Download PDF
Rofo 2019; 191(09): 805-816
DOI: 10.1055/a-0864-2084
Review
© Georg Thieme Verlag KG Stuttgart · New York

Imaging of Multiple Myeloma

Article in several languages: English | deutsch
Aleksander Kosmala
Department of Diagnostic and Interventional Radiology, University-Hospital Würzburg, Germany
,
Thorsten Bley
Department of Diagnostic and Interventional Radiology, University-Hospital Würzburg, Germany
,
Bernhard Petritsch
Department of Diagnostic and Interventional Radiology, University-Hospital Würzburg, Germany
› Author Affiliations
Further Information

Correspondence

Dr. Aleksander Kosmala
Department of Diagnostic and Interventional Radiology, University-Hospital Würzburg
Oberdürrbacher Straße 6
97080 Würzburg
Germany   
Phone: ++ 49/9 31/20 13 40 00   

Publication History

21 November 2018

06 February 2019

Publication Date:
11 June 2019 (online)

Also available at
 
 PDF Download Permissions and Reprints

Abstract

Background Multiple myeloma is a malignant hematological disease characterized by uncontrolled proliferation of monoclonal plasma cells mainly in the bone marrow. Imaging plays a crucial role in diagnosis and follow-up.

Method This literature review provides information about multiple myeloma, its precursor diseases, and available imaging techniques. Advantages and limitations as well as possible prognostic and therapeutic implications of the different imaging methods are presented in the context of the current literature.

Results and Conclusion Cross-sectional imaging has replaced conventional X-ray skeletal survey. Widely available whole-body computed tomography is routinely used to detect osteolytic lesions. Magnetic resonance imaging is the most sensitive technique to identify bone marrow infiltration and is recommended in multiple myeloma precursor diseases. Positron emission computed tomography combines morphological and functional imaging. It is mainly used for follow-up, therapy monitoring, and response evaluation.

Key points:

  • Conventional X-ray skeletal survey is obsolete.

  • Whole-body CT is routinely used to detect osteolysis.

  • MRI is the most sensitive modality to identify bone marrow infiltration.

  • MRI is used for the workup of precursor diseases (alternatively: PET/CT).

  • PET/CT is used for follow-up, therapy monitoring, and response evaluation.

Citation Format

  • Kosmala A, Bley T, Petritsch B. Imaging of Multiple Myeloma. Fortschr Röntgenstr 2019; 191: 805 – 816


#

Key words

myeloma - MGUS - smouldering multiple myeloma - whole-body magnetic resonance imaging (WBMRI) - whole-body low-dose computed tomography (WBLDCT) - PET-CT

Introduction

Multiple myeloma (MM) is a malignant hematological disease characterized by uncontrolled proliferation of monoclonal plasma cells mainly in the bone marrow. With approx. 6500 new cases in Germany each year, MM is one of the most common hematologic neoplasias [1]. The median age of onset is 72 years in men and 74 years in women. Onset prior to the age of 45 is rare (approx. 2 % of cases). Despite therapeutic advances in recent years, the 5-year survival rate continues to be just under 50 % [1]. Bone lesions, which are associated with the most common symptoms like bone pain, fatigue, and anemia due to suppression of normal hematopoiesis, are present in over 80 % of patients at the time of initial diagnosis [2] [3].

Diagnosis is made on the basis of a "myeloma-defining event" with simultaneous biopsy-based confirmation of bone marrow infiltration ≥ 10 % or detection of a plasmacytoma ([Table 1]). In addition to laboratory testing and processing of a bone marrow sample, imaging plays a central role: the presence of osteolysis on conventional radiography, computed tomography (CT) or positron emission tomography combined with CT (PET/CT) or the detection of more than one bone marrow lesion via magnetic resonance imaging (MRI) results in the diagnosis of a myeloma requiring treatment [4]. Modern cross-sectional imaging techniques like MRI and PET/CT can also be used to evaluate prognosis as well as to assess treatment response and disease activity in the clinical course [5] [6] [7].

Table 1

Diagnostic criteria (“myeloma defining events”) for multiple myeloma according to recommendations of the International Myeloma Working Group 2014 (modified after [4]).

evidence of end organ damage („CRAB“) (positive, if one or more of the following are present)

C („hypercalcaemia“)

hypercalcaemia with serum calcium > 0.25 mmol/l above upper limit of normal or > 2.75 mmol/l

R („renal insufficiency“)

renal insufficiency with creatinin clearance < 40 ml/min or serum creatinine > 177 µmol/l

A („anaemia“)

haemoglobin < 100 g/l or value > 20 g/l below the lower limit of normal

B („bone lesions“)

≥ 1 osteolytic lesion (≥ 5 mm) on skeletal radiography, computed tomography or positron emission tomography with computed tomography

Biomarkers of malignancy („SLiM“) (positive, if one or more of the following are present)

S („sixty percent plasma cell percentage“)

clonal plasma cell percentage in the bone marrow ≥ 60 %

Li („light chain ratio“)

ratio of involved/uninvolved serum free light chains (κ/λ-ratio) ≥ 100

M („magnetic resonance imaging“)

more than one focal lesion (≥ 5 mm) on MRI

A manifest multiple myeloma can be diagnosed, if at least one of the above-mentioned criteria is positive. CT = computed tomography, PET/CT = positron emission tomography/computed tomography, MRI = magnetic resonance imaging.

The various imaging modalities are presented in the following with respect to their current importance and their advantages and disadvantages for the diagnosis and follow-up of MM and its initial stages.


#

Imaging for diagnosing MM

Conventional radiography

For a long time, the widely available and comparatively cost-effective conventional X-ray skeletal survey was the established method for detecting osteolytic bone lesions. Scans of the skull, cervical spine, thoracic spine, and lumbar spine on two planes as well as bilateral a. p. scans of the bony thorax, pelvis, and proximal extremities were acquired. In the past, various staging systems and diagnostic guidelines have defined conventional X-ray skeletal survey as a standard [8] [9]. However, current recommendations, e. g. by the European Myeloma Network or the European Society for Medical Oncology, are increasingly abandoning conventional radiography in favor of modern methods [10] [11]. An important weakness of conventional X-ray skeletal survey is the fact that approx. 30–50 % of trabecular bone must be destroyed to be visible as osteolysis. In the meantime, numerous studies have shown that modern cross-sectional techniques like CT, PET/CT and MRI are superior to conventional X-ray for detecting bone disease [12]. Additional disadvantages of conventional projection radiography are the lack of ability to evaluate treatment response or extraosseous involvement and the complicated examination procedure that involves the need to reposition patients who are often in pain multiple times ([Table 2]). As a result, conventional radiography has been replaced by whole-body CT as the basic imaging modality at many centers ([Fig. 1]).

Table 2

Advantages and disadvantages of different imaging modalities in patients with multiple myeloma (modified after [5]).

modality

advantages

disadvantages

X-ray skeletal survey

  • low cost

  • wide availability

  • established by longstanding routine use

  • poor sensitivity

  • advanced osteodestruction necessary to visualize osteolysis

  • time-consuming acquisition, patient discomfort

  • summation effects e. g. in the pelvis impair assessment of lytic lesions

  • no evaluation of non-lytic bone marrow infiltration, extramedullary disease or therapy response

whole body CT

  • high sensitivity for lytic lesions

  • possible depiction of extramedullary disease

  • visualization of bone marrow infiltration in the extremities

  • wide availability

  • short acquisition time

  • high patient comfort

  • relatively low cost

  • useful for planning of surgeries, biopsies or radiation therapy

  • no evaluation of non-lytic bone marrow infiltration in the axial skeleton

  • higher costs and radiation dose compared to X-ray

  • insufficient for monitoring of therapy response

ganzkörper-MRT

  • no radiation exposure

  • high sensitivity for detection of bone marrow infiltration and extramedullary disease

  • depiction of infiltration patterns including diffuse infiltration

  • depiction of non-osteolytic bone marrow infiltration

  • prognostic relevance

  • superior assessment of spinal cord pathologies and nerve root compression

  • possible assessment of therapy response using modern functional techniques

  • high cost

  • long acquisition time

  • limited use in patients with claustrophobia or metal implants

  • limited and delayed evaluation of therapy response using regular morphologic sequences

PET/CT

  • simultaneous morphologic and functional imaging

  • assessment of disease activity and response to therapy

  • pre- and post-therapeutic prognostic significance

  • high sensitivity for extramedullary disease

  • high cost

  • limited availability

  • false-positive diagnoses e. g. due to inflammatory processes

  • limited detection of diffuse bone marrow infiltration

  • need for further standardization

CT = computed tomography, PET/CT = positron emission tomography/computed tomography, MRI = magnetic resonance imaging.

