Introduction

Recent data indicates that musculoskeletal complaints comprise 15% of all emergency department encounters [1]. A small, but potentially urgent percentage of these cases may involve myositis. Myositis is a broad term used to describe inflammation of muscle tissue but has many etiologies. In its chronic form, myositis is associated with connective tissue or autoimmune inflammatory cascades, primarily managed by rheumatologists. Our focus is on the more acute manifestations of myositis that might present to an emergency department, urgent care center, or as a complication of a newly admitted inpatient. Specifically, we look at the spectrum of MRI findings and the role MRI has in the diagnosis, management, and treatment of myositis and other urgent muscle-related disorders. With the increased utilization of MRI, on-call radiologists may need to interpret these cases without the benefit of fellowship-trained musculoskeletal imaging expertise.

MR imaging of myositis

Currently, MR myositis protocols are characteristically brief, using a fluid-sensitive sequence such as short TI inversion recovery (STIR) or proton density with fat saturation in the axial and coronal planes as well as an axial T1 sequence. The brevity of the protocol reflects the inherent sensitivity of MR in the detection of abnormal muscle signal over specificity. The use of composed MR post-processing technique helps to seamlessly link upper and lower components of the arms or legs. Occasionally, paraspinal muscles and shoulders are imaged when clinically indicated.

In general, MRI has been criticized for long scan times, difficulty of access, and lack of specificity. However, with the ever-increasing accessibility, more efficient image acquisition, and the clinical use of techniques formerly reserved for research or less acute entities, emergent MRI could be useful in the diagnosis of myositis and even cases complicated by acute compartment syndrome (ACS). The inconsistent performance of intracompartmental pressure measurements has spawned research into the biochemical markers of impending irreversible muscle ischemia. Pyruvate and phosphocreatine levels have been shown to decrease in the setting of muscle glycolysis (anaerobic respiration). Conversely, lactate concentration has been shown to increase, leading to decreased tissue pH [2]. Efforts are in progress to measure muscle compartment pH by using an indwelling catheter or needle; however, P31 magnetic resonance spectroscopy (MRS) has proven to accurately measure intracellular pH in a noninvasive manner [3, 4]. MRS uses the relative chemical shift of inorganic phosphate (Pi) and phosphocreatine (PCr) to calculate pH using the Henderson-Hasselbalch equation. Sedivy et al. reported a scan time of 4 min using a 3T system [4]. Another emerging technology is MR elastography (MRE). MRE “measures tissue stiffness by encoding displacements due to the propagation of externally induced acoustic waves into the MR phase signal” [5]. The inherent tissue stiffness affects the speed of the wave propagation, with stiffer tissue inducing faster wave speed. It remains to be seen whether the muscle compartment tension associated with myositis and ACS coincides with measurable tissue stiffness afforded by MRE. Ultimately, one could conceive of an abbreviated ACS protocol that uses isotopic 3D volume acquisition combined with P31-MRS and MRE to yield anatomic and biochemical information. Such an endeavor would require specialized software, a streamlined patient selection protocol, and close coordination between the radiologist and technologist; however, with the proper equipment, the idea is imaginable. Incorporating an artificial intelligence automation tool could assist with data processing in order to optimize the turn-around time for these cases. Potentially, cases of suspected but clinically equivocal ACS may benefit from this type of MRI imaging in the future.

Anatomy

A thorough understanding of compartmental anatomy is necessary to adequately describe MR imaging findings of myositis and its complications. Accurate localization of the abnormalities can help clinicians understand the extent of disease and whether the process is affecting adjacent structures such as bone, joint space, bursa, tendons, and neurovascular bundles. The compartments are space-limited areas, confined by the deep and intermuscular fascia.

Upper extremity

The upper extremity anatomy can be divided into the arm and the forearm (Table 1). The muscle compartments of the arm are separated into anterior and posterior compartments by the medial and lateral intermuscular septa, which are fascia thickenings that extend from the humerus to the deep fascia (Fig. 1a). The long and short heads of the biceps make up the superficial muscles of the anterior compartment, while the coracobrachialis and brachialis make up the deeper muscles of the compartment. The three heads of the triceps muscle (long, lateral, and medial) occupy the posterior compartment in toto. The deltoid muscle is not included in the arm compartment schema [6].

