through adolescence from 16 cohort studies found that GA may be important for body size in infancy, but the strength of association attenuates consistently with age. By adolescence, preterm individuals have on average a similar mean BMI to peers born at term., Author(s): Johan L. Vinther 1,*, Tim Cadman 2, Demetris Avraam 3, Claus T. Ekstrøm 4, Thorkild I. A. Sørensen 1,5, Ahmed Elhakeem 2, Ana C. Santos 6,7, Angela Pinot de [...]
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- 2023
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23. Women in Canada are consuming above the upper intake level of folic acid but few are meeting dietary choline recommendations in the second trimester of pregnancy: data from the CHILD cohort study.
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Wiedeman, Alejandra M., Miliku, Kozeta, Moraes, Theo J., Mandhane, Piushkumar J., Simons, Elinor, Subbarao, Padmaja, Turvey, Stuart E., Zwicker, Jill G., and Devlin, Angela M.
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FOLIC acid metabolism ,THERAPEUTIC use of folic acid ,WOMEN ,RESEARCH funding ,FOOD consumption ,FOLIC acid ,SECOND trimester of pregnancy ,MOTHERS ,VITAMIN B12 ,NUTRITIONAL requirements ,DESCRIPTIVE statistics ,CHOLINE ,SURVEYS ,LONGITUDINAL method ,PRENATAL care ,ENRICHED foods ,DIETARY supplements ,PREGNANCY - Abstract
There is concern that during a low-risk pregnancy, women are consuming more than recommended (400 µg/day) supplemental folic acid and may not meet recommendations for other nutrients. The objective of this study was to determine folic acid supplement use and dietary folate intakes in the second trimester (week 18) of pregnancy in women (n = 2996) in the Canadian CHILD cohort study. Vitamin B12 and choline intakes were also assessed because they are metabolically related to folate. The majority of participants (71.6%) were consuming a daily prenatal supplement. Twenty-eight percent of women (n = 847) reported consuming a folic acid supplement and of these women, 45.3% had daily supplemental folic acid intakes above the upper intake level (UL; 1000 µg/day). Daily dietary folate intakes were (mean (SD)) 575 (235) DFE µg/day. In contrast, only 24.8% of women met the dietary choline adequate intake (AI) recommendation (AI ≥ 450 mg/day) with a mean (SD) intake of 375 (151) mg/day. Further understanding of the impact of supplemental folic acid intake above the UL and low choline intake during pregnancy requires further investigation. [ABSTRACT FROM AUTHOR]
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- 2024
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24. The acute care burden of asthma in children was profoundly reduced during the COVID-19 pandemic: A multi-centre Canadian retrospective study.
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McConnery, Jason R, Bone, Jeffrey N, Goldman, Ran D, Hicks, Anne, Seaton, Claire, Subbarao, Padmaja, and Moraes, Theo J
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ASTHMA prevention ,DISEASE exacerbation ,PATIENTS ,HOSPITAL admission & discharge ,RETROSPECTIVE studies ,DESCRIPTIVE statistics ,CHI-squared test ,TIME series analysis ,SEVERITY of illness index ,PEDIATRICS ,STAY-at-home orders ,DISEASES ,MEDICAL appointments ,PUBLIC health ,COMPARATIVE studies ,COVID-19 pandemic ,GOVERNMENT regulation ,CRITICAL care medicine ,COVID-19 ,CHILDREN - Abstract
Objectives Asthma is a chronic lung condition that can be exacerbated when triggered by viruses. Pandemic public health restrictions aimed to reduce COVID-19 transmission indirectly effected other circulating viruses. This study assessed the impact of the pandemic and associated public health measures on acute paediatric asthma across four tertiary sites in three Canadian provinces. We queried whether pandemic-related changes would impair preventive care and delay presentation to care, increasing asthma exacerbation severity. Methods This retrospective study compared the frequency of acute care access and severity of presentation to emergency departments (ED) for acute asthma to four tertiary care children's hospitals during the COVID-19 pandemic (from March 17, 2020 to June 30, 2021) to a pre-lockdown control period (July 1, 2018 to March 16, 2020). Data was subjected to interrupted time series and Chi-square analysis. Results Our study included 26,316 acute asthma visits to ED. Sites experienced a 63% to 89% reduction in acute asthma visits during the pandemic, compared with pre-lockdown controls, and a 17% to 85% reduction in asthma, that is out of proportion as a fraction of all-cause ED visits. For asthma, there was no difference in severity measured by rate of ward admission or rate of Paediatric Intensive Care Unit (PICU) admission. Conclusions Public health measures appear to have resulted in a specific protective association on acute asthma with reduced acute care utilization over and above the reduction in all-cause presentations, without an increase in severity upon presentation. Our study indicates an importance to antiviral public health and engineering strategies to reduce viral transmission and thereby asthma morbidity. [ABSTRACT FROM AUTHOR]
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- 2024
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25. Association of Human Milk Fatty Acid Composition with Maternal Cardiometabolic Diseases: An Exploratory Prospective Cohort Study.
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Scime, Natalie V., Turner, Sarah, Miliku, Kozeta, Simons, Elinor, Moraes, Theo J., Field, Catherine J., Turvey, Stuart E., Subbarao, Padmaja, Mandhane, Piushkumar J., and Azad, Meghan B.
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- 2024
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26. The use of prescription medications and non-prescription medications during lactation in a prospective Canadian cohort study.
