Permeability of the blood-brain barrier in mice
Date:
March 15, 2022
Source:
Harvard Medical School
Summary:
The blood-brain barrier plays an essential role in protecting the
central nervous system from harmful bacteria, toxins, and other
blood-borne pathogens.
FULL STORY ==========================================================================
The blood-brain barrier plays an essential role in protecting the central nervous system from harmful bacteria, toxins, and other blood-borne
pathogens.
========================================================================== Composed of a tight row of endothelial cells, the barrier is semipermeable
and highly selective. It allows small molecules and nutrients to pass from
the blood into the central nervous system, while blocking substances that
might cause infection, inflammation, and otherwise disrupt the system's delicate balance.
However, what exactly controls the permeability of the blood-brain barrier
is a question that has long bedeviled scientists -- and one that Chenghua
Gu, professor of neurobiology in the Blavatnik Institute at Harvard
Medical School and a Howard Hughes Medical Institute investigator,
has been studying for almost a decade.
Previously, Gu and her team at HMS established that a cellular trafficking system called transcytosis plays a key role in controlling blood-brain
barrier permeability by determining how easily molecules can be
transported across it.
Now, new research in mice has revealed more details about how this
process is regulated.
In this new research, published March 15 in Neuron, the scientists
describe a mechanism by which cells in the surrounding environment,
or microenvironment, signal to cells that make up the blood-brain
barrier. They found that this intercellular communication inhibits
transcytosis to keep the barrier less permeable and ensure that molecules cannot easily pass through.
"Our work opens the door to better understand how and why the
microenvironment is important for maintaining the blood-brain barrier,"
Gu said, which could inform the development of better laboratory models
to study the blood-brain barrier.
==========================================================================
Not only that, but the mechanism offers a potential avenue for
manipulating the barrier to make it more or less permeable, the authors
of the study said. If the findings are replicated in further animal
studies and then in humans, they could point to new ways of treating
diseases or delivering medicines into the brain.
Microenvironment matters Contrary to what its name might suggest, the blood-brain barrier is not simply a wall that physically blocks harmful molecules from crossing into the central nervous system. Rather, it
acts more like a self-regulating filtration system, and its permeability changes based on the properties of the endothelial cells it's made of.
In 2014 Gu and her team identified a gene called Mfsd2a, which suppresses transcytosis, the process by which molecules cross the blood-brain barrier
in bubbles called vesicles that are formed in endothelial cells. This suppression maintains the integrity of the barrier by ensuring that
molecules aren't transported across endothelial cells. Building on this
work, in 2017 Gu's teamrevealed that transcytosis may, indeed, be the
main mechanism that controls the permeability of the blood-brain barrier.
However, Gu and colleagues suspected there was more to the story. They
began to wonder how the permeability of the blood-brain barrier is
affected by the surrounding microenvironment, which is composed of cells
that are physically close to the blood vessels in the central nervous
system. More specifically, they became interested in adjacent neural
cells called pericytes that wrap around these blood vessels.
==========================================================================
"We started off asking what are the cells in the microenvironment that
could be conferring these barrier properties to endothelial cells. And
a lot of history and other work prompted us to look at pericytes,"
explained lead author Swathi Ayloo, who conducted the research as a postdoctoral fellow at HMS and is now a senior scientist at Sanofi.
The researchers began by sifting through RNA databases for genes highly expressed in pericytes of the retina and the brain. They identified
a gene in pericytes that makes a protein called vitronectin, found in
the microenvironment of the central nervous system. Then, they turned
to the retina to test the importance of vitronectin in maintaining the blood-brain barrier.
The retina is an ideal model system, Ayloo explained, because in the
first few days after a mouse is born, the blood-retinal barrier is still permeable on the outer edge of the retina, but impermeable in the middle, setting up an easy comparison.
As it turns out, vitronectin was present in the microenvironment near
the endothelial cells in the impermeable part of the barrier, but was
missing at the outer edge of the barrier where the endothelial cells
were permeable.
Furthermore, when the team knocked out the gene that produces vitronectin,
the barrier became leaky.
