Pathophysiological Implication of Pattern Recognition Receptors in Fetal Membranes Rupture: RAGE and NLRP Inflammasome

Choltus, Héléna; Lavergne, Marilyne; Outeiro, Coraline De Sousa Do; Coste, Karen; Belville, Corinne; Blanchon, Loı̈c; Sapin, Vincent

doi:10.3390/biomedicines9091123

Cited by 5 publications

(5 citation statements)

References 176 publications

(208 reference statements)

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“…Intra-amniotic OS, the production of reactive oxygen species (ROS), and sterile inflammation at term and preterm are well-reported phenomena. 6,10,22,[86][87][88][89] In vitro cultures of amnion and chorion cells and ex vivo fetal membrane explant cultures have documented the following multiple biological processes and signaling pathways related to intra-amniotic oxidative imbalance-associated pathologies (i.e., ROS production, DNA fragmentation, p38MAPK activation, EMT, senescence, and inflammation) 21,22,25,27,28,32,50,73,[90][91][92][93][94][95][96] that shift immune status to a pro-inflammatory environment. Changes in the inflammatory environment at the choriodecidua interface have been associated with the suppression of anti-inflammatory hormone (i.e., progesterone) and immune cell regulators (i.e., HLAs) that allow for maternal immune cell infiltration into the membranes.…”

Section: Discussionmentioning

confidence: 99%

Development of oxidative stress‐associated disease models using feto‐maternal interface organ‐on‐a‐chip

et al. 2023

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Oxidative stress (OS) and inflammation arising from cellular derangements at the fetal membrane-decidual interface (feto-maternal interface [FMi]) is a major antecedent to preterm birth (PTB). However, it is impractical to study OS-associated FMi disease state during human pregnancy, and thus it is difficult to develop strategies to reduce the incidences of PTB. A microfluidic organ-on-chip model (FMi-OOC) that mimics the in vivo structure and functions of FMi in vitro was developed to address this challenge. The FMi-OOC contained fetal (amnion epithelial, mesenchymal, and chorion) and maternal (decidua) cells cultured in four compartments interconnected by arrays of microchannels to allow independent but interconnected co-cultivation. Using this model, we tested the effects of OS and inflammation on both fetal (fetal → maternal) and maternal (maternal → fetal) sides of the FMi and determined their differential impact on PTB-associated pathways. OS was induced using cigarette smoke extract (CSE) exposure. The impacts of OS were assessed by measuring cell viability, disruption of immune homeostasis, epithelial-to-mesenchymal transition (EMT), development of senescence, and inflammation. CSE propagated (LC/MS-MS analysis for nicotine) over a 72hour period from the maternal to fetal side, or vice versa. However, they caused How to cite this article: Richardson LS, Kammala AK, Kim S, et al. Development of oxidative stress-associated disease models using feto-maternal interface organ-on-a-chip. The

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Section: Discussionmentioning

confidence: 99%

Development of oxidative stress‐associated disease models using feto‐maternal interface organ‐on‐a‐chip

et al. 2023

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“…The involvement of RAGE in the progression of inflammatory and neurodegenerative disorders has been well studied. Inflammation plays a central role in many physiological processes that are important in the progression of diabetes, lung diseases, and fetal membrane weakening, which are characterized by elevated levels of RAGE in circulation [ 19 , 24 , 25 ]. RAGE exerts its physiological and pathological effects through its ability to bind with a multitude of ligands.…”

Section: The Receptor For Advanced Glycation End Productsmentioning

confidence: 99%

“…Increasingly, it is becoming accepted that RAGE signaling plays a significant role in driving the inflammation that leads to the rupture of the human fetal membranes (FMs) [ 20 , 25 ]. Indeed, this outcome is dependent on the sophisticated communication between the uterus, placenta, and FM, as RAGE signal transduction flows from maternal to fetal tissues, and back again.…”

Section: The Receptor For Advanced Glycation End Productsmentioning

confidence: 99%

“…Thus, inflammation is necessary for many of the key parturition pathways, including fetal membrane weakening, regardless of whether it occurs at the end of normal gestation or preterm (<37 weeks of gestation). RAGE signaling is influential for both preterm and full-term pregnancies’ FM weakening and rupture via its ligand HMGB1 [ 20 , 25 ]. Its binding to RAGE has been identified as an activator of NF-κB, which leads to a release of inflammatory cytokines, such as Interleukin-6 (IL6), Granulocyte Macrophage Stimulating Factor (GM-CSF), and Tumor Necrosis Factor Alpha (TNF-α).…”

Section: The Receptor For Advanced Glycation End Productsmentioning

confidence: 99%

“…Multiple polymorphisms for the receptor have also been identified; however, the most studied, Gly82Ser, is a single-nucleotide polymorphism within the RAGE gene that modifies the ligand-binding structure by increasing its binding affinity for AGEs. This genotype is characterized by lower sRAGE levels and higher risk factors for CVD, which has implicated it in diabetes and autoimmune diseases, such as Kawasaki disease [ 25 ]. Thus, abnormal upregulation and sRAGE activation are indicative of disease development and inflammatory and immune responses in the body [ 28 , 103 , 152 , 153 ].…”

Section: Rage As a Biomarker Or Putative Therapeutic Targetmentioning

confidence: 99%

See 2 more Smart Citations

RAGE against the Machine: Can Increasing Our Understanding of RAGE Help Us to Battle SARS-CoV-2 Infection in Pregnancy?

Kurashima

Kendal-Wright

2022

IJMS

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The receptor of advanced glycation end products (RAGE) is a receptor that is thought to be a key driver of inflammation in pregnancy, SARS-CoV-2, and also in the comorbidities that are known to aggravate these afflictions. In addition to this, vulnerable populations are particularly susceptible to the negative health outcomes when these afflictions are experienced in concert. RAGE binds a number of ligands produced by tissue damage and cellular stress, and its activation triggers the proinflammatory transcription factor Nuclear Factor Kappa B (NF-κB), with the subsequent generation of key proinflammatory cytokines. While this is important for fetal membrane weakening, RAGE is also activated at the end of pregnancy in the uterus, placenta, and cervix. The comorbidities of hypertension, cardiovascular disease, diabetes, and obesity are known to lead to poor pregnancy outcomes, and particularly in populations such as Native Hawaiians and Pacific Islanders. They have also been linked to RAGE activation when individuals are infected with SARS-CoV-2. Therefore, we propose that increasing our understanding of this receptor system will help us to understand how these various afflictions converge, how forms of RAGE could be used as a biomarker, and if its manipulation could be used to develop future therapeutic targets to help those at risk.

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Amniotic fluid CD36 in pregnancies complicated by spontaneous preterm delivery: a retrospective cohort study

Souček

Kacerovský

Musilová

et al. 2023

The Journal of Maternal-Fetal & Neonatal Medicine

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Pathophysiological Implication of Pattern Recognition Receptors in Fetal Membranes Rupture: RAGE and NLRP Inflammasome

Cited by 5 publications

References 176 publications

Development of oxidative stress‐associated disease models using feto‐maternal interface organ‐on‐a‐chip

Development of oxidative stress‐associated disease models using feto‐maternal interface organ‐on‐a‐chip

RAGE against the Machine: Can Increasing Our Understanding of RAGE Help Us to Battle SARS-CoV-2 Infection in Pregnancy?

Amniotic fluid CD36 in pregnancies complicated by spontaneous preterm delivery: a retrospective cohort study

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