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Soliman, Youstina, Yakandawala, Uma, Leong, Christine, Garlock, Emma S., Brinkman, Fiona S.L., Winsor, Geoffrey L., Kozyrskyj, Anita L, Mandhane, Piushkumar J, Turvey, Stuart E., Moraes, Theo J., Subbarao, Padmaja, Nickel, Nathan C., Thiessen, Kellie, Azad, Meghan B, and Kelly, Lauren E
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STEROID drugs ,VITAMIN therapy ,SELF-evaluation ,BREASTFEEDING ,PATIENT safety ,RESEARCH funding ,CHILD health services ,QUESTIONNAIRES ,PIPERIDINE ,DESCRIPTIVE statistics ,LACTATION ,LONGITUDINAL method ,DRUGS ,ONTOLOGIES (Information retrieval) ,NONPRESCRIPTION drugs - Abstract
Background: A lack of safety data on postpartum medication use presents a potential barrier to breastfeeding and may result in infant exposure to medications in breastmilk. The type and extent of medication use by lactating women requires investigation. Methods: Data were collected from the CHILD Cohort Study which enrolled pregnant women across Canada between 2008 and 2012. Participants completed questionnaires regarding medications and non-prescription medications used and breastfeeding status at 3, 6 and 12 months postpartum. Medications, along with self-reported reasons for medication use, were categorized by ontologies [hierarchical controlled vocabulary] as part of a large-scale curation effort to enable more robust investigations of reasons for medication use. Results: A total of 3542 mother-infant dyads were recruited to the CHILD study. Breastfeeding rates were 87.4%, 75.3%, 45.5% at 3, 6 and 12 months respectively. About 40% of women who were breastfeeding at 3 months used at least one prescription medication during the first three months postpartum; this proportion decreased over time to 29.5% % at 6 months and 32.8% at 12 months. The most commonly used prescription medication by breastfeeding women was domperidone at 3 months (9.0%, n = 229/2540) and 6 months (5.6%, n = 109/1948), and norethisterone at 12 months (4.1%, n = 48/1180). The vast majority of domperidone use by breastfeeding women (97.3%) was for lactation purposes which is off-label (signifying unapproved use of an approved medication). Non-prescription medications were more often used among breastfeeding than non-breastfeeding women (67.6% versus 48.9% at 3 months, p < 0.0001), The most commonly used non-prescription medications were multivitamins and Vitamin D at 3, 6 and 12 months postpartum. Conclusions: In Canada, medication use is common postpartum; 40% of breastfeeding women use prescription medications in the first 3 months postpartum. A diverse range of medications were used, with many women taking more than one prescription and non-prescription medicines. The most commonly used prescription medication by breastfeeding women were domperidone for off-label lactation support, signalling a need for more data on the efficacy of domperidone for this indication. This data should inform research priorities and communication strategies developed to optimize care during lactation. [ABSTRACT FROM AUTHOR]
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- 2024
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27. Persistent DNA Methylation Changes across the First Year of Life and Prenatal NO2 Exposure in a Canadian Prospective Birth Study.
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Lee, Samantha, Sbihi, Hind, MacIsaac, Julia L., Balshaw, Robert, Ambalavanan, Amirthagowri, Subbarao, Padmaja, Mandhane, Piushkumar J., Moraes, Theo J., Turvey, Stuart E., Qingling Duan, Brauer, Michael, Brook, Jeffrey R., Kobor, Michael S., and Jones, Meaghan J.
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ASTHMA risk factors ,RISK assessment ,STATISTICAL correlation ,CROSS-sectional method ,PRENATAL exposure delayed effects ,RESEARCH funding ,ACADEMIC medical centers ,DATA analysis ,SECONDARY analysis ,EPIGENOMICS ,PROBABILITY theory ,MULTIPLE regression analysis ,CELL physiology ,QUESTIONNAIRES ,DESCRIPTIVE statistics ,ATTITUDES of mothers ,DNA methylation ,PRENATAL care ,LONGITUDINAL method ,GENE expression ,ENVIRONMENTAL exposure ,RESEARCH ,MICROARRAY technology ,RESEARCH methodology ,ANALYSIS of variance ,STATISTICS ,NITROGEN oxides ,DATA analysis software ,PHENOTYPES - Abstract
BACKGROUND: Evidence suggests that prenatal air pollution exposure alters DNA methylation (DNAm), which could go on to affect long-term health. It remains unclear whether DNAm alterations present at birth persist through early life. Identifying persistent DNAm changes would provide greater insight into the molecular mechanisms contributing to the association of prenatal air pollution exposure with atopic diseases. OBJECTIVES: This study investigated DNAm differences associated with prenatal nitrogen dioxide (NO
2 ) exposure (a surrogate measure of trafficrelated air pollution) at birth and 1 y of age and examined their role in atopic disease. We focused on regions showing persistent DNAm differences from birth to 1 y of age and regions uniquely associated with postnatal NO2 exposure. METHODS: Microarrays measured DNAm at birth and at 1 y of age for an atopy-enriched subset of Canadian Health Infant Longitudinal Development (CHILD) study participants. Individual and regional DNAm differences associated with prenatal NO2 (푛= 128) were identified, and their persistence at age 1 y were investigated using linear mixed effects models (푛= 124). Postnatal-specific DNAm differences (푛= 125) were isolated, and their association with NO2 in the first year of life was examined. Causal mediation investigated whether DNAm differences mediated associations between NO2 and age 1 y atopy or wheeze. Analyses were repeated using biological sex-stratified data. RESULTS: At birth (푛= 128), 18 regions of DNAm were associated with NO2 , with several annotated to HOX genes. Some of these regions were specifically identified in males (푛= 73), but not females (푛= 55). The effect of prenatal NO2 across CpGs within altered regions persisted at 1 y of age. No significant mediation effects were identified. Sex-stratified analyses identified postnatal-specific DNAm alterations. DISCUSSION: Regional cord blood DNAm differences associated with prenatal NO2 persisted through at least the first year of life in CHILD participants. Some differences may represent sex-specific alterations, but replication in larger cohorts is needed. The early postnatal period remained a sensitive window to DNAm perturbations. [ABSTRACT FROM AUTHOR]- Published
- 2024
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28. Association of factors with childhood asthma and allergic diseases using latent class analysis.