Table 1 Anatomy (upper and lower extremities)
Fig. 1
figure 1

Images of anatomic compartments

The description of the forearm is more variable with two, three, and four compartments cited in the literature [7]. In the four compartment classification, there are dorsal, mobile wad of Henry, volar superficial, and volar deep compartments. Anatomically, the forearm compartments are often incompletely separated, and for the purpose of this discussion, can be thought of as either dorsal or volar (Table 1). These two compartments are separated by the radius, ulna, and the intraosseous membrane which spans these bones (Fig. 1b). Due to the porous nature of the forearm compartments, often a single fasciotomy will suffice, releasing tension in the remaining compartments [6].

Lower extremity

The lower extremity anatomy can be divided into the thigh and the lower leg (Table 1). The thigh has three anatomic compartments: anterior, medial, and posterior. The fascia lata defines the circumferential superficial border investing all three compartments. The anterior compartment is separated from the medial and posterior compartments by fascial thickenings called the medial and lateral intermuscular septa that extend from either side of the femur to the fascia lata [8]. The medial compartment is separated from the posterior compartment by a thin fascial plane called the posterior intermuscular septum (Fig. 1c). The gluteus maximus is not included in the thigh compartment schema [9].

The lower leg is comprised of four anatomic compartments: anterior, lateral, superficial posterior, and deep posterior (Table 1). The deep crural fascia defines the circumferential superficial border investing all four compartments, and it fuses with the anterior periosteum of the tibia. The lateral compartment is separated from the anterior and posterior compartments by the anterior and posterior intermuscular septa, respectively. The posterior compartment is divided by the posterior intermuscular fascia into deep and superficial compartments (Fig. 1d). The interosseous membrane bridges the tibia and fibula, separating the anterior and deep posterior compartments [8].

Etiologies and entities

Infectious myositis

Infectious myositis is a type of urgent myositis that can present to the emergency department and can be bacterial or viral. Bacterial pyomyositis typically emanates from hematogenous bacteremia, with patients exhibiting three stages (Table 2). Patients in stage 1 present with localized pain, low-grade pyrexia, and malaise, but purulence is not present. Stage 2 of the disease presents with overt signs of local and systemic infection and usually follows stage 1 by 10 to 21 days. Severe muscle pain, swelling, and skin erythema can be present at this stage. Inflammatory markers and white blood cells become elevated. Frank pus and intramuscular abscesses can be present in stage 2. Stage 3 patients exhibit signs and symptoms of sepsis and complications that may involve other organ systems, including renal failure. Staphylococcus aureus is the most commonly isolated organism in pyomyositis [10, 11].

Table 2 Etiologies, entities, and special features

MRI is the imaging modality of choice for suspected pyomyositis. MRI has inherent qualities that allow us to differentiate tissue properties with marked sensitivity. Combined with intravenous contrast, MRI is excellent at distinguishing the rim-enhancing fluid collections that mark the transition from a phlegmonous stage 1 to a purulent stage 2. In stage 1 pyomyositis, one can expect muscle enlargement with loss of definition and heterogenous increased T2-weighted signal abnormalities (Fig. 2). T1-weighted sequences are usually isointense to slightly hyperintense depending on the proteinaceous nature of the fluid. In the late stage 2, T2-weighted images reveal hyperintensity with corresponding hypointense T1 signal. At this stage, post-contrast T1-weighted images with fat saturation may depict rounded or irregularly shaped rim-enhancing fluid collections that are typical of abscesses. MRI helps to identify percutaneously drainable fluid collections and surgical planning if necessary. Up to 40% of pyomyositis cases involve multiple muscle groups [10, 11].

Fig. 2
figure 2

a Stage 2, pyomyositis in a 36-year-old immunosuppressed patient with an irregularly shaped, multiloculated, peripherally enhancing abscess within the posterior compartment of the proximal thigh on this T1 fat-saturated post-contrast image (arrows). Note the enhancement of the surrounding musculature consistent with infectious myositis (star). Axial proton density with fat saturation at the same level b reveals an abnormal area of increased signal intensity that corresponds to the abscess; however, is less well defined (arrows). Increased signal is also noted in the adjacent muscle (star)