Zoom Image
Fig. 1 Coronal a and sagittal b computed tomography images of the spine and pelvis show multifocal osteolysis in a 60-year-old male patient with multiple myeloma. On the corresponding conventional skeletal radiography images of the thoracic c and lumbar d spine even the largest osteolytic lesion with advanced destruction of the T4 vertebral body is largely occult, while the advanced destruction of the L4 vertebral body is challenging to spot (arrows in b).

#

Whole-body CT

Due to the high intrinsic contrast of bony structures, unenhanced low-dose CT is usually performed for detecting bone involvement in MM. The arms are typically positioned in front of the body. The radiation exposure of such an examination is approx. 3–5 mSv which is two to three times that of a conventional X-ray skeletal survey [13] [14] [15]. In light of the significantly higher sensitivity and improved patient comfort in the typically older patient population, the slightly higher radiation exposure is acceptable. Moreover, it was recently able to be shown that an examination with dose values similar to those of projection radiography (around 1.5 mSv) can be achieved using modern CT techniques [16]. In addition to the high sensitivity, CT has additional advantages such as improved assessment of fracture risk, the ability to visualize extraosseous myeloma, and biopsy, surgery, and radiation planning. Moreover, clinically relevant, non-bone-related secondary diagnoses can be made on CT in approximately one-third of cases ([Table 2]) [17].

In the long bones, CT additionally allows visualization of bone marrow involvement in the form of a focal or diffuse increase in bone marrow density which may be prognostically relevant ([Fig. 2]) [18]. However, in the spine and pelvis, visualization of diffuse or focal non-osteolytic bone marrow involvement is not possible in the case of a preserved trabecular bone structure. Only in advanced osteoporosis can an experienced examiner assess whether the axial skeleton predominantly contains healthy fatty marrow or if bone marrow infiltration is present, particularly over the clinical course. Thus, CT is particularly suitable for treatment monitoring in non-osteolytic bone marrow involvement in the long bones [19], while osteolysis caused by a lack of remineralization in the clinical course does not allow conclusions about treatment response [12]. Only the fat- or soft tissue-equivalent osteolysis "content" allows evaluation of response or determination of a relapse. MRI is the method of choice for visualizing bone marrow infiltration, particularly in the spine and pelvis [20].

Zoom Image
Fig. 2 Coronal computed tomography images of a 64-year-old male patient with multiple myeloma in complete remission a, and 4 months later during relapse b. The humeral metaphyses show subtle osteolysis and scalloping even during remission a, most likely due to a treated infiltration. While the bone marrow of the humerus appears normal and fatty in a without any signs of cellular infiltration, a diffuse hyperdense bone marrow infiltration (arrows) can be readily seen during relapse b.

#

MRI

MRI is usually performed as a whole-body examination including the extremities since almost half of all patients have focal lesions outside the axial skeleton and lesions are seen exclusively in the bones of the extremities in up to 10 % of cases [21]. Coronal and possibly sagittal T1w and T2w sequences as well as fat-saturated T2w sequences are typically used in a clinical examination protocol ([Table 3]). When evaluating images, it is important to always take the age and medical history of the patient into account. Incomplete fatty conversion in comparatively young patients, bone marrow stimulation due to growth factors or chemotherapeutic agents, or allogeneic stem cell transplantation can in some cases only be differentiated from malignant plasma cell infiltration on a conditional basis.

Table 3

Exemplary whole-body MRI protocol (1.5 T MAGNETOM Avanto fit [Siemens Healthineers, Erlangen]).

region

Sequence

TR [ms]

TE [ms]

voxel size [mm3]

bandwidth [Hz/Pixel]

skull, neck, thorax, abdomen, extremities

T2 TIRM coronar

5240

82 (TI: 130)

0.6 × 0.6 × 5.0

 303

T1 VIBE coronar

6.4

4.8

1.5 × 1.5 × 2.5

 740

DWI axial[1]

5000

74

1.9 × 1.9 × 6.0

1628

skull

resolve DWI axial[2]

3220

81/124

1.0 × 1.0 × 6.0

 657

neck

DWI axial1

2900

87

1.7 × 1.7 × 5.0

1644

MRI = magnetic resonance imaging, TR = time to repetition, TE = time to echo, TIRM = turbo inversion recovery magnitude, TI = inversion time, VIBE = volume interpolated breathhold examination, DWI = diffusion weighted imaging.

1 b-values: b50 and b800.


2 b-values: b0 and b1000.


Five different infiltration patterns in myeloma patients can be differentiated on MRI ([Fig. 3], [4]): a normal appearance of the bone marrow, focal infiltration pattern (T1w hypointense lesions with a diameter of at least 5 mm), homogeneous diffuse infiltration (bone marrow on unenhanced T1 image generally more hypointense than adjacent intervertebral disc spaces without degenerative changes), mixed infiltration pattern (focal + diffuse), and the "salt and pepper" pattern (disseminated T1w hypointense lesions in front of an inhomogeneous background of T1w hyperintense normal bone marrow) [20]. Only the plasma cell lesions in the focal or mixed infiltration pattern result in destruction of the surrounding bone substance which is expressed as osteolysis that is potentially visible on projection radiography and CT. Various studies were able to show the prognostic relevance of the MRI patterns of infiltration. A normal appearance of the bone marrow or a "salt and pepper" pattern was usually associated with an early disease stage and a better prognosis, while a diffuse infiltration pattern or numerous focal lesions were associated with genetic high-risk constellations, an advanced disease stage, a higher tumor load, and worse progression-free survival as well as overall survival [22] [23].

Zoom Image
Fig. 3 Bone marrow infiltration patterns of multiple myeloma on magnetic resonance imaging using sagittal fat-saturated T1-weighted images a–e. Normal-appearing bone marrow shows a homogeneously T1w hyperintense distribution due to the fat content a. Focal lesions are visualized with a similar or lower signal intensity compared to the musculature or healthy intervertebral discs (b, arrows with an open arrowhead point to exemplary focal lesions; pathological fractures are seen in T10 and T12 as well as L1, 4, and 5). A diffuse infiltration is indicated by a homogeneous T1w hypointense bone marrow compared to the musculature or neighboring intervertebral discs c. Simultaneous visualization of a generalized T1w hypointense bone marrow and additional focal lesions marks a mixed focal and diffuse infiltration (d, arrows with a closed arrowhead point to exemplary focal lesions, that in this patient appear relatively T1w hyperintense due to high-grade diffuse T1w hypointense infiltration of the surrounding marrow). A “salt-and-pepper” pattern shows a disseminated “micronodular” T1w hypointense infiltration against a background of normal T1w hyperintense fatty bone marrow e, with a simultaneously normal fat-saturated T2w imaging appearance (not shown here).
Zoom Image
Fig. 4 Patterns of bone marrow infiltration in fat-saturated T2-weighted images a–d. Patients with a normal-appearing bone marrow and patients with a salt-and-pepper pattern show homogeneous hypointense bone marrow on T2w images a. Focal lesions appear hyperintense on fat-saturated T2w images b. A diffuse infiltration pattern is marked by homogeneously hyperintense bone marrow on fat-saturated T2w images c. In a mixed imaging pattern, circumscribed focal hyperintense lesions are visualized within homogeneous hyperintense bone marrow on fat-saturated T2w images (arrow in d).

The advantages of MRI are due to the fact that bone marrow infiltration can be visualized even before lytic changes occur ([Table 2]). Therefore, it is not surprising that MRI is superior to conventional radiography with respect to the detection of bone involvement [12]. MRI is at least equivalent to CT and PET/CT, with individual studies showing advantages with respect to MRI [4] [12] [24] [25]. MRI is better suited than PET/CT to detect diffuse bone marrow involvement [25] [26]. A further advantage of MRI is the ability to differentiate uncomplicated osteoporotic fractures from pathological fractures based on the appearance of the bone marrow [27]. Moreover, MRI is highly suitable for visualizing extramedullary myeloma, which occurs in up to one-fifth of all patients and can manifest on a secondary basis (i. e., by spreading from an affected bone) or on a primary basis as an extraosseous finding ([Fig. 5]) [28]. Besides the known disadvantages of MRI in general, like limited availability, high costs, long examination time (depending on the protocol approx. 45 to ≥ 60 minutes) and only conditional applicability in patients with metal implants or claustrophobia, MRI has an additional disadvantage regarding the follow-up of myeloma patients: in purely morphologic sequences it is often not possible to differentiate between vital lesions and non-vital scarring despite possible treatment response since part of the lesions disappears incompletely or only very slowly ([Table 2]) [7] [24] [29]. Therefore, PET/CT has become established for treatment monitoring.

