Placenta-on-a-chip paves the path forward for easy drug screening during pregnancy

Courtesy: Penn State News Letter

Going forward with the concept of ‘organs-on-chip’ that mimic the physiological conditions in-vivo, researchers at the University of Pennsylvania’s School of Engineering and Applied Science have developed ‘placenta-on-a-chip’ to look at the placental barrier and drug transport in pregnancy.  

This is a real breakthrough to study the maternal-fetal drug transport across the placenta, as the placental barrier can never be exactly replicated in the lab and in-vivo studies in humans are not ethical. Pregnant women are not included as research subjects because of the risk of teratogenicity. Animal models are not exactly able to mimic human physiology.

We are all aware of the famous ‘Thalidomide’ disaster, in which a drug for morning sickness, crossed the placental barrier in humans and caused multiple birth defects, collectively known as ‘fetal thalidomide syndrome’ and deaths.

To address these issues, a team of researchers led by Dan Huh, Wilf Family Term Assistant Professor in Bioengineering at Penn and Cassidy Blundell, a graduate student in the Huh lab have developed a placenta-on-a-chip, using microfluidic channels in silicone casing.

The study was also published in the journal Advanced Healthcare Materials.

The two channels house human trophoblast cells on one side and endothelial cells on the other separated by a porous membrane. The unit mimics placental barrier and hence the permeability of the barrier to different drugs can be tested.

A blood-like fluid flows through the maternal side of the channel and the researchers can experiment by adding different drugs to the fluid and see the rate, amount of drug transferred to the fetal side of the channel.

“Ex vivo placental perfusion is a great method,” Huh said, “but it has a pretty high failure rate, and the experimental set-up is complicated: it’s prone to leaks and needs a high level of expertise. Most pharmaceutical companies are not going to be able to test their drugs using this method.”

Currently, to validate their model, the team has tested 2 drugs that they have already studied via ex vivo placental perfusion: heparin, an anticoagulant, and glyburide, used in the treatment of diabetes.

The placenta on the chip was able to simulate the drug transfer of these two drugs as it happens in human placenta and fetal interface. Heparin did not pass through the chip model as it is too large a molecule to breach the placental barrier and glyburide transfer was also limited as in real placenta to protect the fetus.

Huh further added, “We’re getting close, this study has given us confidence that the placenta-on-a-chip has tremendous potential as a screening platform to assess and predict drug transport in the human placenta.”

Besides its use by the pharmaceutical company to test various drugs, the ‘placenta-on-a-chip’ has tremendous potential in testing the transfer of supplements other than drugs like vitamins and nutritional supplement.

Penn State News Release

Abstract in Advanced Healthcare Materials

Placenta-on-a-chip to better understand pregnancy pathology and fetal drug safety.

The human placenta

Human ‘organs on chips’ are microchips lined by human cells, that has revolutionized and accelerated drug development and testing, disease modelling and personalize medicine. The concept ‘organs  on chips’ is a brain child of Donald Ingber,  director of biomedical research center at Harvard’s Wyss  Institute. His team was first to bring about marriage between electronic and biology to design ‘organs on chips’ [1]

In this series of ‘organs on chips’ researchers from NIH’s Eunice Kennedy Shriver National Institute of Child Health and Human Development,[2] the University of Pennsylvania, Wayne State University/Detroit Medical Center, Seoul National University, and Asan Medical Center in South Korea researchers and their colleagues have developed a “placenta-on-a-chip” to study the maternal-fetal interface during pregnancy, its role in pregnancy physiology and pathology and drugs that cross the placental barrier.

On a microlevel, the flash drive size device mimics closely the structure of real placenta and all its selectiveness for allowing the passage of nutrients and harmful substances.

A placenta-on-a-chip microdevice A) The device’s upper (blue) and lower (red) chambers are separated by a semi-permeable membrane. B) Researchers placed maternal cells in one chamber and fetal cells in the other.

The microsystem consists of silicone device with two parallel polydimethylsiloxane (PDMS)microfluidic channels separated by a porous membrane. On one side of those pores are human trophoblast cells and on the other side are human umbilical vein endothelial cells.

The team tested the chip by placing glucose in the maternal compartment and monitoring its movement to the fetal compartment. The glucose transfer mirrored what happens in the body, indicating the chip was an accurate model.[3]

The device was developed by a grant from the ‘March of Dimes’ to identify cause and prevention of preterm births. The study was published in the Journal of Maternal-Fetal & Neonatal Medicine.

Roberto Romero, M.D., chief of the NICHD’s Perinatology Research Branch and one of the study authors said “We believe that this technology may be used to address questions that are difficult to answer with current placenta model systems and help enable research on pregnancy and its complications.”

The new placenta will eliminate the need for animal models to study different dynamics of maternal/fetal interphase especially the exchange of endobiotics and xenobiotics.

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[1] https://cosmosmagazine.com/biology/man-who-built-organs-chips

[2] https://www.nih.gov/news-events/news-releases/researchers-design-placenta-chip-better-understand-pregnancy

[3] http://machinedesign.com/medical/placenta-chip-lets-researchers-better-understand-pregnancy

[4] http://www.tandfonline.com/doi/abs/10.3109/14767058.2015.1038518