Necrotizing fasciitis is an infection that can occur concomitantly with pyomyositis or as a distinct entity. The imaging hallmarks of this type of infection are the result of fascial inflammation and necrosis that leads to fascial thickening, interfascial fluid, and perifascial hyperemic changes, often in multiple compartments [12]. Thickening of the deep and intermuscular fascia greater than 3 mm is associated with 86% of necrotizing fasciitis when compared to non-necrotizing fasciitis [12]. The accumulation of fluid along the fascial planes results in hyperintense T2 signal and hypointense T1 signal. Enhancement is variable, likely due to the disruption of capillary networks traversing the deep fascial planes [12]. Crepitus is the physical sign representing subcutaneous emphysema tracking along fascial planes. This gas is readily identified using conventional radiographs and CT; however, only a minority of cases involves gas-forming organisms. Gradient-echo sequences can help to identity gas on MRI scans. While MRI can yield exquisite tissue contrast and could be useful to map the extent of the disease to aid surgical planning, treatment should not be delayed in lieu of imaging in severely toxic patients [13].

Viral infections are commonly associated with myositis which can range from mild myalgias to rhabdomyolysis, leading to renal failure and cardiac arrhythmias [14]. Multiple viruses have been implicated in myositis and myositis-induced rhabdomyolysis including influenza A/B; parainfluenza; coxsackie; hepatitis A, B, C, and E; and HIV [14,15,16]. Toscana, Dengue, and West Nile viruses have also been documented causes of viral-related myositis [17]. Recently, Beydon et al. presented an MRI documented case of SARS-CoV-2-related myositis of the external obturator and vastus lateralis muscles [18]. The mechanism of viral-related myositis is unclear; however, direct viral invasion, viral-mediated myotoxic cytokines, and viral-induced autoimmune reaction have all been posited [14] (Fig. 3).

Fig. 3
figure 3

Viral myositis (HIV) 48-year-old. Axial STIR images through the mid-thighs reveals heterogeneous hyperintense signal affecting all compartments

The MRI appearance of viral-related myositis varies by extent and distribution; however, streaky or patchy infiltration of muscle by abnormally high T2-weighted signal is a common theme. Heterogeneous or diffuse enhancement of muscle lesions is often seen [17, 18].

Rhabdomyolysis

Rhabdomyolysis can occur as a complication of myositis resulting from a myriad of viral, exertional, toxic, and crush etiologies. Sarcolemma membrane disruption causes myoglobin, potassium, phosphate, creatine kinase (CK), and urate to leak into the systemic circulation [19]. Myoglobin exhibits direct toxic effects that are detrimental to renal blood flow, leading to renal ischemia, and the production of myoglobin casts that cause proximal tubular necrosis [14]. Between 4 and 40% of rhabdomyolysis patients experience acute renal failure [14]. Severe cases exhibit the clinical triad of muscle pain, weakness, and dark-colored urine. Laboratory findings usually include elevated creatine phosphokinase, transaminases, BUN (blood urea nitrogen), creatinine, as well as hyperuricemia and hyperkalemia. Hypocalcemia and hypophosphatemia have also been reported. Compartment syndrome as a complication of rhabdomyolysis can arise due to muscle swelling, compressing nervous and vascular structures within the compartment [19].

Imaging of rhabdomyolysis by MRI is more sensitive than CT or ultrasound, allowing greater detail of the distribution and extent of affected muscles [19] (Fig. 4). Two types of MR imaging findings were described by Lu et al. [20]. Type 1 revealed homogeneously isointense to hyperintense T1-weighted signal, homogenously high T2 and short tau inversion recovery sequences (STIR), and homogenous enhancement after IV contrast administration. Type 1 rhabdomyolysis is associated with overexertion from exercise [20]. While the upper and lower extremities are often involved, axial compartments of the trunk, including the paraspinal, deltoid, abdominal, and gluteal muscle groups, have been reported [21,22,23].

