Regulation of the complement system and immunological tolerance in pregnancy

Laura Teirilä; Jenni Heikkinen-Eloranta; Juha Kotimaa; Seppo Meri; A. Inkeri Lokki

doi:10.1016/j.smim.2019.101337

Regulation of the complement system and immunological tolerance in pregnancy

Laura Teirilä
, Jenni Heikkinen-Eloranta
, Juha Kotimaa
, Seppo Meri
, A. Inkeri Lokki^*

^*Corresponding author for this work

Not published at VTT

University of Helsinki

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

60 Citations (Scopus)

Abstract

Preeclampsia is a serious vascular complication of the human pregnancy, whose etiology is still poorly understood. In preeclampsia, exacerbated apoptosis and fragmentation of the placental tissue occurs due to developmental qualities of the placental trophoblast cells and/or mechanical and oxidative distress to the syncytiotrophoblast, which lines the placental villi. Dysregulation of the complement system is recognized as one of the mechanisms of the disease pathology. Complement has the ability to promote inflammation and facilitate phagocytosis of placenta-derived particles and apoptotic cells by macrophages. In preeclampsia, an overload of placental cell damage or dysregulated complement system may lead to insufficient clearance of apoptotic particles and placenta-derived debris. Excess placental damage may lead to sequestration of microparticles, such as placental vesicles, to capillaries in the glomeruli of the kidney and other vulnerable tissues. This phenomenon could contribute to the manifestations of typical diagnostic symptoms of preeclampsia: proteinuria and new-onset hypertension. In this review we propose that the complement system may serve as a regulator of the complex tolerance and clearance processes that are fundamental in healthy pregnancy. It is therefore recommended that further research be conducted to elucidate the interactions between components of the complement system and immune responses in the context of complicated and healthy pregnancy.

Original language	English
Article number	101337
Journal	Seminars in Immunology
Volume	45
DOIs	https://doi.org/10.1016/j.smim.2019.101337
Publication status	Published - Oct 2019
MoE publication type	A2 Review article in a scientific journal

Funding

This research was funded by VTR research funding (competitive state research financing of the expert responsibility area of Helsinki and Uusimaa Hospital District ; SM fund number: TYH2019311 , JHE fund number: TYH2019213 ), Academy of Finland , the Sigrid Jusélius Foundation and Jane and Aatos Erkko Foundation 4706167 (to SM). We acknowledge the expertise of Assistant Professor Susanna Fagerholm of University of Helsinki for her expertise integrin immunity and are thankful for her suggestions to the manuscript. This research was funded by VTR research funding (competitive state research financing of the expert responsibility area of Helsinki and Uusimaa Hospital District; SM fund number: TYH2019311, JHE fund number: TYH2019213), Academy of Finland, the Sigrid Jus?lius Foundation and Jane and Aatos Erkko Foundation4706167 (to SM).

Keywords

Apoptosis
Complement
Inflammation
Preeclampsia
Pregnancy
Tolerance
Autoimmunity
Complement Activation/genetics
Receptors, Complement/metabolism
Disease Susceptibility
Immunomodulation
Humans
Immune Tolerance
Pre-Eclampsia/diagnosis
Neovascularization, Pathologic/immunology
Complement System Proteins/immunology
Animals
Female

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10.1016/j.smim.2019.101337

Cite this

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title = "Regulation of the complement system and immunological tolerance in pregnancy",

abstract = "Preeclampsia is a serious vascular complication of the human pregnancy, whose etiology is still poorly understood. In preeclampsia, exacerbated apoptosis and fragmentation of the placental tissue occurs due to developmental qualities of the placental trophoblast cells and/or mechanical and oxidative distress to the syncytiotrophoblast, which lines the placental villi. Dysregulation of the complement system is recognized as one of the mechanisms of the disease pathology. Complement has the ability to promote inflammation and facilitate phagocytosis of placenta-derived particles and apoptotic cells by macrophages. In preeclampsia, an overload of placental cell damage or dysregulated complement system may lead to insufficient clearance of apoptotic particles and placenta-derived debris. Excess placental damage may lead to sequestration of microparticles, such as placental vesicles, to capillaries in the glomeruli of the kidney and other vulnerable tissues. This phenomenon could contribute to the manifestations of typical diagnostic symptoms of preeclampsia: proteinuria and new-onset hypertension. In this review we propose that the complement system may serve as a regulator of the complex tolerance and clearance processes that are fundamental in healthy pregnancy. It is therefore recommended that further research be conducted to elucidate the interactions between components of the complement system and immune responses in the context of complicated and healthy pregnancy.",

