Johns Hopkins. US: A Roman philosopher was the first to note the relationship between a
sound mind and a sound body. Now the findings of a new Johns Hopkins
study reveal a possible biochemical explanation behind this ancient
observation.
The research, published ahead of print Jan. 12 in the Proceedings of the National Academy of Sciences,
reveals that a protein already known to act as a natural
antidepressant, enhance learning and memory, power nerve cell growth,
and nourish blood vessels is also a central player in maintaining heart
muscle vitality.
The team’s experiments, conducted in mice and lab-grown heart cells,
show this multi-tasking protein, a nerve-growth factor called BDNF
(brain-derived neurotrophic factor), helps sustain the ability of heart
muscle cells to contract and relax properly. The results reveal that
either BDNF deficiency or cell insensitivity to BDNF’s presence can
precipitate heart muscle dysfunction, particularly under conditions of
chronic or repeated physical stress on the heart, such as endurance
training or high blood pressure. Specifically, the researchers tracked
BDNF’s role in a cascade of molecular signaling events in heart cells,
the disruption of which led to heart muscle failure.
If confirmed in humans, the research team says, the findings could pave
the way to new treatments for certain forms of heart failure, a
disorder that affects nearly 6 million Americans and more than 23
million people worldwide.
In addition, because of BDNF’s well-known antidepressant effects and
its role as a booster of nerve cell health, the research teams says the
results suggest a possible biochemical link between depression and heart
disease, two disorders that tend to occur in concert but whose
relationship remains poorly understood.
“Our results are not only a vivid reminder of the astounding complexity
of the heart’s chemistry and physiology, but also a striking example of
the ability of a single protein to act on multiple fronts and affect
many organs and functions,” says lead investigator Ning Feng, M.D., Ph.D., a cardiology fellow at the Johns Hopkins University School of Medicine.
The findings also can help clarify the biological means behind recent –
and unexplained –observations that heart failure patients whose cardiac
function worsens during physical exertion have low levels of BDNF in
the blood.
“Our observation that BDNF directly controls the ability of heart
muscle cells to ‘beat’ properly offers one possible explanation behind
the declining cardiac function seen in people with heart failure,
especially during exercise,” says senior author Nazareno Paolocci, M.D., Ph.D., assistant professor of medicine at the Johns Hopkins University School of Medicine.
In an initial set of experiments, the scientists isolated cardiac cells
from rodents with either normal or failing hearts in a lab dish and
exposed the cells to BDNF. The normal heart cells responded by
contracting and relaxing vigorously in the presence of BDNF, a
phenomenon marked by peaks of contraction-triggering calcium flow into
the cells. However, cells obtained from failing hearts, even when awash
in BDNF, responded weakly or not at all. To determine why, the
team homed in on BDNF’s receptor, a molecule called TrkB, located on the
surface of cells and responsible for receiving BDNF’s chemical signals
and transmitting them inside the cell. Compared with cardiac cells from
mice with normal hearts, the failing heart cells had a slightly
different version of the TrkB receptor, one that produces less of a
catalyst protein responsible for triggering critical signaling inside
the cardiac cell. This slightly sub-performing version of the receptor
was less responsive to BDNF, rendering the heart cell less sensitive to
it. While this TrkB variant is fairly common and does not necessarily
portend disease, it may render the heart cells of those who carry the
altered version less capable of using BDNF, the researchers say. Mice
engineered to lack TrkB receptors in their heart cells developed
impaired cardiac function. Their hearts contracted poorly, pumped blood
less efficiently and took longer to relax after each beat.
“Taken together, these findings show that any abnormality in the way
BDNF communicates with its receptor appears to unlock a cascade of
chemical glitches that eventually leads to poor cardiac function,” Feng
says.
The investigators say that disruptions in proper BDNF-TrkB signaling can even explain what drives chemotherapy-induced heart failure, a serious and well-established side effect of certain cancer treatments. Such treatments include chemicals that block multiple growth-factor receptors, TrkB among them, to halt tumor growth. And while this approach is critical to stave off cancer progression, it can also inadvertently lead to heart failure by interfering with the ability of cardiac cells to respond to the BDNF circulating in the body.
The investigators say that disruptions in proper BDNF-TrkB signaling can even explain what drives chemotherapy-induced heart failure, a serious and well-established side effect of certain cancer treatments. Such treatments include chemicals that block multiple growth-factor receptors, TrkB among them, to halt tumor growth. And while this approach is critical to stave off cancer progression, it can also inadvertently lead to heart failure by interfering with the ability of cardiac cells to respond to the BDNF circulating in the body.
Another important finding, the researchers say, is that mice with
missing BDNF receptors remained sensitive to adrenaline, the
neurotransmitter released during fight-or-flight situations to infuse
the heart with extra energy needed for peak cardiac performance during
bouts of intense physical or emotional activity. The finding, the
scientists say, means that BDNF affects cardiac function independently
and separately from adrenaline by providing continuous, low-level fuel
for heart contraction under normal conditions or prolonged periods of
slightly elevated cardiac output, such as endurance training.
“Just like a constant low flame can keep a pot on slow simmer, constant
levels of BDNF seem to maintain heart muscle vitality,” Paolocci says.
The researchers point out that low levels of BDNF by themselves may not
be enough to cause immediate heart disease, but chronic BDNF deficiency
or insensitivity, compounded by additional physiologic or pathologic
stressors, is a main culprit in fueling the disease.
“In the absence of chronic stressors, such as hypertension or an
elevated workload of the heart muscle, BDNF deficiency may not cause
full-blown disease, but it could be the proverbial straw that leads to a
‘broken heart,’” Paolocci says.
The research was funded in part by the American Heart Association under
grant number GRNT17070027 and by the National Institutes of Health
under grant number T32HL-0227, with additional funding support from the
Magic That Matters Fund of the Division of Cardiology at Johns Hopkins.
Other investigators involved in the research included Sabine Huke,
Guangshuo Zhu, Carlo Tocchetti, Sa Shi, Takeshi Aiba, Nina Kaludercic,
Donald Hoover, Sarah Beck, Joseph Mankowski, Gordon Tomaselli, Donald
Bers and David Kass.