Hydrocortisone in Preterm Infants and School-Age Functional Outcomes: Follow-Up of a Randomized Clinical Trial

Sara B. DeMauro; Haresh Kirpalani; Susan Hintz; Kristi L. Watterberg; Victoria Watson; Jean Lowe; Seetha Shankaran; Sanjay Chawla; Betty Vohr; Michael E. Msall; Carl T. D'Angio; Bradley A. Yoder; Khanh Lai; Sarah Winter; Tarah T. Colaizy; Stephanie L. Merhar; Kristina Ziolkowski; Carla M. Bann; Marissa Trotta; Jamie E. Newman; Michele C. Walsh; Rosemary D. Higgins; Tanya E. Cahill; Andrea F. Duncan; Deanne E. Wilson-Costello; Myriam Peralta-Carcelen; Hope Arnold; Ricardo A. Mosquera; Roy J. Heyne; Janell Fuller; Elisabeth C. McGowan; Brenna Cavanaugh; Heidi M. Harmon; Nathalie L. Maitre; Mary Lauren Neel; Krisa P. Van Meurs; Laurie A. Richards; Howard W. Kilbride; Abbey C. Hines; Girija Natarajan; Andrea Trembath; Kristen L. Benninger; Kalpashri Kesavan; William F. Malcolm; Dinorah Zanger; Ann Marie Reynolds; Martha Carlson; Abhik Das

doi:10.1001/jamapediatrics.2025.4801

Hydrocortisone in Preterm Infants and School-Age Functional Outcomes: Follow-Up of a Randomized Clinical Trial

Sara B. DeMauro
, Haresh Kirpalani
, Susan Hintz
, Kristi L. Watterberg
, Victoria Watson
, Jean Lowe
, Seetha Shankaran
, Sanjay Chawla
, Betty Vohr
, Michael E. Msall
, Carl T. D'Angio
, Bradley A. Yoder
, Khanh Lai
, Sarah Winter
, Tarah T. Colaizy
, Stephanie L. Merhar
, Kristina Ziolkowski
, Carla M. Bann
, Marissa Trotta
, Jamie E. Newman

Michele C. Walsh, Rosemary D. Higgins, Tanya E. Cahill, Andrea F. Duncan, Deanne E. Wilson-Costello, Myriam Peralta-Carcelen, Hope Arnold, Ricardo A. Mosquera, Roy J. Heyne, Janell Fuller, Elisabeth C. McGowan, Brenna Cavanaugh, Heidi M. Harmon, Nathalie L. Maitre, Mary Lauren Neel, Krisa P. Van Meurs, Laurie A. Richards, Howard W. Kilbride, Abbey C. Hines, Girija Natarajan, Andrea Trembath, Kristen L. Benninger, Kalpashri Kesavan, William F. Malcolm, Dinorah Zanger, Ann Marie Reynolds, Martha Carlson, Abhik Das

Pediatrics

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Research output: Contribution to journal › Article › peer-review

