Characterization of neutrophil subsets in healthy human pregnancies

Aloysius Ssemaganda; Lindsay Kindinger; Philip Bergin; Leslie Nielsen; Juliet Mpendo; Ali Ssetaala; Noah Kiwanuka; Markus Munder; Tiong Ghee Teoh; Pascale Kropf; Ingrid Müller

doi:10.1371/journal.pone.0085696

Characterization of neutrophil subsets in healthy human pregnancies

Aloysius Ssemaganda, Lindsay Kindinger, Philip Bergin, Leslie Nielsen, Juliet Mpendo, Ali Ssetaala, Noah Kiwanuka, Markus Munder, Tiong Ghee Teoh, Pascale Kropf, Ingrid Müller

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

65 Citations (Scopus)

Abstract

We have previously shown that in successful pregnancies increased arginase activity is a mechanism that contributes to the suppression of the maternal immune system. We identified the main type of arginase-expressing cells as a population of activated low-density granulocytes (LDGs) in peripheral blood mononuclear cells and in term placentae. In the present study, we analyzed the phenotype of LDGs and compared it to the phenotype of normal density granulocytes (NDGs) in maternal peripheral blood, placental biopsies and cord blood. Our data reveal that only LDGs but no NDGs could be detected in placental biopsies. Phenotypically, NDGs and LDGs from both maternal and cord blood expressed different levels of maturation, activation and degranulation markers. NDGs from the maternal and cord blood were phenotypically similar, while maternal, cord and placental LDGs showed different expression levels of CD66b. LDGs present in cord blood expressed higher levels of arginase compared to maternal and placental LDGs. In summary, our results show that in maternal and cord blood, two phenotypically different populations of neutrophils can be identified, whereas in term placentae, only activated neutrophils are present.

Original language	English
Pages (from-to)	e85696
Journal	PLoS One
Volume	9
Issue number	2
DOIs	https://doi.org/10.1371/journal.pone.0085696
Publication status	Published - 2014
Externally published	Yes

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title = "Characterization of neutrophil subsets in healthy human pregnancies",

abstract = "We have previously shown that in successful pregnancies increased arginase activity is a mechanism that contributes to the suppression of the maternal immune system. We identified the main type of arginase-expressing cells as a population of activated low-density granulocytes (LDGs) in peripheral blood mononuclear cells and in term placentae. In the present study, we analyzed the phenotype of LDGs and compared it to the phenotype of normal density granulocytes (NDGs) in maternal peripheral blood, placental biopsies and cord blood. Our data reveal that only LDGs but no NDGs could be detected in placental biopsies. Phenotypically, NDGs and LDGs from both maternal and cord blood expressed different levels of maturation, activation and degranulation markers. NDGs from the maternal and cord blood were phenotypically similar, while maternal, cord and placental LDGs showed different expression levels of CD66b. LDGs present in cord blood expressed higher levels of arginase compared to maternal and placental LDGs. In summary, our results show that in maternal and cord blood, two phenotypically different populations of neutrophils can be identified, whereas in term placentae, only activated neutrophils are present.",

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author = "Aloysius Ssemaganda and Lindsay Kindinger and Philip Bergin and Leslie Nielsen and Juliet Mpendo and Ali Ssetaala and Noah Kiwanuka and Markus Munder and Teoh, \{Tiong Ghee\} and Pascale Kropf and Ingrid M{\"u}ller",

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AU - Ssemaganda, Aloysius

AU - Kindinger, Lindsay

AU - Bergin, Philip

AU - Nielsen, Leslie

AU - Mpendo, Juliet

AU - Ssetaala, Ali

AU - Kiwanuka, Noah

AU - Munder, Markus

AU - Teoh, Tiong Ghee

AU - Kropf, Pascale

AU - Müller, Ingrid

PY - 2014

Y1 - 2014

N2 - We have previously shown that in successful pregnancies increased arginase activity is a mechanism that contributes to the suppression of the maternal immune system. We identified the main type of arginase-expressing cells as a population of activated low-density granulocytes (LDGs) in peripheral blood mononuclear cells and in term placentae. In the present study, we analyzed the phenotype of LDGs and compared it to the phenotype of normal density granulocytes (NDGs) in maternal peripheral blood, placental biopsies and cord blood. Our data reveal that only LDGs but no NDGs could be detected in placental biopsies. Phenotypically, NDGs and LDGs from both maternal and cord blood expressed different levels of maturation, activation and degranulation markers. NDGs from the maternal and cord blood were phenotypically similar, while maternal, cord and placental LDGs showed different expression levels of CD66b. LDGs present in cord blood expressed higher levels of arginase compared to maternal and placental LDGs. In summary, our results show that in maternal and cord blood, two phenotypically different populations of neutrophils can be identified, whereas in term placentae, only activated neutrophils are present.

AB - We have previously shown that in successful pregnancies increased arginase activity is a mechanism that contributes to the suppression of the maternal immune system. We identified the main type of arginase-expressing cells as a population of activated low-density granulocytes (LDGs) in peripheral blood mononuclear cells and in term placentae. In the present study, we analyzed the phenotype of LDGs and compared it to the phenotype of normal density granulocytes (NDGs) in maternal peripheral blood, placental biopsies and cord blood. Our data reveal that only LDGs but no NDGs could be detected in placental biopsies. Phenotypically, NDGs and LDGs from both maternal and cord blood expressed different levels of maturation, activation and degranulation markers. NDGs from the maternal and cord blood were phenotypically similar, while maternal, cord and placental LDGs showed different expression levels of CD66b. LDGs present in cord blood expressed higher levels of arginase compared to maternal and placental LDGs. In summary, our results show that in maternal and cord blood, two phenotypically different populations of neutrophils can be identified, whereas in term placentae, only activated neutrophils are present.

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KW - Cell Lineage/immunology

KW - Female

KW - Fetal Blood/cytology

KW - GPI-Linked Proteins/genetics

KW - Gene Expression

KW - Humans

KW - Immune Tolerance

KW - Immunophenotyping

KW - Leukocyte Count

KW - Neutrophil Activation/immunology

KW - Neutrophils/cytology

KW - Phenotype

KW - Placenta/cytology

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SP - e85696

JO - PLoS One

JF - PLoS One

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ER -

Characterization of neutrophil subsets in healthy human pregnancies

Abstract

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