Limited Versus Extended Trophic Feeding (LET-FEED) Trial (LET-FEED)

Study Hypothesis/Question In infants born very preterm, advancing enteral feeds after 24 hours from birth (limited trophic feeds) versus after 72 hours (extended trophic feeds) reduces the risk of all-cause late onset sepsis (LOS) without increasing the risk of other adverse outcomes.

Study Design Type This is a multi-center, open-label, parallel-group, individual randomized controlled trial comparing two different trophic feeding regimens in preterm infants born between 25w0d and 31w6d. These infants will be randomly assigned to either the intervention group, receiving limited trophic feeding (20 to 25 mL/kg/day for one day) or the control group, receiving extended trophic feeding (20 to 25 mL/kg/day for three days) prior to advancing enteral feeds until full feeding volume (140 mL/kg/day) is achieved.

Eligibility Criteria Preterm infants with gestational ages between 25 0/7 and 31 6/7 weeks and a birthweight of <1500 grams who are admitted to six participating neonatal units will be eligible for inclusion. Infants with <5th percentile for weight at birth, vasopressor use within first 24 hours of life major congenital/genetic anomalies affecting enteral feeding, growth, or mortality, and those with a terminal illness in which decisions to withhold or limit support have been made will be excluded. Infants of parents or legal guardians who are unable to provide consent within 36 hours of birth will also be excluded.

Study Intervention/Methods Written parental informed consent will be obtained prenatally or within the first 36 hours of birth. Infants will be randomized to receive limited trophic feeds of 24 to 36 hours or extended trophic feeds for 72 hours prior to the advancement of enteral feeds. Infants will be fed parent's own milk (POM) with donor human milk as the alternative if POM is unavailable.

Primary Outcome Late-onset sepsis, defined as positive blood, urine, and/or cerebrospinal fluid (CSF) cultures in the presence of compatible clinical signs of sepsis, occurring after postnatal day 3 and before hospital discharge, and treated with antibiotics for 5 days or more.

Secondary Outcome(s) The trial will assess various secondary outcomes including length of hospital stay, all-cause in-hospital mortality, duration of IV fluids and central line utilization, necrotizing enterocolitis (Bell's stage IIa or higher), severe intraventricular hemorrhage (grade III or IV either unilaterally or bilaterally), bronchopulmonary dysplasia (oxygen requirement or positive pressure ventilation at 36 weeks corrected gestational age), or retinopathy of prematurity requiring intervention. Additionally, growth metrics throughout hospitalization will be evaluated using change in weight, length, and head circumference z-scores from birth to 36 weeks' corrected gestational age between infants in the limited and extended trophic feeding groups.

Study Overview

• Status: Recruiting
• Conditions: Sepsis; Mortality; Length of Stay
• Intervention / Treatment: Other: Extended Trophic Feeds (3 days of trophics); Other: Limited Trophic Feeds (1 day of trophic feeds)

Detailed Description

Up to 30% of all very preterm (VP; defined as those born before 32 weeks' gestation) newborns born within the United States develop late onset sepsis (LOS), a life-threatening infection that occurs after 72 hours from birth. LOS is the leading cause of morbidity in all very preterm newborns. VP newborns who develop LOS have significantly lower survival rates (adjusted risk ratio [aRR] 0.89, 95% confidence interval [CI] 0.87-0.90), 32% increased risk of being discharged on oxygen (aRR 1.32, 95% CI 1.26-1.38), 288% increased risk of needing a tracheostomy (aRR 2.88, 95% CI 2.47-3.37), and a 209% increased risk of requiring a gastrostomy tube (aRR 2.09, 95% CI 1.93-2.57).27 Thus, clinical practices that can reduce LOS are critically important to ensure VP newborns not only survive, but thrive, living lives free of disability or impairment.