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To, Teresa, Borkhoff, Cornelia M., Anderson, Laura N., Birken, Catherine S., Dell, Sharon D., Janus, Magdalena, Maguire, Jonathon L., Moraes, Theo J., Parkin, Patricia C., Subbarao, Padmaja, Van Dam, Anne, Guttman, Beverly, Terebessy, Emilie, Zhang, Kimball, and Zhu, Jingqin
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ASTHMA in children ,LATENT structure analysis ,LATENT class analysis (Statistics) ,EMERGENCY room visits ,ALLERGIES ,CHILD health services ,LATENT infection ,REFUGEE children - Abstract
We hypothesize that children characterized by deprived factors have poorer health outcomes. We aim to identify clustering of determinants and estimate risk of early childhood diseases. This 1993–2019 longitudinal cohort study combines three Canadian pediatric cohorts and their families. Mothers and children are clustered using latent class analysis (LCA) by 16 indicators in three domains (maternal and newborn; socioeconomic status [SES] and neighbourhood; environmental exposures). Hazard ratios (HR) of childhood asthma, allergic rhinitis (AR), and eczema are quantified with Cox proportional hazard (PH) regression. Rate ratios (RR) of children's health services use (HSU) are estimated with Poisson regression. Here we report the inclusion of 15,724 mother–child pairs; our LCA identifies four mother-clusters. Classes 1 and 2 mothers are older (30–40 s), non-immigrants with university education, living in high SES neighbourhoods; Class 2 mothers have poorer air quality and less greenspace. Classes 3 and 4 mothers are younger (20–30 s), likely an immigrant/refugee, with high school-to-college education, living in lower SES neighborhoods with poorer air quality and less greenspace. Children's outcomes differ by Class, in comparison to Class 1. Classes 3 and 4 children have higher risks of asthma (HR 1.24, 95% CI 1.11–1.37 and HR 1.39, 95% CI 1.22–1.59, respectively), and similar higher risks of AR and eczema. Children with AR in Class 3 have 20% higher all-cause physician visits (RR = 1.20, 95% CI 1.10–1.30) and those with eczema have 18% higher all-cause emergency department visits (RR = 1.18, 95% CI 1.09–1.28) and 14% higher all-cause physician visits (RR = 1.14, 95% CI 1.09–1.19). Multifactorial-LCA mother-clusters may characterize associations of children's health outcomes and care, adjusting for interrelationships. [ABSTRACT FROM AUTHOR]
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- 2024
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29. A Bayesian latent class model for integrating multi-source longitudinal data: application to the CHILD cohort study.
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Lu, Zihang, Subbarao, Padmaja, and Lou, Wendy
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PANEL analysis ,COHORT analysis - Abstract
Multi-source longitudinal data have become increasingly common. This type of data refers to longitudinal datasets collected from multiple sources describing the same set of individuals. Representing distinct features of the individuals, each data source may consist of multiple longitudinal markers of distinct types and measurement frequencies. Motivated by the CHILD cohort study, we develop a model for joint clustering multi-source longitudinal data. The proposed model allows each data source to follow source-specific clustering, and they are aggregated to yield a global clustering. The proposed model is demonstrated through real-data analysis and simulation study. [ABSTRACT FROM AUTHOR]
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- 2024
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30. Divergent maturational patterns of the infant bacterial and fungal gut microbiome in the first year of life are associated with inter-kingdom community dynamics and infant nutrition.
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Mercer, Emily M., Ramay, Hena R., Moossavi, Shirin, Laforest-Lapointe, Isabelle, Reyna, Myrtha E., Becker, Allan B., Simons, Elinor, Mandhane, Piush J., Turvey, Stuart E., Moraes, Theo J., Sears, Malcolm R., Subbarao, Padmaja, Azad, Meghan B., and Arrieta, Marie-Claire
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GUT microbiome ,INFANT nutrition ,INFANTS ,ECOLOGICAL succession ,COLONIZATION (Ecology) ,FUNGAL communities ,PRENATAL influences ,PRENATAL exposure - Abstract
Background: The gut microbiome undergoes primary ecological succession over the course of early life before achieving ecosystem stability around 3 years of age. These maturational patterns have been well-characterized for bacteria, but limited descriptions exist for other microbiota members, such as fungi. Further, our current understanding of the prevalence of different patterns of bacterial and fungal microbiome maturation and how inter-kingdom dynamics influence early-life microbiome establishment is limited. Results: We examined individual shifts in bacterial and fungal alpha diversity from 3 to 12 months of age in 100 infants from the CHILD Cohort Study. We identified divergent patterns of gut bacterial or fungal microbiome maturation in over 40% of infants, which were characterized by differences in community composition, inter-kingdom dynamics, and microbe-derived metabolites in urine, suggestive of alterations in the timing of ecosystem transitions. Known microbiome-modifying factors, such as formula feeding and delivery by C-section, were associated with atypical bacterial, but not fungal, microbiome maturation patterns. Instead, fungal microbiome maturation was influenced by prenatal exposure to artificially sweetened beverages and the bacterial microbiome, emphasizing the importance of inter-kingdom dynamics in early-life colonization patterns. Conclusions: These findings highlight the ecological and environmental factors underlying atypical patterns of microbiome maturation in infants, and the need to incorporate multi-kingdom and individual-level perspectives in microbiome research to improve our understandings of gut microbiome maturation patterns in early life and how they relate to host health. 5AtmDGbifCkZAT-p1B-BuF Video Abstract [ABSTRACT FROM AUTHOR]
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- 2024
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31. Maternal smoking during pregnancy increases the risk of gut microbiome-associated childhood overweight and obesity.
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Ye Peng, Tun, Hein M., Ng, Siew C., Hogan Kok-Fung Wai, Xi Zhang, Parks, Jaclyn, Field, Catherine J, Mandhane, Piush, Moraes, Theo J., Simons, Elinor, Turvey, Stuart E., Subbarao, Padmaja, Brook, Jeffrey R., Takaro, Tim K., Scott, James A., Chan, Francis K. L., and Kozyrskyj, Anita L.