Fig. 4
figure 4

ODCS with type 2, rhabdomyolysis in a 34-year-old. Coronal proton density fat saturation image (a) reveals patchy, heterogeneously hyperintense images of the right hip musculature after being “found down” due to OxyContin overdose. Note the bulging piriformis (star), gluteus minimus (diamond), and gluteus medius (arrowhead) muscles and fluid tracking along the proximal iliotibial band. Coronal T1 image (b) of the same patient

In type 2 rhabdomyolysis, either homogeneous or heterogenous isointense to hyperintense signal on T1 imaging, heterogenous hyperintensity on T2 or STIR sequences, and rim-enhancement daubed the “stipple sign” is seen on post contrast T1-weighted sequences. The rim-enhancing foci represent areas of myonecrosis [20]. The MR findings of type 2 rhabdomyolysis are found in patients with overdose compartment syndrome (ODCS), blunt trauma, vascular occlusion, and carbon monoxide poisoning [24]. Intramuscular hemorrhage can be seen as hyperintense T1-weighted signal abnormalities and signal void or blooming artifacts on gradient-echo sequences [24] (Fig. 4).

Drug-induced and immune-mediated necrotizing myositis

Drug-induced myositis may also be encountered in the emergent or urgent setting. Drugs of abuse, namely, alcohol, cocaine, opiate, phencyclidine, and some wild mushrooms, have been documented causes of myositis [15, 25]. Synthetic cannabinoid-induced myositis leading to rhabdomyolysis has been reported [26] (Fig. 5).

Fig. 5
figure 5

Rhabdomyolysis in a 23-year-old patient who presented to the emergency department 1 week after smoking synthetic cannabinoids with a creatine kinase of 203,700. Axial proton density fat-saturated image reveals selective but symmetric bilateral hyperintensity of all compartments with relative sparing of the adductor longus muscles (star) and vastus intermedius muscles (arrowhead) groups

Even more commonly, prescribed drugs have been implicated in causing myositis and ultimately muscle necrosis such as gabapentin [27], empagliflozin [28], statins, fibrates, cyclosporine, tacrolimus, propofol, labetalol, telbivudine, antipsychotics, voriconazole, entecavir, zidovudine, colchicine, selective serotonin reuptake inhibitors, and lithium, among others [15]. Typically, the myalgias associated with these drugs are self-limiting, resolving when the drug is ceased. However, an increasingly recognized type of inflammatory myopathy is immune-mediated necrotizing myopathy (IMNM). IMNM is a novel subset of the family of inflammatory myopathies of which polymyositis, dermatomyositis, and inclusion body myositis are most well-known. In distinction to the other drug-induced causes of myositis, IMNM is difficult to treat because the drug, most commonly a statin, produces anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase antibodies (anti-HMGCR) or anti-signal recognition particle (SRP) that continue to circulate long after the discontinuation of the offending agent [29]. Unlike, other inflammatory myopathies such as dermatomyositis, polymyositis, and inclusion body myositis which are the product of T cell-mediated attack of the muscle fibers, IMNM is an antibody-mediated response to the muscle fibers characterized by the presence of macrophages. These antibodies can be detected by immunoassays, obviating the need for muscle biopsy [30].

Patients can present to the emergency department with extreme fatigue, muscle soreness, and extremity weakness. Laboratory findings include markedly elevated CK and transaminase levels. The addition of myoglobinuria suggests progression to rhabdomyolysis. Of note, in contradistinction to non-inflammatory myopathies, IMNM patients CK levels fail to improve despite aggressive hydration. Long-term, aggressive, immunosuppressive therapies are the current treatment, and several months of therapy may be required before CK levels normalize [30]. MRI examination may reveal diffusely hyperintense T2-weighted signal within affected muscle groups, consistent with muscle edema of myositis [30]. Additional findings include muscle atrophy and fatty replacement which is more severe in patients with anti-SRP antibodies [29]. Elessawy et al. utilized whole-body MRI for a variety of chronic myositis. He used coronal STIR and T1 sequences with a total scan time ranging from 15 to 20 min [31]. Using a whole-body technique allowed for the detection of bilateral and early asymptomatic myositis muscles groups.

Diabetic myonecrosis

Diabetic myonecrosis (DMN), also called diabetic muscle infarcts, is a sequela seen in patients that have longstanding, suboptimal glycemic control [32]. Characterized by acute onset pain with or without a focal mass and reduced range of mobility, these patients may have a low-grade fever and a mildly elevated CK; however, leukocytosis is usually absent. Chronic diabetic renal disease seems to be the common factor, predicting incidence and recurrence of DMN [32]. Other stigmata of uncontrolled diabetes are often present such as neuropathy and retinopathy. Jelinek et al. studied 21 patients and found that the thigh was most commonly affected site (81%), followed by the calf (19%). Up to 38% of these patients had bilateral infarcts, 62% had multicompartmental involvement, and 86% had more than three muscles involved. Combined thigh and calf involvement were present in 10% of patients [33].

