Modeling preeclampsia using human induced pluripotent stem cells

Horii, Mariko; Morey, Robert; Bui, Tony; Touma, Ojeni; Nelson, Katelyn N.; Cho, Hee-Young; Rishik, Hannah; Laurent, Louise C.; Parast, Mana M.

doi:10.1038/s41598-021-85230-5

Cited by 30 publications

(46 citation statements)

References 97 publications

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“…For instance, hiPSCs generated from umbilical cords and exposed to culture conditions that promote trophoblast formation show stark differences in the transcriptome (as determined by RNA-seq) if the cords are collected from pregnancies with early onset preeclampsia. In particular, expression of genes associated with O 2 responsiveness and STB formation is impaired in cells from preeclampsia, without marked changes in the DNA methylome ( Sheridan et al, 2019 ; Horii et al, 2021 ).…”

Section: Omics Technologies For the Study Of Early Stb Developmentmentioning

confidence: 99%

Omics Approaches to Study Formation and Function of Human Placental Syncytiotrophoblast

Jaremek

Jeyarajah

Bhattad

et al. 2021

Front. Cell Dev. Biol.

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Proper development of the placenta is vital for pregnancy success. The placenta regulates exchange of nutrients and gases between maternal and fetal blood and produces hormones essential to maintain pregnancy. The placental cell lineage primarily responsible for performing these functions is a multinucleated entity called syncytiotrophoblast. Syncytiotrophoblast is continuously replenished throughout pregnancy by fusion of underlying progenitor cells called cytotrophoblasts. Dysregulated syncytiotrophoblast formation disrupts the integrity of the placental exchange surface, which can be detrimental to maternal and fetal health. Moreover, various factors produced by syncytiotrophoblast enter into maternal circulation, where they profoundly impact maternal physiology and are promising diagnostic indicators of pregnancy health. Despite the multifunctional importance of syncytiotrophoblast for pregnancy success, there is still much to learn about how its formation is regulated in normal and diseased states. ‘Omics’ approaches are gaining traction in many fields to provide a more holistic perspective of cell, tissue, and organ function. Herein, we review human syncytiotrophoblast development and current model systems used for its study, discuss how ‘omics’ strategies have been used to provide multidimensional insights into its formation and function, and highlight limitations of current platforms as well as consider future avenues for exploration.

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Section: Omics Technologies For the Study Of Early Stb Developmentmentioning

confidence: 99%

Omics Approaches to Study Formation and Function of Human Placental Syncytiotrophoblast

Jaremek

Jeyarajah

Bhattad

et al. 2021

Front. Cell Dev. Biol.

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“…Since hiPSCs can be used as starting cells in addition to preexisting hESCs, generation of patient-specific hTSLCs is feasible by sequential establishment of hiPSCs from patients' somatic cells followed by conversion of the hiPSCs to hTSLCs. In turn, the approaches using trisomy 21 hPSCs and PE-derived hiPSCs successfully model trophoblast differentiation defects (Horii et al, 2016(Horii et al, , 2021. Since many hiPSC lines have been established or can be established from human patients with various symptoms, similar approaches can be employed to understand previously unknown links between human diseases and the events during early placentation.…”

Section: Bmp4-induced Htslcsmentioning

confidence: 99%

Integrating High-Throughput Approaches and in vitro Human Trophoblast Models to Decipher Mechanisms Underlying Early Human Placenta Development

Lee

Kim

2021

Front. Cell Dev. Biol.

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The placenta is a temporary but pivotal organ for human pregnancy. It consists of multiple specialized trophoblast cell types originating from the trophectoderm of the blastocyst stage of the embryo. While impaired trophoblast differentiation results in pregnancy disorders affecting both mother and fetus, the molecular mechanisms underlying early human placenta development have been poorly understood, partially due to the limited access to developing human placentas and the lack of suitable human in vitro trophoblast models. Recent success in establishing human trophoblast stem cells and other human in vitro trophoblast models with their differentiation protocols into more specialized cell types, such as syncytiotrophoblast and extravillous trophoblast, has provided a tremendous opportunity to understand early human placenta development. Unfortunately, while high-throughput research methods and omics tools have addressed numerous molecular-level questions in various research fields, these tools have not been widely applied to the above-mentioned human trophoblast models. This review aims to provide an overview of various omics approaches that can be utilized in the study of human in vitro placenta models by exemplifying some important lessons obtained from omics studies of mouse model systems and introducing recently available human in vitro trophoblast model systems. We also highlight some key unknown questions that might be addressed by such techniques. Integrating high-throughput omics approaches and human in vitro model systems will facilitate our understanding of molecular-level regulatory mechanisms underlying early human placenta development as well as placenta-associated complications.

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“…Horii et al have published reproducible models for differentiating human iPSCs into trophoblasts [ 60 ]. More recently, iPSC-derived trophoblasts have been used to study preeclampsia (PE), demonstrating changes in the syncytialization process, as well as differential gene expression in response to hypoxia [ 61 ]. This study underpins the utility of human iPSCs in studying placental disorders and gaining a better understanding of the pathways involved.…”

Section: In Vitro Placental Modelsmentioning

confidence: 99%

“…Modeling the transfer, and more generally the absorption, distribution, metabolism and excretion (ADME), of xenobiotics from the mother to fetus through the placenta has become one of the efforts in the DART field. To this end, different in silico approaches have been developed, such as statistics-based QSAR analysis and PBPK models [ 61 ].…”

Section: In Silico Placental Modelsmentioning

confidence: 99%

The Role of the 3Rs for Understanding and Modeling the Human Placenta

Costa

Mackay

Greca

et al. 2021

JCM

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Modeling the physiology of the human placenta is still a challenge, despite the great number of scientific advancements made in the field. Animal models cannot fully replicate the structure and function of the human placenta and pose ethical and financial hurdles. In addition, increasingly stricter animal welfare legislation worldwide is incentivizing the use of 3R (reduction, refinement, replacement) practices. What efforts have been made to develop alternative models for the placenta so far? How effective are they? How can we improve them to make them more predictive of human pathophysiology? To address these questions, this review aims at presenting and discussing the current models used to study phenomena at the placenta level: in vivo, ex vivo, in vitro and in silico. We describe the main achievements and opportunities for improvement of each type of model and critically assess their individual and collective impact on the pursuit of predictive studies of the placenta in line with the 3Rs and European legislation.

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Modeling preeclampsia using human induced pluripotent stem cells

Cited by 30 publications

References 97 publications

Omics Approaches to Study Formation and Function of Human Placental Syncytiotrophoblast

Omics Approaches to Study Formation and Function of Human Placental Syncytiotrophoblast

Integrating High-Throughput Approaches and in vitro Human Trophoblast Models to Decipher Mechanisms Underlying Early Human Placenta Development

The Role of the 3Rs for Understanding and Modeling the Human Placenta

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