b2815 Tissue Engineering and Nanotheranostics “9.61x6.69”2 Tissue Engineering and Nanotheranosticsand it is hoped that regenerating or replacing the muscle tissue will
mitigate these negative outcomes. Of the many opportunities for
intervention, two classes are particularly prominent in the clinic. The
first of these is wasting disorders, which result in muscle loss on a
large scale throughout the body. The second is volumetric muscle loss
(VML), which can be the result of injury or surgery.
1.1. W asting Diseases and Disorders
There are several diseases and disorders that can cause muscular wast-
ing, including a class known as muscular dystrophy (MD). Duchenne’s
muscular dystrophy (DMD), for example, is caused by a defective
DMD gene, which encodes the protein dystrophin. Dystrophin is an
integral member of the dystrophin-associated protein complex, which
connects a myocyte’s actin cytoskeleton to the extracellular matrix
(ECM).^1 It is thought that this connection shields the sarcolemma
from excessive stress, especially during eccentric contraction.2,
In DMD, mutations result in a non-functional dystrophin protein,
which is unable to fulfill its mechanical role. This, in turn, is thought
to lead to higher sarcolemmal stresses, eventually resulting in elevated
intracellular Ca2+.^4 Although work is still underway to understand all
of the underlying processes, the end result on the organ level is myo-
cyte death, fat deposition, and fibrosis. Due to these changes to the
muscle tissue, patients with DMD experience pronounced muscle
weakness. The diagnosis is generally made at a young age as the chil-
dren are unable to keep up with their peers, and most of them are
confined to wheelchairs by the age of 10.5,6 Although treatment for
DMD patients is improving, many succumb to respiratory or cardiac
complications by the age of 20. DMD is recessive, and because the
DMD gene is located on the X chromosome, it affects men more
often than women. Female carriers can experience similar symptoms
to males in some cases.^7 In 2015, it was determined that the com-
bined prevalence of DMD and Becker’s muscular dystrophy (BMD)
(another prevalent dystrophy) among boys aged 5–9 was about 2 in
10,000.^8 Although DMD is the most common, there are many other
dystrophies. BMD is very similar to DMD, and results in partially
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