Zoom Image
Fig. 5 Axial FDG PET/CT image a and corresponding b800 DWI image b of a 69-year-old male patient with multiple myeloma. Primary extramedullary disease of the pleura and of the liver in segment 4a (short arrows in a and b) as well as secondary extraosseous lesions adjacent to the ribs show a vivid hypermetabolism on PET/CT (a) and appear hyperintense on DWI b. Note: FDG = 18F-fluorodeoxyglucose, PET/CT = positron emission tomography/computed tomography, DWI = diffusion-weighted imaging.

#

PET/CT

18F-fluorodeoxyglucose (FDG) PET/CT is an imaging modality that visualizes the glucose hypermetabolism of medullary and extramedullary myeloma in addition to the morphological detection of osteolysis as an additional functional component ([Fig. 5]) [6] [12] [30]. Even though non-osteolytic lesions can also be detected on PET/CT, the persistence of at least one osteolytic lesion (≥ 5 mm) continues to be necessary according to current diagnostic guidelines for formal diagnosis of bone involvement [4]. The diagnostic performance of PET/CT for detecting focal lesions is significantly greater than that of conventional radiography and is largely comparable with MRI [12]. PET/CT is inferior to MRI only with respect to the detection of diffuse bone marrow infiltration [25] [26] since the cellular uptake rate of FDG as well as the percentage of myeloma cells in the examined volume plays a role. Given a low cell density, e. g. in the case of low-grade diffuse involvement, the FDG uptake must also be low.

PET/CT has become established primarily for treatment monitoring. Based on the visualization of metabolic activity in myeloma lesions, a differentiation between hypermetabolism suspicious for malignancy and inactive scarring is possible, while a difference often cannot be observed on a purely morphological basis on CT or MRI [7] [29] [31] [32]. Moreover, PET/CT makes it possible to make prognostic statements both in the initial diagnosis and in the course of treatment. Therefore, for example, the detection of more than 3 hypermetabolic focal lesions at the initial diagnosis or shortly after the start of treatment is an independent predictor of a worse survival rate so that certain patients may benefit from a targeted early change of treatment [33] [34] [35]. Moreover, better treatment results were observed in patients with complete normalization of the metabolism in focal lesions after induction chemotherapy [33]. An unremarkable PET/CT examination is predictive of a long-term relapse-free survival even after autologous stem cell transplantation while the detection of active lesions is an independent predictor of a worse progression-free survival [35] [36] [37]. Despite these promising results, PET/CT is not yet established as a routine method in the clinical routine in many places due to the high costs and the limited availability ([Table 2]).


#
#

Imaging of precursors to multiple myeloma

Monoclonal gammopathy of unclear significance (MGUS)

MGUS is an asymptomatic precursor disease of MM that does not require treatment and is usually identified incidentally after the 50th year of life on the basis of an M-gradient in routine laboratory testing and has an annual risk of progressing to myeloma requiring treatment of approx. 1 % [3]. By definition, patients with monoclonal gammopathy differ from patients with "smoldering multiple myeloma" (SMM) and symptomatic MM on the basis of a lower M-protein and a plasma cell infiltration < 10 % in the bone marrow biopsy. In addition, these patients may not exhibit a "myeloma-defining event" ([Table 1]) [3] [4]. Although patients with MGUS per definition do not have myeloma-related osteolysis, at least one focal lesion could be detected via whole-body MRI in 23 % of cases in a study including 137 patients, which proved to be an independent predictive factor for disease progression to symptomatic MM in the course of the disease [23]. To identify such cases in a timely manner and to be able to monitor them closely, MRI should be performed in the case of a diagnosis of MGUS.


#

"Smoldering multiple myeloma“

SMM is also an asymptomatic precursor to MM without the presence of end-organ damage. However, compared to MGUS, it has higher laboratory parameters, a plasma cell infiltration of 10–60 % in the bone marrow and an annual risk of progressing to MM of 10 % [3] [4]. In recent years, two studies showed that focal lesions can be detected on MRI in up to 28 % of patients with SMM [38] [39]. The presence of more than one focal lesion was an independent predictor of faster progression to symptomatic MM in both studies. The International Myeloma Working Group (IMWG) recommends performing MRI in the case of diagnosis of SMM accordingly early in order to be able to treat high-risk patients in a timely manner. Therefore, the presence of more than one focal lesion on MRI is included in the latest version of the IMWG recommendations as a "myeloma-defining event", resulting in treatment as symptomatic myeloma [4]. In the case of unclear MRI findings, a diffuse infiltration, or the presence of only one focal lesion, a follow-up MRI should be performed at an interval of 3–6 months for better assessment of the risk of disease progression [4]. Alternatively FDG PET/CT can be performed in the case of contraindications or a lack of availability.


#

Solitary plasmacytoma

Solitary plasmacytoma can be divided into primary bone plasmacytoma and primary extramedullary plasmacytoma, with the primary bone plasmacytoma being associated with a higher risk of progression to MM. Besides bone marrow biopsy, the presence of osteolytic lesions in addition to the primary lesion should be ruled out on whole-body CT or PET/CT. Moreover, MRI or PET/CT, which is also suitable for visualizing extramedullary and non-osteolytic lesions and can detect additional lesions in up to one-third of all patients resulting in a change in the therapeutic approach, should be performed [4] [40].


#
#

Follow-up imaging and assessment of treatment response and minimal residual disease

Projection radiography and CT are only conditionally suitable for follow-up in patients with MM. Since remineralization of osteolytic lesions cannot be expected even after successful treatment, these two modalities can only show disease progression with new or larger osteolytic lesions or complications like fracture of vertebral bodies [12]. Treatment response can be identified on CT only on the basis of regression of extraosseous or paraosseous soft-tissue manifestations or on the basis of regression of medullary plasma cell infiltrations in the long bones of the extremities. In the case of treatment response, increasing normalization of the bone marrow appearance or regression of focal lesions with respect to number and size can be expected on MRI. However, it cannot be assumed in all cases that focal lesions will completely disappear since non-vital scarring can continue to be visible and cannot be differentiated from plasma cell nests with residual vitality on a purely morphological basis without functional sequences [32]. In addition, MRI shows a possible treatment response only with a slight time delay of 1–3 months [24]. Response can be detected much more quickly, namely after just a few days, and with significantly higher specificity with PET/CT which is why this technique has also become established for follow-up [7] [24] [31] [32] [35].

Effective treatments have increasingly resulted in a majority of patients achieving complete remission according to the conventional definition. However, since multiple myeloma is not a uniform disease, vital plasma cell nests can continue to be visible at other locations despite response according to laboratory testing and unremarkable blind puncture of the bone marrow of the iliac crest or sternum [7] [41]. In one study including 282 patients, it was able to be shown for example that patients with complete remission according to the conventional definition and remaining vital lesions on PET/CT have a significantly shorter progression-free survival than those without vital lesions. However, an unremarkable PET/CT after the conclusion of treatment was an independent predictor of a longer progression-free survival and overall survival [42]. Based on the increasingly clinically established treatment monitoring in lymphoma diseases, IMWG recently published criteria for the assessment of minimal residual disease using PET/CT among other things and thus highlighted the importance of functional imaging for defining remission [31]. In the future, further standardization of the criteria regarding the quantitative and visual evaluation of PET/CT examinations would be desirable.


#

Future developments

Since MRI with purely morphological sequences cannot differentiate vital lesions from non-vital ones with sufficient certainty, additional functional MRI techniques like dynamic contrast-enhanced (DCE) MRI and diffusion-weighted imaging (DWI) are being tested at some centers. DCE-MRI after intravenous administration of a gadolinium-containing contrast agent allows conclusions about local microcirculation in bone marrow. Correlations with disease activity, disease stage, treatment response, progression-free survival, and overall survival could be shown in studies [43] [44]. However, the fact that DCE-MRI requires dedicated software for evaluation and quantification is problematic because the software can be associated with high procurement costs and software from different providers can yield inconsistent results even using the same source data. The molecular movement of hydrogen in tissue can be shown on DWI-MRI allowing tissue characterization without the administration of contrast agent. Primarily cell-rich focal myeloma lesions and diffuse infiltration of bone marrow by monoclonal plasma cells have a high signal due to their diffusion restriction in the DWI sequence which is why it is highly suitable as a search sequence [45] [46]. Moreover, a correlation between quantitative DWI parameters and the degree of bone marrow infiltration as well as treatment response could be shown ([Fig. 6]) [44] [47] [48] [49]. A general problem of DWI is its general susceptibility to interference. Both techniques are not yet widely established for routine use.