One of the most protective factors in preventing LOS is an exclusive human milk-based diet. Common clinical practice for VP newborns includes starting human milk-based enteral feeds at approximately 20 mL/kg/day (e.g. "trophic feeds") and then progressively advancing the volume of enteral feeds daily until reaching a sufficient quantity to achieve adequate hydration and nutrition (e.g. "full feeds"). While enteral feeds are being advanced, VP newborns receive additional supplementary fluids and nutrition via intravenous (IV) infusions. Yet, any indwelling catheter to provide IV nutrition inherently increases the risk of LOS because the catheter breaches the newborn's protective skin barrier, thereby increasing risk of invasive infection from skin microbes.

One way to reduce the need for IV fluids is to initiate enteral human milk feeds earlier and advance feeds faster, thereby limiting the duration of indwelling IV catheters. An additional benefit of this approach is that early introduction of human milk prevents dysbiosis of the neonatal microbiome that is associated with LOS. By preventing the growth of harmful, pathogenic, sepsis-causing bacteria within the gut of VP newborns, these newborns have overall less risk of developing LOS. Yet, these benefits are with an exclusive human milk-based diet as meta-analyses and systematic reviews have demonstrated that feeding formula significantly increases the risk of necrotizing enterocolitis (NEC), a devastating inflammatory process within the gastrointestinal system that is associated with a 30-50% mortality rate.

A Gerber-funded (AA Salas PI, novice research award), pilot randomized trial that compared early versus delayed progressive feeding in 60 extremely preterm infants born at the University of Alabama Hospital showed that early progressive feeding reduced the need for central venous access (p=0.0001) and parenteral nutrition by 4 days (p=0.0005). Culture-proven sepsis (10% vs. 27%; p= 0.18) tended to be lower in the early progressive feeding group but did not reach statistical significance due to the limited power and sample size of the study.

Thus, the natural next question is whether early progression of enteral feeds in a multi-center trial improves clinical outcomes, namely prevention of invasive infection, without increased risk of adverse outcomes including mortality. The lack of multi-center clinical trials evaluating faster advancement of enteral feeds to full volume feeds has left clinicians with uncertainty about the risks and benefits of this approach and resulted in a lack of uniformity in clinical practice. This has led to significant differences in how VP newborns are fed across the US and globally, with some centers initiating and advancing feeds within the first few hours after birth and others continuing small volume "trophic" feeds without any advancement until day 4 after birth. Thus, clinicians caring for VP newborns are in dire need of evidence to determine the optimal feeding advancement strategy to improve their short- and long-term outcomes.

Study Population:

Investigators will enroll 350 very preterm infants born at 25 0/7 to 31 6/7 weeks' gestation admitted to the six participating neonatal intensive care units. All newborns will be eligible for this study without regards to gender, ethnicity, race, socioeconomic status, or language spoken. This study population has been selected based on the frequency of newborn admissions, sepsis, and overall mortality observed at these gestational ages. The participating centers include: (1) St. Joseph's Medical Center (Tacoma, WA), (2) Baylor College of Medicine (Houston, TX), (3) University of Alabama (Birmingham, AL), (4) University of South Florida (Tampa, FL), and (5) University of Oklahoma (Oklahoma City, OK).

Consent and Randomization:

To ensure timely enrollment, written informed consent will be obtained no later than 36 hours following birth, with a goal of enrollment within 24 hours of birth or prenatally. Identification of potential participants will prompt a visit from a study team member, who will meet with the parent(s) in their room or the baby's room to explain the study. During this meeting, the risks and benefits associated with participation will be thoroughly discussed, and ample time will be allocated for the parents to ask any questions they may have. The consent will include that the newborn will be fed parent's own milk as the prioritized enteral feed with donor milk as the alternative if POM is of insufficient quantity.

Importantly, participants will be assured that their infant will receive all necessary treatments irrespective of their involvement in the study. The process of randomization will then determine the assignment of each participant to their respective study group.

Participants will be randomly assigned to one of the study groups following computer generated random-block sequences. The University of Washington will develop the sequence and implement stratified randomization by gestational age using a computerized central telephone system. Twin and multiple infants will be randomized individually.

