Maternal activation of the EGFR prevents translocation of gut-residing pathogenic Escherichia coli in a model of late-onset neonatal sepsis

Kathryn A. Knoop; Paige E. Coughlin; Alexandria N. Floyd; I. Malick Ndao; Carla Hall-Moore; Nurmohammad Shaikh; Andrew J. Gasparrini; Brigida Rusconi; Marilyn Escobedo; Misty Good; Barbara B. Warner; Phillip I. Tarr; Rodney D. Newberry

doi:10.1073/pnas.1912022117

Maternal activation of the EGFR prevents translocation of gut-residing pathogenic Escherichia coli in a model of late-onset neonatal sepsis

Kathryn A. Knoop, Paige E. Coughlin, Alexandria N. Floyd, I. Malick Ndao, Carla Hall-Moore, Nurmohammad Shaikh, Andrew J. Gasparrini, Brigida Rusconi, Marilyn Escobedo, Misty Good, Barbara B. Warner, Phillip I. Tarr, Rodney D. Newberry

Immunology

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

Abstract

Late-onset sepsis (LOS) is a highly consequential complication of preterm birth and is defined by a positive blood culture obtained after 72 h of age. The causative bacteria can be found in patients' intestinal tracts days before dissemination, and cohort studies suggest reduced LOS risk in breastfed preterm infants through unknown mechanisms. Reduced concentrations of epidermal growth factor (EGF) of maternal origin within the intestinal tract of mice correlated to the translocation of a gut-resident human pathogen Escherichia coli, which spreads systemically and caused a rapid, fatal disease in pups. Translocation of Escherichia coli was associated with the formation of colonic goblet cell-associated antigen passages (GAPs), which translocate enteric bacteria across the intestinal epithelium. Thus, maternally derived EGF, and potentially other EGFR ligands, prevents dissemination of a gut-resident pathogen by inhibiting goblet cell-mediated bacterial translocation. Through manipulation of maternally derived EGF and alteration of the earliest gut defenses, we have developed an animal model of pathogen dissemination which recapitulates gut-origin neonatal LOS.

Original language	English (US)
Pages (from-to)	7941-7949
Number of pages	9
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	117
Issue number	14
DOIs	https://doi.org/10.1073/pnas.1912022117
State	Published - Apr 7 2020

Keywords

Bloodstream infections
Breast milk
Goblet cells
Neonate
Sepsis

ASJC Scopus subject areas

General

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10.1073/pnas.1912022117

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Knoop, K. A., Coughlin, P. E., Floyd, A. N., Malick Ndao, I., Hall-Moore, C., Shaikh, N., Gasparrini, A. J., Rusconi, B., Escobedo, M., Good, M., Warner, B. B., Tarr, P. I., & Newberry, R. D. (2020). Maternal activation of the EGFR prevents translocation of gut-residing pathogenic Escherichia coli in a model of late-onset neonatal sepsis. Proceedings of the National Academy of Sciences of the United States of America, 117(14), 7941-7949. https://doi.org/10.1073/pnas.1912022117

Maternal activation of the EGFR prevents translocation of gut-residing pathogenic Escherichia coli in a model of late-onset neonatal sepsis. / Knoop, Kathryn A.; Coughlin, Paige E.; Floyd, Alexandria N. et al.
In: Proceedings of the National Academy of Sciences of the United States of America, Vol. 117, No. 14, 07.04.2020, p. 7941-7949.

Research output: Contribution to journal › Article › peer-review

Knoop, KA, Coughlin, PE, Floyd, AN, Malick Ndao, I, Hall-Moore, C, Shaikh, N, Gasparrini, AJ, Rusconi, B, Escobedo, M, Good, M, Warner, BB, Tarr, PI & Newberry, RD 2020, 'Maternal activation of the EGFR prevents translocation of gut-residing pathogenic Escherichia coli in a model of late-onset neonatal sepsis', Proceedings of the National Academy of Sciences of the United States of America, vol. 117, no. 14, pp. 7941-7949. https://doi.org/10.1073/pnas.1912022117

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abstract = "Late-onset sepsis (LOS) is a highly consequential complication of preterm birth and is defined by a positive blood culture obtained after 72 h of age. The causative bacteria can be found in patients' intestinal tracts days before dissemination, and cohort studies suggest reduced LOS risk in breastfed preterm infants through unknown mechanisms. Reduced concentrations of epidermal growth factor (EGF) of maternal origin within the intestinal tract of mice correlated to the translocation of a gut-resident human pathogen Escherichia coli, which spreads systemically and caused a rapid, fatal disease in pups. Translocation of Escherichia coli was associated with the formation of colonic goblet cell-associated antigen passages (GAPs), which translocate enteric bacteria across the intestinal epithelium. Thus, maternally derived EGF, and potentially other EGFR ligands, prevents dissemination of a gut-resident pathogen by inhibiting goblet cell-mediated bacterial translocation. Through manipulation of maternally derived EGF and alteration of the earliest gut defenses, we have developed an animal model of pathogen dissemination which recapitulates gut-origin neonatal LOS.",

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AU - Shaikh, Nurmohammad

AU - Gasparrini, Andrew J.

AU - Rusconi, Brigida

AU - Escobedo, Marilyn

AU - Good, Misty

AU - Warner, Barbara B.

AU - Tarr, Phillip I.

AU - Newberry, Rodney D.

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N2 - Late-onset sepsis (LOS) is a highly consequential complication of preterm birth and is defined by a positive blood culture obtained after 72 h of age. The causative bacteria can be found in patients' intestinal tracts days before dissemination, and cohort studies suggest reduced LOS risk in breastfed preterm infants through unknown mechanisms. Reduced concentrations of epidermal growth factor (EGF) of maternal origin within the intestinal tract of mice correlated to the translocation of a gut-resident human pathogen Escherichia coli, which spreads systemically and caused a rapid, fatal disease in pups. Translocation of Escherichia coli was associated with the formation of colonic goblet cell-associated antigen passages (GAPs), which translocate enteric bacteria across the intestinal epithelium. Thus, maternally derived EGF, and potentially other EGFR ligands, prevents dissemination of a gut-resident pathogen by inhibiting goblet cell-mediated bacterial translocation. Through manipulation of maternally derived EGF and alteration of the earliest gut defenses, we have developed an animal model of pathogen dissemination which recapitulates gut-origin neonatal LOS.

AB - Late-onset sepsis (LOS) is a highly consequential complication of preterm birth and is defined by a positive blood culture obtained after 72 h of age. The causative bacteria can be found in patients' intestinal tracts days before dissemination, and cohort studies suggest reduced LOS risk in breastfed preterm infants through unknown mechanisms. Reduced concentrations of epidermal growth factor (EGF) of maternal origin within the intestinal tract of mice correlated to the translocation of a gut-resident human pathogen Escherichia coli, which spreads systemically and caused a rapid, fatal disease in pups. Translocation of Escherichia coli was associated with the formation of colonic goblet cell-associated antigen passages (GAPs), which translocate enteric bacteria across the intestinal epithelium. Thus, maternally derived EGF, and potentially other EGFR ligands, prevents dissemination of a gut-resident pathogen by inhibiting goblet cell-mediated bacterial translocation. Through manipulation of maternally derived EGF and alteration of the earliest gut defenses, we have developed an animal model of pathogen dissemination which recapitulates gut-origin neonatal LOS.

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Maternal activation of the EGFR prevents translocation of gut-residing pathogenic Escherichia coli in a model of late-onset neonatal sepsis

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Keywords

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