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Linking Human Milk Oligosaccharides, Infant Fecal Community Types, and Later Risk To Require Antibiotics
by
Descombes, Patrick
, Alliet, Philippe
, Porta, Nadine
, Mercenier, Annick
, Grathwohl, Dominik
, Sprenger, Norbert
, Berger, Bernard
, Steenhout, Philippe
, Foata, Francis
, Puccio, Giuseppe
, Siegwald, Léa
, Delley, Michèle
, Moine, Deborah
, Charpagne, Aline
in
2′FL
/ Acids
/ Anti-Bacterial Agents - administration & dosage
/ Antibiotics
/ Babies
/ Baby foods
/ Bacteria - classification
/ Breast Feeding
/ Breast milk
/ Breastfeeding & lactation
/ Clinical trials
/ Digestive system
/ Double-Blind Method
/ Feces
/ Feces - microbiology
/ Female
/ formula
/ Gastrointestinal Microbiome
/ Gastrointestinal tract
/ Gene amplification
/ Gestational age
/ Gut microbiota
/ Host-Microbe Biology
/ human milk oligosaccharides
/ Humans
/ Immune system
/ Infant
/ Infant Formula - analysis
/ Infant formulas
/ Infant, Newborn
/ Infants
/ Infections
/ Intestinal microflora
/ LNnT
/ Male
/ Microbiomes
/ Microbiota
/ Milk
/ Milk, Human - chemistry
/ Oligosaccharides
/ Oligosaccharides - administration & dosage
/ Oligosaccharides - chemistry
/ RNA, Ribosomal, 16S
/ rRNA 16S
/ Standard deviation
/ Taxonomy
2020
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Linking Human Milk Oligosaccharides, Infant Fecal Community Types, and Later Risk To Require Antibiotics
by
Descombes, Patrick
, Alliet, Philippe
, Porta, Nadine
, Mercenier, Annick
, Grathwohl, Dominik
, Sprenger, Norbert
, Berger, Bernard
, Steenhout, Philippe
, Foata, Francis
, Puccio, Giuseppe
, Siegwald, Léa
, Delley, Michèle
, Moine, Deborah
, Charpagne, Aline
in
2′FL
/ Acids
/ Anti-Bacterial Agents - administration & dosage
/ Antibiotics
/ Babies
/ Baby foods
/ Bacteria - classification
/ Breast Feeding
/ Breast milk
/ Breastfeeding & lactation
/ Clinical trials
/ Digestive system
/ Double-Blind Method
/ Feces
/ Feces - microbiology
/ Female
/ formula
/ Gastrointestinal Microbiome
/ Gastrointestinal tract
/ Gene amplification
/ Gestational age
/ Gut microbiota
/ Host-Microbe Biology
/ human milk oligosaccharides
/ Humans
/ Immune system
/ Infant
/ Infant Formula - analysis
/ Infant formulas
/ Infant, Newborn
/ Infants
/ Infections
/ Intestinal microflora
/ LNnT
/ Male
/ Microbiomes
/ Microbiota
/ Milk
/ Milk, Human - chemistry
/ Oligosaccharides
/ Oligosaccharides - administration & dosage
/ Oligosaccharides - chemistry
/ RNA, Ribosomal, 16S
/ rRNA 16S
/ Standard deviation
/ Taxonomy
2020
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Linking Human Milk Oligosaccharides, Infant Fecal Community Types, and Later Risk To Require Antibiotics
by
Descombes, Patrick
, Alliet, Philippe
, Porta, Nadine
, Mercenier, Annick
, Grathwohl, Dominik
, Sprenger, Norbert
, Berger, Bernard
, Steenhout, Philippe
, Foata, Francis
, Puccio, Giuseppe
, Siegwald, Léa
, Delley, Michèle
, Moine, Deborah
, Charpagne, Aline
in
2′FL
/ Acids
/ Anti-Bacterial Agents - administration & dosage
/ Antibiotics
/ Babies
/ Baby foods
/ Bacteria - classification
/ Breast Feeding
/ Breast milk
/ Breastfeeding & lactation
/ Clinical trials
/ Digestive system
/ Double-Blind Method
/ Feces
/ Feces - microbiology
/ Female
/ formula
/ Gastrointestinal Microbiome
/ Gastrointestinal tract
/ Gene amplification
/ Gestational age
/ Gut microbiota
/ Host-Microbe Biology
/ human milk oligosaccharides
/ Humans
/ Immune system
/ Infant
/ Infant Formula - analysis
/ Infant formulas
/ Infant, Newborn
/ Infants
/ Infections
/ Intestinal microflora
/ LNnT
/ Male
/ Microbiomes
/ Microbiota
/ Milk
/ Milk, Human - chemistry
/ Oligosaccharides
/ Oligosaccharides - administration & dosage
/ Oligosaccharides - chemistry
/ RNA, Ribosomal, 16S
/ rRNA 16S
/ Standard deviation
/ Taxonomy
2020
