CMR in inflammatory vasculitis.

Vasculitis, the inflammation of blood vessels, can produce devastating complications such as blindness, renal failure, aortic rupture and heart failure through a variety of end-organ effects. Noninvasive imaging with cardiovascular magnetic resonance (CMR) has contributed to improved and earlier diagnosis. CMR may also be used in serial evaluation of such patients as a marker of treatment response and as an indicator of subsequent complications. Unique strengths of CMR favoring its use in such conditions are its abilities to noninvasively visualize both lumen and vessel wall with high resolution. This case-based review focuses on the large- and medium-vessel vasculitides where MR angiography has the greatest utility. Because of increasing recognition of cardiac involvement in small-vessel vasculitides, this review also presents evidence supporting greater consideration of CMR to detect and quantify myocardial microvascular disease. CMR's complementary role amidst traditional clinical, serological and other diagnostic techniques in personalized care for patients with vasculitis is emphasized. Specifically, the CMR laboratory can address questions related to extent and severity of vascular involvement. As ongoing basic and translational studies better elucidate poorly-defined underlying molecular mechanisms, this review concludes with a discussion of potential directions for the development of more targeted imaging approaches.

Introduction

Vasculitis, the inflammation of blood vessels, is rare [1,2], yet those affected may suffer high rates of morbidity and mortality. A significant contributor to poor outcomes is delay in diagnosis. While advances in serologic testing have afforded somewhat earlier diagnosis, there remains a need for better techniques to detect vasculitis and improve outcomes. Advances in non-invasive imaging are poised to fill this gap, particularly in vasculitis involving large- and medium-sized arteries where these studies can play a significant role in i) establishing the correct diagnosis, ii) determining disease extent and activity and iii) measuring treatment response [3].

Recognition that not only vascular but also cardiac sequelae occur in certain vasculitides makes cardiovascular magnetic resonance (CMR) appealing amidst the various imaging options available [4]. Some clinicians may not consider CMR due to concerns surrounding the use of gadolinium-based contrast in vasculitis patients who frequently present with significant renal dysfunction. The availability of excellent non-contrast MR angiography techniques can allay such concerns, allowing CMR in high-risk patients who may have the most to benefit from timely use of the technology.

The paucity of well-defined pathogenic mechanisms for many of these disorders renders in some respect inadequate each of the many vasculitis classification schemes. In this review, we use the common approach that focuses on the sizes of the involved blood vessel that can guide CMR protocols and afford differential diagnosis of imaging findings. This approach, however, requires an appreciation that while specific types of vasculitis classically affect certain-sized blood vessels, there remains a spectrum of involvement across the various levels of the vasculature. What follows is a brief summary of the techniques most relevant to the CMR vasculitis examination followed by case-based illustrations of the major primary inflammatory vasculitides.

While this review focuses on the primary vasculitides, secondary vasculitis and mimics of vasculitis warrant consideration when evaluating a patient with suspected vasculitis [5]. Secondary vasculitis may occur in the setting of infection, malignancy, connective tissue disease [6], drugs and environmental exposure. Another consideration with vasculitis of medium and small vessels is primary central nervous system (CNS) angiitis or involvement of the CNS with a systemic vasculitis. This, too, is beyond the scope of this review but can be pursued in greater depth in several recent publications of MR’s role in the diagnosis and serial assessment of cerebral vasculitis [7,8].

CMR techniques in the vasculitis examination

The evaluation of vasculitis by CMR may include angiography, vessel wall imaging and occasionally myocardial assessment (Figure 1, Table 1). The typical patient presenting with a vasculitis query to the CMR laboratory is one whose clinical, serological and even histopathological evaluations may have already led to diagnosis of a particular condition. For instance, a patient who initially presented with classic signs and symptoms of giant cell arteritis (GCA), underwent definitive temporal artery biopsy and received prednisone therapy, may subsequently be referred for CMR to define the extent of aortic involvement. Less commonly, the CMR laboratory is the first to propose vasculitis as a mechanism underlying the observed findings (Figure 2).

Figure 1

CMR provides a variety of techniques for noninvasive, three-dimensional imaging of the entire vascular tree that may be useful in patients with known or suspected vasculitis such as contrast-enhanced bright blood angiography. (A), noncontrast dark blood angiography (B and C, with lines indicating planes of reformatting of data from the 3D acquisition) and noncontrast bright blood angiography (D, shown in inverted grayscale).

