Human Milk Fortification in Extremely Preterm Infants (N-forte)
Primary Purpose
Necrotizing Enterocolitis, Sepsis, Mortality
Status
Active
Phase
Phase 2
Locations
Sweden
Study Type
Interventional
Intervention
H2MF
Bovine milk-based fortifier
Sponsored by
About this trial
This is an interventional prevention trial for Necrotizing Enterocolitis
Eligibility Criteria
Inclusion Criteria:
- Gestational age at birth 22+0-27+6: based on prenatal ultrasonography.
- Enteral feeds < 100 mL/kg/day at the day of randomisation.
- Written informed consent from the legal guardians of the infant.
- The home clinic of the infant has the logistics of maintaining the intervention until gestational week 34+0
Exclusion Criteria:
- Lethal or complicated malformation known at the time of inclusion
- Chromosomal anomalies known at the time of inclusion
- No realistic hope for survival at the time of inclusion
- Gastrointestinal malformation known at the time of inclusion
- Abdominal surgery before the time of inclusion
- Participation in another intervention trial aiming at having an effect on growth, nutrition, feeding intolerance or severe complications such as NEC and sepsis
- Infants having nutrient fortifier or formula prior to randomisation
Sites / Locations
- Queen Silvia Children´s Hospital
- Crown Princess Victoria Children´s Hospital
- Karolinska Hospital
- Norrlands Universitetssjukhus
- Akademiska Barnsjukhuset
Arms of the Study
Arm 1
Arm 2
Arm Type
Experimental
Active Comparator
Arm Label
H2MF
Standard fortifier
Arm Description
Human milk-based breast milk fortifier
Standard care: bovine milk-based breast milk fortifier
Outcomes
Primary Outcome Measures
The incidence of the composite of necrotizing enterocolitis, culture-proven sepsis and mortality
An infant should have had any of these diagnoses to fulfil the criterion
Secondary Outcome Measures
The incidence of the composite of necrotizing enterocolitis and culture-proven sepsis
An infant should have had any of these diagnoses to fulfil the criterion
The incidence of the composite of necrotizing enterocolitis culture-proven sepsis, bronchopulmonary dysplasia, retinopathy of prematurity and mortality (Mortality and morbidity index)
An infant should have had any of these diagnoses to fulfil the criterion
Time to reach full enteral feeds
The day of life the infant has received at least 150 mL/kg enteral feeds
Number of feeding interruptions
Number of days feedings held for ≥12 hours or feeds reduced by >50% (ml/kg/d) not due to a clinical procedure or transitioning to the breast
Numbers of days with parenteral nutrition
Number of days of parental amino acid and/or lipid infusion. Only days when the enteral feed <150mL/kg/day should be included
Number of large gastric aspirates per day
≥100% pre-feed volume (2 hours feeding volume if continuous feeding). Lower limit=2 ml/kg.
Stool frequency
Time to regain birth weight
Change in head circumference in centimeters
Change in weight in gram
Change in length in centimeters
The mortality incidence
The incidence of necrotising enterocolitis: Bell´s stage II-III
The incidence spontaneous intestinal perforation
The incidence of abdominal surgery
The incidence culture-proven sepsis
The incidence of suspected sepsis, not culture-proven
The incidence of pneumonia
Pathological X-ray confirmed by an independent radiologist, need of increased respiratory support/oxygen and laboratory inflammatory response
The incidence of bronchopulmonary dysplasia
Need of extra oxygen, continuous positive air pressure (CPAP) or ventilator at gestational week 36+0
The incidence of retinopathy of the prematurity
Classified into stage I-V. The diagnosis is set after gestational week 42+0
The incidence of intraventricular haemorrhage
Classified into grade I-IV according to Papile
The incidence of periventricular leukomalacia
Criteria according to de Vries
Number of days with intensive care
Need of respirator or CPAP until discharge (not later than gestational week 44+0).
Length of stay at the hospital
Gestational week and day at discharge (not later than gestational week 44+0).