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- 2024
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32. Author Correction: The maternal serum metabolome by multisegment injection-capillary electrophoresis-mass spectrometry: a high-throughput platform and standardized data workflow for large-scale epidemiological studies
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Shanmuganathan, Meera, Kroezen, Zachary, Gill, Biban, Azab, Sandi, de Souza, Russell J., Teo, Koon K., Atkinson, Stephanie, Subbarao, Padmaja, Desai, Dipika, Anand, Sonia S., and Britz-McKibbin, Philip
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- 2021
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33. Erratum:Gestational age at birth and body size from infancy through adolescence: An individual participant data meta-analysis on 253, 810 singletons in 16 birth cohort studies (PLoS Med (2023) 20:1 (e1004036) DOI: 10.1371/journal.pmed.1004036)
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Vinther, Johan L., Cadman, Tim, Avraam, Demetris, Ekstrøm, Claus T., Sørensen, Thorkild I. A., Elhakeem, Ahmed, Santos, Ana C., de Moira, Angela Pinot, Heude, Barbara, Iñiguez, Carmen, Pizzi, Costanza, Simons, Elinor, Voerman, Ellis, Corpeleijn, Eva, Zariouh, Faryal, Santorelli, Gilian, Inskip, Hazel M., Barros, Henrique, Carson, Jennie, Harris, Jennifer R., Nader, Johanna L., Ronkainen, Justiina, Strandberg-Larsen, Katrine, Santa-Marina, Loreto, Calas, Lucinda, Cederkvist, Luise, Popovic, Maja, Charles, Marie-Aline, Welten, Marieke, Vrijheid, Martine, Azad, Meghan, Subbarao, Padmaja, Burton, Paul, Mandhane, Puishkumar J., Huang, Rae-Chi, Wilson, Rebecca C., Haakma, Sido, Fernández-Barrés, S. lvia, Turvey, Stuart, Santos, Susana, Tough, Suzanne C., Sebert, Sylvain, Moraes, Theo J., Salika, Theodosia, Jaddoe, Vincent W. V., Lawlor, Deborah A., Nybo Andersen, Anne-Marie, and VU University medical center
- Abstract
The fifth author's name is indexed incorrectly. The author's name should be indexed as Sørensen TIA. The correct citation is: Vinther JL, Cadman T, Avraam D, Ekstrøm CT, Sørensen TIA, Elhakeem A, et al. (2023) Gestational age at birth and body size from infancy through adolescence: An individual participant data meta-analysis on 253, 810 singletons in 16 birth cohort studies. PLoS Med 20(1): e1004036. https://doi.org/10.1371/journal.pmed.1004036.
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- 2023
34. Di-(2-Ethylhexyl) Phthalate (DEHP) in House Dust in Canadian Homes: Behaviors and Associations with Housing Characteristics and Consumer Products.
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Zhang, Luyao, Navaranjan, Garthika, Takaro, Tim K., Bernstein, Sarah, Jantunen, Liisa, Lou, Wendy, Mandhane, Piush J., Moraes, Theo J., Scott, James A., Simons, Elinor, Turvey, Stuart E., Subbarao, Padmaja, and Brook, Jeffrey R.
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DUST ,CONSUMER goods ,PLASTIC flooring ,PRODUCT attributes ,ASTHMA in children ,DUST measurement - Abstract
Background. Di-(2-ethylhexyl) phthalate (DEHP), which is ubiquitous in indoor environments, was the predominant phthalate measured in house dust in the Canadian CHILD Cohort and was found to be associated with a large increased risk of childhood asthma. Objective. To inform interventions by identifying sources of DEHP in dust and assessing behaviors related to DEHP concentrations in house dust. Methods. DEHP levels were measured in 726 dust samples collected at ~3 months of age in CHILD as well as in ~50 homes at two time points (June and November) in the CHILD pilot study. DEHP metabolites were measured in urine for a subset of the ~3-month-old infants. Housing characteristics were assessed at the time of dust and urine collection. Numerous factors from these surveys were investigated as potential sources of DEHP using univariate analyses and multivariable regressions. Correlations between DEHP in dust and urinary metabolites and between repeat dust samples were examined to study the relationship between dust measurement and DEHP exposure. Results. Overall, DEHP dust concentrations were higher for lower-income families. Homes with vinyl flooring in the kitchen and bathroom showed higher levels of DEHP than those without vinyl flooring. The quantity of vinyl furniture and the presence of mold were associated with higher DEHP concentrations, while the use of mattress covers reduced concentration. No other significant associations were found. DEHP concentrations in dust were consistent over 6 months, although the correlation between dust and DEHP metabolites in urine was low. Conclusion. DEHP in house dust persisted over multiple months, contributed to infant internal exposure, and was associated with specific housing characteristics. These findings may inform the public on their choice of building materials and products, as well as future policies, aimed at reducing the health risk associated with exposures in the indoor environment especially for children. [ABSTRACT FROM AUTHOR]
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- 2023
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35. A Joint Modeling Approach for Clustering Mixed-Type Multivariate Longitudinal Data: Application to the CHILD Cohort Study
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Tan, Zhiwen, Shen, Chang, Subbarao, Padmaja, Lou, Wendy, and Lu, Zihang
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Methodology (stat.ME) ,FOS: Computer and information sciences ,Applications (stat.AP) ,Statistics - Applications ,Statistics - Methodology - Abstract
In epidemiological and clinical studies, identifying patients' phenotypes based on longitudinal profiles is critical to understanding the disease's developmental patterns. The current study was motivated by data from a Canadian birth cohort study, the CHILD Cohort Study. Our goal was to use multiple longitudinal respiratory traits to cluster the participants into subgroups with similar longitudinal respiratory profiles in order to identify clinically relevant disease phenotypes. To appropriately account for distinct structures and types of these longitudinal markers, we proposed a novel joint model for clustering mixed-type (continuous, discrete and categorical) multivariate longitudinal data. We also developed a Markov Chain Monte Carlo algorithm to estimate the posterior distribution of model parameters. Analysis of the CHILD Cohort data and simulated data were presented and discussed. Our study demonstrated that the proposed model serves as a useful analytical tool for clustering multivariate mixed-type longitudinal data. We developed an R package BCClong to implement the proposed model efficiently., 21 pages, 4 figures, 2 tables
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- 2022
36. Maturational patterns of the infant gut mycobiome are associated with early-life body mass index
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Gutierrez, Mackenzie W., Mercer, Emily M., Moossavi, Shirin, Laforest-Lapointe, Isabelle, Reyna, Myrtha E., Becker, Allan B., Simons, Elinor, Mandhane, Piush J., Turvey, Stuart E., Moraes, Theo J., Sears, Malcolm R., Subbarao, Padmaja, Azad, Meghan B., and Arrieta, Marie-Claire
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- 2023
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37. DNA methylation is not associated with sensitization to or dietary introduction of highly allergenic foods in a subset of the CHILD cohort at age 1 year
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Kolsun, Kurt P., Lee, Samantha, MacIsaac, Julia L., Subbarao, Padmaja, Moraes, Theo J., Mandhane, Piushkumar J., Turvey, Stuart E., Kobor, Michael S., Jones, Meaghan J., and Simons, Elinor
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- 2023
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38. Natural Green Spaces, Sensitization to Allergens, and the Role of Gut Microbiota during Infancy.
