Activation of Nod1 Signaling Induces Fetal Growth Restriction and Death through Fetal and Maternal Vasculopathy

Intrauterine fetal growth restriction (IUGR) and death (IUFD) are both serious problems in the perinatal medicine. Fetal vasculopathy is currently considered to account for a pathogenic mechanism of IUGR and IUFD. We previously demonstrated that an innate immune receptor, the nucleotide-binding olig...

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Published in	The Journal of immunology (1950) Vol. 196; no. 6; pp. 2779 - 2787
Main Authors	Inoue, Hirosuke, Nishio, Hisanori, Takada, Hidetoshi, Sakai, Yasunari, Nanishi, Etsuro, Ochiai, Masayuki, Onimaru, Mitsuho, Chen, Si Jing, Matsui, Toshiro, Hara, Toshiro
Format	Journal Article
Language	English
Published	United States AAI 15.03.2016
Subjects	Animals Chemokine CCL2 - metabolism Female Fetal Death - etiology Fetal Death - prevention & control Fetal Growth Retardation - chemically induced Fetal Growth Retardation - immunology Humans Innate Immunity and Inflammation Interleukin-6 - metabolism Ligands Maternal Exposure - adverse effects Mice Mice, Inbred C57BL Mice, Knockout Nod1 Signaling Adaptor Protein - agonists Nod1 Signaling Adaptor Protein - genetics Nod1 Signaling Adaptor Protein - metabolism Oligopeptides - administration & dosage Pregnancy Signal Transduction - drug effects Tumor Necrosis Factor-alpha - metabolism Vasculitis - chemically induced Vasculitis - immunology
Online Access	Get full text
ISSN	0022-1767 1550-6606 1550-6606
DOI	10.4049/jimmunol.1500295