Length of need of feeding tube
Gestational week and day when the infant does not need it anymore (not later than gestational week 44+0)
Neurocognitive development at 2 years
Bayleys III, PARCA-R (Parental Report of Children´s Abilities-Revised) and ASQ-3 (Ages and stages questionnaire)
Prevalence of cerebral palsy at 2 years
Prevalence of epilepsy at 2 years
Prevalence of squint and/or impaired vision at 2 years
Prevalence of impaired hearing at 2 years
The number of infants needing extra oxygen and/or ventilatory support after discharge from the hospital at the neonatal period
The incidence of wheeze and/or asthma
The incidence of severe infections after discharge from the neonatal unit
The number of infants needing feeding tube after discharge from the hospital at the neonatal period
The number of infants needing extra nutritional support after discharge from the hospital at the neonatal period
The prevalence of neurocognitive development at 5.5 years
Wechsler Preschool and Primary Scale of Intelligence IV (WPPSI-IV TM) and Movement ABC-2: the total scale points as well as the points of sub scales (motor, cognitive, language) will be presented. The prevalence of infants with a realist below 2 standard deviations will be defined to have mental retardation.
The prevalence of cerebral palsy at 5.5 years
The prevalence of epilepsy at 5.5 years of age
The prevalence of squint and/or impaired vision at 5.5 years of age
The prevalence of children with impaired hearing at 5.5 years of age
The prevalence of wheeze and/or asthma at 5.5 years of age
Microbiome composition in stool samples
The relative abundance and diversity of microbial taxa will be analyses with next generation sequencing and be related till the study intervention
Levels of subclasses of T and B cells and granulocytes in blood samples
T helper subsets (TH1, Th2, TH17, Treg), T cells subsets associated with the intestinal mucosa (gamma/delta-T cells, MAIT cells) and neutrophils will be assessed using masscytometry
Levels of immune markers in plasma
Pre planned analyses are anti-inflammatory (e.g. IL-10) and proinflammatory (e.g. TNF) cytokines and chemokines (e.g. CXCL11, CCL18).
Levels of growth factors in plasma samples
The levels of growth factors such as IGF-1 and the associated IGFBP-3 will be analysed.
Levels of lipids in plasma samples
Fatty acids in plasma
Levels of neurotransmitters in plasma samples
Neurotransmitters such as GABA and serotonin in plasma
Levels of metabolic peptides in urine samples
Metabolic peptide will be measured with proton nuclear magnetic resonance spectroscopy (NMR), liquid chromatography (LC) and mass spectroscopy couple to gas chromatography (GC-MC).
Levels of markers of central nervous system (CNS) damage in plasma samples
Markers of CNS damage such as neurofilament light protein will be measured in plasma
Levels of proteins in breast milk samples
Protein composition will be measured with multiplex methods
Levels of human milk oligosaccharides in breast milk samples
The levels of human milk oligosaccharides will be measured with high-performance anion-exchange chromatography with pulsed amperometric detection.
Health care costs
The number of days at each level of care will be recorded until discharge from the hospital (not longer than gestational week 44+0). The cost will be calculated by multiplying the number of days at each level of care by the average cost
Full Information
NCT ID
NCT03797157
First Posted
December 17, 2018
Last Updated
December 12, 2022
Sponsor
Thomas Abrahamsson, MD, PhD
Collaborators
Sahlgrenska University Hospital, Sweden, Region Uppsala, Vasterbottens lans landsting, Prolacta Bioscience, Region Stockholm
1. Study Identification
Unique Protocol Identification Number
NCT03797157
Brief Title
Human Milk Fortification in Extremely Preterm Infants
Acronym
N-forte
Official Title
Nordic Study on Human Milk Fortification in Extremely Preterm Infants: a Randomized Controlled Trial
Study Type
Interventional
2. Study Status
Record Verification Date
December 2022
Overall Recruitment Status
Active, not recruiting
Study Start Date
February 1, 2019 (Actual)
Primary Completion Date
September 1, 2022 (Actual)
Study Completion Date
December 31, 2027 (Anticipated)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor-Investigator
Name of the Sponsor
Thomas Abrahamsson, MD, PhD
Collaborators
Sahlgrenska University Hospital, Sweden, Region Uppsala, Vasterbottens lans landsting, Prolacta Bioscience, Region Stockholm
4. Oversight
Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes
5. Study Description
Brief Summary
This is a randomised controlled multi-centre trial comparing the effect of diet supplementation of a human breast milk-based nutrient fortifier (H2MF®) with standard bovine protein-based nutrient fortifier in 222 extremely preterm infants (born before gestational week 28+0) exclusively fed with human breast milk (own mother´s milk and/or donor milk). The infants will be randomised to receive either the human breast-milk based H2MF® or the standard bovine protein-based nutrient fortifier when oral feeds have reached <100 ml/kg/day.