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Buchholz, Vienna, Bridgman, Sarah L., Nielsen, Charlene C., Gascon, Mireia, Tun, Hein M., Simons, Elinor, Turvey, Stuart E., Subbarao, Padmaja, Takaro, Tim K., Broo, Jeffrey R., Scott, James A., Mandhane, Piush J., and Kozyrskyj, Anita L.
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- 2023
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39. Infant Vitamin D Supplements, Fecal Microbiota and Their Metabolites at 3 Months of Age in the CHILD Study Cohort.
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Zhao, Xin, Bridgman, Sarah L., Drall, Kelsea M., Tun, Hein M., Mandhane, Piush J., Moraes, Theo J., Simons, Elinor, Turvey, Stuart E., Subbarao, Padmaja, Scott, James A., and Kozyrskyj, Anita L.
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DIETARY supplements ,NUCLEAR magnetic resonance spectroscopy ,VITAMIN D ,BREASTFEEDING ,INFANTS ,GLYCERIN ,MICROBIAL metabolites ,METABOLITES ,HUMAN microbiota - Abstract
Infant vitamin D liquid formulations often contain non-medicinal excipients such as glycerin (ie. glycerol) and 1,2-propanediol (1,2-PD). We examined whether infant vitamin D supplementation is associated with fecal glycerol and 1,2-PD concentrations at 3 months of age and characterized associations between these two molecules, and gut microbiota and their metabolites. Fecal metabolites and microbiota were quantified using Nuclear Magnetic Resonance Spectroscopy and 16S rRNA sequencing, respectively, in 575 infants from the CHILD Study at 3 months of age. Vitamin D supplement use was determined using questionnaires. Vitamin D supplementation was associated with greater odds of high 1,2-PD (adjusted OR 1.65 95% CI: 1.06, 2.53) and with decreased odds of high fecal glycerol (adjusted OR: 0.62 95% CI: 0.42, 0.90) after adjustment for breastfeeding and other covariates. Our findings were confirmed in linear regression models; vitamin D supplementation was positively associated with fecal 1,2-PD and inversely associated with glycerol (aβ: 0.37, 95% CI 0.03, 0.71 & aβ: −0.23 95% CI −0.44, −0.03, respectively). Fecal 1,2-PD and glycerol concentrations were negatively correlated with each other. Positive correlations between fecal 1,2-PD, Bifidobacteriaceae, Lactobacillaceae, Enterobacteriaceae and acetate levels were observed. Our research demonstrates that infant vitamin D supplement administration may differentially and independently influence infant gut microbiota metabolites. [ABSTRACT FROM AUTHOR]
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- 2023
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40. The maternal prenatal and offspring early‐life gut microbiome of childhood asthma phenotypes.
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Lee‐Sarwar, Kathleen A., Chen, Yih‐Chieh, Chen, Yuan Yao, Kozyrskyj, Anita L., Mandhane, Piush J., Turvey, Stuart E., Subbarao, Padmaja, Bisgaard, Hans, Stokholm, Jakob, Chawes, Bo, Sørensen, Søren J., Kelly, Rachel S., Lasky‐Su, Jessica, Zeiger, Robert S., O'Connor, George T., Sandel, Megan T., Bacharier, Leonard B., Beigelman, Avraham, Carey, Vincent J., and Harshfield, Benjamin J.
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ASTHMA in children ,GUT microbiome ,THIRD trimester of pregnancy ,CESAREAN section ,FISHER exact test - Abstract
Background: The infant fecal microbiome is known to impact subsequent asthma risk, but the environmental exposures impacting this association, the role of the maternal microbiome, and how the microbiome impacts different childhood asthma phenotypes are unknown. Methods: Our objective was to identify associations between features of the prenatal and early‐life fecal microbiomes and child asthma phenotypes. We analyzed fecal 16 s rRNA microbiome profiling and fecal metabolomic profiling from stool samples collected from mothers during the third trimester of pregnancy (n = 120) and offspring at ages 3–6 months (n = 265), 1 (n = 436) and 3 years (n = 506) in a total of 657 mother–child pairs participating in the Vitamin D Antenatal Asthma Reduction Trial. We used clinical data from birth to age 6 years to characterize subjects with asthma as having early, transient or active asthma phenotypes. In addition to identifying specific genera that were robustly associated with asthma phenotypes in multiple covariate‐adjusted models, we clustered subjects by their longitudinal microbiome composition and sought associations between fecal metabolites and relevant microbiome and clinical features. Results: Seven maternal and two infant fecal microbial taxa were robustly associated with at least one asthma phenotype, and a longitudinal gut microenvironment profile was associated with early asthma (Fisher exact test p =.03). Though mode of delivery was not directly associated with asthma, we found substantial evidence for a pathway whereby cesarean section reduces fecal Bacteroides and microbial sphingolipids, increasing susceptibility to early asthma. Conclusion: Overall, our results suggest that the early‐life, including prenatal, fecal microbiome modifies risk of asthma, especially asthma with onset by age 3 years. [ABSTRACT FROM AUTHOR]
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- 2023
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41. Impact of Cesarean Delivery and Breastfeeding on Secretory Immunoglobulin A in the Infant Gut Is Mediated by Gut Microbiota and Metabolites.
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Chen, Yuan Yao, Tun, Hein M., Field, Catherine J., Mandhane, Piushkumar J., Moraes, Theo J., Simons, Elinor, Turvey, Stuart E., Subbarao, Padmaja, Scott, James A., and Kozyrskyj, Anita L.
