Clinical Trial Details
— Status: Enrolling by invitation
Administrative data
| NCT number |
NCT05521958 |
| Other study ID # |
152310 |
| Secondary ID |
|
| Status |
Enrolling by invitation |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
June 10, 2022 |
| Est. completion date |
June 2028 |
Study information
| Verified date |
November 2023 |
| Source |
University of Utah |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The purpose of this study is to evaluate both genotypic differences and differences in local
gene expression in individuals who develop acute traumatic compartment syndrome relative to
control patients with at-risk lower extremity fractures who do not develop compartment
syndrome.
Description:
Acute compartment syndrome is associated with infection, contractures, fracture non-union,
and chronic pain syndromes. The most common cause of acute compartment syndrome is fracture.
Individuals with compartment syndrome associated with a lower extremity fracture have
demonstrated worse patient reported outcome scores compared to individuals who suffer lower
extremity fractures alone.
The pathophysiology of compartment syndrome has been traditionally described as loss of
tissue perfusion and subsequent cellular anoxia related to supra-physiologic pressure within
a closed myofascial space. Both animal and clinical studies have suggested that compartment
syndrome develops when the intra-compartmental pressure approaches systemic diastolic blood
pressure. However, other studies have demonstrated that high absolute compartment pressures
and/or narrowed delta pressures have poor sensitivity for predicting compartment syndrome,
suggesting that the pathophysiology of compartment syndrome is likely more complex than the
currently accepted understanding of the disease process.
Animal models suggest that fracture promotes inflammation and exacerbates microvascular
dysfunction, which may act synergistically with elevated intra-compartmental pressures to
create clinical compartment syndrome. It is known that fracture causes microvascular damage
and inflammation in surrounding muscle tissue. Several models have demonstrated that the
microvascular environment in compartment syndrome is characterized by tenuous, intermittent
blood supply to the musculature, which displays asymmetric microvascular dysfunction in
response to elevated compartment pressures. Similarly, recent animal research has
demonstrated that elevated intra-compartmental pressure is associated with a pro-inflammatory
state, which directly contributes to skeletal muscle injury and may exacerbate microvascular
injury.
It is unknown whether individual genomic and/or transcriptomic variability is clinically
relevant with respect to response to fracture or the development of compartment syndrome.
However, there is evidence from the vascular surgery literature in both animal and human
models that individual variability in gene expression meaningfully affects skeletal muscle
response to acute ischemia. The investigators hypothesize that there may be an individual
pre-disposition to developing clinical compartment syndrome in the setting of at-risk
fractures which manifests itself in the cellular response to inflammation and low grade
ischemia. The overarching goal of this study is to characterize cellular level dysfunction in
human compartment syndrome and to determine whether there are unique gene expression profiles
associated with the development of clinical compartment syndrome. Specific aim 1 of this
study is to compare genetic and transcriptomic differences individuals with high-risk tibia
fractures who do not develop compartment syndrome and individuals with high-risk tibia
fractures who do develop clinical compartment syndrome. Specific aim 2 of this study is to to
compare genetic differences between acute compartment syndrome patients and chronic
exertional compartment syndrome patients.