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Linking Human Milk Oligosaccharides, Infant Fecal Community Types, and Later Risk To Require Antibiotics
Journal Article
Linking Human Milk Oligosaccharides, Infant Fecal Community Types, and Later Risk To Require Antibiotics
2020
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Overview
Human milk is the sole and recommended nutrition for the newborn infant and contains one of the largest constituents of diverse oligosaccharides, dubbed human milk oligosaccharides (HMOs). Preclinical and clinical association studies indicate that HMOs have multiple physiological functions largely mediated through the establishment of the gut microbiome. Until recently, HMOs were not available to investigate their role in randomized controlled intervention trials. To our knowledge, this is the first report on the effects of 2 HMOs on establishing microbiota in newborn infants. We provide a detailed description of the microbiota changes observed upon feeding a formula with 2 HMOs in comparison to breastfed reference infants' microbiota. Then, we associate the microbiota to long-term health as assessed by prescribed antibiotic use. Human milk oligosaccharides (HMOs) may provide health benefits to infants partly by shaping the development of the early-life intestinal microbiota. In a randomized double-blinded controlled multicentric clinical trial, healthy term infants received either infant formula (control) or the same formula with two HMOs (2′-fucosyllactose and lacto-N- neo tetraose; test) from enrollment (0 to 14 days) to 6 months. Then, all infants received the same follow-up formula without HMOs until 12 months of age. Breastfed infants (BF) served as a reference group. Stool microbiota at 3 and 12 months, analyzed by 16S rRNA gene sequencing, clustered into seven fecal community types (FCTs) with marked differences in total microbial abundances. Three of the four 12-month FCTs were likely precursors of the adult enterotypes. At 3 months, microbiota composition in the test group ( n = 58) appeared closer to that of BF ( n = 35) than control ( n = 63) by microbiota alpha (within group) and beta (between groups) diversity analyses and distribution of FCTs. While bifidobacteriaceae dominated two FCTs, its abundance was significantly higher in one (FCT BiH for Bifidobacteriaceae at high abundance) than in the other (FCT Bi for Bifidobacteriaceae ). HMO supplementation increased the number of infants with FCT BiH (predominant in BF) at the expense of FCT Bi (predominant in control). We explored the association of the FCTs with reported morbidities and medication use up to 12 months. Formula-fed infants with FCT BiH at 3 months were significantly less likely to require antibiotics during the first year than those with FCT Bi. Previously reported lower rates of infection-related medication use with HMOs may therefore be linked to gut microbiota community types. (This study has been registered at ClinicalTrials.gov under registration number NCT01715246.) IMPORTANCE Human milk is the sole and recommended nutrition for the newborn infant and contains one of the largest constituents of diverse oligosaccharides, dubbed human milk oligosaccharides (HMOs). Preclinical and clinical association studies indicate that HMOs have multiple physiological functions largely mediated through the establishment of the gut microbiome. Until recently, HMOs were not available to investigate their role in randomized controlled intervention trials. To our knowledge, this is the first report on the effects of 2 HMOs on establishing microbiota in newborn infants. We provide a detailed description of the microbiota changes observed upon feeding a formula with 2 HMOs in comparison to breastfed reference infants' microbiota. Then, we associate the microbiota to long-term health as assessed by prescribed antibiotic use.
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