MRI is the study of choice for imaging DMN because it clearly identifies the location, number, and extent of disease involvement. Muscle swelling, exhibiting isointense T1-weighted signal and hyperintense T2-weighted/inversion-recovery signal are the usual imaging characteristics (Fig. 6). Subfascial and subcutaneous edema may be present [33]. Diffuse enhancement on gadolinium-enhanced T1-weighted imaging typically corresponds to the hyperintense T2-weighted signal abnormalities; however, 29% of the patients studied by Jelinek et al. exhibited small rim-enhancing foci with low central T1-weighted signal. These rim-enhancing components represent muscle infarction and necrosis. Fourteen percent of patients had small foci of both hyperintensity T1-weighted and T2-weighted signal abnormalities corresponding with post-infarct hemorrhage [33].

Fig. 6
figure 6

Diabetic myonecrosis in a 48-year-old patient who presented to the emergency department with acute calf pain and a long history of uncontrolled diabetes, including nephropathy and retinopathy. Sagittal STIR image (a) reveals heterogeneous, hyperintense signal within the superficial posterior compartment (arrow). Axial PD fat saturation images through the calf (b) reveals heterogenous hyperintense T2-weighted signal throughout the lateral gastrocnemius muscle (arrows). Axial T1 image (c) notes isointense effacement of intermuscular fat within the lateral gastrocnemius relative to the surrounding musculature (arrowhead)

While highly sensitive, the specificity of MRI is limited by an extensive differential diagnosis, including soft tissue abscess, pyomyositis, necrotizing fasciitis, inflammatory myositis, and primary muscle lymphoma. Therefore, DMN remains a clinical and imaging diagnosis [33]. A clinical history of uncontrolled, insulin-dependent, complicated diabetes with sudden onset thigh and/or calf pain without overt signs of infection should raise the suspicion of DMN. These findings, in addition to bilateral or simultaneously discontinuous sites of disease on MRI imaging, can lead one to the diagnosis of DMN. In contradistinction to DMN, necrotizing fasciitis is more likely to have fever, cellulitis, and leukocytosis [33]. Occasionally, histopathologic diagnosis via a percutaneous biopsy is required for cases of diagnostic dilemma.

Paraneoplastic myositis and polymyositis

While a rare disease, with an incidence of approximately 1/100,000, adult-onset dermatomyositis is associated with a concomitant malignancy in 15–30% [34]. Paraneoplastic polymyositis may herald a yet undiagnosed malignancy or coincide with a tumor diagnosis. Occasionally, paraneoplastic dermatomyositis or polymyositis patients can present to the emergency department or urgent care center experiencing proximal muscle weakness, myalgias, and elevated muscle enzymes. Croce et al. report a case of severe paraneoplastic polymyositis in a 38-year-old patient who presented with myalgias and proximal muscle weakness and ultimately was diagnosed with a breast mass [35]. Min et al. reported a similar clinical scenario of 45-year-old patient presenting to an emergency department who exhibited significantly elevated muscle enzymes and myoglobin. Min et al.’s patient was discovered to have a serous ovarian carcinoma that caused a rapidly progressing paraneoplastic necrotizing myopathy [36]. Given the rarity of paraneoplastic polymyositis, MRI imaging of such cases are sparse; however, the clinical expression of paraneoplastic polymyositis does not differ from polymyositis without cancer [35]. One could presume that the MRI appearance would be similar to that of non-paraneoplastic myositis or rhabdomyolysis depending on the severity of the disease (Figs. 7, 8, and 9).