Table 1

Components of the CMR Examination of Vasculitis

Technique	Comments
PRECONTRAST
Dark blood stacks typically in axial, coronal and sagittal planes e.g. HASTE	Provides vessel wall imaging as well as complementary information to CE-MRA regarding lumen
Noncontrast bright blood stack(s) e.g. SSFP
	CONTRAST
3D contrast-enhanced magnetic resonance angiography e.g. spoiled gradient echo	Appropriate vasculature should be covered depending on clinical questions and known or suspected diagnosis (see Table 2)
	POSTCONTRAST
T1-weighted vessel wall imaging e.g. VIBE or FAME	Additional vessel wall imaging, particularly useful to delineate thickening and thrombus
	CARDIAC ACQUISITIONS
Multiplane cine imaging e.g. SSFP Aortic valve velocity-encoded cine Myocardial imaging: T2 precontrast, T1W early post contrast, late post-gadolinium imaging	May be appropriate when aortic root disease involves the aortic valve or when myocardial inflammation is suspected, particularly in small-vessel vasculitides

Figure 2

Vasculitis was identified in a 28 year-old female with unrelenting back pain initially referred for MR examination to rule out aortic dissection; additional history revealed recent unintentional 5 kg weight loss.A. Contrast-enhanced magnetic resonance angiography (CE-MRA) showed diffuse luminal irregularities (arrows). B. Pre-contrast dark blood imaging indicated marked aortic wall thickening to 9–10 mm (arrowheads). There was marked elevation of inflammatory markers including erythrocyte sedimentation rate (ESR, 94 mm/hr) and c-reactive protein (7.3 mg/L) levels. Symptoms markedly improved with prednisone, with reduced ESR (12 mm/hr) and aortic wall thickness at 12-month follow-up.

Techniques for angiography include both contrast-enhanced MR angiography (CE-MRA) as well as non-contrast approaches, both recently summarized in this journal by Hartung et al[9]. MRA’s sensitivity is typically at or near 100% while specificity tends to be lower, underscoring the potential to overestimate degree of stenosis particularly in branch vessels of the aorta. The workhorse technique for demonstration of luminal stenosis remains CE-MRA, with improved spatial resolution, better vessel-to-background contrast and reduced volume requirement for exogenous contrast material with higher field strength. These advantages offset limitations imposed by radiofrequency field inhomogeneity that increases with field strength. Technical developments in coil hardware and parallel acquisition techniques make higher field scanners appealing platforms for CE-MRA.

Non-contrast approaches for angiography abound, starting with traditional time-of-flight (TOF) angiography. While infrequently relied upon for stenosis assessment in extracranial arteries, TOF angiography does provide complementary information to CE-MRA. Rapid, lower-resolution 3D TOF imaging prescribed over a large volume helps identify sites of disease for higher-resolution 2D dark blood scans for vessel wall imaging. Our laboratory and many others have found 3D navigator SSFP imaging to be tremendously useful for non-contrast bright blood MRA of the thoracic aorta [10], particularly when CE-MRA may not be feasible due to contraindications to gadolinium-based contrast administration. Similarly, 3D non-contrast dark blood MRA may be useful in certain settings, particularly when higher heart rate, greater field strength or other approaches help shorten what are typically longer scan times [11]. Dark blood imaging is also preferable when susceptibility artifact obscures interpretation of bright blood images. Another SSFP-based non-contrast approach that is particularly appealing for lower extremity imaging is non-enhanced quiescent-interval single-shot MR angiography (Figure 1) [12]. While initially developed for atherosclerosis imaging of the peripheral arteries, it warrants consideration in vasculitides where peripheral vascular involvement is not uncommon. Some of the more commonly used elements of the CMR vasculitis protocol are listed in Table 1. Table 2 suggests which segments of the arterial tree should be imaged in the most common primary vasculitides. Table 3 summarizes studies comparing magnetic resonance to other modalities commonly used to evaluate the inflammatory vasculitidies.

Table 2

Typical arterial segments involved in the major primary vasculitides

	Thoracic Aorta	Abdominal Aorta	Pulmonary Arteries	Carotid Arteries	Upper Extremities	Mesenteric arteries	Renal arteries	Lower Extremities	Coronary Arteries
Giant cell arteritis	X	X		X	X
Takayasu arteritis	X	X	X	X	X
Polyarteritis nodosa						X	X
Kawasaki disease									X
Behçet disease			X					X

The most common conditions prompting referral for MR examination are shown with X indicating typically-involved segments of the extracranial arterial tree. This scope warrants consideration when prescribing the imaging protocol. Note that atypical manifestations have been reported in virtually all vessel territories for these disorders.