"That set the stage for us to say, OK, we know that vitronectin is
important for barrier permeability, but why is it functioning like this,
what is the mechanism," Ayloo said.
Through a series of genetic experiments in mice, the researchers
established that vitronectin binds to a receptor called integrin ?5 in endothelial cells to form a signaling pathway. This signaling pathway
inhibits transcytosis by telling endothelial cells in the blood-brain
barrier to maintain the tension of their membranes, which prevents the formation of vesicles that can transport molecules across the barrier.
"When we zoom out, it totally makes sense, because this mechanism is
basically controlling the biophysical properties of the membrane, and
that determines how easy or how difficult it is to form those vesicles,"
Gu said.
"The big punch line is that there is this very active ligand-receptor
signaling between pericytes and endothelial cells, and you need that
active interaction for the maintenance of the barrier," Ayloo added.
Completing the picture Gu describes the microenvironment, also known as
the extracellular matrix, as "a really mysterious thing" that is present
around all tissues yet is exceedingly difficult to study. For her, the
paper not only reveals a specific mechanism in the microenvironment
that controls permeability of the blood-brain barrier, but opens the
door for more research on cellular signaling in the extracellular matrix.
Moreover, the extracellular matrix is known to break down in
neurodegenerative diseases such as multiple sclerosis.
"That's one of the hallmark features of neurodegenerative diseases,
so I think we need to do more extracellular matrix research," Ayloo
said. She added that there are many protein-to-protein interactions
between the microenvironment and the blood-brain barrier that need to
be better understood, especially within the context of disease.
Understanding the microenvironment could also lead to better laboratory
models to study the blood-brain barrier. Right now, Gu explained, these
models typically include only endothelial cells, and don't incorporate
the microenvironment.
"You cannot just put endothelial cells together in an in vitro model
and claim that this is the blood-brain barrier," Gu said. "Billions
of dollars are being spent on inaccurate models." Once researchers
identify the full collection of proteins in the microenvironment that
influence the permeability of the blood-brain barrier, she added, "we can re-create those factors in a model to more accurately mimic the barrier."
If the findings are affirmed in further experiments and, eventually,
in humans, the specific interaction between vitronectin and integrin ?5
may offer a new molecular target for manipulating the permeability of
the blood-brain barrier.
Gu estimates that around 90 percent of retinal diseases are related
to barrier leakage, necessitating treatments that make the barrier
less permeable - - something that also appears to be true for certain neurodegenerative diseases. On the flip side, in some conditions, the
barrier needs to become temporarily more permeable so that medicines
can be delivered into the brain.
"By identifying this basic molecular mechanism, now maybe we can find
agonists that target this mechanism to tighten the barrier, and inhibitors
that target this mechanism to open it," Gu said.
Perhaps most importantly, the work highlights the fundamental role of
the microenvironment in controlling the permeability of the blood-brain
barrier and brings researchers another step closer to a complete
understanding of how the blood-brain barrier works.
The study was funded by a Mahoney Postdoctoral Fellowship, Fidelity
Biosciences Research Initiative, an Allen Distinguished Investigator
Award, the NIH (DP1NS092473 Pioneer Award; R01 HL153261; RF1 DA048786),
and the Howard Hughes Medical Institute.
Additional authors on the study include Christopher Gallego Lazo of HMS
and the Howard Hughes Medical Institute; Shenghuan Sun, formerly of HMS
and the Howard Hughes Medical Institute; and Wei Zhang and Bianxiao Cui
of Stanford University.
========================================================================== Story Source: Materials provided by Harvard_Medical_School. Original
written by Catherine Caruso. Note: Content may be edited for style
and length.
========================================================================== Journal Reference:
1. Swathi Ayloo, Christopher Gallego Lazo, Shenghuan Sun, Wei Zhang,
Bianxiao Cui, Chenghua Gu. Pericyte-to-endothelial cell signaling
via vitronectin-integrin regulates blood-CNS barrier. Neuron,
2022; DOI: 10.1016/j.neuron.2022.02.017 ==========================================================================
Link to news story:
https://www.sciencedaily.com/releases/2022/03/220315113020.htm
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