The randomised intervention, stratified by centre, will continue until the target gestational week 34+0. The infant must not be fed with formula during the intervention period. The allocation will be concealed before inclusion, but after randomisation the study is not blinded.
Primary endpoint of the intervention is the composite variable necrotizing enterocolitis (NEC), sepsis and mortality.
The enrolled infants are characterised with clinical data including growth, feeding intolerance, use of enteral and parenteral nutrition, treatment, antibiotics and complications collected daily in a study specific case report form from birth until discharge from the hospital (not longer than gestational week 44+0). A follow up focusing on neurological development, growth and feeding problems will be performed at 2 years of age (corrected) and 5.5 years of age.
Detailed Description
This is a randomised controlled multi-centre trial comparing the effect of diet supplementation of a human breast milk-based nutrient fortifier (H2MF®) with standard bovine protein-based nutrient fortifier in 222 extremely preterm infants (born before gestational week 28+0) exclusively fed with human breast milk (own mother´s milk and/or donor milk). The infants will be randomised to receive either the human breast-milk based H2MF® or the standard bovine protein-based nutrient fortifier when oral feeds have reached <100 ml/kg/day. If fortification with extra enteral lipids is needed during the intervention period, the infants receiving H2MF® will be supplemented with the human milk-based Prolact CR®, while the infants receiving standard bovine protein-based fortification will be supplemented with the standard lipid products used at the unit. The study subject will be enrolled at level III neonatal intensive care unit (NICU)s. Only infants with a home clinic with the logistics to maintain the intervention until gestational week 34+0 will be included.
The randomised intervention, stratified by centre, will continue until the target gestational week 34+0. The infant must not be fed with formula during the intervention period. The allocation will be concealed before inclusion, but after randomisation the study is not blinded. It would not be possible to prescribe the fortifier and prepare of the breast milk in a blinded fashion, since the fortifiers are not exactly equal in nutrient content and also look different. Instead the assessment of several of the outcomes will be made blinded, such as the assessment of X-ray images in NEC cases.
The enrolled infants are characterised with clinical data including growth, feeding intolerance, use of enteral and parenteral nutrition, treatment, antibiotics and complications collected daily in a study specific case report form from birth until discharge from the hospital (not longer than gestational week 44+0). A follow up focusing on neurological development, growth and feeding problems will be performed at 2 years of age (corrected).
Since it is often difficult to distinguish between the diagnoses of NEC and sepsis, and their clinical consequences, the investigator's primary endpoint of the intervention is the composite variable NEC, sepsis and mortality. Secondary endpoints are feeding intolerance and other severe complication such as Bronchopulmonary dysplasia (BPD), Retinopathy of prematurity (ROP) and neurological impairment. Stool, urine and blood samples are also collected for microbiology, metabolomic and immunology analysis in order to study underlying mechanisms. Health economic analyses will be made to evaluate the costs and benefits of an introduction of human milk-based fortifier in NICUs in the Nordic countries.