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Abstract

Importance: Bronchopulmonary dysplasia (BPD) is the most common in-hospital morbidity of prematurity, associated with significant long-term medical and neurodevelopmental sequelae and health resource utilization. The Neonatal Research Network (NRN) Hydrocortisone for BPD Trial evaluated the efficacy and safety of hydrocortisone to prevent BPD in high-risk very preterm infants; the impact of hydrocortisone on school-age outcomes in this trial cohort is previously unreported. Objective: To evaluate the impact of neonatal hydrocortisone treatment on early school-age functional motor, cognitive, academic, and pulmonary outcomes among children who participated in the Hydrocortisone for BPD Trial. Design, Setting, and Participants: This prospective long-term cohort study is a follow-up of a randomized clinical trial, the Hydrocortisone for BPD Trial, conducted at 19 centers of the Eunice Kennedy Shriver National Institute of Child Health and Human Development NRN. Participants, enrolled from August 2011 to February 2018, included intubated infants who had been born before 30 weeks' gestational age and had been mechanically ventilated for at least 7 days by postnatal day 14 to 28. They were eligible for a single, in-person, early school-age visit between corrected age 5 years 0 months and 7 years 11 months, conducted from September 2017 to July 2024. Data analysis was performed from July 2024 to September 2025. Intervention: Participants were randomized to a 10-day tapering course of hydrocortisone or placebo beginning at 14 to 28 postnatal days. Main Outcomes and Measures: Early school-age study visits were performed by certified, masked assessors. The primary outcome of functional impairment was defined as any of the following: cognitive delay, motor delay, academic delay, or poor functional exercise capacity. Results: The primary outcome was available for 545 of 674 eligible children (80.9%), including 272 children in the hydrocortisone group (152 [55.9%] female; mean [SD] gestational age, 24.9 [1.5] weeks; mean [SD] age at visit, 5.3 [0.6] years) and 273 in the placebo group (108 [39.6%] female; mean [SD] gestational age, 24.8 [1.5] weeks; mean [SD] age at visit, 5.4 [0.6] years). There was no difference in the rate of functional impairment between the hydrocortisone group (194 of 272 children [71.3%]) and the placebo group (200 of 273 children [73.3%]) (adjusted relative risk, 0.99; 95% CI, 0.89-1.10), nor were there differences in the rates of the individual components. Motor delay was the most common impairment (308 of 510 children [60.4%]), followed by poor functional exercise capacity (175 of 484 children [36.2%]). Conclusions and Relevance: In this study, neonatal hydrocortisone treatment of preterm infants with high risk for BPD did not impact functional impairment or its components; nearly three-quarters of the children demonstrated functional impairment at school age. Trial Registration: ClinicalTrials.gov

Original language	English
Journal	JAMA Pediatrics
DOIs	https://doi.org/10.1001/jamapediatrics.2025.4801
State	Accepted/In press - 2025

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10.1001/jamapediatrics.2025.4801

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DeMauro, S. B., Kirpalani, H., Hintz, S., Watterberg, K. L., Watson, V., Lowe, J., Shankaran, S., Chawla, S., Vohr, B., Msall, M. E., D'Angio, C. T., Yoder, B. A., Lai, K., Winter, S., Colaizy, T. T., Merhar, S. L., Ziolkowski, K., Bann, C. M., Trotta, M., ... Das, A. (Accepted/In press). Hydrocortisone in Preterm Infants and School-Age Functional Outcomes: Follow-Up of a Randomized Clinical Trial. JAMA Pediatrics. https://doi.org/10.1001/jamapediatrics.2025.4801

@article{ade89097a79b4c6c8c8b6c127143efb2,

title = "Hydrocortisone in Preterm Infants and School-Age Functional Outcomes: Follow-Up of a Randomized Clinical Trial",

abstract = "Importance: Bronchopulmonary dysplasia (BPD) is the most common in-hospital morbidity of prematurity, associated with significant long-term medical and neurodevelopmental sequelae and health resource utilization. The Neonatal Research Network (NRN) Hydrocortisone for BPD Trial evaluated the efficacy and safety of hydrocortisone to prevent BPD in high-risk very preterm infants; the impact of hydrocortisone on school-age outcomes in this trial cohort is previously unreported. Objective: To evaluate the impact of neonatal hydrocortisone treatment on early school-age functional motor, cognitive, academic, and pulmonary outcomes among children who participated in the Hydrocortisone for BPD Trial. Design, Setting, and Participants: This prospective long-term cohort study is a follow-up of a randomized clinical trial, the Hydrocortisone for BPD Trial, conducted at 19 centers of the Eunice Kennedy Shriver National Institute of Child Health and Human Development NRN. Participants, enrolled from August 2011 to February 2018, included intubated infants who had been born before 30 weeks' gestational age and had been mechanically ventilated for at least 7 days by postnatal day 14 to 28. They were eligible for a single, in-person, early school-age visit between corrected age 5 years 0 months and 7 years 11 months, conducted from September 2017 to July 2024. Data analysis was performed from July 2024 to September 2025. Intervention: Participants were randomized to a 10-day tapering course of hydrocortisone or placebo beginning at 14 to 28 postnatal days. Main Outcomes and Measures: Early school-age study visits were performed by certified, masked assessors. The primary outcome of functional impairment was defined as any of the following: cognitive delay, motor delay, academic delay, or poor functional exercise capacity. Results: The primary outcome was available for 545 of 674 eligible children (80.9\%), including 272 children in the hydrocortisone group (152 [55.9\%] female; mean [SD] gestational age, 24.9 [1.5] weeks; mean [SD] age at visit, 5.3 [0.6] years) and 273 in the placebo group (108 [39.6\%] female; mean [SD] gestational age, 24.8 [1.5] weeks; mean [SD] age at visit, 5.4 [0.6] years). There was no difference in the rate of functional impairment between the hydrocortisone group (194 of 272 children [71.3\%]) and the placebo group (200 of 273 children [73.3\%]) (adjusted relative risk, 0.99; 95\% CI, 0.89-1.10), nor were there differences in the rates of the individual components. Motor delay was the most common impairment (308 of 510 children [60.4\%]), followed by poor functional exercise capacity (175 of 484 children [36.2\%]). Conclusions and Relevance: In this study, neonatal hydrocortisone treatment of preterm infants with high risk for BPD did not impact functional impairment or its components; nearly three-quarters of the children demonstrated functional impairment at school age. Trial Registration: ClinicalTrials.gov",