Study Intervention and Active Comparator:

After consenting, information about the pregnancy and participating infant will be collected, including contact information for the parent(s), race/ethnicity, medical history, family history, education level, employment status, marital status, and other information to assess baseline characteristics of study participants.

All consented and enrolled infants will be randomly assigned to receive either limited trophic feeds of 24 hours or extended trophic feeds of 72 hours after birth prior to the advancement of enteral feeds. Given that IV fluids and parenteral nutrition need to be ordered up to 12 hours prior to the implemented change, investigators have included a 12-hour period of advancement (24 to 36 hours versus 72 to 84 hours after birth) to account for these logistics and ensure the generalizability of the trial's findings. Feeding volumes will be advanced by 25 to 30 mL/kg/day until full feeds (140 mL/kg/day) are reached within two weeks of birth.

All participating centers will provide parent's own milk as the prioritized feed, with human donor milk provided inn cases where POM is not available in sufficient quantities. Preterm formula will not be used. The trial will recommend that fortification occurs once enteral feeding volumes of 40 to 60 mL/kg/day or higher are achieved and that IV catheters will be removed once the newborn is above 120 mL/kg/day of enteral feeds.

Deviations from the feeding protocol will be allowed if signs of feeding intolerance are present before establishment of full enteral feeding. Feeding intolerance will be defined as an interruption or cessation of enteral feeds for a period greater than 12 hours for abnormal abdominal examination within 14 days of birth. Information will also be collected on the percentage of enteral feeds that had a >50% reduction in planned volume over each 24-hour period to serve as an additional metric of feeding intolerance.

The primary outcome will be culture-proven late onset sepsis. Culture-proven LOS will be defined as positive blood, urine, and/or cerebrospinal fluid (CSF) cultures in the presence of compatible clinical signs of sepsis, occurring between postnatal day 3 and hospital discharge, necessitating treatment with antibiotics for 5 days or more.

• Study Type: Interventional
• Enrollment (Estimated): 350
• Phase: Phase 3

Contacts and Locations

• Study Contact: Name: Gregory C Valentine, MD MED FAAP; Phone Number: (206) 543-3200; Email: gcvalent@uw.edu
• Study Contact Backup: Name: Ariel Salas, MD, MSPH; Email: asalas@uabmc.edu

Study Locations

• United States
  • Alabama
    • Birmingham, Alabama, United States, 35233
      • Not yet recruiting
      • University of Alabama at Birmingham
      • Contact: Ariel Salas, MD MSPH; Phone Number: 205.934.4680; Email: asalas@uabmc.edu
  • Florida
    • Tampa, Florida, United States, 33606
      • Not yet recruiting
      • University of South Florida
      • Contact: Steven Ford, MD; Phone Number: (813) 844-7493; Email: slford2@usf.edu
  • Oklahoma
    • Oklahoma City, Oklahoma, United States, 73104
      • Not yet recruiting
      • University of Oklahoma
      • Contact: Erynn Bergner, MD; Phone Number: (405) 271-5215; Email: erynn-bergner@ouhsc.edu
  • Texas
    • Houston, Texas, United States, 77030
      • Not yet recruiting
      • Baylor College of Medicine
      • Contact: Amy B Hair, MD; Phone Number: 832-826-1380; Email: abhair@texaschildrens.org
      • Contact: Murali Premkumar, MBBS, DCH,DNB,MRCPCH, MS; Phone Number: 832-826-1380; Email: premkuma@bcm.edu
  • Washington
    • Seattle, Washington, United States, 98195
      • Not yet recruiting
      • University of Washington
      • Contact: Gregory C Valentine, MD MED FAAP; Phone Number: (206) 543-3200; Email: gcvalent@uw.edu
    • Tacoma, Washington, United States, 98405
      • Recruiting
      • St. Joseph's Medical Center
      • Contact: Gregory C Valentine, MD MED FAAP; Phone Number: 2534266740; Email: gcvalent@uw.edu
      • Contact: Stephen Welty, MD; Phone Number: 2534266740; Email: stephen.welty@vmfh.org