Analyses will be conducted using an intention to treat approach. An evaluation will be performed when 20 infants have been included to evaluate feasibility and make it possible to adjust the protocol for the remaining part of the study. Safety analyses will be performed by an independent data and safety monitoring board (DSMB) when 50, 100 and 150 infants have been included. A sample size re-estimation will be made by an independent statistician when 150 infants have been included. Thus, the definitive sample size might be increased (never decreased) based on this interim analysis. The study can be terminated before 322 infants have been enrolled based on a decision of the sponsor and the DSMB, if the primary outcome is significantly lower (with a significance level <0.001) in the H2MF® than in the standard fortification group in the interim analysis made after 150 infants have completed the neonatal period. The study subject will be enrolled at level III NICUs in the Nordic Countries. All study subjects will be followed during the neonatal period until discharge (not longer than gestational week 44+0) and also be included in a follow up at 2 and 5.5 years of age based on the national follow up program for extremely preterm infants.
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Necrotizing Enterocolitis, Sepsis, Mortality
7. Study Design
Primary Purpose
Prevention
Study Phase
Phase 2, Phase 3
Interventional Study Model
Parallel Assignment
Masking
None (Open Label)
Allocation
Randomized
Enrollment
229 (Actual)
8. Arms, Groups, and Interventions
Arm Title
H2MF
Arm Type
Experimental
Arm Description
Human milk-based breast milk fortifier
Arm Title
Standard fortifier
Arm Type
Active Comparator
Arm Description
Standard care: bovine milk-based breast milk fortifier
Intervention Type
Dietary Supplement
Intervention Name(s)
H2MF
Intervention Description
H2MF is a human milk-based breastmilk fortifier for preterm infants
Intervention Type
Dietary Supplement
Intervention Name(s)
Bovine milk-based fortifier
Intervention Description
Bovine milk-based fortifier is the standard breast milk fortifier in Sweden
Primary Outcome Measure Information:
Title
The incidence of the composite of necrotizing enterocolitis, culture-proven sepsis and mortality
Description
An infant should have had any of these diagnoses to fulfil the criterion
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Secondary Outcome Measure Information:
Title
The incidence of the composite of necrotizing enterocolitis and culture-proven sepsis
Description
An infant should have had any of these diagnoses to fulfil the criterion
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
The incidence of the composite of necrotizing enterocolitis culture-proven sepsis, bronchopulmonary dysplasia, retinopathy of prematurity and mortality (Mortality and morbidity index)
Description
An infant should have had any of these diagnoses to fulfil the criterion
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
Time to reach full enteral feeds
Description
The day of life the infant has received at least 150 mL/kg enteral feeds
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
Number of feeding interruptions
Description
Number of days feedings held for ≥12 hours or feeds reduced by >50% (ml/kg/d) not due to a clinical procedure or transitioning to the breast
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
Numbers of days with parenteral nutrition
Description
Number of days of parental amino acid and/or lipid infusion. Only days when the enteral feed <150mL/kg/day should be included
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
Number of large gastric aspirates per day
Description
≥100% pre-feed volume (2 hours feeding volume if continuous feeding). Lower limit=2 ml/kg.
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
Stool frequency
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
Time to regain birth weight
Time Frame
From birth until discharge from hospital (but not longer than gestational week 44+0)
Title
Change in head circumference in centimeters
Time Frame
At 7, 14, 21 and 28 days, the end of intervention (gestational week 34+0), gestational week 36+0, at discharge from neonatal ward (or at gestational week 44+0, whatever comes first) and at 2 years of age (corrected) and 5.5 years of age (uncorrected).
Title
Change in weight in gram
Time Frame
At 7, 14, 21 and 28 days, the end of intervention (gestational week 34+0), gestational week 36+0, at discharge from neonatal ward (or at gestational week 44+0, whatever comes first) and at 2 years of age (corrected) and 5.5 years of age (uncorrected).
Title
Change in length in centimeters
Time Frame
At 7, 14, 21 and 28 days, the end of intervention (gestational week 34+0), gestational week 36+0, at discharge from neonatal ward (or at gestational week 44+0, whatever comes first) and at 2 years of age (corrected) and 5.5 years of age (uncorrected).