Zoom Image
Fig. 6 Axial b800 a, c and ADC b, d DWI images of a 69-year-old patient with multiple myeloma. The baseline exam a, b before initiation of therapy reveals multiple osseous and extraosseous lesions, which show restricted diffusion on the ADC-map (arrows in b). 10 days after VCD therapy onset, myeloma lesions become less hyperintense in the b800 images and show increasing ADC values (arrows in d), which can be attributed to a decline in cellularity due to early therapy response. Note: DWI = diffusion-weighted imaging, ADC = apparent diffusion coefficient, VCD = Velcade® (bortezomib), cyclophosphamide, dexamethasone.

Moreover, technical advances also in morphological MRI sequences (e. g. ultrashort echo time UTE technique) could make it possible in the future to visualize even small osteolytic lesions with dedicated, high-resolution sequences, which has only been possible with CT until now. This would mean, for example, a significant reduction in radiation dose in the case of suspected SMM or MGUS where to date end-organ damage in the form of osteolytic lesions has been ruled out via CT. However, data from prospective studies in this regard are currently lacking.

Another promising hybrid technique is PET/MRI which combines the metabolic information of PET with the excellent soft-tissue contrast of MRI. Although PET/MRI lacks the ability to visualize mineralized bone, which would seem to be a disadvantage compared, for example, to PET/CT, MRI alone has excellent sensitivity for detecting osseous, particularly intramedullary, lesions, as confirmed by the results of initial studies on the PET/MRI hybrid method, which showed comparable diagnostic performance to that of PET/CT in myeloma patients, with larger studies still lacking due in part to the low availability of such scanners [50].

Alternative tracers for PET that can be used instead of FDG provide a further development opportunity. 11C-methionine is absorbed to a greater degree for example by plasma cells and can be successfully used for imaging in MM. The results of recent studies confirm that 11C-methionine has a better diagnostic performance and better performance in relation to the assessment of treatment response compared to FDG [51] [52]. However, due to the short half-life of the tracer, this technique has only been available on a limited basis to date.

There have also been further developments regarding CT in recent years. Examinations using the dual-energy technique make it possible to create virtual calcium-free datasets ([Fig. 7]). Using this technique, it was able to be shown that even non-osteolytic bone marrow involvement in the axial skeleton can be detected on CT [53] [54]. Moreover, the technique can be used for the targeted biopsy of focal bone lesions that are occult on conventional CT [55]. In the future this could be relevant for MM with its highly heterogeneous intraindividual distribution, for example, for examining individual lesions in a targeted manner in addition to blind puncture of the iliac crest.

Zoom Image
Fig. 7 Axial CT of the pelvis in a 76-year-old male patient with multiple myeloma. The non-lytic lesions (arrows in a and b) can barely be seen in the bone window a or soft tissue window b settings. Both lesions show hypermetabolism on PET/CT (arrows in c). Using the dual-energy CT color overlay after virtual calcium removal, both lesions can readily be seen depicted in green (arrows in d). Note: CT = computed tomography, PET/CT = positron emission tomography/computed tomography.

#
#

Conflict of Interest

The authors received research support from a research cooperation of the Institute of Diagnostic and Interventional Radiology with Siemens Healthineers AG.

Acknowledgment

A special thank you to Professor Buck from the Department of Nuclear Medicine, University Hospital Würzburg.