Participation Criteria

Eligibility Criteria

• Ages Eligible for Study: Child
• Accepts Healthy Volunteers: Yes

Description

Inclusion Criteria:

• <1500 gram birthweight
• 25w0d-31w6d at birth
• Consent to feed donor milk when parent's own milk is not available or of insufficient quantity

Exclusion Criteria:

• <5th percentile for weight at birth (Fenton growth curve)
• Parent or legal guardian unable to provide consent within 36 hours after birth
• Congenital anomaly affecting decisions on enteral feedings (e.g. gastroschisis, omphalocele, congenital diaphragmatic hernia, congenital heart disease, etc.)
• Known genetic condition affecting growth, feeding, or mortality
• Vasopressor use within first 24 hours after birth (not including hydrocortisone)
• Considered terminally ill

Study Plan

How is the study designed?

Design Details

• Primary Purpose: Prevention
• Allocation: Randomized
• Interventional Model: Parallel Assignment
• Masking: None (Open Label)

Number of Arms

2

Arms and Interventions

Participant Group / Arm	Intervention / Treatment
Active Comparator: Extended Trophic Feeding; Advancing enteral feeds after 3 days of trophic feeds of 20-25 mL/kg birthweight/day. Advancement of enteral feeds will be by approximately 30 mL/kg birthweight/day after 3 days of trophic feeds. Advancement will occur until achieving at least 140 mL/kg birthweight/day of enteral feeds. Enteral feeds will consist of parent's own milk or donor human milk.	Other: Extended Trophic Feeds (3 days of trophics); Advancing enteral feeds after 3 days of trophic feeds of 20-25 mL/kg birthweight/day. Advancement of enteral feeds will be by approximately 30 mL/kg birthweight/day after 3 days of trophic feeds. Advancement will occur until achieving at least 140 mL/kg birthweight/day of enteral feeds. Enteral feeds will consist of parent's own milk or donor human milk.
Experimental: Limited Trophic Feeds; Advancing enteral feeds after 1 day of trophic feeds of 20-25 mL/kg birthweight/day. Advancement of enteral feeds will be by approximately 30 mL/kg birthweight/day until achieving at least 140 mL/kg birthweight/day of enteral feeds. Enteral feeds will consist of parent's own milk or donor human milk.	Other: Limited Trophic Feeds (1 day of trophic feeds); Advancing enteral feeds after 1 day of trophic feeds of 20-25 mL/kg birthweight/day. Advancement of enteral feeds will be by approximately 30 mL/kg birthweight/day until achieving at least 140 mL/kg birthweight/day of enteral feeds. Enteral feeds will consist of parent's own milk or donor human milk.; Other Names: Limited Trophic Feeds

What is the study measuring?

Primary Outcome Measures

Outcome Measure	Measure Description	Time Frame
Late Onset Sepsis	Defining LOS: For the purposes of this study, a positive finding of LOS will be defined as the following: a body fluid culture (e.g. blood, urine, CSF) that returns positive, obtained in the presence of compatible clinical signs of sepsis (e.g. hypotension, apnea/bradycardia, increasing oxygen requirements, increasing metabolic acidosis, lactic acidosis, hypoglycemia, hyperglycemia, etc.) occurring after 72 hours from birth and before hospital discharge that was treated with antibiotics for a minimum of 5 days.	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation