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CESAREAN section ,BREASTFEEDING ,GUT microbiome ,INFANTS ,MICROBIAL metabolites ,DELIVERY (Obstetrics) ,METABOLITES - Abstract
How gut immunity in early life is shaped by birth in relation to delivery mode, intrapartum antibiotic prophylaxis (IAP) and labor remains undetermined. We aimed to address this gap with a study of secretory Immunoglobulin A (SIgA) in the infant gut that also tested SIgA-stimulating pathways mediated by gut microbiota and metabolites. Among 1017 Canadian full-term infants, gut microbiota of fecal samples collected at 3 and 12 months were profiled using 16S rRNA sequencing; C. difficile was quantified by qPCR; fecal metabolites and SIgA levels were measured by NMR and SIgA enzyme-linked immunosorbent assay, respectively. We assessed the putative causal relationships from birth events to gut microbiota and metabolites, and ultimately to SIgA, in statistical sequential mediation models, adjusted for maternal gravida status in 551 infants. As birth mode influences the ability to breastfeed, the statistical mediating role of breastfeeding status and milk metabolites was also evaluated. Relative to vaginal birth without maternal IAP, cesarean section (CS) after labor was associated with reduced infant gut SIgA levels at 3 months (6.27 vs. 4.85 mg/g feces, p < 0.05); this association was sequentially mediated through gut microbiota and metabolites of microbial or milk origin. Mediating gut microbiota included Enterobacteriaceae, C. difficile, and Streptococcus. The milk or microbial metabolites in CS-SIgA mediating pathways were galactose, fucose, GABA, choline, lactate, pyruvate and 1,2-propanediol. This cohort study documented the impact of birth on infant gut mucosal SIgA. It is the first to characterize gut microbe-metabolite mediated pathways for early-life SIgA maturation, pathways that require experimental verification. [ABSTRACT FROM AUTHOR]
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- 2023
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42. Lung Function as a Biomarker of Health: An Old Concept Rediscovered.
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Reyna, Myrtha E., Bedard, Marc-Antoine, and Subbarao, Padmaja
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An editorial is presented on the concept of asthma as multiple related disorders rather than a single disease diagnosis, with declining lung function as a trait of moderate to severe asthma. It emphasize the importance of understanding these phenotypes to inform disease prevention strategies and underscore the significance of investigating lung function decline, symptoms, and morbidity in asthma management.
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- 2023
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43. The human milk proteome and allergy of mother and child: Exploring associations with protein abundances and protein network connectivity.
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Dekker, Pieter M., Azad, Meghan B., Boeren, Sjef, Mandhane, Piushkumar J., Moraes, Theo J., Simons, Elinor, Subbarao, Padmaja, Turvey, Stuart E., Saccenti, Edoardo, and Hettinga, Kasper A.
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MILK allergy ,BREAST milk ,MOTHER-child relationship ,FOOD allergy ,MILK proteins ,BABY foods ,GOAT milk - Abstract
Background: The human milk proteome comprises a vast number of proteins with immunomodulatory functions, but it is not clear how this relates to allergy of the mother or allergy development in the breastfed infant. This study aimed to explore the relation between the human milk proteome and allergy of both mother and child. Methods: Proteins were analyzed in milk samples from a subset of 300 motherchild dyads from the Canadian CHILD Cohort Study, selected based on maternal and child allergy phenotypes. For this selection, the definition of "allergy" included food allergy, eczema, allergic rhinitis, and asthma. Proteins were analyzed with non-targeted shotgun proteomics using filter-aided sample preparation (FASP) and nanoLC-Orbitrap-MS/MS. Protein abundances, based on label-free quantification, were compared using multiple statistical approaches, including univariate, multivariate, and network analyses. Results: Using univariate analysis, we observed a trend that milk for infants who develop an allergy by 3 years of age contains higher abundances of immunoglobulin chains, irrespective of the allergy status of the mother. This observation suggests a difference in the milk's immunological potential, which might be related to the development of the infant's immune system. Furthermore, network analysis showed overall increased connectivity of proteins in the milk of allergic mothers and milk for infants who ultimately develop an allergy. This difference in connectivity was especially noted for proteins involved in the protein translation machinery and may be due to the physiological status of the mother, which is reflected in the interconnectedness of proteins in her milk. In addition, it was shown that network analysis complements the other methods for data analysis by revealing complex associations between the milk proteome and mother-child allergy status. Conclusion: Together, these findings give new insights into how the human milk proteome, through differences in the abundance of individual proteins and protein-protein associations, relates to the allergy status of mother and child. In addition, these results inspire new research directions into the complex interplay of the mother-milk-infant triad and allergy. [ABSTRACT FROM AUTHOR]
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- 2022
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44. Prediction of odds for emergency cesarean section: A secondary analysis of the CHILD term birth cohort study.
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Tun, Mon H., Chari, Radha, Kaul, Padma, Mamede, Fabiana V., Paulden, Mike, Lefebvre, Diana L., Turvey, Stuart E., Moraes, Theo J., Sears, Malcolm R., Subbarao, Padmaja, and Mandhane, Piush J.
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CHILDBIRTH ,DELIVERY (Obstetrics) ,CESAREAN section ,RECEIVER operating characteristic curves ,COHORT analysis ,SECONDARY analysis - Abstract
Introduction: Previously developed cesarean section (CS) and emergency CS prediction tools use antenatal and intrapartum risk factors. We aimed to develop a predictive model for the risk of emergency CS before the onset of labour utilizing antenatal obstetric and non-obstetric factors. Methods: We completed a secondary analysis of data collected from the CHILD Cohort Study. The analysis was limited to term (≥37 weeks), singleton pregnant women with cephalic presentation. The sample was divided into a training and validation dataset. The emergency CS prediction model was developed in the training dataset and the performance accuracy was assessed by the area under the receiver operating characteristic curve(AUC) of the receiver operating characteristic analysis (ROC). Our final model was subsequently evaluated in the validation dataset. Results: The participant sample consisted of 2,836 pregnant women. Mean age of participants was 32 years, mean BMI of 25.4 kg/m2 and 39% were nulliparous. 14% had emergency CS delivery. Each year of increasing maternal age increased the odds of emergency CS by 6% (adjusted Odds Ratio (aOR 1.06,1.02–1.08). Likewise, there was a 4% increase odds of emergency CS for each unit increase in BMI (aOR 1.04,1.02–1.06). In contrast, increase in maternal height has a negative association with emergency CS. The final emergency CS delivery predictive model included six variables (hypertensive disorders of pregnancy, antenatal depression, previous vaginal delivery, age, height, BMI). The AUC for our final prediction model was 0.74 (0.72–0.77) in the training set with a similar AUC in the validation dataset (0.77; 0.71–0.82). Conclusion: The developed and validated emergency CS delivery prediction model can be used in counselling prospective parents around their CS risk and healthcare resource planning. Further validation of the tool is suggested. [ABSTRACT FROM AUTHOR]
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- 2022
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45. Factors associated with breast-feeding initiation and continuation in Canadian-born and non-Canadian-born women: a multi-centre study.