  • References

  • 1 Krebs in Deutschland für 2013/2014. Robert Koch-Institut; 2017 11th ed.
    PubMedGoogle Scholar
  • 2 Kyle RA, Gertz MA, Witzig TE. et al. Review of 1027 patients with newly diagnosed multiple myeloma. Mayo Clin Proc 2003; 78: 21-33
    CrossrefPubMedGoogle Scholar
  • 3 Rajkumar SV, Kumar S. Multiple Myeloma: Diagnosis and Treatment. Mayo Clin Proc 2016; 91: 101-119
    CrossrefPubMedGoogle Scholar
  • 4 Rajkumar SV, Dimopoulos MA, Palumbo A. et al. International Myeloma Working Group updated criteria for the diagnosis of multiple myeloma. Lancet Oncol 2014; 15: e538-e548
    CrossrefPubMedGoogle Scholar
  • 5 Terpos E, Dimopoulos MA, Moulopoulos LA. The Role of Imaging in the Treatment of Patients With Multiple Myeloma in 2016. Am Soc Clin Oncol Educ B 2016; 36: e407-e417
    PubMedGoogle Scholar
  • 6 Mihailovic J, Goldsmith SJ. Multiple myeloma:18F-FDG-PET/CT and diagnostic imaging. In: Semin Nucl Med. W.B. Saunders 2015: 16-31
    PubMedGoogle Scholar
  • 7 Hillengass J, Merz M, Delorme S. Minimal residual disease in multiple myeloma: use of magnetic resonance imaging. Semin Hematol 2018; 55: 19-21
    CrossrefPubMedGoogle Scholar
  • 8 Durie BGM, Salmon SE. A clinical staging system for multiple myeloma. Cancer 1975; 36: 842-854
    CrossrefPubMedGoogle Scholar
  • 9 Dimopoulos M, Terpos E, Comenzo RL. et al. International myeloma working group consensus statement and guidelines regarding the current role of imaging techniques in the diagnosis and monitoring of multiple Myeloma. Leukemia 2009; 23: 1545-1556
    CrossrefPubMedGoogle Scholar
  • 10 Moreau P, San Miguel J, Sonneveld P. et al. Multiple myeloma: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up. Ann Oncol 2017; 28: iv52-iv61
    CrossrefPubMedGoogle Scholar
  • 11 Terpos E, Kleber M, Engelhardt M. et al. European myeloma network guidelines for the management of multiple myeloma-related complications. Haematologica 2015; 100: 1254-1266
    CrossrefPubMedGoogle Scholar
  • 12 Regelink JC, Minnema MC, Terpos E. et al. Comparison of modern and conventional imaging techniques in establishing multiple myeloma-related bone disease: A systematic review. Br J Haematol 2013; 162: 50-61
    CrossrefPubMedGoogle Scholar
  • 13 Cretti F, Perugini G. Patient dose evaluation for the whole-body low-dose multidetector CT (WBLDMDCT) skeleton study in multiple myeloma (MM). Radiol Medica 2016; 121: 93-105
    PubMedGoogle Scholar
  • 14 Gleeson TG, Moriarty J, Shortt CP. et al. Accuracy of whole-body low-dose multidetector CT (WBLDCT) versus skeletal survey in the detection of myelomatous lesions, and correlation of disease distribution with whole-body MRI (WBMRI). Skeletal Radiol 2009; 38: 225-236
    CrossrefPubMedGoogle Scholar
  • 15 Hansford BG, Silbermann R. Advanced Imaging of Multiple Myeloma Bone Disease. Front Endocrinol (Lausanne) 2018; 9: 436
    CrossrefPubMedGoogle Scholar
  • 16 Suntharalingam S, Mikat C, Wetter A. et al. Whole-body ultra-low dose CT using spectral shaping for detection of osteolytic lesion in multiple myeloma. Eur Radiol 2018; 28: 1-8
    CrossrefPubMedGoogle Scholar
  • 17 Surov A, Bach AG, Tcherkes A. et al. Non-osseous incidental findings in low-dose whole-body CT in patients with multiple myeloma. Br J Radiol 2014; 87: 20140185
    CrossrefPubMedGoogle Scholar
  • 18 Matsue K, Kobayashi H, Matsue Y. et al. Prognostic significance of bone marrow abnormalities in the appendicular skeleton of patients with multiple myeloma. Blood Adv 2018; 2: 1032-1039
    CrossrefPubMedGoogle Scholar
  • 19 Horger M, Kanz L, Denecke B. et al. The benefit of using whole-body, low-close, nonenhanced, multidetector computed tomography for follow-up and therapy response monitoring in patients with multiple myeloma. Cancer 2007; 109: 1617-1626
    CrossrefPubMedGoogle Scholar
  • 20 Dimopoulos MA, Hillengass J, Usmani S. et al. Role of magnetic resonance imaging in the management of patients with multiple myeloma: a consensus statement. J Clin Oncol 2015; 33: 657-664
    CrossrefPubMedGoogle Scholar
  • 21 Bäuerle T, Hillengass J, Fechtner K. et al. Multiple Myeloma and Monoclonal Gammopathy of Undetermined Significance: Importance of Whole-Body versus Spinal MR Imaging. Radiology 2009; 252: 477-485
    CrossrefPubMedGoogle Scholar
  • 22 Mai EK, Hielscher T, Kloth JK. et al. A magnetic resonance imaging-based prognostic scoring system to predict outcome in transplant-eligible patients with multiple myeloma. Haematologica 2015; 100: 818-825
    CrossrefPubMedGoogle Scholar
  • 23 Hillengass J, Weber MA, Kilk K. et al. Prognostic significance of whole-body MRI in patients with monoclonal gammopathy of undetermined significance. Leukemia 2014; 28: 174-178
    CrossrefPubMedGoogle Scholar
  • 24 Spinnato P, Bazzocchi A, Brioli A. et al. Contrast enhanced MRI and18F-FDG PET-CT in the assessment of multiple myeloma: A comparison of results in different phases of the disease. Eur J Radiol 2012; 81: 4013-4018
    CrossrefPubMedGoogle Scholar
  • 25 Zamagni E, Nanni C, Patriarca F. et al. A prospective comparison of 18F-fluorodeoxyglucose positron emission tomography-computed tomography, magnetic resonance imaging and whole-body planar radiographs in the assessment of bone disease in newly diagnosed multiple myeloma. Haematologica 2007; 92: 50-55
    CrossrefPubMedGoogle Scholar
  • 26 Breyer RJ, Mulligan ME, Smith SE. et al. Comparison of imaging with FDG PET/CT with other imaging modalities in myeloma. Skeletal Radiol 2006; 35: 632-640
    CrossrefPubMedGoogle Scholar
  • 27 Baur A, Stäbler A, Brüning R. et al. Diffusion-weighted MR imaging of bone marrow: differentiation of benign versus pathologic compression fractures. Radiology 1998; 207: 349-356
    CrossrefPubMedGoogle Scholar
  • 28 Varettoni M, Corso A, Pica G. et al. Incidence, presenting features and outcome of extramedullary disease in multiple myeloma: A longitudinal study on 1003 consecutive patients. Ann Oncol 2010; 21: 325-330
    CrossrefPubMedGoogle Scholar
  • 29 Walker R, Barlogie B, Haessler J. et al. Magnetic Resonance Imaging in Multiple Myeloma: Diagnostic and Clinical Implications. J Clin Oncol 2007; 25: 1121-1128
    CrossrefPubMedGoogle Scholar
  • 30 Nanni C, Zamagni E, Farsad M. et al. Role of 18F-FDG PET/CT in the assessment of bone involvement in newly diagnosed multiple myeloma: preliminary results. Eur J Nucl Med Mol Imaging 2006; 33: 525-531
    CrossrefPubMedGoogle Scholar
  • 31 Kumar S, Paiva B, Anderson KC. et al. International Myeloma Working Group consensus criteria for response and minimal residual disease assessment in multiple myeloma. Lancet Oncol 2016; 17: e328-e346
    CrossrefPubMedGoogle Scholar
  • 32 Derlin T, Peldschus K, Münster S. et al. Comparative diagnostic performance of18F-FDG PET/CT versus whole-body MRI for determination of remission status in multiple myeloma after stem cell transplantation. Eur Radiol 2013; 23: 570-578
    CrossrefPubMedGoogle Scholar
  • 33 Bartel TB, Haessler J, Brown TLY. et al. F18-fluorodeoxyglucose positron emission tomography in the context of other imaging techniques and prognostic factors in multiple myeloma. Blood 2009; 114: 2068-2076
    PubMedGoogle Scholar
  • 34 Usmani SZ, Mitchell A, Waheed S. et al. Prognostic implications of serial 18-fluoro-deoxyglucose emission tomography in multiple myeloma treated with total therapy 3. Blood 2013; 121: 1819-1823
    CrossrefPubMedGoogle Scholar
  • 35 Zamagni E, Patriarca F, Nanni C. et al. Prognostic relevance of 18-F FDG PET/CT in newly diagnosed multiple myeloma patients treated with up-front autologous transplantation. Blood 2011; 118: 5989-5995
    CrossrefPubMedGoogle Scholar
  • 36 Nanni C, Zamagni E, Celli M. et al. The value of 18F-FDG PET/CT after autologous stem cell transplantation (ASCT) in patients affected by multiple myeloma (MM): Experience with 77 patients. Clin Nucl Med 2013; 38: e74-e79
    CrossrefPubMedGoogle Scholar
  • 37 Lapa C, Lückerath K, Malzahn U. et al. 18 FDG-PET/CT for prognostic stratification of patients with multiple myeloma relapse after stem cell transplantation. Oncotarget 2014; 5: 7381-7391
    CrossrefPubMedGoogle Scholar
  • 38 Hillengass J, Fechtner K, Weber MA. et al. Prognostic significance of focal lesions in whole-body magnetic resonance imaging in patients with asymptomatic multiple myeloma. J Clin Oncol 2010; 28: 1606-1610
    CrossrefPubMedGoogle Scholar
  • 39 Kastritis E, Moulopoulos LA, Terpos E. et al. The prognostic importance of the presence of more than one focal lesion in spine MRI of patients with asymptomatic (smoldering) multiple myeloma. Leukemia 2014; 28: 2402-2403
    CrossrefPubMedGoogle Scholar
  • 40 Moulopoulos LA, Dimopoulos MA, Weber D. et al. Magnetic resonance imaging in the staging of solitary plasmacytoma of bone. J Clin Oncol 1993; 11: 1311-1315
    CrossrefPubMedGoogle Scholar
  • 41 Rasche L, Chavan SS, Stephens OW. et al. Spatial genomic heterogeneity in multiple myeloma revealed by multi-region sequencing. Nat Commun 2017; 8: 268
    CrossrefPubMedGoogle Scholar
  • 42 Zamagni E, Nanni C, Mancuso K. et al. PET/CT improves the definition of complete response and allows to detect otherwise unidentifiable skeletal progression in multiple myeloma. Clin Cancer Res 2015; 21: 4384-4390
    CrossrefPubMedGoogle Scholar
  • 43 Hillengass J, Ritsch J, Merz M. et al. Prognostic Significance Of Parameters Of Dynamic Contrast-Enhanced MRI Detecting Increased Bone Marrow Microcirculation In Monoclonal Plasma Cell Disorders. Blood 2013; 122: 3146
    CrossrefPubMedGoogle Scholar
  • 44 Dutoit JC, Claus E, Offner F. et al. Combined evaluation of conventional MRI, dynamic contrast-enhanced MRI and diffusion weighted imaging for response evaluation of patients with multiple myeloma. Eur J Radiol 2016; 85: 373-382
    CrossrefPubMedGoogle Scholar
  • 45 Pawlyn C, Fowkes L, Otero S. et al. Whole-body diffusion-weighted MRI: A new gold standard for assessing disease burden in patients with multiple myeloma?. Leukemia 2016; 30: 1446-1448
    CrossrefPubMedGoogle Scholar
  • 46 Sachpekidis C, Mosebach J, Freitag MT. et al. Application of 18 F-FDG PET and diffusion weighted imaging (DWI) in multiple myeloma: comparison of functional imaging modalities. Am J Nucl Med Mol Imaging 2015; 5: 479-492
    PubMedGoogle Scholar
  • 47 Horger M, Weisel K, Horger W. et al. Whole-body diffusion-weighted MRI with apparent diffusion coefficient mapping for early response monitoring in multiple myeloma: preliminary results. Am J Roentgenol 2011; 196: W790-W795
    CrossrefPubMedGoogle Scholar
  • 48 Giles SL, Messiou C, Collins DJ. et al. Whole-Body Diffusion-weighted MR Imaging for Assessment of Treatment Response in Myeloma. Radiology 2014; 271: 785-794
    CrossrefPubMedGoogle Scholar
  • 49 Hillengass J, Bäuerle T, Bartl R. et al. Diffusion-weighted imaging for non-invasive and quantitative monitoring of bone marrow infiltration in patients with monoclonal plasma cell disease: A comparative study with histology. Br J Haematol 2011; 153: 721-728
    CrossrefPubMedGoogle Scholar
  • 50 Sachpekidis C, Hillengass J, Goldschmidt H. et al. Comparison of (18)F-FDG PET/CT and PET/MRI in patients with multiple myeloma. Am J Nucl Med Mol Imaging 2015; 5: 469-478
    PubMedGoogle Scholar
  • 51 Lapa C, Knop S, Schreder M. et al. 11C-methionine-PET in multiple myeloma: Correlation with clinical parameters and bone marrow involvement. Theranostics 2016; 6: 254-261
    CrossrefPubMedGoogle Scholar
  • 52 Luckerath K, Lapa C, Albert C. et al. 11C-Methionine-PET: a novel and sensitive tool for monitoring of early response to treatment in multiple myeloma. Oncotarget 2015; 6: 8418-8429
    CrossrefPubMedGoogle Scholar
  • 53 Kosmala A, Weng AM, Heidemeier A. et al. Multiple Myeloma and Dual-Energy CT: Diagnostic Accuracy of Virtual Noncalcium Technique for Detection of Bone Marrow Infiltration of the Spine and Pelvis. Radiology 2018; 286: 205-213
    CrossrefPubMedGoogle Scholar
  • 54 Kosmala A, Weng AM, Krauss B. et al. Dual-energy CT of the bone marrow in multiple myeloma: diagnostic accuracy for quantitative differentiation of infiltration patterns. Eur Radiol 2018; 28: 5083-5090
    CrossrefPubMedGoogle Scholar
  • 55 Burke MC, Garg A, Youngner JM. et al. Initial experience with dual-energy computed tomography-guided bone biopsies of bone lesions that are occult on monoenergetic CT. Skeletal Radiol 2018; 48: 605-613
    PubMedGoogle Scholar

