Placental malperfusion in response to intrauterine inflammation and its connection to fetal sequelae

Solange N. Eloundou; Ji Yeon Lee; Dan Wu; Jun Lei; Mia C. Feller; Maide Ozen; Yan Zhu; Misun Hwang; Bei Jia; Han Xie; Julia L. Clemens; Michael W. McLane; Samar AlSaggaf; Nita Nair; Marsha Wills-Karp; Xiaobin Wang; Ernest M. Graham; Ahmet Baschat; Irina Burd

doi:10.1371/journal.pone.0214951

Placental malperfusion in response to intrauterine inflammation and its connection to fetal sequelae

Solange N. Eloundou, Ji Yeon Lee, Dan Wu, Jun Lei, Mia C. Feller, Maide Ozen, Yan Zhu, Misun Hwang, Bei Jia, Han Xie, Julia L. Clemens, Michael W. McLane, Samar AlSaggaf, Nita Nair, Marsha Wills-Karp, Xiaobin Wang, Ernest M. Graham, Ahmet Baschat, Irina Burd

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Abstract

Exposure to intrauterine inflammation (IUI) is associated with short- and long-term adverse perinatal outcomes. However, little data exist on utilizing placenta to prognosticate fetal injury in this scenario. Our study aimed to utilize imaging modalities to evaluate mechanisms contributing to placental injury following IUI exposure and correlated it to concomitant fetal brain injury. CD1 pregnant dams underwent laparotomies and received intrauterine injections of either lipopolysaccharide (LPS; a model of IUI) or phosphate-buffered saline (PBS). In utero ultrasound Doppler velocimetry of uterine and umbilical arteries and magnetic resonance imaging (MRI) of placental volumes with confirmatory immunohistochemical (vimentin) and histochemistry (fibrin) analyses were performed. ELISA for thrombosis markers, fibrinogen and fibrin was performed to analyze thrombi in placenta. Fetal brain immunohistochemistry was performed to detect microglial activation (ionized calcium-binding adaptor molecule 1, Iba1). On ultrasound, LPS group demonstrated elevated resistance indices, pulsatility indices and a greater occurrence of absent end-diastolic flow in the umbilical and uterine arteries. In the fetus, there was an increased cardiac Tei indices in the LPS group. MRI revealed decreased volume of placenta in the LPS group associated with placental thinning and placental endothelial damage on immunohistochemistry. Decreased fibrinogen content and more thrombi staining in placenta exposed to maternal LPS indicated the hypercoagulability. Furthermore, the expression of Iba1was significantly associated with placental thickness (r = -0.7890, Pearson correlation coefficient). Our data indicate that IUI can trigger events leading to maternal placental malperfusion and fetal vessel resistance, as well as predispose the developing fetus to cardiac dysfunction and brain damage. Furthermore, our data suggest that prenatal ultrasound can be a real-time clinical tool for assessing fetal risk for adverse neurologic outcomes following the potential IUI exposure.

Original language	English (US)
Article number	e0214951
Journal	PloS one
Volume	14
Issue number	4
DOIs	https://doi.org/10.1371/journal.pone.0214951
State	Published - Apr 2019

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Eloundou, S. N., Lee, J. Y., Wu, D., Lei, J., Feller, M. C., Ozen, M., Zhu, Y., Hwang, M., Jia, B., Xie, H., Clemens, J. L., McLane, M. W., AlSaggaf, S., Nair, N., Wills-Karp, M., Wang, X., Graham, E. M., Baschat, A., & Burd, I. (2019). Placental malperfusion in response to intrauterine inflammation and its connection to fetal sequelae. PloS one, 14(4), Article e0214951. https://doi.org/10.1371/journal.pone.0214951

Eloundou, SN, Lee, JY, Wu, D, Lei, J, Feller, MC, Ozen, M, Zhu, Y, Hwang, M, Jia, B, Xie, H, Clemens, JL, McLane, MW, AlSaggaf, S, Nair, N, Wills-Karp, M , Wang, X , Graham, EM , Baschat, A & Burd, I 2019, 'Placental malperfusion in response to intrauterine inflammation and its connection to fetal sequelae', PloS one, vol. 14, no. 4, e0214951. https://doi.org/10.1371/journal.pone.0214951

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title = "Placental malperfusion in response to intrauterine inflammation and its connection to fetal sequelae",

abstract = "Exposure to intrauterine inflammation (IUI) is associated with short- and long-term adverse perinatal outcomes. However, little data exist on utilizing placenta to prognosticate fetal injury in this scenario. Our study aimed to utilize imaging modalities to evaluate mechanisms contributing to placental injury following IUI exposure and correlated it to concomitant fetal brain injury. CD1 pregnant dams underwent laparotomies and received intrauterine injections of either lipopolysaccharide (LPS; a model of IUI) or phosphate-buffered saline (PBS). In utero ultrasound Doppler velocimetry of uterine and umbilical arteries and magnetic resonance imaging (MRI) of placental volumes with confirmatory immunohistochemical (vimentin) and histochemistry (fibrin) analyses were performed. ELISA for thrombosis markers, fibrinogen and fibrin was performed to analyze thrombi in placenta. Fetal brain immunohistochemistry was performed to detect microglial activation (ionized calcium-binding adaptor molecule 1, Iba1). On ultrasound, LPS group demonstrated elevated resistance indices, pulsatility indices and a greater occurrence of absent end-diastolic flow in the umbilical and uterine arteries. In the fetus, there was an increased cardiac Tei indices in the LPS group. MRI revealed decreased volume of placenta in the LPS group associated with placental thinning and placental endothelial damage on immunohistochemistry. Decreased fibrinogen content and more thrombi staining in placenta exposed to maternal LPS indicated the hypercoagulability. Furthermore, the expression of Iba1was significantly associated with placental thickness (r = -0.7890, Pearson correlation coefficient). Our data indicate that IUI can trigger events leading to maternal placental malperfusion and fetal vessel resistance, as well as predispose the developing fetus to cardiac dysfunction and brain damage. Furthermore, our data suggest that prenatal ultrasound can be a real-time clinical tool for assessing fetal risk for adverse neurologic outcomes following the potential IUI exposure.",