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Chooniedass, Rishma, Tarrant, Marie, Turner, Sarah, Lok Fan, Heidi Sze, Del Buono, Katie, Masina, Stephanie, Becker, Allan B, Mandhane, Piushkumar, Turvey, Stuart E, Moraes, Theo, Sears, Malcolm R, Subbarao, Padmaja, and Azad, Meghan B
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BREASTFEEDING ,MATERNAL age ,INFANT development ,CANADIAN provinces ,PREGNANT women ,COMMUNITIES - Abstract
Objective: To identify factors associated with breast-feeding initiation and continuation in Canadian-born and non-Canadian-born women. Design: Prospective cohort of mothers and infants born from 2008 to 2012: the Canadian Healthy Infant Longitudinal Development (CHILD) Cohort Study. Setting: General community setting in four Canadian provinces. Participants: In total, 3455 pregnant women from Vancouver, Edmonton, Winnipeg and Toronto between 2008 and 2012. Results: Of 3010 participants included in the current study, the majority were Canadian-born (75·5 %). Breast-feeding initiation rates were high in both non-Canadian-born (95·5 %) and Canadian-born participants (92·7 %). The median breast-feeding duration was 10 months in Canadian-born participants and 11 months in non-Canadian-born participants. Among Canadian-born participants, factors associated with breast-feeding initiation and continuation were older maternal age, higher maternal education, living with their partner and recruitment site. Rooming-in during the hospital stay was also associated with higher rates of breast-feeding initiation, but not continuation at 6-month postpartum. Factors associated with non-initiation of breast-feeding and cessation at 6-month postpartum were maternal smoking, living with a current smoker, caesarean birth and early-term birth. Among non-Canadian-born participants, maternal smoking during pregnancy was associated with lower odds of breast-feeding initiation and lower odds of breast-feeding continuation at 6 months, and older maternal age and recruitment site were associated with breast-feeding continuation at 6 months. Conclusions: Although Canadian-born and non-Canadian-born women in the CHILD cohort have similar breast-feeding initiation rates, breast-feeding initiation and continuation are more strongly associated with socio-demographic characteristics in Canadian-born participants. Recruitment site was strongly associated with breast-feeding continuation in both groups and may indicate geographic disparities in breast-feeding rates nationally. [ABSTRACT FROM AUTHOR]
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- 2022
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46. From Prescription Drugs to Natural Health Products: Medication Use in Canadian Infants.
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Bedard, Pascal, Winsor, Geoffrey L., Garlock, Emma S., Azad, Meghan B., Becker, Allan B., Mandhane, Piush J., Moraes, Theo J., Sears, Malcolm R., Turvey, Stuart E., Subbarao, Padmaja, Brinkman, Fiona S. L., and Kozyrskyj, Anita L.
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BIOTHERAPY ,RESEARCH ,RESEARCH methodology ,PEDIATRICS ,SURVEYS ,DRUGS ,DESCRIPTIVE statistics ,RESEARCH funding ,LONGITUDINAL method ,PARENTS ,CHILDREN - Abstract
Limited data exist on pharmaceutical product use by infants, although available data suggests higher prevalence of use among children under 12 months of age. We conducted a descriptive study of 3050 infants recruited in the CHILD Cohort Study, a prospective, multicenter, longitudinal cohort following children from pregnancy through childhood. Parents were surveyed for use of prescription and over-the-counter drugs, and natural health products (NHPs, including homeopathic products and vitamins) at 3, 6, and 12 months after delivery. By one year of age, 96.0% of children had taken at least one pharmaceutical product. Among 307 reported products, 32 were given to at least 1% of cohort infants. Vitamin D, acetaminophen, ibuprofen, topical hydrocortisone, amoxicillin, and nystatin were the most common medications and natural health products (NHPs) received, with 8/32 of the most frequently used products being NHPs. Overall, 14.7% of pharmaceutical products administered to children were off-label and 35.8% were NHPs or products without a Drug Identification Number (DIN). The use of over-the-counter medications and NHPs is common and off-label use of drugs is frequent, even in the first year of life. This study highlights the importance of conducting studies on medication use in infants, and of infant medication use monitoring by healthcare providers. [ABSTRACT FROM AUTHOR]
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- 2022
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47. Early Life Antimicrobial Exposure: Impact on Clostridioides difficile Colonization in Infants.
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Obiakor, Chinwe Vivien, Parks, Jaclyn, Takaro, Tim K., Tun, Hein M., Morales-Lizcano, Nadia, Azad, Meghan B., Mandhane, Piushkumar J., Moraes, Theo J., Simons, Elinor, Turvey, Stuart E., Subbarao, Padmaja, Scott, James A., and Kozyrskyj, Anita L.
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BACTERIAL colonies ,INFANTS ,CLOSTRIDIOIDES difficile ,RNA ,COHORT analysis - Abstract
The relationship between antibiotic use and Clostridioides difficile (C. difficile) has been well established in adults and older children but remains unclear and is yet to be fully examined in infant populations. This study aimed to determine the separate and cumulative impact from antibiotics and household cleaning products on C. difficile colonization in infants. This study included 1429 infants at 3–4 months of age and 1728 infants at 12 months of age from the Canadian Healthy Infant Longitudinal Development (CHILD) birth cohort. The levels of infant antimicrobial exposure were obtained from hospital birth charts and standardized questionnaires. Infant gut microbiota was characterized by Illumina 16S ribosomal ribonucleic acid (rRNA) gene sequencing. Analysis of C. difficile was performed using a quantitative polymerase chain reaction (qPCR). Overall, C. difficile colonized 31% and 46% of infants at 3–4 months and 12 months, respectively. At 3–4 months, C. difficile colonization was significantly higher in infants exposed to both antibiotics and higher (above average) usage of household cleaning products (adjusted odds ratio (aOR) 1.50, 95% CI 1.03–2.17; p = 0.032) than in infants who had the least antimicrobial exposure. This higher colonization persisted up to 12 months of age. Our study suggests that cumulative exposure to systemic antibiotics and higher usage of household cleaning products facilitates C. difficile colonization in infants. Further research is needed to understand the future health impacts. [ABSTRACT FROM AUTHOR]
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- 2022
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48. Wheeze trajectories: Determinants and outcomes in the CHILD Cohort Study.
