Cluff K, Miserlis D, Naganathan GK, Pipinos II, Koutakis P, Samal A, McComb RD, Subbiah J, Casale GP. Morphometric analysis of gastrocnemius muscle biopsies from patients with peripheral arterial disease: objective grading of muscle degeneration.
Background
Peripheral artery disease (PAD), which affects an estimated 27 million people in Europe and North America, is caused by atherosclerotic plaques that limit blood flow to the legs. Chronic,repeated ischemia in the lower leg muscles of PAD patients is associated with loss of normal myofiber morphology and myofiber degradation. In this study, we tested the hypothesis that myofiber morphometrics of PAD calf muscle are significantly different from normal calf muscle and correlate with reduced calf muscle strength and walking performance.
Methods
Gastrocnemius biopsies were collected from 154 PAD patients (Fontaine stage II) and 85 control subjects. Morphometric parameters of gastrocnemius fibers were determined and evaluated for associations with walking distances and calf muscle strength.
Results
Compared with control myofibers, PAD myofiber cross-sectional area, major and minor axes, equivalent diameter, perimeter, solidity, and density were significantly decreased (P < 0.005), whereas roundness was significantly increased (P < 0.005). Myofiber morphometric parameters correlated with walking distances and calf muscle strength. Multiple regression analyses demonstrated myofiber cross-sectional area, roundness, and solidity as the best predictors of calf muscle strength and 6-min walking distance, whereas cross-sectional area was the main predictor of maximum walking distance.
Conclusions
Myofiber morphometrics of PAD gastrocnemius differ significantly from those of control muscle and predict calf muscle strength and walking distances of the PAD patients. Morphometric parameters of gastrocnemius myofibers may serve as objective criteria for diagnosis, staging, and treatment of PAD.
Elevated intracranial fluid volume can drive intracranial pressure increases, which can potentially result in numerous neurological complications or death. This study’s focus was to develop a passive skin patch sensor for the head that would non-invasively measure cranial fluid volume shifts. The sensor consists of a single baseline component configured into a rectangular planar spiral with a self-resonant frequency response when impinged upon by external radio frequency sweeps. Fluid volume changes (10 mL increments) were detected through cranial bone using the sensor on a dry human skull model. Preliminary human tests utilized two sensors to determine feasibility of detecting fluid volume shifts in the complex environment of the human body. The correlation between fluid volume changes and shifts in the first resonance frequency using the dry human skull was classified as a second order polynomial with R2 = 0.97. During preliminary and secondary human tests, a ≈24 MHz and an average of ≈45.07 MHz shifts in the principal resonant frequency were measured respectively, corresponding to the induced cephalad bio-fluid shifts. This electromagnetic resonant sensor may provide a non-invasive method to monitor shifts in fluid volume and assist with medical scenarios including stroke, cerebral hemorrhage, concussion, or monitoring intracranial pressure.
The open-circuit resonant sensor design leverages the architecture of a thin planar spiral which is passive (does not require batteries), robust and lightweight (does not have electrical components or electrical connections), and may be able to wirelessly monitor cardiovascular health and limb hemodynamics.
The
interconnected porous structures that mimic the extracellular
matrix support cell growth in tissue engineering. Nanofibers generated
by electrospinning can act as a vehicle for therapeutic cell delivery
to a neural lesion. The incorporation of carbon nanomaterials with
excellent electrical conductivity in nanofibers is an attractive aspect
for design of a nanodevice for neural tissue regeneration. In this
study, nanoscaffolds were created by electrospinning poly(ε-caprolactone)
(PCL) and three different types of carbon nanomaterials, which are
carbon nanotubes, graphene, and fullerene. The component of carbon
nanomaterials in nanofibers was confirmed by Fourier transform infrared
spectroscopy. The fiber diameter was determined by scanning electron
microscopy, and it was found that the diameter varied depending on
the type of nanomaterial in the fibers. The incorporation of carbon
nanotubes and graphene in the PCL fibers increased the contact angle
significantly, while the incorporation of fullerene reduced the contact
angle significantly. Incorporation of CNT, fullerene, and graphene
in the PCL fibers increased dielectric constant. Astrocytes isolated
from neonatal rats were cultured on PCL-nanomaterial nanofibers. The
cell viability assay showed that the PCL-nanomaterial nanofibers were
not toxic to the cultured astrocytes. The immunolabeling showed the
growth and morphology of astrocytes on nanofiber scaffolds. SEM was
performed to determine the cell attachment and interaction with the
nanoscaffolds. This study indicates that PCL nanofibers containing
nanomaterials are biocompatible and could be used for cell and drug
delivery into the nervous system.
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