Fig. 7
figure 7

Polymyositis. Axial T1-weighted image (a) through the mid-thigh reveals mildly increased but isointense bilateral muscle swelling. Axial proton density fat-saturated image (b) through the same level reveals patchy hyperintense signal within all compartments with relatively sparing of some posterior and medial compartment muscles

Fig. 8
figure 8

Dermatomyositis in 59-year-old. Axial STIR image of the lower pelvis reveals patient with diffusely increased hyperintensity of the obturator internus (circle) and obturator externus muscles (arrowhead) due to chronic, steroid-resistant dermatomyositis. Patient succumbed to respiratory failure within 1 month of this image

Fig. 9
figure 9

A 59-year-old with rheumatoid arthritis and polymyositis. Axial STIR image of the left mid-thigh reveals patchy hyperintense involvement of all three compartments with some muscle sparing in the medial and posterior compartments. Note relative atrophy of the hyperintense muscles

Muscle compartment syndromes

Acute compartment syndrome

While some cases of myositis can develop into acute compartment syndrome (ACS), the most common cause of ACS are tibial diaphyseal fractures due to blunt, crush, or penetrating trauma. The anterior compartment of the lower leg is the most commonly involved compartment [37]. The classic physical signs and symptoms of compartment syndrome are pain with passive stretching, increased pressure, pallor, paresthesia, paralysis, and pulselessness (six P’s) [38]. An intracompartmental monitoring device can be used to quantitate the compartment pressures. A sustained intracompartment pressure (ICP) of (> 30 mmHg) or perfusion pressure (diastolic BP–ICP) of less than 30 mmHg is considered abnormal [38]. The medicolegal risks associated with a “missed or delayed compartment releases have resulted in some of the highest indemnity payments in orthopedic litigation” [39].

While MR should not delay surgery in manifest ACS cases for more than 1 h, if signs and symptoms are equivocal, MR can play an adjunctive diagnostic role [40]. Rominger et al. described a loss of normal muscle septation or architecture on T1 imaging and diffuse increased signal intensity on T2-weighted images in cases of compartment syndrome. Contrast enhancement of these cases was variable, but intense muscle enhancement was noted early in the process. As tissue became devitalized, enhancement patterns became more variable. The development of fluid collections may have represented muscle necrosis. Late or follow-up imaging revealed areas of fibrosis and fatty infiltration [40] (Fig. 10).

Fig. 10
figure 10

Dorsal compartment syndrome of the forearm. Coronal proton density fat-saturation image (a) reveals heterogeneously hyperintense signal affecting the dorsal compartment due to blunt trauma. Axial short TI inversion recovery (STIR) (b) reveals bowing of the superficial deep fascia secondary to the swollen muscles throughout the dorsal compartment (arrows)

Overdose compartment syndrome

Nontraumatic or less acute causes of compartment syndrome can pose more of a diagnostic dilemma. This type of compartment syndrome often produces vague symptoms, and obtunded patients may require more of an investigative work-up to elucidate the cause and extent of the disease process. The physical signs and symptoms classically associated with compartment syndrome (six P’s) may be either late findings or cannot be elicited due the patient’s level of consciousness [38].

The combination of legally prescribed and illicit drug use has caused an opioid epidemic in North America. Eighty percent of the world’s prescription opioids are consumed by Canadians and Americans, and there are 467,000 heroin addicts in the USA [41, 42]. A common scenario is the patient that is “found down” presenting with muscle compartment tension, varying degrees of functional deficit, and varying degrees of obtundation. Overdose compartment syndrome (ODCS) patients present differently than acute traumatic compartment syndrome, and there are no clear guidelines for treatment [42]. Parzych et al. prepared a retrospective analysis of 30 patients “found down” with clinical concern for compartment syndrome and found that these patients present with special diagnostic challenges. These patients are often unexaminable, have been immobile for an unspecified amount of time, and are often of “lower socioeconomic health status, leading to increased complication profile and less-reliable long-term follow-up” [42]. Compartment ischemia due to long-term immobility, lying on a hard-noncompliant surface, ultimately causes cell membrane destruction, tissue inflammation and damage (myositis), muscle necrosis, rhabdomyolysis, elevated compartment pressure, and compartment syndrome [38]. Parzych et al.’s group reserved compartmental pressure measurements for patients who were unexaminable, believed to be down for a relatively short period of time, and who had compartments that were not frankly tense but had clinical concern for ongoing muscle necrosis [42]. Laboratory findings most often revealed an elevated creatinine, creatine phosphokinase, and lactate; however, there was no significant relationship between the laboratory findings and the degree of muscle necrosis found at surgery [42]. Compared to acute traumatic compartment syndrome, the gluteus muscles are more often affected with ODCS [43].