Table 3

MRI in inflammatory vasculitidies

Author (Reference #)	Year published	Design	Comparison Groups	N	Role of CMR
Giant Cell Arteritis
Kornigkam-Santos [21]	2011	Retrospective	MRA in patients vs. retrospective normal controls	28	MRA detected GCA in 67% with good inter-observer agreement
Bley [25]	2005	Prospective	MRA vs. Biopsy	20	16/17 GCA + by biopsy were MRA +, all 3 GCA – were MRA -
Bley [26]	2005	Unclear	MRA in diagnosed GCA patients	21	MRA demonstrated vascular involvement in all previously diagnosed 9 patients
Walter [27]	2005	Unclear	PET in GCA	30 patients and 31 controls	PET had a sensitivity of 73.3% and specificity of 83.9%
Meller [28]	2005	Unclear	PET vs. MRA	15 FUO patients	MRA and PET had comparable sensitivity and specificity for detecting inflammation. Identical vascular territories were identified in the majority but disparate territories in a large minority
Cyran [29]	2011	Prospective	PET vs. MRI	17	Both Dynamic Contrast Enhanced MRI and PET had identical sensitivity and specificity (86 and 90% respectively) in assessing carotid and vertebral inflammation
Both [31]	2008	Prospective	PET vs. MRI	25	MRI and PET found unreliable for assessing large-vessel inflammation in GCA patients on pre-existing immunosuppressive therapy
Takayasu’s Arteritis
Li [37]	2011	Retrospective	Whole body MRI	42	Wall thickness and post-contrast intensity by MRI higher in active group than remissive group (6.12 vs. 4.31 mm and 1.56 vs. 1.17)
Desai [38]	2005	Retrospective case series	MRA-inversion recovery prepared gradient-echo MR pulse sequence	7	All patients had increased wall thickness and 5 had enhancement with contrast (4 had clinically active disease)
Choe [39]	2000	Prospective	MRI	26 patients and 16 controls	MR imaging was concordant with clinical findings in 23 patients (88.5%), with laboratory findings in most patients (ESR in 92.3% [24/26] and CRP in 84.6% [22/26])
Jiang [40]	2012	Prospective	MRA	26 patients-16 classified as active and 10 as inactive	Active group had more stenosis in left SCA than the inactive group (14/16, 87.5% vs. 2/10, 20%; p<0.01) greater vessel wall thickness in left CCA (11/16, 68.75% vs. 1/10, 10%; p<0.01) and left SCA (9/16, 56.25% vs. 0/10, 0%; p<0.01)
Tso [41]	2002	Retrospective	MRA	24	MRA revealed vessel wall edema in 94% (17 of 18), 81% (13 of 16), and 56% (24 of 43) of studies during periods of unequivocally active disease, uncertain disease activity, and apparent clinical remission, respectively. ESR and CRP did not correlate with clinical assessment or MR evidence of vascular edema
Yamada [34]	2000	Prospective	MRA vs. CA	30	Takayasu arteritis was diagnosed in 20 patients - MRA accurately revealed 323 (98%) of 330 arteries, but 7 (2%) stenotic lesions were overestimated as occluded. The sensitivity and specificity of MRA for diagnosis of Takayasu arteritis were 100%. PA lesions were demonstrated in 10 (50%) of the 20 patients.
Garg [35]	2011	Prospective	MRA vs. DSA	22	Diagnosis confirmed by MRA in all patients. MRA with sensitivity, specificity, PPV, NPV and DA for detection of a >50% lesion was 98.33%, 97.25%, 92.18%, 99.43% and 97.52% respectively.
Kawasaki Disease
Greil [54]	2007	Prospective	MRA vs. CA	6	Complete agreement between MRA and CA in detection of coronary aneurysms (n=15).Excellent agreement for aneurysm diameter, length, and distance from the ostium.
Tacke [55]	2011	Prospective	MRA vs. Echocardiography	63	MRA detected coronary aneurysms in 15 patients, whereas echo detected aneurysms in 11.
Greil [56]	2002	Prospective	MRA vs. CA	6	Excellent agreement for assessment of coronary aneurysm maximal diameter and length
Mavrogeni [57]	2004	Prospective	MRA vs. CA	13	6 patients had coronary aneurysms and 7 had ectasia. MRA and CA agreed completely for the diagnosis of aneurysms
Suzuki [58]	2006	Retrospective	MRA vs. CA	106	MRA agreed well with CA for detecting aneurysms and stenoses
Arnold [59]	2007	Prospective	MRA vs. Multidetector CT vs. CA	16	100% agreement between MDCT and CA in the detection of aneurysms and stenoses. MRI and CA had 93% agreement for the detection of aneurysms. MRI missed one stenosis.
Mavrogeni [61]	2011	Unclear	MRA in Kawasaki disease patients in convalescence	13	MRA revealed high prevalence of coronary ectasia and myocarditis in 46% (n=13) of convalescing Kawasaki disease patients