author = "DeMauro, \{Sara B.\} and Haresh Kirpalani and Susan Hintz and Watterberg, \{Kristi L.\} and Victoria Watson and Jean Lowe and Seetha Shankaran and Sanjay Chawla and Betty Vohr and Msall, \{Michael E.\} and D'Angio, \{Carl T.\} and Yoder, \{Bradley A.\} and Khanh Lai and Sarah Winter and Colaizy, \{Tarah T.\} and Merhar, \{Stephanie L.\} and Kristina Ziolkowski and Bann, \{Carla M.\} and Marissa Trotta and Newman, \{Jamie E.\} and Walsh, \{Michele C.\} and Higgins, \{Rosemary D.\} and Cahill, \{Tanya E.\} and Duncan, \{Andrea F.\} and Wilson-Costello, \{Deanne E.\} and Myriam Peralta-Carcelen and Hope Arnold and Mosquera, \{Ricardo A.\} and Heyne, \{Roy J.\} and Janell Fuller and McGowan, \{Elisabeth C.\} and Brenna Cavanaugh and Harmon, \{Heidi M.\} and Maitre, \{Nathalie L.\} and Neel, \{Mary Lauren\} and \{Van Meurs\}, \{Krisa P.\} and Richards, \{Laurie A.\} and Kilbride, \{Howard W.\} and Hines, \{Abbey C.\} and Girija Natarajan and Andrea Trembath and Benninger, \{Kristen L.\} and Kalpashri Kesavan and Malcolm, \{William F.\} and Dinorah Zanger and Reynolds, \{Ann Marie\} and Martha Carlson and Abhik Das",

note = "Publisher Copyright: {\textcopyright} 2026 American Medical Association.",

year = "2025",

doi = "10.1001/jamapediatrics.2025.4801",

language = "English",

journal = "JAMA Pediatrics",

issn = "2168-6203",

publisher = "American Medical Association",

}

DeMauro, SB, Kirpalani, H, Hintz, S, Watterberg, KL, Watson, V, Lowe, J, Shankaran, S, Chawla, S, Vohr, B, Msall, ME, D'Angio, CT, Yoder, BA, Lai, K, Winter, S, Colaizy, TT, Merhar, SL, Ziolkowski, K, Bann, CM, Trotta, M, Newman, JE, Walsh, MC, Higgins, RD, Cahill, TE, Duncan, AF, Wilson-Costello, DE, Peralta-Carcelen, M, Arnold, H, Mosquera, RA, Heyne, RJ, Fuller, J, McGowan, EC, Cavanaugh, B, Harmon, HM, Maitre, NL, Neel, ML, Van Meurs, KP, Richards, LA, Kilbride, HW, Hines, AC, Natarajan, G, Trembath, A, Benninger, KL, Kesavan, K, Malcolm, WF, Zanger, D, Reynolds, AM, Carlson, M & Das, A 2025, 'Hydrocortisone in Preterm Infants and School-Age Functional Outcomes: Follow-Up of a Randomized Clinical Trial', JAMA Pediatrics. https://doi.org/10.1001/jamapediatrics.2025.4801

TY - JOUR

T1 - Hydrocortisone in Preterm Infants and School-Age Functional Outcomes

T2 - Follow-Up of a Randomized Clinical Trial

AU - DeMauro, Sara B.

