Abstract
Malignant bone tumors are either primary or metastatic in nature. The high sensitivity and accuracy of 99mTc-MDP bone scintigraphy in diagnosing bone metastasis were established as long ago as 1961 (Fleming et al., Radiology 77:635–636, 1961). In contrast, its usefulness in the investigation of primary bone tumors, both malignant and benign, appears not to be fully appreciated. The main reason is the low diagnostic yield of conventional planar bone scintigraphy; this is true. However, recognizing the fact that the magnified images of pinhole scintigraphy can depict anatomy in amazing detail along with unique metabolic information, a number of primary tumors and tumorlike diseases of bone have become among the most important and challenging indications for bone scanning.
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Malignant bone tumors are either primary or metastatic in nature. The high sensitivity and accuracy of 99mTc-MDP bone scintigraphy in diagnosing bone metastasis were established as long ago as 1961 (Fleming et al. 1961) (Fig. 1.2). In contrast, its usefulness in the investigation of primary bone tumors, both malignant and benign, appears not to be fully appreciated. The main reason is the low diagnostic yield of conventional planar bone scintigraphy; this is true. However, recognizing the fact that the magnified images of pinhole scintigraphy can depict anatomy in amazing detail along with unique metabolic information, a number of primary tumors and tumorlike diseases of bone have become among the most important and challenging indications for bone scanning.
In actuality 99mTc-MDP bone scintigraphy reinforced with the pinhole magnification technique and nuclear angiography has been demonstrated to be helpful in the diagnosis of primary bone tumors. The malignant tumors so far studied by this means include skeletal metastases and primary osteosarcoma, fibrosarcoma, Ewing’s sarcoma, multiple myeloma, leukemia, and lymphoma, and the benign tumors comprise osteoid osteoma, enchondroma, osteochondroma, simple bone cyst, and giant cell tumor (Bahk 1996; Bahk 1998; Kim et al. 1992). The method has also been applied to (a) the mapping of the multiple lesions in polyostotic diseases such as enchondromatosis or Ollier’s disease, familial exostosis, fibrous dysplasia, and histiocytosis X (Kirchner and Simon 1981); (b) preoperative localization of the nidus in osteoid osteoma in flat or irregular bones in particular (Lisbona and Rosenthall 1979); (c) detection of the intramedullary skip metastasis in osteosarcoma and giant cell tumor (Levine et al. 1984); (d) assessment of regional tumor extent; (e) evaluation of tumors with ambiguous radiographic and histological findings; (f) distinction among osteosarcoma, Ewing’s sarcoma, and chondrosarcoma (McLean and Murray 1984) and between bone cyst and cystic bone lesions (Hudson 1984); and (g) unexplained bone pains.
The use of gallium-67 citrate, thallium-201 chloride, 99mTc-MIBI, and other agents for bone tumors is not considered in this chapter since these radiopharmaceuticals have fully been described in numerous publications including standard nuclear medicine textbooks and a number of excellent review articles (Nadel and Rossleigh 1995; Neumann et al. 1995; Waxman 1995; Focacci et al. 1998; Pinkas et al. 2001).
17.1 Metastasis
Radiography plays a relatively less crucial role in bone metastases in the early phase when bone changes are minimal or undetectable. It is also true that radiography is less suitable for the diagnosis of metastases in anatomically complex and thickly overshadowed bones or conversely in small or thin bones such as the cervical and thoracic vertebrae, the sternum, the ribs, the lumbosacral junction, and the sacroiliac joints. The reason is simply that osteolysis or neoplastic osteogenesis in those bones and structures is easily hidden unless the change is overt. Severe porosis in elderly and bed-ridden patients prevents radiographic detection of metastases and often makes conventional or computed tomography powerless. Not infrequently, however, 99mTc-MDP bone scintigraphy diagnoses radiographically invisible or uncertain metastases because they accumulate tracer emitting enough γ-rays from within porotic or thin bones (Fig. 17.1) or through thick or superimposed bones (Fig. 17.2). In addition, whole-body scanning advantageously permits scrutiny of the entire skeleton. In particular, the early metastasis of pediatric malignant tumors deserves a high index of suspicion in differential diagnosis (Bahk et al. 2017). For example, if only the skull is radiographed for local swelling on the forehead, the true state of affairs may be disguised as a local pathology, while the cranial lesion is just one of multiple metastases (Fig. 17.3).