Abbreviations. MRA: magnetic resonance angiography, PET: positron emission tomography, MRI: Magnetic resonance imaging, ESR: erythrocyte sedimentation rate, CRP: C-reactive protein, SCA: subclavian artery, CCA: common carotid artery, CA: conventional angiography, PPV: positive predictive value, NPV: negative predictive value, DA: diagnostic accuracy.

Large vessel vasculitis

Giant cell arteritis (GCA)

GCA is a granulomatous, large-vessel vasculitis with a predilection for individuals aged ≥70 years. Up to 60% of patients with GCA have findings consistent with polymyalgia rheumatica such as proximal muscle morning stiffness and aching [13]. The overall incidence is highest in individuals of Scandinavian descent, where it occurs in 18 to 20 per 100,000 individuals [14]. GCA can be diagnosed as present if 3 of the following 5 classical findings are observed: i) age ≥50 years; ii) new-onset or new type of localized pain in the head; iii) temporal artery tenderness; iv) erythrocyte sedimentation rate ≥50 mm/h; and v) arterial biopsy specimen showing vasculitis [15]. However, appreciating that non-classic symptoms may be the initial manifestation of GCA, high clinical suspicion and rapid institution of, for instance, steroid therapy is needed to avoid dreaded complications such as vision loss. Examination of the retina with fluorescein angiography holds particular value in diagnosis [16].

Classically, GCA affects the extracranial branches of the carotid artery, notably the temporal artery. Risk of developing thoracic and abdominal aortic aneurysms is 17 and 2 times higher, respectively, in patients with GCA compared to age-matched individuals without GCA [17]. Aortic involvement in GCA carries a very high risk of rupture and death, with an average survival of 1 year in GCA patients with thoracic aortic dissection [18]. This considerable increase in mortality due to aortic involvement mandates a low threshold for aortic imaging in this disease [19,20]. Subclavian artery and axillary artery involvement are not uncommon in GCA, and MR performs well in delineating such [21]. GCA affected lower extremities alone in 17% of patients in a recent series [22]. Recognition of long stenotic segments and vessel wall thickening with MR can prompt specific treatment (e.g., prednisone) in such GCA patients who may present solely with claudication. Follow-up MR may identify reduced vessel wall thickening indicating a favorable response to therapy [4].

The sensitivity and specificity of Doppler ultrasonography (US) compared to the clinical diagnosis of temporal arteritis in a meta-analysis of 23 studies was 69 and 82% respectively [23]. Additionally, since US assessment was confined to detection of the “halo” sign in the temporal artery, it cannot reliably assess the thoracic aorta, whose involvement can lead to the serious and fatal complications as discussed above. Nonetheless, European League Against Rheumatism (EULAR) guidelines assign US a class Ia recommendation for the diagnosis of GCA vs. IIa for MRA [24]. Alternatively, 3T MRI of the cranial arteries has a high sensitivity and specificity in detecting vessel wall inflammation when compared with temporal artery biopsy (89-94%, and 92-100% respectively), albeit in small studies [25,26]. Positron emission tomography (PET) may have a higher sensitivity than MRI in detecting GCA according to some retrospective studies [27,28]. However, PET is limited in its ability to demonstrate temporal artery inflammation because of inadequate spatial resolution and inability to distinguish luminal changes in close proximity to glucose-avid brain tissue. In addition, it involves considerable exposure to ionizing radiation. Recently, high resolution dynamic contrast-enhanced (DCE) MRI performed well in detecting vessel inflammation in patients with suspected arteritis [29]. The abnormal extraction fraction computed from first-pass MR imaging, implying increased endothelial leakiness, correlated well with FDG-uptake in arterial walls by PET-CT.

Current data suggest no clear role for either CMR or PET in GCA patient follow up. PET does detect decline in activity with treatment, but in most cases the uptake does not disappear. This is thought to arise from chronic changes associated with vessel wall remodeling. In one GCA study including patients with a complicated course, PET findings correlated poorly with clinical and laboratory criteria of disease activity and MRI findings. In the same study, PET could not predict disease relapse [30]. Of note, MRI with dark blood imaging may demonstrate wall thickening and edema that persists despite clinical and laboratory improvements [31].

