Muscle wastage
is a core killer of the elderly and this is not observed in any other species
who typically sustain muscle integrity to almost the end. Thus an outright remedy is very desirous and
will lead to substantially more people surviving to the century mark.
The good news is
that we may have a simple and safe fix for this where the body gets to do what
it was supposed to do. This continues to
be independent of actual life extension research as that is a different problem. This is the problem we should not have
anyway.
This also
eliminates natural bone deterioration as well.
That has always been about healthy muscles stimulating bone growth and
renewal.
A New Approach
to Myostatin-Related Muscle Growth
Blocking myostatin has been
shown to boost muscle growth and regeneration in various species. There are
even a few natural human myostatin mutants, but that is a rare genetic occurrence. For some
years now researchers have been investigating means to manipulate myostatin levels
and related signaling as a therapy for age-related loss of muscle mass and
strength, as well as for various other medical conditions in which wasting of
muscles plays a role. This, like many forms of modern medical research, aims to
produce a form of compensatory change, potentially beneficial but in no way
addressing root causes to prevent progression of the underlying condition.
Researchers here have moved on past myostatin and
further down the chain of signals and molecular mechanisms to find a novel
place to intervene in order to boost muscle growth in mice and humans. So far
results are promising: if this treatment turns out to produce few to no
side-effects, it is the sort of thing that everyone could benefit from. That
said, again, it doesn't address root causes of degenerative muscle loss with
aging - something that needs to be accomplished in order to reliably and most effectively extend
healthy life.
Quote:
The new compound (BYM338) acts to prevent muscle
wasting by blocking a receptor that
engages a cellular signaling system that exists to put the brakes on muscle
development when appropriate. But sometimes those brakes are activated
inappropriately, or are stuck on.
A variety of signals can activate the receptor.
Prior to development of BYM338, compounds developed to block these molecules
were blunt instruments, either trapping all incoming signals (which stimulated
muscle growth but also caused harmful side effects) or blocking just a single
receptor activator (providing only tepid growth stimulation.) BYM338 was
designed to be in the Goldilocks zone (just right.)
In the study the compound boosted muscle mass 25 to
50 percent and increased strength in animal models. Those gains were
significantly superior to those of compounds that blocked a single receptor
activator. Clinical trials are currently underway. Preliminary data on the
antibody was promising enough to have it designated a breakthrough therapy by
the US Food and Drug Administration for sporadic inclusion body myositis, a rare muscle wasting disease with no approved
therapies.
Here is a link to the paper - the PDF format full version is also presently available if you'd like to
wade in to the details.
Quote:
The myostatin/Activin type II
receptor (ActRII) pathway has been identified as critical in
regulating skeletal muscle size. Several other ligands, including GDF11 and the Activins, signal through this
pathway, suggesting that the ActRII receptors are major regulatory nodes in the
regulation of muscle mass.
We have developed a novel, human anti-ActRII antibody ("Bimagrumab", aka BYM338) to
prevent binding of ligands to the receptors, and thus inhibit downstream
signaling. BYM338 enhances differentiation of primary human skeletal myoblasts, and counteracts the inhibition of differentiationinduced
by myostatin or Activin A.
BYM338 dramatically increases skeletal muscle mass
in mice, beyond sole inhibition of myostatin as detected by comparing the
antibody with a myostatin inhibitor. A mouse version of the antibody induces
enhanced muscle hypertrophy in myostatin-mutant mice, further confirming a
beneficial effect on muscle growth through blockade of ActRII ligands beyond
myostatin inhibition alone.
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