Three basic radiographic changes of malignant metastases are osteolysis, osteogenesis, and a combination of both. The individual bone change is not specific by itself, but certain features or patterns are of diagnostic value. For example, the metastasis from renal cell carcinoma is often lytic and solitary (Fig. 17.4a), and the metastases from prostate carcinoma are usually osteoblastic and multiple or diffuse (Fig. 17.5a). It is also worth remembering that bronchogenic carcinomas, the squamous cell variety in particular (Greenspan and Norman 1988) (Fig. 17.6a), strongly tend to eccentrically metastasize to the cortex (Deutch and Resnick 1980), and multiple myeloma produces characteristic punched-out or soap bubble-like lytic lesions in the skull, spine, pelvis, and proximal limb bones (Fig. 17.7a).
99mTc-MDP bone scanning is highly regarded for its ability to diagnose metastases, especially when the primary tumor has a great propensity toward early dissemination (Pistenma et al. 1975; Kirchner and Simon 1981). Its usefulness in detecting both distant and local intramedullary spread of a malignancy is well appreciated, making the study a sine qua non in the staging and managing of many malignant tumors (Fogelman and McKillop 1991) (Fig. 17.8). It should also be emphasized that ordinary scintigraphy has three pitfalls: relatively high false-negative results, ambiguous photopenic manifestation, and the lack of specificity in the majority of individual lesions. Previously, the incidence of false-negative bone scintigraphy in metastases was reported to be as high as 3% (Pistenma et al. 1975; Citrin and McKillop 1978). Publications also indicated that in a small percentage of patients, radiography could detect metastases that were not visualized on scintigraph. The main reasons are the smallness and photopenic presentation. However, many such lesions can correctly be diagnosed by properly using pinhole scintigraphy (the closer the detector to the objects, the higher the resolution and the greater the sensitivity), dramatically reducing the incidence of false-negative scans. Indeed, magnified scintigraphy can visualize not only tiny bone metastases (Fig. 17.9) but also soft-tissue invasion when richly vascularized or mineralized (Fig. 17.10).
On the other hand, elusive photopenic metastases can be identified as such by noting reactive tracer uptake in the periphery of the lesion on the pinhole scintigraph (Fig. 17.11). Among the primary malignancies whose metastatic lesions are often photopenic, carcinomas of the kidney (Kim et al. 1983) (Figs. 17.4 and 17.11), stomach (Fig. 17.12a), breast (Fig. 17.12b), larynx (Fig. 17.12c), and biliary tract (Fig. 17.12d) deserve mention. In addition, the involvement of certain bones has been related to malignant metastases. Examples are the “hot” areas in the calvaria, the scapula, the sternum, the pelvis, the vertebra, and the long-bone shaft (Kirchner and Simon 1981). Generally, however, no tumor-specific pattern of bone metastases has been recognized because the metastatic behavior of malignant tumors is so diverse and unpredictable. As shown in Fig. 17.13, different carcinomas can cause metastasis that shows exactly the same scintigraphic sign such as fusiform intracortical tracer uptake: the primary tumors were bronchogenic carcinoma in Fig. 17.13a and renal cell carcinoma in Fig. 17.13b. Conversely, it is also true that the same primary carcinomas create metastases of different types in two different bones at the same time (Fig. 17.14) or simultaneous mixed-type metastasis in the same bone (Fig. 17.15).
The multiplicity is a distinctive feature of metastasis. Indeed, the diagnosis becomes likelier if lesions are scattered randomly with the heavier involvement of the bones containing active hematopoietic marrow (Fig. 17.16). Metastases are called the “superscan” when diffuse and extensive (Fig. 17.17). Cranial spread of carcinoma may be considered as a modified expression of widespread metastasis that is not yet systemic. The number of bone metastases may vary from a few to numerous and even innumerable, and the scintigraphic expression may be either “hot” or “cold.” Radiographic changes are predominantly osteolytic, mixed, or osteoblastic. Figure 17.18 demonstrates innumerable radiographically geographic and scintigraphically photopenic cranial metastases from esophageal carcinoma, and Fig. 17.19 is an example of scanty mixed-type cranial metastases from breast carcinoma.