Takayasu arteritis (TA)

TA shares many of the vascular findings of GCA but occurs in considerably younger patients, classically women more often than men under the age of 50 years. Diagnosis requires angiographic abnormalities [32] plus one of the following four findings: i) decreased peripheral artery pulse(s) and/or claudication of extremities; ii) blood pressure difference >10 mm Hg between extremities; iii) bruits over aorta and/or its major branches; or iv) hypertension. The mandate for angiographic evidence of disease makes MR an important component of the TA evaluation, especially in children where invasive angiography and CT hold considerably less appeal.

TA, previously termed “pulseless disease” because bilateral subclavian artery occlusion eliminates the radial pulse (Figure 3), can also affect the aorta, pulmonary arteries and renal arteries; some data suggest a predilection for bilateral vessel involvement [33]. In a direct comparison of MRI with invasive angiography, Yamada et al. demonstrated accurate evaluation of 98% vascular territories and also demonstrated pulmonary artery involvement in 50% of patients, identical to the distribution delineated by conventional angiography [34]. Similarly, Garg et al. have also shown a high correlation between MRA and digital subtraction angiography in detecting stenosis and aneurysm formation [35].

Figure 3

A 42 year-old female presented with bilateral arm fatigue, worse with lifting above the head. Physical examination showing absent radial pulses, and serum inflammatory markers including erythrocyte sedimentation rate and c-reactive protein levels were elevated. Anemia was also present (hematocrit 30%). With a presumptive diagnosis of Takayasu arteritis, treatment with prednisone was initiated and CE-MRA was requested. A. Volume rendering shows patency of the common brachiocephalic trunk (C); the proximal portion of the left subclavian artery (L SC, arrow) is patent while distally it is occluded (open arrow). B. Maximum intensity projection (MIP) shows reconstitution of the distal L SC (arrows) via collaterals. C. Similarly, a MIP image shows that the right subclavian artery is occluded (open arrow) and fills distally (filled arrows) via collaterals. D. Volume rendering demonstrates high-grade stenosis (arrow) of the left vertebral artery (V).

Using MR’s ability to assess vessel wall thickening and disease activity, Andrews et al. underscored the utility of MR over traditional x-ray angiography in facilitating early diagnosis and guiding treatment [36]. Given the extent of potential arterial involvement and the requirement for accurate diagnosis (Figures 3, 4, 5), complete aortic imaging with visualization of all major branches should be performed in every TA patient [13]. Li and colleagues demonstrated the diagnostic utility in patients with confirmed TA of whole-body MRA combined with dark blood axial plane vessel wall imaging from neck to pelvis [37]. A correlation with disease activity (clinical and laboratory) with inflammation on MRI was demonstrated by Desai et al., Choe et al., and Jiang et al. using primarily pre-contrast T1W and T2W dark blood imaging but also post-gadolinium T1W imaging [38-40], but not replicated by Tso et al., who with T2W-STIR demonstrated evidence of inflammation by MRI when the disease was clinically quiescent [41]. With histological evidence of ongoing inflammation in Takayasu patients when the disease is clinically quiescent [42], imaging-based detection of vessel wall inflammation warrants further evaluation in clinical trials that examine the effect of treating subclinical disease on outcomes.

Figure 4

Images of the thoracic aorta in a patient with Takayasu arteritis are shown.A. CE-MRA in the sagittal plane demonstrates diffuse, mild dilatation of the descending aorta that measured 33 mm at the level indicated by arrows vs. 25 mm more proximally (arrowheads). Vessel wall thickening can be appreciated using techniques such as non-contrast inversion recovery dark blood imaging (B, showing thickening of 4–5 mm of the thoracic aorta wall, arrows). Additional post-contrast T1-weighted imaging such as the volumetric interpolated breathhold technique (C, same location as B) further confirm vessel wall thickening in this patient.

Figure 5

Images of the abdominal aorta in a patient with Takayasu arteritis are shown.A. Volume rendering viewed in the antero-posterior direction of a CE-MRA acquired using a coronal slab demonstrates marked irregularity of the infraceliac abdominal aorta. B. Maximum intensity projection of a CE-MRA obtained using a sagittal slab at a subsequent visit shows ostial disease of the celiac trunk (arrow) and absence of the superior mesenteric artery (SMA, open triangle). C. Post-contrast volumetric interpolated breathhold T1-weighted image shows thickening of the wall of the abdominal aorta (arrow) and obliteration of the SMA ostium (notched arrow).