Secondary Outcome Measures

Outcome Measure	Measure Description	Time Frame
All-Cause In-Hospital Mortality	all-cause in-hospital mortality	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Duration of parenteral nutrition	Days of parenteral nutrition during hospitalization	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Duration of Central Venous Access	Days of central venous access throughout hospitalization	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Length of hospitalization	Length of hospitalization (days)	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Time to reach full enteral feeding volumes	Full enteral feeding volumes defined as ≥120 mL/kg birthweight/day	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Number of culture-proven late onset sepsis episodes	Will be assess per participant throughout hospitalization	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Type of late-onset sepsis	Hematogenous/sepsis, urinary tract infection, meningitis, combination, or other	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Necrotizing Enterocolitis	Modified Bell's stage IIa or higher	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Spontaneous Intestinal Perforation (SIP)	SIP diagnosed during hospitalization	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Severe Intraventricular Hemorrhage (IVH)	Defined as Grade III or IV unilaterally or bilaterally	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Bronchopulmonary Dysplasia	Defined as needing supplemental oxygen or non-invasive administration of positive pressure, or invasive ventilation at 36 weeks corrected gestational age	At 36 weeks corrected gestational age
Retinopathy of Prematurity requiring Intervention	Medical or surgical intervention	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Patent Ductus Arteriosus Requiring Intervention	Medical or surgical intervention (not including prophylactic)	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Type of pathogen detected in culture-positive late-onset sepsis	Bacteria, fungal, or viral pathogen detected in any culture-positive late-onset sepsis event detected after 72 hours from birth and during hospitalization	Through study completion, the end of NICU hospitalization, an average of 40 weeks' gestation
Change in Z-score of weight	From birth to 36 weeks corrected gestational age weight Z-score change	From admission to 36 weeks corrected gestational age
Change in Z-score of length	From birth to 36 weeks corrected gestational age length Z-score change	From admission to 36 weeks corrected gestational age
Change in Z-score of head circumference	From birth to 36 weeks corrected gestational age head circumference Z-score change	From admission to 36 weeks corrected gestational age

Collaborators and Investigators

• Sponsor: University of Washington
• Collaborators: Baylor College of Medicine; University of South Florida; University of Alabama at Birmingham; University of Oklahoma; St. Joseph's Medical Center
• Investigators: Principal Investigator: Gregory C Valentine, University of Washington