Correspondence

Dr. Aleksander Kosmala
Department of Diagnostic and Interventional Radiology, University-Hospital Würzburg
Oberdürrbacher Straße 6
97080 Würzburg
Germany   
Phone: ++ 49/9 31/20 13 40 00   

  • References

  • 1 Krebs in Deutschland für 2013/2014. Robert Koch-Institut; 2017 11th ed.
    PubMedGoogle Scholar
  • 2 Kyle RA, Gertz MA, Witzig TE. et al. Review of 1027 patients with newly diagnosed multiple myeloma. Mayo Clin Proc 2003; 78: 21-33
    CrossrefPubMedGoogle Scholar
  • 3 Rajkumar SV, Kumar S. Multiple Myeloma: Diagnosis and Treatment. Mayo Clin Proc 2016; 91: 101-119
    CrossrefPubMedGoogle Scholar
  • 4 Rajkumar SV, Dimopoulos MA, Palumbo A. et al. International Myeloma Working Group updated criteria for the diagnosis of multiple myeloma. Lancet Oncol 2014; 15: e538-e548
    CrossrefPubMedGoogle Scholar
  • 5 Terpos E, Dimopoulos MA, Moulopoulos LA. The Role of Imaging in the Treatment of Patients With Multiple Myeloma in 2016. Am Soc Clin Oncol Educ B 2016; 36: e407-e417
    PubMedGoogle Scholar
  • 6 Mihailovic J, Goldsmith SJ. Multiple myeloma:18F-FDG-PET/CT and diagnostic imaging. In: Semin Nucl Med. W.B. Saunders 2015: 16-31
    PubMedGoogle Scholar
  • 7 Hillengass J, Merz M, Delorme S. Minimal residual disease in multiple myeloma: use of magnetic resonance imaging. Semin Hematol 2018; 55: 19-21
    CrossrefPubMedGoogle Scholar
  • 8 Durie BGM, Salmon SE. A clinical staging system for multiple myeloma. Cancer 1975; 36: 842-854
    CrossrefPubMedGoogle Scholar
  • 9 Dimopoulos M, Terpos E, Comenzo RL. et al. International myeloma working group consensus statement and guidelines regarding the current role of imaging techniques in the diagnosis and monitoring of multiple Myeloma. Leukemia 2009; 23: 1545-1556
    CrossrefPubMedGoogle Scholar
  • 10 Moreau P, San Miguel J, Sonneveld P. et al. Multiple myeloma: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up. Ann Oncol 2017; 28: iv52-iv61
    CrossrefPubMedGoogle Scholar
  • 11 Terpos E, Kleber M, Engelhardt M. et al. European myeloma network guidelines for the management of multiple myeloma-related complications. Haematologica 2015; 100: 1254-1266
    CrossrefPubMedGoogle Scholar
  • 12 Regelink JC, Minnema MC, Terpos E. et al. Comparison of modern and conventional imaging techniques in establishing multiple myeloma-related bone disease: A systematic review. Br J Haematol 2013; 162: 50-61
    CrossrefPubMedGoogle Scholar
  • 13 Cretti F, Perugini G. Patient dose evaluation for the whole-body low-dose multidetector CT (WBLDMDCT) skeleton study in multiple myeloma (MM). Radiol Medica 2016; 121: 93-105
    PubMedGoogle Scholar
  • 14 Gleeson TG, Moriarty J, Shortt CP. et al. Accuracy of whole-body low-dose multidetector CT (WBLDCT) versus skeletal survey in the detection of myelomatous lesions, and correlation of disease distribution with whole-body MRI (WBMRI). Skeletal Radiol 2009; 38: 225-236
    CrossrefPubMedGoogle Scholar
  • 15 Hansford BG, Silbermann R. Advanced Imaging of Multiple Myeloma Bone Disease. Front Endocrinol (Lausanne) 2018; 9: 436
    CrossrefPubMedGoogle Scholar
  • 16 Suntharalingam S, Mikat C, Wetter A. et al. Whole-body ultra-low dose CT using spectral shaping for detection of osteolytic lesion in multiple myeloma. Eur Radiol 2018; 28: 1-8
    CrossrefPubMedGoogle Scholar
  • 17 Surov A, Bach AG, Tcherkes A. et al. Non-osseous incidental findings in low-dose whole-body CT in patients with multiple myeloma. Br J Radiol 2014; 87: 20140185
    CrossrefPubMedGoogle Scholar
  • 18 Matsue K, Kobayashi H, Matsue Y. et al. Prognostic significance of bone marrow abnormalities in the appendicular skeleton of patients with multiple myeloma. Blood Adv 2018; 2: 1032-1039
    CrossrefPubMedGoogle Scholar
  • 19 Horger M, Kanz L, Denecke B. et al. The benefit of using whole-body, low-close, nonenhanced, multidetector computed tomography for follow-up and therapy response monitoring in patients with multiple myeloma. Cancer 2007; 109: 1617-1626
    CrossrefPubMedGoogle Scholar
  • 20 Dimopoulos MA, Hillengass J, Usmani S. et al. Role of magnetic resonance imaging in the management of patients with multiple myeloma: a consensus statement. J Clin Oncol 2015; 33: 657-664
    CrossrefPubMedGoogle Scholar
  • 21 Bäuerle T, Hillengass J, Fechtner K. et al. Multiple Myeloma and Monoclonal Gammopathy of Undetermined Significance: Importance of Whole-Body versus Spinal MR Imaging. Radiology 2009; 252: 477-485
    CrossrefPubMedGoogle Scholar
  • 22 Mai EK, Hielscher T, Kloth JK. et al. A magnetic resonance imaging-based prognostic scoring system to predict outcome in transplant-eligible patients with multiple myeloma. Haematologica 2015; 100: 818-825
    CrossrefPubMedGoogle Scholar
  • 23 Hillengass J, Weber MA, Kilk K. et al. Prognostic significance of whole-body MRI in patients with monoclonal gammopathy of undetermined significance. Leukemia 2014; 28: 174-178
    CrossrefPubMedGoogle Scholar
  • 24 Spinnato P, Bazzocchi A, Brioli A. et al. Contrast enhanced MRI and18F-FDG PET-CT in the assessment of multiple myeloma: A comparison of results in different phases of the disease. Eur J Radiol 2012; 81: 4013-4018
    CrossrefPubMedGoogle Scholar
  • 25 Zamagni E, Nanni C, Patriarca F. et al. A prospective comparison of 18F-fluorodeoxyglucose positron emission tomography-computed tomography, magnetic resonance imaging and whole-body planar radiographs in the assessment of bone disease in newly diagnosed multiple myeloma. Haematologica 2007; 92: 50-55
    CrossrefPubMedGoogle Scholar
  • 26 Breyer RJ, Mulligan ME, Smith SE. et al. Comparison of imaging with FDG PET/CT with other imaging modalities in myeloma. Skeletal Radiol 2006; 35: 632-640
    CrossrefPubMedGoogle Scholar
  • 27 Baur A, Stäbler A, Brüning R. et al. Diffusion-weighted MR imaging of bone marrow: differentiation of benign versus pathologic compression fractures. Radiology 1998; 207: 349-356
    CrossrefPubMedGoogle Scholar
  • 28 Varettoni M, Corso A, Pica G. et al. Incidence, presenting features and outcome of extramedullary disease in multiple myeloma: A longitudinal study on 1003 consecutive patients. Ann Oncol 2010; 21: 325-330
    CrossrefPubMedGoogle Scholar
  • 29 Walker R, Barlogie B, Haessler J. et al. Magnetic Resonance Imaging in Multiple Myeloma: Diagnostic and Clinical Implications. J Clin Oncol 2007; 25: 1121-1128
