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Human milk antibodies to global pathogens reveal geographic and interindividual variations in IgA and IgG
Joseph J. Campo, … , William A. Petri Jr., Kirsi M. Järvinen
Joseph J. Campo, … , William A. Petri Jr., Kirsi M. Järvinen
Published August 1, 2024
Citation Information: J Clin Invest. 2024;134(15):e168789. https://doi.org/10.1172/JCI168789.
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Clinical Research and Public Health Infectious disease Article has an altmetric score of 144

Human milk antibodies to global pathogens reveal geographic and interindividual variations in IgA and IgG

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Abstract

BACKGROUND The use of high-throughput technologies has enabled rapid advancement in the knowledge of host immune responses to pathogens. Our objective was to compare the repertoire, protection, and maternal factors associated with human milk antibodies to infectious pathogens in different economic and geographic locations.METHODS Using multipathogen protein microarrays, 878 milk and 94 paired serum samples collected from 695 women in 5 high and low-to-middle income countries (Bangladesh, Finland, Peru, Pakistan, and the United States) were assessed for specific IgA and IgG antibodies to 1,607 proteins from 30 enteric, respiratory, and bloodborne pathogens.RESULTS The antibody coverage across enteric and respiratory pathogens was highest in Bangladeshi and Pakistani cohorts and lowest in the U.S. and Finland. While some pathogens induced a dominant IgA response (Campylobacter, Klebsiella, Acinetobacter, Cryptosporidium, and pertussis), others elicited both IgA and IgG antibodies in milk and serum, possibly related to the invasiveness of the infection (Shigella, enteropathogenic E. coli “EPEC”, Streptococcus pneumoniae, Staphylococcus aureus, and Group B Streptococcus). Besides the differences between economic regions and decreases in concentrations over time, human milk IgA and IgG antibody concentrations were lower in mothers with high BMI and higher parity, respectively. In Bangladeshi infants, a higher specific IgA concentration in human milk was associated with delayed time to rotavirus infection, implying protective properties of antirotavirus antibodies, whereas a higher IgA antibody concentration was associated with greater incidence of Campylobacter infection.CONCLUSION This comprehensive assessment of human milk antibody profiles may be used to guide the development of passive protection strategies against infant morbidity and mortality.FUNDING Bill and Melinda Gates Foundation grant OPP1172222 (to KMJ); Bill and Melinda Gates Foundation grant OPP1066764 funded the MDIG trial (to DER); University of Rochester CTSI and Environmental Health Sciences Center funded the Rochester Lifestyle study (to RJL); and R01 AI043596 funded PROVIDE (to WAP).

Authors

Joseph J. Campo, Antti E. Seppo, Arlo Z. Randall, Jozelyn Pablo, Chris Hung, Andy Teng, Adam D. Shandling, Johnathon Truong, Amit Oberai, James Miller, Najeeha Talat Iqbal, Pablo Peñataro Yori, Anna Kaarina Kukkonen, Mikael Kuitunen, L. Beryl Guterman, Shaun K. Morris, Lisa G. Pell, Abdullah Al Mahmud, Girija Ramakrishan, Eva Heinz, Beth D. Kirkpatrick, Abu S.G. Faruque, Rashidul Haque, R. John Looney, Margaret N. Kosek, Erkki Savilahti, Saad B. Omer, Daniel E. Roth, William A. Petri Jr., Kirsi M. Järvinen

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Figure 9

Validation of human milk IgA correlates of risk in an independent mother-infant birth cohort.

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Validation of human milk IgA correlates of risk in an independent mother...
(A) Hazard ratio of infants during the first year of life divided into the top and bottom halves of mothers’ milk IgA responses for antigens included in a validation mini-protein microarray. Milk samples were from women in the independent Cryptosporidium Burden Study cohort (Validation set, n = 144 milk samples). Only proteins that were reactive in at least 10% of women in the Cryptosporidium Burden Study are shown. (B) Hazard ratio and 95% CIs from Cox proportional hazards models of infants during the first year of life divided into the top and bottom half of mothers’ milk IgA responders against Campylobacter jejuni PEB4 and Rotavirus A VP4. P,Cox regression P value; FDR, adjusted P value.

Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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