author = "Eloundou, {Solange N.} and Lee, {Ji Yeon} and Dan Wu and Jun Lei and Feller, {Mia C.} and Maide Ozen and Yan Zhu and Misun Hwang and Bei Jia and Han Xie and Clemens, {Julia L.} and McLane, {Michael W.} and Samar AlSaggaf and Nita Nair and Marsha Wills-Karp and Xiaobin Wang and Graham, {Ernest M.} and Ahmet Baschat and Irina Burd",

note = "Publisher Copyright: {\textcopyright} 2019 Eloundou et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.",

year = "2019",

month = apr,

doi = "10.1371/journal.pone.0214951",

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T1 - Placental malperfusion in response to intrauterine inflammation and its connection to fetal sequelae

AU - Eloundou, Solange N.

AU - Lee, Ji Yeon

AU - Wu, Dan

AU - Lei, Jun

AU - Feller, Mia C.

AU - Ozen, Maide

AU - Zhu, Yan

AU - Hwang, Misun

AU - Jia, Bei

AU - Xie, Han

AU - Clemens, Julia L.

AU - McLane, Michael W.

AU - AlSaggaf, Samar

AU - Nair, Nita

AU - Wills-Karp, Marsha

AU - Wang, Xiaobin

AU - Graham, Ernest M.

AU - Baschat, Ahmet

AU - Burd, Irina

N1 - Publisher Copyright: © 2019 Eloundou et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

PY - 2019/4

Y1 - 2019/4

N2 - Exposure to intrauterine inflammation (IUI) is associated with short- and long-term adverse perinatal outcomes. However, little data exist on utilizing placenta to prognosticate fetal injury in this scenario. Our study aimed to utilize imaging modalities to evaluate mechanisms contributing to placental injury following IUI exposure and correlated it to concomitant fetal brain injury. CD1 pregnant dams underwent laparotomies and received intrauterine injections of either lipopolysaccharide (LPS; a model of IUI) or phosphate-buffered saline (PBS). In utero ultrasound Doppler velocimetry of uterine and umbilical arteries and magnetic resonance imaging (MRI) of placental volumes with confirmatory immunohistochemical (vimentin) and histochemistry (fibrin) analyses were performed. ELISA for thrombosis markers, fibrinogen and fibrin was performed to analyze thrombi in placenta. Fetal brain immunohistochemistry was performed to detect microglial activation (ionized calcium-binding adaptor molecule 1, Iba1). On ultrasound, LPS group demonstrated elevated resistance indices, pulsatility indices and a greater occurrence of absent end-diastolic flow in the umbilical and uterine arteries. In the fetus, there was an increased cardiac Tei indices in the LPS group. MRI revealed decreased volume of placenta in the LPS group associated with placental thinning and placental endothelial damage on immunohistochemistry. Decreased fibrinogen content and more thrombi staining in placenta exposed to maternal LPS indicated the hypercoagulability. Furthermore, the expression of Iba1was significantly associated with placental thickness (r = -0.7890, Pearson correlation coefficient). Our data indicate that IUI can trigger events leading to maternal placental malperfusion and fetal vessel resistance, as well as predispose the developing fetus to cardiac dysfunction and brain damage. Furthermore, our data suggest that prenatal ultrasound can be a real-time clinical tool for assessing fetal risk for adverse neurologic outcomes following the potential IUI exposure.

AB - Exposure to intrauterine inflammation (IUI) is associated with short- and long-term adverse perinatal outcomes. However, little data exist on utilizing placenta to prognosticate fetal injury in this scenario. Our study aimed to utilize imaging modalities to evaluate mechanisms contributing to placental injury following IUI exposure and correlated it to concomitant fetal brain injury. CD1 pregnant dams underwent laparotomies and received intrauterine injections of either lipopolysaccharide (LPS; a model of IUI) or phosphate-buffered saline (PBS). In utero ultrasound Doppler velocimetry of uterine and umbilical arteries and magnetic resonance imaging (MRI) of placental volumes with confirmatory immunohistochemical (vimentin) and histochemistry (fibrin) analyses were performed. ELISA for thrombosis markers, fibrinogen and fibrin was performed to analyze thrombi in placenta. Fetal brain immunohistochemistry was performed to detect microglial activation (ionized calcium-binding adaptor molecule 1, Iba1). On ultrasound, LPS group demonstrated elevated resistance indices, pulsatility indices and a greater occurrence of absent end-diastolic flow in the umbilical and uterine arteries. In the fetus, there was an increased cardiac Tei indices in the LPS group. MRI revealed decreased volume of placenta in the LPS group associated with placental thinning and placental endothelial damage on immunohistochemistry. Decreased fibrinogen content and more thrombi staining in placenta exposed to maternal LPS indicated the hypercoagulability. Furthermore, the expression of Iba1was significantly associated with placental thickness (r = -0.7890, Pearson correlation coefficient). Our data indicate that IUI can trigger events leading to maternal placental malperfusion and fetal vessel resistance, as well as predispose the developing fetus to cardiac dysfunction and brain damage. Furthermore, our data suggest that prenatal ultrasound can be a real-time clinical tool for assessing fetal risk for adverse neurologic outcomes following the potential IUI exposure.

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Placental malperfusion in response to intrauterine inflammation and its connection to fetal sequelae

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