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author = "Laura Teiril{\"a} and Jenni Heikkinen-Eloranta and Juha Kotimaa and Seppo Meri and Lokki, \{A. Inkeri\}",

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AU - Heikkinen-Eloranta, Jenni

AU - Kotimaa, Juha

AU - Meri, Seppo

AU - Lokki, A. Inkeri

PY - 2019/10

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N2 - Preeclampsia is a serious vascular complication of the human pregnancy, whose etiology is still poorly understood. In preeclampsia, exacerbated apoptosis and fragmentation of the placental tissue occurs due to developmental qualities of the placental trophoblast cells and/or mechanical and oxidative distress to the syncytiotrophoblast, which lines the placental villi. Dysregulation of the complement system is recognized as one of the mechanisms of the disease pathology. Complement has the ability to promote inflammation and facilitate phagocytosis of placenta-derived particles and apoptotic cells by macrophages. In preeclampsia, an overload of placental cell damage or dysregulated complement system may lead to insufficient clearance of apoptotic particles and placenta-derived debris. Excess placental damage may lead to sequestration of microparticles, such as placental vesicles, to capillaries in the glomeruli of the kidney and other vulnerable tissues. This phenomenon could contribute to the manifestations of typical diagnostic symptoms of preeclampsia: proteinuria and new-onset hypertension. In this review we propose that the complement system may serve as a regulator of the complex tolerance and clearance processes that are fundamental in healthy pregnancy. It is therefore recommended that further research be conducted to elucidate the interactions between components of the complement system and immune responses in the context of complicated and healthy pregnancy.

AB - Preeclampsia is a serious vascular complication of the human pregnancy, whose etiology is still poorly understood. In preeclampsia, exacerbated apoptosis and fragmentation of the placental tissue occurs due to developmental qualities of the placental trophoblast cells and/or mechanical and oxidative distress to the syncytiotrophoblast, which lines the placental villi. Dysregulation of the complement system is recognized as one of the mechanisms of the disease pathology. Complement has the ability to promote inflammation and facilitate phagocytosis of placenta-derived particles and apoptotic cells by macrophages. In preeclampsia, an overload of placental cell damage or dysregulated complement system may lead to insufficient clearance of apoptotic particles and placenta-derived debris. Excess placental damage may lead to sequestration of microparticles, such as placental vesicles, to capillaries in the glomeruli of the kidney and other vulnerable tissues. This phenomenon could contribute to the manifestations of typical diagnostic symptoms of preeclampsia: proteinuria and new-onset hypertension. In this review we propose that the complement system may serve as a regulator of the complex tolerance and clearance processes that are fundamental in healthy pregnancy. It is therefore recommended that further research be conducted to elucidate the interactions between components of the complement system and immune responses in the context of complicated and healthy pregnancy.

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KW - Preeclampsia

KW - Pregnancy

KW - Tolerance

KW - Autoimmunity

KW - Complement Activation/genetics

KW - Receptors, Complement/metabolism

KW - Disease Susceptibility

KW - Immunomodulation

KW - Humans

KW - Immune Tolerance

KW - Pre-Eclampsia/diagnosis

KW - Neovascularization, Pathologic/immunology

KW - Complement System Proteins/immunology

KW - Animals

KW - Female

UR - https://www.scopus.com/pages/publications/85075714054

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DO - 10.1016/j.smim.2019.101337

M3 - Review Article

C2 - 31757607

AN - SCOPUS:85075714054

SN - 1044-5323

VL - 45

JO - Seminars in Immunology

JF - Seminars in Immunology

M1 - 101337

ER -

Regulation of the complement system and immunological tolerance in pregnancy

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