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Pixabay/CC0 Public Domain
A team of scientists have developed a simple method for automated
manufacturing of lung organoids which could revolutionize the development of
treatments for lung disease. These organoids, miniature structures containing
the cells that real lungs do, could be used to test early-stage experimental
drugs more effectively, without needing to use animal material.
In the future, patients could even have personalized organoids grown from
their own tissue to try out potential treatments in advance.
"The best result for now—quite simply—is that it works," said
Professor Diana Klein of University of Duisburg-Essen, first author of the
article in Frontiers in Bioengineering and Biotechnology.
"This means that, in principle, lung organoids can be produced using
an automated process. These complex structures represent the in vivo situation
better than conventional cell lines and thus serve as an excellent disease
model."
"In the next step, the organoids could also be used to test potential
therapeutics using high-throughput methods," said Klein.
"Which ones are effective and at what concentration? This could
accelerate the development of specific medications for patients. Furthermore,
the organoids could also be used to predict patient-specific reactions to
radiotherapy or other potential treatments."
Stem cells step up
Finding better treatments for lung diseases would save millions of lives
worldwide. But lungs are a complex structure, difficult to model in the lab so
that treatments can be tested quickly and effectively. Lung organoids are a
promising option for research, but until now, they required too much
painstaking manual work for them to be used in preclinical medical testing.
"You take a starting cell, in our case, a stem cell, and multiply
it—the cells grow in a suitable plastic dish," explained Klein.
"Once the cells have grown sufficiently, you then detach them from the
plastic dish and 'animate' the cells to form small cellular aggregates. We do
this by placing a certain number of cells in an anti-adhesive dish. The cells
then float together and form embryoid bodies.
"These structures are then treated with various growth factors,
substances that are typically found in the lungs or during lung development. In
the presence of these substances, the cells transform into various cell types
that are found in the lungs."
The scientists put their embryoid bodies into a special tank with a
continuously stirring membrane, which contained a suitable medium for growing
the organoids. They also manually cultured a control set of organoids on a
conventional growth plate.
The organoids spent four weeks in the tank, and were then analyzed using
microscopy, immunofluorescence, immunohistochemistry, and RNA sequencing to see
how the organoids had developed, what cells had formed, and how comparable they
were to conventionally-grown organoids.
Analysis confirmed that both sets of organoids had developed the lung-like
structures representing airways and alveoli that scientists were looking for,
and RNA sequencing showed that they had developed characteristic epithelial and
mesodermal lung cells.
Both sets developed the same types of cells, although in slightly different
proportions—for instance, manually generated lung organoids contained more
alveolar cells. The organoids developed in the bioreactor seemed to be larger,
with fewer alveolar spheres.
Mini lungs to maximize research?
The fact that the bioreactor can produce more organoids at a time, with
less manual work, could be a gamechanger for lung disease research. However,
more testing will be needed to establish the best conditions for organoid
development, and the organoids themselves will need to be improved to mimic
real-life conditions within the body better.
"Organoids can't yet fully recapitulate the lung cellular
composition," said Klein. "Some cells are still missing from the 'big
picture,' such as infiltrating immune cells and blood vessels. But the
organoids themselves show very good bronchiolar and alveolar structures. We
obviously don't have blood flow, meaning the conditions are rather static.
"But for a patient-oriented screening platform, this may not be
necessary, if important insights into the cells' fate during a certain
treatment can be obtained. These systems may not yet be as complex as an entire
organism, but they are human-based—we have the cells that we also find in
patients."
"There is still a lot of room for optimization," added Klein. "We need robust and scalable protocols for large-scale organoid production. This requires careful consideration of the bioreactor design, the cell types to be used, and the conditions under which the organoids are cultivated. But we're working on it."
Provided by Frontiers
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