Title
The mortality incidence
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence of necrotising enterocolitis: Bell´s stage II-III
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence spontaneous intestinal perforation
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence of abdominal surgery
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence culture-proven sepsis
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence of suspected sepsis, not culture-proven
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence of pneumonia
Description
Pathological X-ray confirmed by an independent radiologist, need of increased respiratory support/oxygen and laboratory inflammatory response
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence of bronchopulmonary dysplasia
Description
Need of extra oxygen, continuous positive air pressure (CPAP) or ventilator at gestational week 36+0
Time Frame
At gestational week 36+0
Title
The incidence of retinopathy of the prematurity
Description
Classified into stage I-V. The diagnosis is set after gestational week 42+0
Time Frame
From birth until gestational week 42+0
Title
The incidence of intraventricular haemorrhage
Description
Classified into grade I-IV according to Papile
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
The incidence of periventricular leukomalacia
Description
Criteria according to de Vries
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
Number of days with intensive care
Description
Need of respirator or CPAP until discharge (not later than gestational week 44+0).
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
Length of stay at the hospital
Description
Gestational week and day at discharge (not later than gestational week 44+0).
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
Length of need of feeding tube
Description
Gestational week and day when the infant does not need it anymore (not later than gestational week 44+0)
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
Title
Neurocognitive development at 2 years
Description
Bayleys III, PARCA-R (Parental Report of Children´s Abilities-Revised) and ASQ-3 (Ages and stages questionnaire)
Time Frame
At 2 years of age
Title
Prevalence of cerebral palsy at 2 years
Time Frame
At 2 years of age
Title
Prevalence of epilepsy at 2 years
Time Frame
At 2 years of age
Title
Prevalence of squint and/or impaired vision at 2 years
Time Frame
At 2 years of age
Title
Prevalence of impaired hearing at 2 years
Time Frame
At 2 years of age
Title
The number of infants needing extra oxygen and/or ventilatory support after discharge from the hospital at the neonatal period
Time Frame
From gestational week 44 until 2 years of age
Title
The incidence of wheeze and/or asthma
Time Frame
From birth until 2 years of life
Title
The incidence of severe infections after discharge from the neonatal unit
Time Frame
From gestational week 44 until 2 years of age
Title
The number of infants needing feeding tube after discharge from the hospital at the neonatal period
Time Frame
From gestational week 44 until 2 years of age
Title
The number of infants needing extra nutritional support after discharge from the hospital at the neonatal period
Time Frame
From gestational week 44 until 2 years of age
Title
The prevalence of neurocognitive development at 5.5 years
Description
Wechsler Preschool and Primary Scale of Intelligence IV (WPPSI-IV TM) and Movement ABC-2: the total scale points as well as the points of sub scales (motor, cognitive, language) will be presented. The prevalence of infants with a realist below 2 standard deviations will be defined to have mental retardation.
Time Frame
At 5.5 years of age
Title
The prevalence of cerebral palsy at 5.5 years
Time Frame
At 5.5 years of age
Title
The prevalence of epilepsy at 5.5 years of age
Time Frame
At 5.5 years of age
Title
The prevalence of squint and/or impaired vision at 5.5 years of age
Time Frame
At 5.5 years of age
Title
The prevalence of children with impaired hearing at 5.5 years of age
Time Frame
At 5.5 years of age
Title
The prevalence of wheeze and/or asthma at 5.5 years of age
Time Frame
At 5.5 years of age
Title
Microbiome composition in stool samples
Description
The relative abundance and diversity of microbial taxa will be analyses with next generation sequencing and be related till the study intervention
Time Frame
At 1, 2, 3 and 4 weeks of age and gestational week 36+0
Title
Levels of subclasses of T and B cells and granulocytes in blood samples
Description
T helper subsets (TH1, Th2, TH17, Treg), T cells subsets associated with the intestinal mucosa (gamma/delta-T cells, MAIT cells) and neutrophils will be assessed using masscytometry
Time Frame
At 1, 2 and 4 weeks of age and gestational week 36+0
Title
Levels of immune markers in plasma
Description
Pre planned analyses are anti-inflammatory (e.g. IL-10) and proinflammatory (e.g. TNF) cytokines and chemokines (e.g. CXCL11, CCL18).