    CrossrefPubMedGoogle Scholar
  • 30 Nanni C, Zamagni E, Farsad M. et al. Role of 18F-FDG PET/CT in the assessment of bone involvement in newly diagnosed multiple myeloma: preliminary results. Eur J Nucl Med Mol Imaging 2006; 33: 525-531
    CrossrefPubMedGoogle Scholar
  • 31 Kumar S, Paiva B, Anderson KC. et al. International Myeloma Working Group consensus criteria for response and minimal residual disease assessment in multiple myeloma. Lancet Oncol 2016; 17: e328-e346
    CrossrefPubMedGoogle Scholar
  • 32 Derlin T, Peldschus K, Münster S. et al. Comparative diagnostic performance of18F-FDG PET/CT versus whole-body MRI for determination of remission status in multiple myeloma after stem cell transplantation. Eur Radiol 2013; 23: 570-578
    CrossrefPubMedGoogle Scholar
  • 33 Bartel TB, Haessler J, Brown TLY. et al. F18-fluorodeoxyglucose positron emission tomography in the context of other imaging techniques and prognostic factors in multiple myeloma. Blood 2009; 114: 2068-2076
    PubMedGoogle Scholar
  • 34 Usmani SZ, Mitchell A, Waheed S. et al. Prognostic implications of serial 18-fluoro-deoxyglucose emission tomography in multiple myeloma treated with total therapy 3. Blood 2013; 121: 1819-1823
    CrossrefPubMedGoogle Scholar
  • 35 Zamagni E, Patriarca F, Nanni C. et al. Prognostic relevance of 18-F FDG PET/CT in newly diagnosed multiple myeloma patients treated with up-front autologous transplantation. Blood 2011; 118: 5989-5995
    CrossrefPubMedGoogle Scholar
  • 36 Nanni C, Zamagni E, Celli M. et al. The value of 18F-FDG PET/CT after autologous stem cell transplantation (ASCT) in patients affected by multiple myeloma (MM): Experience with 77 patients. Clin Nucl Med 2013; 38: e74-e79
    CrossrefPubMedGoogle Scholar
  • 37 Lapa C, Lückerath K, Malzahn U. et al. 18 FDG-PET/CT for prognostic stratification of patients with multiple myeloma relapse after stem cell transplantation. Oncotarget 2014; 5: 7381-7391
    CrossrefPubMedGoogle Scholar
  • 38 Hillengass J, Fechtner K, Weber MA. et al. Prognostic significance of focal lesions in whole-body magnetic resonance imaging in patients with asymptomatic multiple myeloma. J Clin Oncol 2010; 28: 1606-1610
    CrossrefPubMedGoogle Scholar
  • 39 Kastritis E, Moulopoulos LA, Terpos E. et al. The prognostic importance of the presence of more than one focal lesion in spine MRI of patients with asymptomatic (smoldering) multiple myeloma. Leukemia 2014; 28: 2402-2403
    CrossrefPubMedGoogle Scholar
  • 40 Moulopoulos LA, Dimopoulos MA, Weber D. et al. Magnetic resonance imaging in the staging of solitary plasmacytoma of bone. J Clin Oncol 1993; 11: 1311-1315
    CrossrefPubMedGoogle Scholar
  • 41 Rasche L, Chavan SS, Stephens OW. et al. Spatial genomic heterogeneity in multiple myeloma revealed by multi-region sequencing. Nat Commun 2017; 8: 268
    CrossrefPubMedGoogle Scholar
  • 42 Zamagni E, Nanni C, Mancuso K. et al. PET/CT improves the definition of complete response and allows to detect otherwise unidentifiable skeletal progression in multiple myeloma. Clin Cancer Res 2015; 21: 4384-4390
    CrossrefPubMedGoogle Scholar
  • 43 Hillengass J, Ritsch J, Merz M. et al. Prognostic Significance Of Parameters Of Dynamic Contrast-Enhanced MRI Detecting Increased Bone Marrow Microcirculation In Monoclonal Plasma Cell Disorders. Blood 2013; 122: 3146
    CrossrefPubMedGoogle Scholar
  • 44 Dutoit JC, Claus E, Offner F. et al. Combined evaluation of conventional MRI, dynamic contrast-enhanced MRI and diffusion weighted imaging for response evaluation of patients with multiple myeloma. Eur J Radiol 2016; 85: 373-382
    CrossrefPubMedGoogle Scholar
  • 45 Pawlyn C, Fowkes L, Otero S. et al. Whole-body diffusion-weighted MRI: A new gold standard for assessing disease burden in patients with multiple myeloma?. Leukemia 2016; 30: 1446-1448
    CrossrefPubMedGoogle Scholar
  • 46 Sachpekidis C, Mosebach J, Freitag MT. et al. Application of 18 F-FDG PET and diffusion weighted imaging (DWI) in multiple myeloma: comparison of functional imaging modalities. Am J Nucl Med Mol Imaging 2015; 5: 479-492
    PubMedGoogle Scholar
  • 47 Horger M, Weisel K, Horger W. et al. Whole-body diffusion-weighted MRI with apparent diffusion coefficient mapping for early response monitoring in multiple myeloma: preliminary results. Am J Roentgenol 2011; 196: W790-W795
    CrossrefPubMedGoogle Scholar
  • 48 Giles SL, Messiou C, Collins DJ. et al. Whole-Body Diffusion-weighted MR Imaging for Assessment of Treatment Response in Myeloma. Radiology 2014; 271: 785-794
    CrossrefPubMedGoogle Scholar
  • 49 Hillengass J, Bäuerle T, Bartl R. et al. Diffusion-weighted imaging for non-invasive and quantitative monitoring of bone marrow infiltration in patients with monoclonal plasma cell disease: A comparative study with histology. Br J Haematol 2011; 153: 721-728
    CrossrefPubMedGoogle Scholar
  • 50 Sachpekidis C, Hillengass J, Goldschmidt H. et al. Comparison of (18)F-FDG PET/CT and PET/MRI in patients with multiple myeloma. Am J Nucl Med Mol Imaging 2015; 5: 469-478
    PubMedGoogle Scholar
  • 51 Lapa C, Knop S, Schreder M. et al. 11C-methionine-PET in multiple myeloma: Correlation with clinical parameters and bone marrow involvement. Theranostics 2016; 6: 254-261
    CrossrefPubMedGoogle Scholar
  • 52 Luckerath K, Lapa C, Albert C. et al. 11C-Methionine-PET: a novel and sensitive tool for monitoring of early response to treatment in multiple myeloma. Oncotarget 2015; 6: 8418-8429
    CrossrefPubMedGoogle Scholar
  • 53 Kosmala A, Weng AM, Heidemeier A. et al. Multiple Myeloma and Dual-Energy CT: Diagnostic Accuracy of Virtual Noncalcium Technique for Detection of Bone Marrow Infiltration of the Spine and Pelvis. Radiology 2018; 286: 205-213
    CrossrefPubMedGoogle Scholar
  • 54 Kosmala A, Weng AM, Krauss B. et al. Dual-energy CT of the bone marrow in multiple myeloma: diagnostic accuracy for quantitative differentiation of infiltration patterns. Eur Radiol 2018; 28: 5083-5090
    CrossrefPubMedGoogle Scholar
  • 55 Burke MC, Garg A, Youngner JM. et al. Initial experience with dual-energy computed tomography-guided bone biopsies of bone lesions that are occult on monoenergetic CT. Skeletal Radiol 2018; 48: 605-613
    PubMedGoogle Scholar