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Abstract	Intrauterine fetal growth restriction (IUGR) and death (IUFD) are both serious problems in the perinatal medicine. Fetal vasculopathy is currently considered to account for a pathogenic mechanism of IUGR and IUFD. We previously demonstrated that an innate immune receptor, the nucleotide-binding oligomerization domain-1 (Nod1), contributed to the development of vascular inflammations in mice at postnatal stages. However, little is known about the deleterious effects of activated Nod1 signaling on embryonic growth and development. We report that administration of FK565, one of the Nod1 ligands, to pregnant C57BL/6 mice induced IUGR and IUFD. Mass spectrometry analysis revealed that maternally injected FK565 was distributed to the fetal tissues across placenta. In addition, maternal injection of FK565 induced robust increases in the amounts of CCL2, IL-6, and TNF proteins as well as NO in maternal, placental and fetal tissues. Nod1 was highly expressed in fetal vascular tissues, where significantly higher levels of CCL2 and IL-6 mRNAs were induced with maternal injection of FK565 than those in other tissues. Using Nod1-knockout mice, we verified that both maternal and fetal tissues were involved in the development of IUGR and IUFD. Furthermore, FK565 induced upregulation of genes associated with immune response, inflammation, and apoptosis in fetal vascular tissues. Our data thus provided new evidence for the pathogenic role of Nod1 in the development of IUGR and IUFD at the maternal-fetal interface.
AbstractList	Intrauterine fetal growth restriction (IUGR) and death (IUFD) are both serious problems in the perinatal medicine. Fetal vasculopathy is currently considered to account for a pathogenic mechanism of IUGR and IUFD. We previously demonstrated that an innate immune receptor, the nucleotide-binding oligomerization domain-1 (Nod1), contributed to the development of vascular inflammations in mice at postnatal stages. However, little is known about the deleterious effects of activated Nod1 signaling on embryonic growth and development. We report that administration of FK565, one of the Nod1 ligands, to pregnant C57BL/6 mice induced IUGR and IUFD. Mass spectrometry analysis revealed that maternally injected FK565 was distributed to the fetal tissues across placenta. In addition, maternal injection of FK565 induced robust increases in the amounts of CCL2, IL-6, and TNF proteins as well as NO in maternal, placental and fetal tissues. Nod1 was highly expressed in fetal vascular tissues, where significantly higher levels of CCL2 and IL-6 mRNAs were induced with maternal injection of FK565 than those in other tissues. Using Nod1-knockout mice, we verified that both maternal and fetal tissues were involved in the development of IUGR and IUFD. Furthermore, FK565 induced upregulation of genes associated with immune response, inflammation, and apoptosis in fetal vascular tissues. Our data thus provided new evidence for the pathogenic role of Nod1 in the development of IUGR and IUFD at the maternal-fetal interface. Intrauterine fetal growth restriction (IUGR) and death (IUFD) are both serious problems in the perinatal medicine. Fetal vasculopathy is currently considered to account for a pathogenic mechanism of IUGR and IUFD. We previously demonstrated that an innate immune receptor, the nucleotide-binding oligomerization domain-1 (Nod1), contributed to the development of vascular inflammations in mice at postnatal stages. However, little is known about the deleterious effects of activated Nod1 signaling on embryonic growth and development. We report that administration of FK565, one of the Nod1 ligands, to pregnant C57BL/6 mice induced IUGR and IUFD. Mass spectrometry analysis revealed that maternally injected FK565 was distributed to the fetal tissues across placenta. In addition, maternal injection of FK565 induced robust increases in the amounts of CCL2, IL-6, and TNF proteins as well as NO in maternal, placental and fetal tissues. Nod1 was highly expressed in fetal vascular tissues, where significantly higher levels of CCL2 and IL-6 mRNAs were induced with maternal injection of FK565 than those in other tissues. Using Nod1 -knockout mice, we verified that both maternal and fetal tissues were involved in the development of IUGR and IUFD. Furthermore, FK565 induced upregulation of genes associated with immune response, inflammation, and apoptosis in fetal vascular tissues. Our data thus provided new evidence for the pathogenic role of Nod1 in the development of IUGR and IUFD at the maternal-fetal interface. Intrauterine fetal growth restriction (IUGR) and death (IUFD) are both serious problems in the perinatal medicine. Fetal vasculopathy is currently considered to account for a pathogenic mechanism of IUGR and IUFD. We previously demonstrated that an innate immune receptor, the nucleotide-binding oligomerization domain-1 (Nod1), contributed to the development of vascular inflammations in mice at postnatal stages. However, little is known about the deleterious effects of activated Nod1 signaling on embryonic growth and development. We report that administration of FK565, one of the Nod1 ligands, to pregnant C57BL/6 mice induced IUGR and IUFD. Mass spectrometry analysis revealed that maternally injected FK565 was distributed to the fetal tissues across placenta. In addition, maternal injection of FK565 induced robust increases in the amounts of CCL2, IL-6, and TNF proteins as well as NO in maternal, placental and fetal tissues. Nod1 was highly expressed in fetal vascular tissues, where significantly higher levels of CCL2 and IL-6 mRNAs were induced with maternal injection of FK565 than those in other tissues. Using Nod1-knockout mice, we verified that both maternal and fetal tissues were involved in the development of IUGR and IUFD. Furthermore, FK565 induced upregulation of genes associated with immune response, inflammation, and apoptosis in fetal vascular tissues. Our data thus provided new evidence for the pathogenic role of Nod1 in the development of IUGR and IUFD at the maternal-fetal interface.Intrauterine fetal growth restriction (IUGR) and death (IUFD) are both serious problems in the perinatal medicine. Fetal vasculopathy is currently considered to account for a pathogenic mechanism of IUGR and IUFD. We previously demonstrated that an innate immune receptor, the nucleotide-binding oligomerization domain-1 (Nod1), contributed to the development of vascular inflammations in mice at postnatal stages. However, little is known about the deleterious effects of activated Nod1 signaling on embryonic growth and development. We report that administration of FK565, one of the Nod1 ligands, to pregnant C57BL/6 mice induced IUGR and IUFD. Mass spectrometry analysis revealed that maternally injected FK565 was distributed to the fetal tissues across placenta. In addition, maternal injection of FK565 induced robust increases in the amounts of CCL2, IL-6, and TNF proteins as well as NO in maternal, placental and fetal tissues. Nod1 was highly expressed in fetal vascular tissues, where significantly higher levels of CCL2 and IL-6 mRNAs were induced with maternal injection of FK565 than those in other tissues. Using Nod1-knockout mice, we verified that both maternal and fetal tissues were involved in the development of IUGR and IUFD. Furthermore, FK565 induced upregulation of genes associated with immune response, inflammation, and apoptosis in fetal vascular tissues. Our data thus provided new evidence for the pathogenic role of Nod1 in the development of IUGR and IUFD at the maternal-fetal interface.
Author	Hara, Toshiro Takada, Hidetoshi Matsui, Toshiro Inoue, Hirosuke Nishio, Hisanori Nanishi, Etsuro Sakai, Yasunari Ochiai, Masayuki Onimaru, Mitsuho Chen, Si Jing
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Cites_doi	10.1038/nri2075 10.1111/j.0001-6349.2004.00602.x 10.1111/j.1471-0528.2010.02737.x 10.4049/jimmunol.1302841 10.1159/000321933 10.1074/jbc.274.21.14560 10.1016/S0140-6736(89)90710-1 10.1016/j.immuni.2012.10.014 10.1111/j.1476-5381.2010.00814.x 10.4049/jimmunol.1100578 10.1126/science.1095292 10.1111/apa.12559 10.1016/j.immuni.2014.12.010 10.1074/jbc.M602638200 10.1111/j.1600-0897.2010.00848.x 10.1016/j.immuni.2007.03.009 10.1007/s00216-013-7071-2 10.1021/ac400294q 10.1038/nm.2087 10.1111/j.1365-2249.2009.04073.x 10.2202/1544-6115.1027 10.1164/rccm.200608-1103OC 10.1038/nri3565 10.1182/blood-2010-12-325142 10.1007/s13669-013-0041-z 10.1136/bmj.38629.587639.7C 10.1155/2011/364381 10.1161/ATVBAHA.110.216325 10.1016/j.bpobgyn.2009.06.005
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Snippet	Intrauterine fetal growth restriction (IUGR) and death (IUFD) are both serious problems in the perinatal medicine. Fetal vasculopathy is currently considered...
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SubjectTerms	Animals Chemokine CCL2 - metabolism Female Fetal Death - etiology Fetal Death - prevention & control Fetal Growth Retardation - chemically induced Fetal Growth Retardation - immunology Humans Innate Immunity and Inflammation Interleukin-6 - metabolism Ligands Maternal Exposure - adverse effects Mice Mice, Inbred C57BL Mice, Knockout Nod1 Signaling Adaptor Protein - agonists Nod1 Signaling Adaptor Protein - genetics Nod1 Signaling Adaptor Protein - metabolism Oligopeptides - administration & dosage Pregnancy Signal Transduction - drug effects Tumor Necrosis Factor-alpha - metabolism Vasculitis - chemically induced Vasculitis - immunology
Title	Activation of Nod1 Signaling Induces Fetal Growth Restriction and Death through Fetal and Maternal Vasculopathy
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