Time Frame
At 1, 2 and 4 weeks of age and gestational week 36+0
Title
Levels of growth factors in plasma samples
Description
The levels of growth factors such as IGF-1 and the associated IGFBP-3 will be analysed.
Time Frame
At 1, 2 and 4 weeks of age and gestational week 36+0
Title
Levels of lipids in plasma samples
Description
Fatty acids in plasma
Time Frame
At 1, 2 and 4 weeks of age and gestational week 36+0
Title
Levels of neurotransmitters in plasma samples
Description
Neurotransmitters such as GABA and serotonin in plasma
Time Frame
At 1, 2 and 4 weeks of age and gestational week 36+0
Title
Levels of metabolic peptides in urine samples
Description
Metabolic peptide will be measured with proton nuclear magnetic resonance spectroscopy (NMR), liquid chromatography (LC) and mass spectroscopy couple to gas chromatography (GC-MC).
Time Frame
At 1, 2, 3 and 4 weeks of age and gestational week 36+0
Title
Levels of markers of central nervous system (CNS) damage in plasma samples
Description
Markers of CNS damage such as neurofilament light protein will be measured in plasma
Time Frame
At 1, 2 and 4 weeks of age and gestational week 36+0
Title
Levels of proteins in breast milk samples
Description
Protein composition will be measured with multiplex methods
Time Frame
At 1, 2, 3 and 4 weeks of age and gestational week 36+0
Title
Levels of human milk oligosaccharides in breast milk samples
Description
The levels of human milk oligosaccharides will be measured with high-performance anion-exchange chromatography with pulsed amperometric detection.
Time Frame
At 1, 2, 3 and 4 weeks of age and gestational week 36+0
Title
Health care costs
Description
The number of days at each level of care will be recorded until discharge from the hospital (not longer than gestational week 44+0). The cost will be calculated by multiplying the number of days at each level of care by the average cost
Time Frame
From birth until discharge from hospital (but not loner than gestational week 44+0)
10. Eligibility
Sex
All
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria:
Gestational age at birth 22+0-27+6: based on prenatal ultrasonography.
Enteral feeds < 100 mL/kg/day at the day of randomisation.
Written informed consent from the legal guardians of the infant.
The home clinic of the infant has the logistics of maintaining the intervention until gestational week 34+0
Exclusion Criteria:
Lethal or complicated malformation known at the time of inclusion
Chromosomal anomalies known at the time of inclusion
No realistic hope for survival at the time of inclusion
Gastrointestinal malformation known at the time of inclusion
Abdominal surgery before the time of inclusion
Participation in another intervention trial aiming at having an effect on growth, nutrition, feeding intolerance or severe complications such as NEC and sepsis
Infants having nutrient fortifier or formula prior to randomisation
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Thomas R Abrahamsson, MD, PhD
Organizational Affiliation
Region Östergötland
Official's Role
Principal Investigator
Facility Information:
Facility Name
Queen Silvia Children´s Hospital
City
Göteborg
Country
Sweden
Facility Name
Crown Princess Victoria Children´s Hospital
City
Linköping
Country
Sweden
Facility Name
Karolinska Hospital
City
Stockholm
Country
Sweden
Facility Name
Norrlands Universitetssjukhus
City
Umeå
Country
Sweden
Facility Name
Akademiska Barnsjukhuset
City
Uppsala
Country
Sweden
12. IPD Sharing Statement
Plan to Share IPD
No
Citations:
PubMed Identifier
34815288
Citation
Jensen GB, Ahlsson F, Domellof M, Elfvin A, Naver L, Abrahamsson T. Nordic study on human milk fortification in extremely preterm infants: a randomised controlled trial-the N-forte trial. BMJ Open. 2021 Nov 23;11(11):e053400. doi: 10.1136/bmjopen-2021-053400.
Results Reference
derived
Learn more about this trial
Human Milk Fortification in Extremely Preterm Infants
We'll reach out to this number within 24 hrs