   Permissions and Reprints
Zoom Image
Fig. 1 Coronal a and sagittal b computed tomography images of the spine and pelvis show multifocal osteolysis in a 60-year-old male patient with multiple myeloma. On the corresponding conventional skeletal radiography images of the thoracic c and lumbar d spine even the largest osteolytic lesion with advanced destruction of the T4 vertebral body is largely occult, while the advanced destruction of the L4 vertebral body is challenging to spot (arrows in b).
Zoom Image
Fig. 2 Coronal computed tomography images of a 64-year-old male patient with multiple myeloma in complete remission a, and 4 months later during relapse b. The humeral metaphyses show subtle osteolysis and scalloping even during remission a, most likely due to a treated infiltration. While the bone marrow of the humerus appears normal and fatty in a without any signs of cellular infiltration, a diffuse hyperdense bone marrow infiltration (arrows) can be readily seen during relapse b.
Zoom Image
Fig. 3 Bone marrow infiltration patterns of multiple myeloma on magnetic resonance imaging using sagittal fat-saturated T1-weighted images a–e. Normal-appearing bone marrow shows a homogeneously T1w hyperintense distribution due to the fat content a. Focal lesions are visualized with a similar or lower signal intensity compared to the musculature or healthy intervertebral discs (b, arrows with an open arrowhead point to exemplary focal lesions; pathological fractures are seen in T10 and T12 as well as L1, 4, and 5). A diffuse infiltration is indicated by a homogeneous T1w hypointense bone marrow compared to the musculature or neighboring intervertebral discs c. Simultaneous visualization of a generalized T1w hypointense bone marrow and additional focal lesions marks a mixed focal and diffuse infiltration (d, arrows with a closed arrowhead point to exemplary focal lesions, that in this patient appear relatively T1w hyperintense due to high-grade diffuse T1w hypointense infiltration of the surrounding marrow). A “salt-and-pepper” pattern shows a disseminated “micronodular” T1w hypointense infiltration against a background of normal T1w hyperintense fatty bone marrow e, with a simultaneously normal fat-saturated T2w imaging appearance (not shown here).
Zoom Image
Fig. 4 Patterns of bone marrow infiltration in fat-saturated T2-weighted images a–d. Patients with a normal-appearing bone marrow and patients with a salt-and-pepper pattern show homogeneous hypointense bone marrow on T2w images a. Focal lesions appear hyperintense on fat-saturated T2w images b. A diffuse infiltration pattern is marked by homogeneously hyperintense bone marrow on fat-saturated T2w images c. In a mixed imaging pattern, circumscribed focal hyperintense lesions are visualized within homogeneous hyperintense bone marrow on fat-saturated T2w images (arrow in d).
Zoom Image
Fig. 5 Axial FDG PET/CT image a and corresponding b800 DWI image b of a 69-year-old male patient with multiple myeloma. Primary extramedullary disease of the pleura and of the liver in segment 4a (short arrows in a and b) as well as secondary extraosseous lesions adjacent to the ribs show a vivid hypermetabolism on PET/CT (a) and appear hyperintense on DWI b. Note: FDG = 18F-fluorodeoxyglucose, PET/CT = positron emission tomography/computed tomography, DWI = diffusion-weighted imaging.
Zoom Image
Fig. 6 Axial b800 a, c and ADC b, d DWI images of a 69-year-old patient with multiple myeloma. The baseline exam a, b before initiation of therapy reveals multiple osseous and extraosseous lesions, which show restricted diffusion on the ADC-map (arrows in b). 10 days after VCD therapy onset, myeloma lesions become less hyperintense in the b800 images and show increasing ADC values (arrows in d), which can be attributed to a decline in cellularity due to early therapy response. Note: DWI = diffusion-weighted imaging, ADC = apparent diffusion coefficient, VCD = Velcade® (bortezomib), cyclophosphamide, dexamethasone.
Zoom Image
Fig. 7 Axial CT of the pelvis in a 76-year-old male patient with multiple myeloma. The non-lytic lesions (arrows in a and b) can barely be seen in the bone window a or soft tissue window b settings. Both lesions show hypermetabolism on PET/CT (arrows in c). Using the dual-energy CT color overlay after virtual calcium removal, both lesions can readily be seen depicted in green (arrows in d). Note: CT = computed tomography, PET/CT = positron emission tomography/computed tomography.
Zoom Image
Abb. 1 Koronare a und sagittale b Computertomografie von Wirbelsäule und Becken, auf der zahlreiche Osteolysen bei einem 60-jährigen Patienten mit Multiplem Myelom zu erkennen sind. Auf den entsprechenden konventionellen seitlichen Aufnahmen von BWS c und LWS d ist die größte Osteolyse mit fortgeschrittener Destruktion von BWK 4 weitgehend okkult, die ausgeprägte Destruktion der Vorderkante von LWK 4 nur schwer erkennbar (Pfeile in b).
Zoom Image
Abb. 2 Koronare Computertomografie eines 64-jährigen Patienten mit Multiplem Myelom in stringenter Komplettremission a sowie 4 Monate später in der Rezidiv-Situation b. An den Metaphysen der Humeri lassen sich bereits in a feine Osteolysen sowie ein Scallopping abgrenzen, vermutlich durch einen früheren, inzwischen behandelten Befall. Während sich der Markraum des Humerus beidseits in a altersentsprechend fetthaltig und daher ohne Hinweis auf ein zelluläres Infiltrat darstellt, ist in der Rezidiv-Situation b eine deutliche diffuse Dichteanhebung im Sinne einer Markrauminfiltration abzugrenzen (Pfeile).
Zoom Image
Abb. 3 Muster der Knochenmarkinfiltration des Multiplen Myeloms in der Magnetresonanztomografie anhand von sagittalen T1-gewichteten, nicht fettgesättigten Bildern a–e. Ein normales Knochenmarkbild erscheint aufgrund des Fettgehalts T1w recht homogen hyperintens a. Fokale Läsionen zeigen T1w eine ähnliche oder niedrigere Signalintensität wie Muskulatur oder normale Bandscheiben (b, pathologische Sinterungsfrakturen von BWK 10 und 12 sowie LWK 1, 4 und 5; Pfeile mit offener Spitze zeigen exemplarische fokale Läsionen). Ein im Vergleich zu Muskel bzw. angrenzenden Bandscheibenfächern T1w homogen hypointenses Knochenmarkbild kennzeichnet eine diffuse Infiltration c. Das gleichzeitige Vorliegen eines T1w-generalisiert homogen hypointensen Knochenmarkbildes und zusätzlich abgrenzbarer fokaler Läsionen kennzeichnet den gemischt fokal/diffusen Befall (d, Pfeile mit geschlossener Spitze zeigen exemplarische fokale Läsionen, die bei diesem Patienten aufgrund des hochgradig diffus infiltrierten T1w-hypointensen Knochenmarks verhältnismäßig signalreich erscheinen). Das „salt-and-pepper“-Muster zeigt disseminiert kleinnoduläre, T1w-hypointense Herde vor dem Hintergrund eines normalen T1w-hyperintensen Fettmarks e bei gleichzeitig normalem fettgesättigtem T2w-Bild (hier nicht gezeigt).
Zoom Image
Abb. 4 Muster der Knochenmarkinfiltration in fettgesättigten T2-gewichteten Aufnahmen a–d. Patienten mit einem normalen Knochenmarkbild und Patienten mit einer Infiltration nach „salt-and-pepper“-Muster weisen ein homogen T2w-hypointenses Knochenmark auf a. Fokale Läsionen erscheinen in fettgesättigten T2-gewichteten Aufnahmen hyperintens b. Ein diffuses Knochenmarkinfiltrationsmuster ist gekennzeichnet durch eine homogene Signalanhebung des Knochenmarks in fettgesättigten T2-gewichteten Aufnahmen c. Beim gemischten Befalls-Muster sind in fettgesättigten T2-gewichteten Aufnahmen zusätzlich zur homogenen Signalanhebung des Knochenmarks auch umschriebene, hyperintense fokale Läsionen abgrenzbar (Pfeil in d).
Zoom Image
Abb. 5 Axiales FDG PET/CT-Bild a und korrelierendes b800-Bild der DWI b eines 69-jährigen Patienten mit Multiplem Myelom. Primär extraossärer Myelom-Befall der Pleura sowie der Leber in Segment 4a (jeweils kurze Pfeile in a und b) sowie sekundär extraossäre Herde angrenzend an die Rippen beidseits (jeweils lange Pfeile in a und b) zeigen einen Hypermetabolismus im PET/CT a und kommen analog in der DWI hyperintens zur Darstellung b. Anmerkung: FDG = 18F-Fluorodeoxyglukose, PET/CT = Positronen-Emissionstomografie/Computertomografie, DWI = Diffusionsbildgebung.
Zoom Image
Abb. 6 Axiale b800- a, c und ADC b, d -Bilder der DWI eines 69-jährigen Patienten mit Multiplem Myelom. In der Baseline-Untersuchung vor Therapiebeginn a, b zeigen sich multiple ossäre und extraossäre, in der ADC-Map diffusionseingeschränkte Herde (Pfeile in b). 10 Tage nach Beginn der VCD-Therapie imponieren die Herde in den b800-Bildern weniger hyperintens mit einem Anstieg der ADC-Werte (Pfeile in d), was man auf eine Abnahme der Zelldichte aufgrund eines frühen Therapieansprechens zurückführen kann. Anmerkung: DWI = Diffusionsbildgebung, ADC = apparenter Diffusionskoeffizient, VCD = Velcade® (Bortezomib), Cyclophosphamid, Dexamethason.
Zoom Image
Abb. 7 Axiales CT des Beckens bei einem 76-jährigen Patienten mit Multiplem Myelom. Im Knochenfenster a und Weichteilfenster b sind die nicht lytischen Herde kaum erkennbar (Pfeile in a und b). Im PET/CT-Bild zeigen beide Herde einen Hypermetabolismus (Pfeile in c). Im Farb-Overlay der Dual-Energy-CT nach virtueller Kalziumentfernung kommen beide Herde grün demarkiert zur Darstellung (Pfeile in d). Anmerkung: CT = Computertomografie, PET/CT = Positronen-Emissionstomografie/Computertomografie.