AU - Kirpalani, Haresh

AU - Hintz, Susan

AU - Watterberg, Kristi L.

AU - Watson, Victoria

AU - Lowe, Jean

AU - Shankaran, Seetha

AU - Chawla, Sanjay

AU - Vohr, Betty

AU - Msall, Michael E.

AU - D'Angio, Carl T.

AU - Yoder, Bradley A.

AU - Lai, Khanh

AU - Winter, Sarah

AU - Colaizy, Tarah T.

AU - Merhar, Stephanie L.

AU - Ziolkowski, Kristina

AU - Bann, Carla M.

AU - Trotta, Marissa

AU - Newman, Jamie E.

AU - Walsh, Michele C.

AU - Higgins, Rosemary D.

AU - Cahill, Tanya E.

AU - Duncan, Andrea F.

AU - Wilson-Costello, Deanne E.

AU - Peralta-Carcelen, Myriam

AU - Arnold, Hope

AU - Mosquera, Ricardo A.

AU - Heyne, Roy J.

AU - Fuller, Janell

AU - McGowan, Elisabeth C.

AU - Cavanaugh, Brenna

AU - Harmon, Heidi M.

AU - Maitre, Nathalie L.

AU - Neel, Mary Lauren

AU - Van Meurs, Krisa P.

AU - Richards, Laurie A.

AU - Kilbride, Howard W.

AU - Hines, Abbey C.

AU - Natarajan, Girija

AU - Trembath, Andrea

AU - Benninger, Kristen L.

AU - Kesavan, Kalpashri

AU - Malcolm, William F.

AU - Zanger, Dinorah

AU - Reynolds, Ann Marie

AU - Carlson, Martha

AU - Das, Abhik

PY - 2025

Y1 - 2025

N2 - Importance: Bronchopulmonary dysplasia (BPD) is the most common in-hospital morbidity of prematurity, associated with significant long-term medical and neurodevelopmental sequelae and health resource utilization. The Neonatal Research Network (NRN) Hydrocortisone for BPD Trial evaluated the efficacy and safety of hydrocortisone to prevent BPD in high-risk very preterm infants; the impact of hydrocortisone on school-age outcomes in this trial cohort is previously unreported. Objective: To evaluate the impact of neonatal hydrocortisone treatment on early school-age functional motor, cognitive, academic, and pulmonary outcomes among children who participated in the Hydrocortisone for BPD Trial. Design, Setting, and Participants: This prospective long-term cohort study is a follow-up of a randomized clinical trial, the Hydrocortisone for BPD Trial, conducted at 19 centers of the Eunice Kennedy Shriver National Institute of Child Health and Human Development NRN. Participants, enrolled from August 2011 to February 2018, included intubated infants who had been born before 30 weeks' gestational age and had been mechanically ventilated for at least 7 days by postnatal day 14 to 28. They were eligible for a single, in-person, early school-age visit between corrected age 5 years 0 months and 7 years 11 months, conducted from September 2017 to July 2024. Data analysis was performed from July 2024 to September 2025. Intervention: Participants were randomized to a 10-day tapering course of hydrocortisone or placebo beginning at 14 to 28 postnatal days. Main Outcomes and Measures: Early school-age study visits were performed by certified, masked assessors. The primary outcome of functional impairment was defined as any of the following: cognitive delay, motor delay, academic delay, or poor functional exercise capacity. Results: The primary outcome was available for 545 of 674 eligible children (80.9%), including 272 children in the hydrocortisone group (152 [55.9%] female; mean [SD] gestational age, 24.9 [1.5] weeks; mean [SD] age at visit, 5.3 [0.6] years) and 273 in the placebo group (108 [39.6%] female; mean [SD] gestational age, 24.8 [1.5] weeks; mean [SD] age at visit, 5.4 [0.6] years). There was no difference in the rate of functional impairment between the hydrocortisone group (194 of 272 children [71.3%]) and the placebo group (200 of 273 children [73.3%]) (adjusted relative risk, 0.99; 95% CI, 0.89-1.10), nor were there differences in the rates of the individual components. Motor delay was the most common impairment (308 of 510 children [60.4%]), followed by poor functional exercise capacity (175 of 484 children [36.2%]). Conclusions and Relevance: In this study, neonatal hydrocortisone treatment of preterm infants with high risk for BPD did not impact functional impairment or its components; nearly three-quarters of the children demonstrated functional impairment at school age. Trial Registration: ClinicalTrials.gov

