Delayed wound healing is a Type 2 diabetes mellitus (DM) complication caused by hyperglycemia, systemic inflammation, and decreased blood microcirculation. Skeletal muscles are also affected by hyperglycemia, resulting in reduced blood flow and glucose uptake. Low Magnitude High Frequency Vibration (LMHFV) has been proven to be beneficial to muscle contractility and blood microcirculation. We hypothesized that LMHFV could accelerate the wound healing of n5-streptozotocin (n5-STZ)-induced DM rats by enhancing muscle activity and blood microcirculation. This study investigated the effects of LMHFV in an open foot wound created on the footpad of n5-STZ-induced DM rats (DM_V), compared with no-treatment DM (DM), non-DM vibration (Ctrl_V) and non-DM control rats (Ctrl) on Days 1, 4, 8 and 13. Results showed that the foot wounds of DM_V and Ctrl_V rats were significantly reduced in size compared to DM and Ctrl rats, respectively, at Day 13. The blood glucose level of DM_V rats was significantly reduced, while the glucose transporter 4 (GLUT4) expression and blood microcirculation of DM_V rats were significantly enhanced in comparison to those of DM rats. In conclusion, LMHFV can accelerate the foot wound healing process of n5-STZ rats.
Delayed foot wound healing is a major complication attributed to hyperglycemia in type 2
diabetes mellitus (DM) patients, and these wounds may develop into foot ulcers. There are
at least two types of DM wound models used in rodents to study delayed wound healing.
However, clinically relevant animal models are not common. Most models use type 1 DM
rodents or wounds created on the back rather than on the foot. An open full-thickness
excision wound on the footpad of type 2 DM rats is more clinically relevant, but such a
model has not yet been characterized systematically. The objective of this study was to
investigate and characterize how DM affected a full-thickness excision open foot wound in
n5-streptozotocin (n5-STZ)-induced type 2 DM rats. We hypothesized that elevated
inflammation, reduced blood circulation, and cell proliferation due to hyperglycemia could
delay the wound healing of DM rats. The wounds of DM rats were compared with those of
non-DM rats (Ctrl) at Days 1 and 8 post wounding. The wound healing process of the DM rats
was significantly delayed compared with that of the Ctrl rats. The DM rats also had higher
C-reactive protein (CRP) and lower blood circulation and proliferating cell nuclear
antigen (PCNA) in DM wounds. This confirmed that elevated inflammation and reduced blood
flow and cell proliferation delayed foot wound healing in the n5-STZ rats. Hence, this
open foot wound animal model provides a good approach to study the process of delayed
wound healing.
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