Idiopathic aortitis

This inflammatory, noninfectious aortitis has been described both as an isolated aortic disease at one end a spectrum that includes GCA-TA at the other end [43]. However, unlike GCA and TA, idiopathic aortitis infrequently presents with constitutional symptoms but more likely manifests as aortic aneurysm in the setting of asthma or eczema [44]. With recognition that tissue-infiltrating IgG4-positive plasma cells represent the sine qua non of this disease [45], it has been more appropriately included in the spectrum of IgG4-mediated disorders [46]. Typical manifestations include aneurysms of the ascending thoracic or abdominal aorta (Figure 6), and two large studies reported a prevalence of 4 to 6% when examining surgical aortic specimens [47,48]. When histology is available, the diagnosis can be made by demonstration of an abundance of plasma cells spanning the intima, media and adventitia and by their positive staining for IgG4 (Figures 7, 8). An association with retroperitoneal fibrosis has also been described that may lead to ureteral obstruction. CMR in a patient with idiopathic aortitis should span the thorax and abdomen, with attention paid not only to aortic dimensions and wall morphology but also other potentially affected abdominal organs [46].

Figure 6

A 58 year-old male with fatigue and palpitations underwent transthoracic echocardiography that indicated dilatation of the aortic root. CMR was ordered to assess the aorta. A. MIP of the CE-MRA shows marked dilatation of the ascending aorta, which measured up to 6 cm in diameter compared to the 2.5 cm arch. B. Single heartbeat true FISP bright blood image shows thickening of the aortic wall (arrowhead), also evident on HASTE dark blood imaging in the axial (C) and sagittal planes (D).

Figure 7

A. Histopathological examination of the aortic wall in a patient with idiopathic aortitis demonstrates an abundance of plasma cells in the intima.B. Low power light microscopy demonstrates inflammatory cells in media (right side) and adventitia (left side). Warthin-Starry stain was negative for spirochetes. Images courtesy of Drs. Mark Brownell and Anne Albers.

Figure 8

A. Inflammatory infiltrate in a patient with idiopathic aortitis is seen to extend from the adventitia into the mediastinal fat.B. Immunohistochemistry demonstrates IgG4-positive plasma cells. Images courtesy of Drs. Mark Brownell and Anne Albers.

Medium vessel vasculitis

Kawasaki disease (KD)

This leading cause of acquired heart disease in children begins with fever persisting for at least four days. Additionally, diagnosis requires 4 of the following 5 features: i) desquamative rash of the extremities or perineal area; ii) polymorphous exanthema; iii) bilateral conjunctival injection; iv) injection of oral and pharyngeal mucosa; and v) cervical lymphadenopathy [32,49]. Involvement of the coronary arteries produces much of KD’s mortality and morbidity via myocardial infarction and heart failure. Coronary artery aneurysms develop in up to 25% of untreated children [50]; intravenous immunoglobulin therapy reduces this incidence to 3 or 4% [51].

As cardiovascular death has been reported up to 18 years after the initial illness [52], both pediatric and adult cardiovascular specialists should be attuned to the essential elements of follow-up evaluation. The initial evaluation of the child with acute KD includes echocardiography for coronary artery imaging, which is particularly feasible at high volume centers and in smaller children who receive sedation [53]. Because the presence and extent of coronary artery involvement dictate follow-up treatment and testing [49], poor visualization by echo should prompt consideration of CMR for coronary artery imaging in KD [54]. CMR’s lack of ionizing radiation and noninvasive nature make it preferable in children and young adults with KD over modalities such as computed tomography and invasive x-ray angiography (Figures 9, 10). Tacke et al. recently demonstrated the utility of a more comprehensive assessment afforded by CMR that included rest and stress perfusion imaging, cine imaging for wall motion abnormality and late post-gadolinium imaging for infarct scar [55]. Greil et al. first demonstrated equivalence of MRI with conventional angiography in detecting coronary aneurysms, stenosis and complete occlusions using a free-breathing, T2-prepared, 3D bright-blood sequence with navigator gating and tracking [56]. Subsequently, Mavrogeni et al. confirmed complete agreement between conventional angiography and this MRA technique in demonstrating coronary ectasia and aneurysms [57]. Using bright-blood and dark-blood imaging, Suzuki et al. replicated the equivalence of MRI with conventional angiography and superiority over echocardiography in detecting aneurysms and stenosis in patients ranging from 4 months to 37 years [58].