AB - Importance: Bronchopulmonary dysplasia (BPD) is the most common in-hospital morbidity of prematurity, associated with significant long-term medical and neurodevelopmental sequelae and health resource utilization. The Neonatal Research Network (NRN) Hydrocortisone for BPD Trial evaluated the efficacy and safety of hydrocortisone to prevent BPD in high-risk very preterm infants; the impact of hydrocortisone on school-age outcomes in this trial cohort is previously unreported. Objective: To evaluate the impact of neonatal hydrocortisone treatment on early school-age functional motor, cognitive, academic, and pulmonary outcomes among children who participated in the Hydrocortisone for BPD Trial. Design, Setting, and Participants: This prospective long-term cohort study is a follow-up of a randomized clinical trial, the Hydrocortisone for BPD Trial, conducted at 19 centers of the Eunice Kennedy Shriver National Institute of Child Health and Human Development NRN. Participants, enrolled from August 2011 to February 2018, included intubated infants who had been born before 30 weeks' gestational age and had been mechanically ventilated for at least 7 days by postnatal day 14 to 28. They were eligible for a single, in-person, early school-age visit between corrected age 5 years 0 months and 7 years 11 months, conducted from September 2017 to July 2024. Data analysis was performed from July 2024 to September 2025. Intervention: Participants were randomized to a 10-day tapering course of hydrocortisone or placebo beginning at 14 to 28 postnatal days. Main Outcomes and Measures: Early school-age study visits were performed by certified, masked assessors. The primary outcome of functional impairment was defined as any of the following: cognitive delay, motor delay, academic delay, or poor functional exercise capacity. Results: The primary outcome was available for 545 of 674 eligible children (80.9%), including 272 children in the hydrocortisone group (152 [55.9%] female; mean [SD] gestational age, 24.9 [1.5] weeks; mean [SD] age at visit, 5.3 [0.6] years) and 273 in the placebo group (108 [39.6%] female; mean [SD] gestational age, 24.8 [1.5] weeks; mean [SD] age at visit, 5.4 [0.6] years). There was no difference in the rate of functional impairment between the hydrocortisone group (194 of 272 children [71.3%]) and the placebo group (200 of 273 children [73.3%]) (adjusted relative risk, 0.99; 95% CI, 0.89-1.10), nor were there differences in the rates of the individual components. Motor delay was the most common impairment (308 of 510 children [60.4%]), followed by poor functional exercise capacity (175 of 484 children [36.2%]). Conclusions and Relevance: In this study, neonatal hydrocortisone treatment of preterm infants with high risk for BPD did not impact functional impairment or its components; nearly three-quarters of the children demonstrated functional impairment at school age. Trial Registration: ClinicalTrials.gov

UR - https://www.scopus.com/pages/publications/105024328853

U2 - 10.1001/jamapediatrics.2025.4801

DO - 10.1001/jamapediatrics.2025.4801

M3 - Article

C2 - 41359352

SN - 2168-6203

JO - JAMA Pediatrics

JF - JAMA Pediatrics

ER -

Hydrocortisone in Preterm Infants and School-Age Functional Outcomes: Follow-Up of a Randomized Clinical Trial

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