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Dai, Ruixue, Miliku, Kozeta, Gaddipati, Sirisha, Choi, Jihoon, Ambalavanan, Amirthagowri, Tran, Maxwell M., Reyna, Myrtha, Sbihi, Hind, Lou, Wendy, Parvulescu, Paula, Lefebvre, Diana L., Becker, Allan B., Azad, Meghan B., Mandhane, Piush J., Turvey, Stuart E., Duan, Qingling, Moraes, Theo J., Sears, Malcolm R., and Subbarao, Padmaja
- Abstract
Wheezing in early life is associated with asthma in adulthood; however, the determinants of wheezing trajectories and their associations with asthma and lung function in childhood remain poorly understood. In the CHILD Cohort Study, we aimed to identify wheezing trajectories and examine the associations between these trajectories, risk factors, and clinical outcomes at age 5 years. Wheeze data were collected at 8 time points from 3 months to 5 years of age. We used group-based trajectory models to derive wheeze trajectories among 3154 children. Associations with risk factors and clinical outcomes were analyzed by weighted regression models. We identified 4 trajectories: a never/infrequent trajectory, transient wheeze, intermediate-onset (preschool) wheeze, and persistent wheeze. Higher body mass index was a common risk factor for all wheeze trajectories compared with that in the never/infrequent group. The unique predictors for specific wheeze trajectories included male sex, lower respiratory tract infections, and day care attendance for transient wheeze; paternal history of asthma, atopic sensitization, and child genetic risk score of asthma for intermediate wheeze; and maternal asthma for persistent wheeze. Blood eosinophil counts were higher in children with the intermediate wheeze trajectory than in those children with the other trajectories at the ages of 1 and 5 years. All wheeze trajectories were associated with decreased lung function and increased risk of asthma at age 5 years. We identified 4 distinct trajectories in children from 3 months to 5 years of age, reflecting different phenotypes of early childhood wheeze. These trajectories were characterized by different biologic and physiologic traits and risk factors. [Display omitted] [ABSTRACT FROM AUTHOR]
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- 2022
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49. Lung clearance index predicts persistence of preschool wheeze.
- Author
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Safavi, Shahideh, Dai, Ruixue, Breton, Vanessa L., Emmerson, Melanie N., Kowalik, Krzysztof, Lu, Zihang, Lou, Wendy, Dubeau, Aimée, DeLorenzo, Stephanie, Azad, Meghan B., Becker, Allan B., Mandhane, Piush J., Turvey, Stuart E., Gustafsson, Per, Lefebvre, Diana L., Sears, Malcolm R., Moraes, Theo J., Subbarao, Padmaja, and Kalayci, Ömer
- Subjects
WHEEZE ,PRESCHOOL children ,LUNGS ,MASS spectrometry - Abstract
Background: The lung clearance index (LCI) is a measure of pulmonary function. Variable feasibility (50‐>80%) in preschool children has been reported. There are limited studies exploring its relationship to respiratory symptoms and how it predicts persistent wheeze. We aimed to assess the association with respiratory symptoms in preschool‐aged children with LCI and determine its utility in predicting persistent wheeze. Methods: LCI was measured in a subcohort of the CHILD Cohort Study at age 3 years using SF6 multiple breath washout test mass spectrometry. Respiratory symptom phenotypes at age 3 were derived from children's respiratory symptoms reported by their parents. Responses were used to categorize children into 4 symptom groups: recurrent wheeze (3RW), recurrent cough (3RC), infrequent symptoms (IS), and no current symptoms (NCS). At age 5 years, these children were seen by a specialist clinician and assessed for persistent wheeze (PW). Results: At age 3 years, 69% (234/340) had feasible LCI. Excluding two children with missing data, 232 participants were categorized as follows: 33 (14%) 3RW; 28 (12%) 3RC; 17 (7%) IS; and 154 (66%) NCS. LCI z‐score at age 3 years was highest in children with 3RW compared to 3RC (mean (SD): 1.14 (1.56) vs. 0.09 (0.95), p <.01), IS (mean (SD): −0.14 (0.59), p <.01), and NCS (mean (SD): −0.08 (1.06), p <.01). LCI z‐score at age 3 was predictive of persistent wheeze at age 5 (PW) (AUROC: 0.87). Conclusions: LCI at age 3 was strongly associated with recurrent wheeze at age 3, and predictive of its persistence to age 5. [ABSTRACT FROM AUTHOR]
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- 2022
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50. Early‐life cytomegalovirus infection is associated with gut microbiota perturbations and increased risk of atopy.
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Sbihi, Hind, Simmons, Karen E., Sears, Malcolm R., Moraes, Theo J., Becker, Allan B., Mandhane, Piush J., Subbarao, Padmaja, Dai, Darlene L. Y., Finlay, B. Brett, Turvey, Stuart E., Gantt, Soren, and Genuneit, Jon
- Subjects
CYTOMEGALOVIRUS diseases ,ATOPY ,GUT microbiome ,JUVENILE diseases ,ALLERGIES ,URINALYSIS - Abstract
Background: The "old friends" hypothesis posits that reduced exposure to previously ubiquitous microorganisms is one factor involved in the increased rates of allergic diseases. Cytomegalovirus (CMV) may be one of the "old friends" hypothesized to help prevent allergic diseases. We sought to elucidate whether early‐life CMV infection is associated with childhood atopy via perturbations of the gut microbiota. Methods: Participants were recruited from a population‐based birth cohort (CHILD study) and followed prospectively until age 5 years in four Canadian cities. A total of 928 participants provided stool microbiome data, urine for CMV testing, skin prick tests, and questionnaire‐based detailed environmental exposures. Cytomegalovirus infection was assessed in the first year of life while the main outcome was defined by persistent sensitization to any allergen at ages 1, 3, and 5 years. Results: Early CMV infection was associated with increased beta and decreased alpha diversity of the gut microbiota. Both changes in diversity measures and early CMV infection were associated with persistent allergic sensitization at age 5 years (aOR = 2.08; 95% CI: 1, 4.33). Mediation analysis demonstrated that perturbation of gut microbial composition explains 30% of the association. Conclusions: Early‐life CMV infection is associated with an alteration in the intestinal microbiota, which mediates the effect of the infection on childhood atopy. This work indicates that preventing CMV infection would not put children at increased risk of developing atopy. Rather, a CMV vaccine, in addition to preventing CMV‐associated morbidity and mortality, might reduce the risk of childhood allergic diseases. [ABSTRACT FROM AUTHOR]
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- 2022
- Full Text
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