Efficacy and Safety of Enteral Recombinant Human Insulin in Preterm Infants: A Randomized Clinical Trial.

Birth Weight Enteral Nutrition / methods Enterocolitis, Necrotizing Female Humans Infant Infant, Newborn Infant, Premature Insulin Male Milk, Human

Journal

JAMA pediatrics

ISSN: 2168-6211

Titre abrégé: JAMA Pediatr

Pays: United States

ID NLM: 101589544

Informations de publication

Date de publication:
01 05 2022

Historique:

pubmed: 1 3 2022

medline: 6 5 2022

entrez: 28 2 2022

Statut: ppublish

Résumé

Feeding intolerance is a common condition among preterm infants owing to immaturity of the gastrointestinal tract. Enteral insulin appears to promote intestinal maturation. The insulin concentration in human milk declines rapidly post partum and insulin is absent in formula; therefore, recombinant human (rh) insulin for enteral administration as a supplement to human milk and formula may reduce feeding intolerance in preterm infants. To assess the efficacy and safety of 2 different dosages of rh insulin as a supplement to both human milk and preterm formula. The FIT-04 multicenter, double-blind, placebo-controlled randomized clinical trial was conducted at 46 neonatal intensive care units throughout Europe, Israel, and the US. Preterm infants with a gestational age (GA) of 26 to 32 weeks and a birth weight of 500 g or more were enrolled between October 9, 2016, and April 25, 2018. Data were analyzed in January 2020. Preterm infants were randomly assigned to receive low-dose rh insulin (400-μIU/mL milk), high-dose rh insulin (2000-μIU/mL milk), or placebo for 28 days. The primary outcome was time to achieve full enteral feeding (FEF) defined as an enteral intake of 150 mL/kg per day or more for 3 consecutive days. The final intention-to-treat analysis included 303 preterm infants (low-dose group: median [IQR] GA, 29.1 [28.1-30.4] weeks; 65 boys [59%]; median [IQR] birth weight, 1200 [976-1425] g; high-dose group: median [IQR] GA, 29.0 [27.7-30.5] weeks; 52 boys [55%]; median [IQR] birth weight, 1250 [1020-1445] g; placebo group: median [IQR] GA, 28.8 [27.6-30.4] weeks; 54 boys [55%]; median [IQR] birth weight, 1208 [1021-1430] g). The data safety monitoring board advised to discontinue the study early based on interim futility analysis (including the first 225 randomized infants), as the conditional power did not reach the prespecified threshold of 35% for both rh-insulin dosages. The study continued while the data safety monitoring board analyzed and discussed the data. In the final intention-to-treat analysis, the median (IQR) time to achieve FEF was significantly reduced in 94 infants receiving low-dose rh insulin (10.0 [7.0-21.8] days; P = .03) and in 82 infants receiving high-dose rh insulin (10.0 [6.0-15.0] days; P = .001) compared with 85 infants receiving placebo (14.0 [8.0-28.0] days). Compared with placebo, the difference in median (95% CI) time to FEF was 4.0 (1.0-8.0) days for the low-dose group and 4.0 (1.0-7.0) days for the high-dose group. Weight gain rates did not differ significantly between groups. Necrotizing enterocolitis (Bell stage 2 or 3) occurred in 7 of 108 infants (6%) in the low-dose group, 4 of 88 infants (5%) in the high-dose group, and 10 of 97 infants (10%) in the placebo group. None of the infants developed serum insulin antibodies. Results of this randomized clinical trial revealed that enteral administration of 2 different rh-insulin dosages was safe and compared with placebo, significantly reduced time to FEF in preterm infants with a GA of 26 to 32 weeks. These findings support the use of rh insulin as a supplement to human milk and preterm formula. ClinicalTrials.gov Identifier: NCT02510560.

Identifiants

DOI: 10.1001/jamapediatrics.2022.0020 PMID: 35226099 PMC: PMC8886453

pubmed: 35226099

pii: 2789461

doi: 10.1001/jamapediatrics.2022.0020

pmc: PMC8886453

doi:

Substances chimiques

Insulin 0

Banques de données

ClinicalTrials.gov

['NCT02510560']

Types de publication

Journal Article Multicenter Study Randomized Controlled Trial Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

Pagination

452-460

Investigateurs

Johannes B van Goudoever (JB)

Elise Mank (E)

Letty van Toledo (L)

Elisabeth M W Kooi (EMW)

Arend F Bos (AF)

Richard A van Lingen (RA)

Astrid Giezen (A)

Miguel Sáenz de Pipáon (M)

Marta Cabrera Lafuente (M)

Esperanza Escribano (E)

Manuel Sánchez Luna (M)

María Del Carmen Sánchez Gómez de Orgaz (M)

Felix Castillo (F)

Manuel Cidrás (M)

Macarena Quesada (M)

Maria L Couce (ML)

Olalla López-Suárez (O)

Máximo Vento (M)

María Gormaz (M)

Alexandre Lapillonne (A)

Agnes Giuseppi (A)

Virginie Rigourd (V)

Jean-Michel Hascoet (JM)

Emily Greze (E)

Alain Beuchée (A)

Nadia Mazille (N)

Virgilio P Carnielli (VP)

Chiara Biagetti (C)

Maria P Bellagamba (MP)

Gianluca Lista (G)

Paola Roggero (P)

Orsola Amato (O)

Paolo Tagliabue (P)

Giovanni Vento (G)

Simonetta Costa (S)

Massimo Agosti (M)

Laura Morlacchi (L)

Thibault Senterre (T)

Anne Vervoort (A)

Pierre Maton (P)

Christine Vandeputte (C)

Katleen Plaskie (K)

Luc M G I Cornette (LMGI)

James D'haese (J)

Filip Cools (F)

Michel Sonnaert (M)

Raanan Shamir (R)

Ruben Bromiker (R)

Gil Klinger (G)

Shmuel Zangen (S)

Mara Troitzky (M)

Kyla Marks (K)

Eilon Shany (E)

Arieh Riskin (A)

Ori Hochwald (O)

Huda Jubran (H)

Naim Shehadeh (N)

Strauss Tzipora (S)

Leibovitch Leah (L)

Dror Mandel (D)

Alon Haham (A)

Victoria G Atanasova (VG)

Lyuben G Veskov (LG)

Donka P Uzunova (DP)

Zornica T Malinova (ZT)

Frank Jochum (F)

Mario Rüdiger (M)

Katrin Weber (K)

Walter A Mihatsch (WA)

Rahel Schuler (R)

Andrea Nagy (A)

Gergely Balázs (G)

Judit Kiss (J)

Anna Gajda (A)

Hajnalka Szabó (H)

Eva Szabo (E)

Tamas Tenk (T)

Sam Oddie (S)

Rachel Wane (R)

Elaine M Boyle (EM)

Marie Hubbard (M)

Stephen P Wardle (SP)

Dushyant Batra (D)

Tim Scorrer (T)

Charlotte Groves (C)

Joern-Hendrik Weitkamp (JH)

Theresa J Rogers (TJ)

Ryan T Moore (RT)

Devon Kuehn (D)

Kimberly D Ernst (KD)

Commentaires et corrections

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