Figure 9

An 11 year-old boy presented to a pediatric hospital with chest and jaw pain while playing one year after a prolonged febrile illness. Initially, CT angiography was performed (A, image courtesy of Dr. Christopher Learn) that showed thrombus in a calcified aneurysm of the left anterior descending coronary artery (LAD, arrow). In the setting of elevation of the serum troponin and possible need for coronary intervention, the patient was transferred to a nearby adult hospital. Invasive angiography (B) showed thrombus nearly occluding LAD that was treated with angioplasty and stent placement. C. Coronary MRA performed in another patient with KD using a navigator-triggered slab prescribed perpendicular to the aortic root demonstrates a 9 mm proximal LAD aneurysm (arrow). LV = left ventricle Ao = aorta.

Figure 10

LGE-CMR in three-chamber (left), mid short-axis (center) and vertical long axis (right) planes show LAD-territory infarct scar in a boy with Kawasaki disease.

Arnold et al. compared conventional angiography, multi-detector CT (MDCT) and MRI in 16 patients and showed 100% concordance between conventional angiography and MDCT, and 93% concordance between MRI and coronary angiography for aneurysm detection [59]. MRI missed one stenotic lesion, while providing additional information regarding myocardial inflammation and injury. Kan et al. recently summarized the safety and accuracy of contemporary CT with ultra-low radiation exposure for pediatric patients [60], including 5 with suspected coronary involvement in KD with nondiagnostic CMR examination. More recently, using free-breathing, T2-prepared, 3D-SSFP, whole heart approach with navigator gating and tracking, Greil et al. demonstrated complete and excellent agreement between MRA and coronary angiography [54].

Mavrogeni et al. reported comprehensive CMR findings using both coronary and myocardial evaluation in 13 KD patients thought to be in convalescence (stage II and III, 20–25 days after disease onset) [61]. Of the six patients with demonstrable myocardial inflammation by T2W STIR (which had resolved in all 6 by repeat CMR 3 months later), only three had evident abnormality by LGE yet all had lower LV ejection fraction by cine imaging. Additional 3D ECG-gated steady state free precession navigator-gated non-contrast coronary MRA identified coronary aneurysms and intracoronary thrombus, some of which were missed by echocardiography. In joint guidelines issued by the American Academy of Pediatrics and the American Heart Association in 2004, echocardiography, MRI, and conventional coronary angiography were all accorded level of evidence C for detection of coronary abnormalities due to lack of prospective data [62].

Polyarteritis nodosa (PAN)

Whereas KD is considered an acute medium vessel vasculitis, PAN is typically a subacute disorder affecting adults more than children. While all the vasculitides are relatively rare, higher incidences of PAN have been reported in Alaskan and Kuwaiti natives [1]. PAN classically affects visceral arteries such as renal, hepatic and mesenteric arteries. Presenting findings often include hypertension, fever, musculoskeletal symptoms, abdominal angina and neuropathy, occasionally with hepatitis B antigen or DNA in the serum [63].

While invasive x-ray angiography may traditionally be used to demonstrate renal artery involvement in PAN, especially when therapy via coil embolization is being considered (Figure 11), CMR may uncover both coronary involvement and its sequelae. Mavrogeni and colleagues identified coronary artery aneurysms in 4 of 16 PAN patients using 3D whole heart navigator MRA [64], and resultant myocardial injury was demonstrated in a patient with PAN by Kobayashi et al. using T2-weighted and LGE imaging of the myocardium [65]. In a longitudinal study of patients with immune-mediated disease comparing incident coronary heart disease (CHD) hospitalization to the entire population of Sweden, Zöller et al. found in 248 patients with PAN a standardized incidence ratio for CHD of 3.81 (95% CI 2.72–5.19) in the first year after PAN hospitalization [66]. Prospective studies are needed to better define the utility of CMR in earlier detection and targeted intervention to prevent CHD complications in PAN.

Figure 11

Traditional x-ray angiography may still be employed in most centers to diagnose polyarteritis nodosa involving the visceral arteries, such as the focal, segmental aneurysms (left panel, up to 4.5 cm in diameter) of the hepatic artery seen in this 77 year-old woman with acute abdominal pain, syncope and bleeding within the liver parenchyma by CT. The angiographic appearance was consistent with PAN. Coil embolization (right panel) was performed with resolution of bleeding. Images courtesy Dr. Leslie Cooper.

Behçet disease (BD)

This disorder is notorious for involving both arteries and veins across vessel sizes, and typically affects young males of Asian and Eastern Mediterranean descent. Presentation with recurrent venous thrombi in a young male with aphthous ulcers and/or uveitis should raise one’s suspicion of BD (Figure 12). Of note, vascular involvement may precede the more classical findings [67].