Given the difficulty assessing the signs and symptoms of ODCS, MRI may play a greater role in assessing these patients than in acute compartment syndrome. MRI may help to differentiate equivocal cases of compartment syndrome by revealing whether single or multiple muscle compartments are involved, by guiding selective compartment fasciotomies and avoiding unnecessary fasciotomies [40]. In addition, information on the overall extent of the process, detection of fascial bowing, muscle herniation, or focal fluid collections may prove useful.

MR findings of ODCS overlap with rhabdomyolysis and compartment syndrome exhibiting isointense to faintly hyperintense T1-weighted findings with muscle swelling, fascial bowing, and decreased definition of compartmental architectural detail. T2-weighted finding include diffuse or patchy hyperintensity. Post-contrast administration reveals variable levels of enhancement which may depend on the degree of tissue devitalization.

Diagnosis of compartment syndrome

Acute compartment syndrome (ACS) is the most severe complication of the entities we have described; however, many sources state that it is a “clinical diagnosis” [44, 45]. Despite this assertion, a study performed by Ulmer found the signs and symptoms use to diagnose acute compartment syndrome were debatable [46]. Specifically, Ulmer’s research found a low sensitivity of 13% to 19%; a positive predictive value of 11% to 15%; specificity of 97%; and a negative predictive value of 98%. He concluded that the “clinical features of compartment syndrome of the lower leg are more useful by their absence in excluding the diagnosis then they are when present in confirming the diagnosis” [46].

The measurement of intracompartmental pressure is an attempt to objectify the diagnosis of ACS. Large et al. considered a compartment pressure difference of greater than 5 mmHg from the standard to be a significant deviation in their study. They found that the most competent operators, using correct technique, achieved the acceptable standard only 60% of the time. Accuracy decreased to 42% if there were small errors in technique and 22% when catastrophic errors were committed [47]. Moreover, additional errors led to sampling unintended compartments and failure to penetrate the fascia with the needle [47].

The lack of sensitivity of the classic clinical signs and symptoms for ACS, combined with the questionable accuracy of intracompartmental pressure tests, raises concerns when deciding whether to perform a fasciotomy. Fitzgerald et al. performed a retrospective study of 60 patients and concluded that wounds sustained secondary to fasciotomy were “associated with marked morbidity and of such an appearance that their lifestyles were altered” [48]. Similarly, Lim et al. concluded that “as necessary as they are, fasciotomies are not benign procedures” and that “less invasive tests” may help to reduce unnecessary fasciotomies [49].

As discussed, MRI can play an adjunct role in in the diagnosis of myositis by identifying the location, distribution, and extension of the disease process. MRI is also useful in presurgical planning by accurately revealing vital information about the proximity of anatomic structures and by identifying fluid collections that may indicate abscesses or tissue necrosis. MRI is the imaging modality of choice in many cases of myositis, especially in cases that do not involve imminent intervention in order to prevent tissue devitalization. However, given the aforementioned limitations in diagnosis, invasive testing, and treatment morbidity, we posit that MRI may have a role yet to play in ACS. We have seen how rapid MRI scans play an important role in acute brain ischemia, using abbreviated protocols to quickly discriminate between strokes to be treated with IV-tPA and stroke mimics [50]. Similarly, the shorter length of time from injury to fasciotomy portends a better outcome for patients with ACS. A common mantra is that skeletal muscle ischemia for less than 3 h is reversible, and that ischemia for more than 4–8 h is irreversible. However, Vaillancourt et al. stated that these parameters did not comport with their intraoperative findings of tissue necrosis [51].

Conclusion

Myositis and other urgent muscle disorders can present in the emergent setting in several forms with varying levels of severity. Patients usually present with an array of complaints that range from myalgias and muscle swelling to decreased range of motion and weakness. Specific entities may include fever and leukocytosis, and many exhibit increased CK levels. Some patients are unresponsive due to their level of consciousness, precluding adequate assessment of history and physical exam. In addition, the classic physical signs and symptoms for the detection of ACS are low in sensitivity but high in specificity. Given the spectrum of findings, MRI remains a useful, sensitive, diagnostic tool that should be correlated with the available clinical and laboratory data. While some patients require urgent surgical intervention, most can be safely imaged using MR with relative haste considering the efficiency of modern protocols. Potential research incorporating 3D-isotropic volume sets with spectroscopy and elastography could be promising and help to refine the future specificity of MR imaging in this field.