Defining the lipid profiles of human milk, infant formula, and animal milk: implications for infant feeding

George, Alexandra; Paul, Sudip; Wang, Tingting; Huynh, Kevin; Giles, Corey; Mellett, Natalie; Duong, Thy; Nguyen, Anh; Geddes, Donna; Mansell, Toby; Saffery, Richard; Vuillermin, Peter; Ponsonby, Anne-Louise; Burgner, David; Burugupalli, Satvika; Meikle, Peter; Team, Barwon Infant Study Investigator

doi:10.26181/25124249.v1

1341447_George,A_2023.pdf (2.96 MB)

Defining the lipid profiles of human milk, infant formula, and animal milk: implications for infant feeding

journal contribution

posted on 2024-02-01, 06:18 authored by Alexandra GeorgeAlexandra George, Sudip PaulSudip Paul, Tingting Wang, Kevin HuynhKevin Huynh, Corey GilesCorey Giles, Natalie Mellett, Thy Duong, Anh Nguyen, Donna Geddes, Toby Mansell, Richard Saffery, Peter Vuillermin, Anne-Louise Ponsonby, David Burgner, Satvika Burugupalli, Peter MeiklePeter Meikle, Barwon Infant Study Investigator Team

Background: Breastfed infants have lower disease risk compared to formula-fed infants, however, the mechanisms behind this protection are unknown. Human milk has a complex lipidome which may have many critical roles in health and disease risk. However, human milk lipidomics is challenging, and research is still required to fully understand the lipidome and to interpret and translate findings. This study aimed to address key human milk lipidome knowledge gaps and discuss possible implications for early life health. Methods: Human milk samples from two birth cohorts, the Barwon Infant Study (n = 312) and University of Western Australia birth cohort (n = 342), were analysed using four liquid chromatography-mass spectrometry (LC–MS) methods (lipidome, triacylglycerol, total fatty acid, alkylglycerol). Bovine, goat, and soy-based infant formula, and bovine and goat milk were analysed for comparison. Composition was explored as concentrations, relative abundance, and infant lipid intake. Statistical analyses included principal component analysis, mixed effects modelling, and correlation, with false discovery rate correction, to explore human milk lipidome longitudinal trends and inter and intra-individual variation, differences between sample types, lipid intakes, and correlations between infant plasma and human milk lipids. Results: Lipidomics analysis identified 979 lipids. The human milk lipidome was distinct from that of infant formula and animal milk. Ether lipids were of particular interest, as they were significantly higher, in concentration and relative abundance, in human milk than in formula and animal milk, if present in the latter samples at all. Many ether lipids were highest in colostrum, and some changed significantly through lactation. Significant correlations were identified between human milk and infant circulating lipids (40% of which were ether lipids), and specific ether lipid intake by exclusively breastfed infants was 200-fold higher than that of an exclusively formula-fed infant. Conclusion: There are marked differences between the lipidomes of human milk, infant formula, and animal milk, with notable distinctions between ether lipids that are reflected in the infant plasma lipidome. These findings have potential implications for early life health, and may reveal why breast and formula-fed infants are not afforded the same protections. Comprehensive lipidomics studies with outcomes are required to understand the impacts on infant health and tailor translation.

Funding

AG is supported by International Society for Research in Human Milk and Lactation-Family Larsson-Rosenquist Foundation funding. KH is supported by a National Health and Medical Research Council (NHMRC) investigator grant (1197190). DG receives an unrestricted research grant from Medela AG, administered by the University of Western Australia. TM is supported by an early-career fellowship from the Murdoch Children's Research Institute. PV is supported by an NHMRC Career Development Fellowship. A-LP is supported by an NHMRC Investigator Grant. DB is supported by an NHMRC Investigator Grant. PM is supported by an NHMRC Investigator grant (2009965). This work was supported by LEW Carty grant and by the Victorian Government's Operational Infrastructure Support Program. The funding bodies had no input in design or publication of this study.

History

Publication Date

2023-08-30

Journal

Frontiers in Nutrition

Volume

10

Article Number

1227340

Pagination

15p.

Publisher

Frontiers

ISSN

2296-861X

Rights Statement

© 2023 George, Paul, Wang, Huynh, Giles, Mellett, Duong, Nguyen, Geddes, Mansell, Saffery, Vuillermin, Ponsonby, Burgner, Burugupalli, Meikle and Barwon Infant Study Investigator Team. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.