Figure 12

A 25 year-old Middle Eastern male with a 6 year history of recurrent deep venous thrombi despite therapeutic anticoagulation presented to a vascular medicine specialist. Physical examination demonstrated painful erythematous lesions over the lateral aspect of the calf (A, Courtesy Dr. Steven Dean) and oral ulcerations. B. Subsequent contrast-enhanced magnetic resonance venogram showed occlusion of a previously placed filter in the inferior vena cava (arrowhead). Extensive venous collaterals are evident. C. Coronal plane post-contrast volumetric interpolated breathhold T1-weighted image shows signal void delineating the IVC filter (arrows).

Pulmonary artery aneurysms contribute to excess mortality via rupture; aggressive treatment with steroids, immunosuppression and occasionally surgery has reduced mortality [68]. Recognizing such, vascular imaging of the patient with BD should at some point include the pulmonary arteries. A recent study identified cardiac complications in 6% of patients with this disease including pericarditis, right ventricular thrombus, myocardial infarction and endomyocardial fibrosis [69] – all of which can be readily demonstrated with a suitably-prescribed CMR examination.

Small vessel vasculitis: Churg-Strauss syndrome (CSS)

Patients with small vessel vasculitis have significant constitutional symptoms. Other more specific complaints are related to the particular bed that is affected. For example, palpable purpura is the hallmark dermatological manifestation of small vessel vasculitis, whereas alveolar hemorrhage may occur if the lung parenchyma is involved. Clinical clues to the diagnosis of CSS may include asthma, hypereosinophilia and fever, and half of these patients test positive for anti-neutrophilic cytoplasmic antibody(ANCA) [3]. CSS warrants particular attention in this review given that rates of cardiac involvement have been reported to be as high as 75 to 90%. Cardiovascular involvement in CSS consists of pericarditis, myocarditis, cardiomyopathies and intracavitary thrombi [70,71].In a series of 11 patients undergoing CMR, various forms of myocardial injury was detected in all patients. Mean LVEF was 45% with impairment of LV function in 6 patients, edema in 4, pericardial effusion in 7, and LGE-positivity in 9 including some with normal LV size and EF [72]. The subendocardial pattern of myocardial involvement in CSS can be readily detected by LGE-CMR but not echocardiography [73,74]. Existing data support the use of LGE and T2 myocardial imaging in defining the presence and extent of cardiac disease (Figure 13) [70,72]. Future studies using perfusion CMR may help elucidate to what extent microvascular disease contributes to myocardial involvement.

Figure 13

A 37-year-old female with biopsy-proven Churg-Strauss-vasculitis was referred for CMR examination The left ventricle was slightly enlarged with mild systolic dysfunction: LV ejection fraction was 45%. Late post-gadolinium myocardial enhancement images in various planes show septal intramural and anteroseptal and anterior subendocardial lesions. Images courtesy Drs. Ralf Waβmuth and Jeanette Schulz-Menger.

Review and Conclusions

Su and colleagues, in one of the few studies of molecular imaging specifically targeting non-atherosclerotic vascular inflammation, showed feasibility of targeting the enzyme myeloperoxidase that is a marker of certain vasculitides [75]. Ongoing advances in understanding the molecular bases for these varied conditions may translate into novel diagnostic imaging approaches. Remarkably, diagnosis still heavily relies on direct tissue examination; development of MR agents that target IgG4 or ANCA could hopefully improve the diagnostic specificity of noninvasive imaging and reduce the need for histopathology.

In conclusion, diagnosis and serial assessment of patients with inflammatory vasculitis require clinical, laboratory and imaging assessments. The CMR laboratory in particular offers a spectrum of techniques for noninvasive angiography and vessel wall imaging, both with and without need for exogenous contrast administration. The utility of these techniques in patients with inflammatory vasculitis is realized only through 1) their timely use at initial presentation for accurate delineation of both presence and extent of disease and 2) an ongoing dialog among CMR specialists and the clinicians charged with initial diagnosis and long-term management. Such efforts coupled with continued advances in molecular understanding and treatment warrant further investigation given the considerable morbidity and mortality for patients with primary vasculitis.

Competing interests

Dr. Raman receives research support from Siemens. Drs. Jarjour and Aneja have no competing interests to report.

Authors’ contributions

SVR drafted the manuscript and figures. WNJ and AA contributed to manuscript preparation and revision. All authors read and approved the final manuscript.