Publications and helpful links

General Publications

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• Perez KM, Strobel KM, Hendrixson DT, Brandon O, Hair AB, Workneh R, Abayneh M, Nangia S, Hoban R, Kolnik S, Rent S, Salas A, Ojha S, Valentine GC. Nutrition and the gut-brain axis in neonatal brain injury and development. Semin Perinatol. 2024 Aug;48(5):151927. doi: 10.1016/j.semperi.2024.151927. Epub 2024 Jun 13.
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• Singer JR, Blosser EG, Zindl CL, Silberger DJ, Conlan S, Laufer VA, DiToro D, Deming C, Kumar R, Morrow CD, Segre JA, Gray MJ, Randolph DA, Weaver CT. Preventing dysbiosis of the neonatal mouse intestinal microbiome protects against late-onset sepsis. Nat Med. 2019 Nov;25(11):1772-1782. doi: 10.1038/s41591-019-0640-y. Epub 2019 Nov 7.
• Stewart CJ, Embleton ND, Marrs ECL, Smith DP, Fofanova T, Nelson A, Skeath T, Perry JD, Petrosino JF, Berrington JE, Cummings SP. Longitudinal development of the gut microbiome and metabolome in preterm neonates with late onset sepsis and healthy controls. Microbiome. 2017 Jul 12;5(1):75. doi: 10.1186/s40168-017-0295-1.
• Lee CC, Feng Y, Yeh YM, Lien R, Chen CL, Zhou YL, Chiu CH. Gut Dysbiosis, Bacterial Colonization and Translocation, and Neonatal Sepsis in Very-Low-Birth-Weight Preterm Infants. Front Microbiol. 2021 Oct 7;12:746111. doi: 10.3389/fmicb.2021.746111. eCollection 2021.
• Quigley M, Embleton ND, Meader N, McGuire W. Donor human milk for preventing necrotising enterocolitis in very preterm or very low-birthweight infants. Cochrane Database Syst Rev. 2024 Sep 6;9(9):CD002971. doi: 10.1002/14651858.CD002971.pub6.
• Ruiz-Giardin JM, Ochoa Chamorro I, Velazquez Rios L, Jaqueti Aroca J, Garcia Arata MI, SanMartin Lopez JV, Guerrero Santillan M. Blood stream infections associated with central and peripheral venous catheters. BMC Infect Dis. 2019 Oct 15;19(1):841. doi: 10.1186/s12879-019-4505-2.
• Heilmann C, Ziebuhr W, Becker K. Are coagulase-negative staphylococci virulent? Clin Microbiol Infect. 2019 Sep;25(9):1071-1080. doi: 10.1016/j.cmi.2018.11.012. Epub 2018 Nov 29.
• Shalabi M, Adel M, Yoon E, Aziz K, Lee S, Shah PS; Canadian Neonatal Network. Risk of Infection Using Peripherally Inserted Central and Umbilical Catheters in Preterm Neonates. Pediatrics. 2015 Dec;136(6):1073-9. doi: 10.1542/peds.2015-2710. Epub 2015 Nov 16.
• Marchant EA, Boyce GK, Sadarangani M, Lavoie PM. Neonatal sepsis due to coagulase-negative staphylococci. Clin Dev Immunol. 2013;2013:586076. doi: 10.1155/2013/586076. Epub 2013 May 22.
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• Hair AB, Peluso AM, Hawthorne KM, Perez J, Smith DP, Khan JY, O'Donnell A, Powers RJ, Lee ML, Abrams SA. Beyond Necrotizing Enterocolitis Prevention: Improving Outcomes with an Exclusive Human Milk-Based Diet. Breastfeed Med. 2016 Mar;11(2):70-4. doi: 10.1089/bfm.2015.0134. Epub 2016 Jan 20.

Study record dates

Study Major Dates

• Study Start (Actual): July 3, 2025
• Primary Completion (Estimated): January 1, 2028
• Study Completion (Estimated): March 31, 2028

Study Registration Dates

• First Submitted: March 11, 2025
• First Submitted That Met QC Criteria: March 18, 2025
• First Posted (Actual): March 25, 2025

Study Record Updates

• Last Update Posted (Actual): July 28, 2025
• Last Update Submitted That Met QC Criteria: July 23, 2025
• Last Verified: July 1, 2025

More Information

Terms related to this study

• Keywords: Nutrition; sepsis; Prematurity; Feeding; enteral feeds; Very preterm; Trophic; Trophic feeds; Trophic feeding
• Additional Relevant MeSH Terms: Pathologic Processes; Infections; Systemic Inflammatory Response Syndrome; Inflammation; Sepsis
• Other Study ID Numbers: STUDY00021132

Plan for Individual participant data (IPD)

• Plan to Share Individual Participant Data (IPD)?: YES
• IPD Plan Description: De-identified data may be shared with other researchers if a scientifically sound and reasonable plan is provided to the study team investigators and Co-PIs. A data sharing or transfer use agreement may be required per institutional policy if sharing of data occurs.
• IPD Sharing Time Frame: Deidentified data will be shared with researchers requesting access to the data if they have a scientifically sound and reasonable plan. The data will be shared within 6-12 months of receiving the request by the researchers and a determination is made.
• IPD Sharing Access Criteria: Deidentified data will be shared with researchers requesting access to the data if they have a scientifically sound and reasonable plan. The data will be shared within 6-12 months of receiving the request by the researchers and a determination is made. The data will be transferred via a HIPAA secure format.
• IPD Sharing Supporting Information Type: STUDY_PROTOCOL; SAP; ICF; ANALYTIC_CODE; CSR

Drug and device information, study documents

• Studies a U.S. FDA-regulated drug product: No
• Studies a U.S. FDA-regulated device product: No
• product manufactured in and exported from the U.S.: No