As in certain primary bone tumors (McLean and Murray 1984; Goodgold et al. 1984; Hudson 1984), the characteristics of metastasis can be analyzed scintigraphically by the pinhole technique (Bahk et al. 1987). As predicted by McKillop (1987), it is not uncommon that pinhole scintigraphy depicts a photopenic component within apparently “hot” lesions shown on an ordinary scintigraph, giving rise to a ringlike or picture frame-like appearance. Pathologically, photopenia is related to osteonecrosis, hypovascularity, and aggressive invasion and is typically seen in metastases from carcinoma of the lung (Fig. 17.20a), breast (Fig. 17.20b), stomach, and kidney. The “ring” may be single or double and simple or signet shaped. Conversely, the pinhole scan occasionally discloses septum-like or mottled areas of tracer uptake within photopenic metastases. The bone metastasis from follicular thyroid carcinoma is a typical example (Kim et al. 1993) (Fig. 17.21). As discussed above, photopenic changes are encountered more commonly in metastases from renal cell carcinoma and occasionally in those from carcinomas of the lung, stomach, breast, and head and neck.
Pinhole scintigraphy plays a decisive role in discriminating vertebral metastasis (Fig. 17.22) from infection (Fig. 17.23) and fracture (Fig. 17.24), all of which radiographically manifest as bone destruction (Bahk et al. 1987). Pinhole scanning is also extremely valuable in the staging of malignant tumors and searching for distant metastases since the entire skeleton can be scrutinized (Fig. 17.25). In the investigation of an early metastasis, a high index of suspicion and keen judgment cannot be overemphasized. However, trifling a lesion may appear at first scanning; it should not be dismissed at once but rather be closely followed up with great concern preferably in 3 months at first, particularly when the primary tumor has a strong proclivity toward early and high-rate bone metastasis (Tanaka et al. 1991). One notorious tumor of this kind is breast carcinoma. The case presented in Fig. 17.26 was a 47-year-old female patient with well-differentiated invasive ductal adenocarcinoma of the right breast with positive axillary nodes. The first follow-up scintigraph was taken 10 months after mastectomy. There was a tiny, ambiguous uptake in the lateral edge of the right 11th rib. The second follow-up was 8 months later and showed unmistakable metastasis. Fortunately, the lesion had remained solitary.
Direct invasion of local bone is another mode of metastasis. Well-known examples are Pancoast’s tumor of the thoracic inlet (Fig. 17.27) and peripherally located lung carcinomas with contiguous invasion of the local rib (Fig. 17.28), rectal carcinoma with spread to the sacrum, and nasopharyngeal cancer with neighboring bone invasion (see “Nasopharyngeal Cancer” in Chap. 20). The direct rib invasion may (Fig. 17.27) or may not show tracer uptake (Fig. 17.28), requiring pinhole scintigraphy for accurate diagnosis (Fig. 17.27). Pinhole scintigraphy is very useful for the separate delineation of individual metastatic lesions that are closely positioned on the planar scintigraph (Fig. 17.29).
Cortical bone metastases occur as the result of hematogenous dissemination of tumor cells from almost any kind of carcinoma (Coerkamp and Kroon 1988). Extended application of the pinhole technique by us to the analysis of long-bone metastases has been shown to be highly rewarding. Indeed, pinhole scanning distinguishes selective involvement of the cortex (Fig. 17.30), periosteum (Fig. 17.6), endosteum (Fig. 17.31), panosteum or all bone layers (Fig. 17.32), and medullary space (Fig. 17.33). In contrast to the absolute high prevalence of axial bone involvement, metastases are extremely rare in the bones of the hands and feet (Asthana et al. 2001; Bahk et al. 2006) (Fig. 17.34) and uncommon in the patella (Fig. 17.35) and mandible (Fig. 17.11).
The last but not least important use of bone scintigraphy in skeletal metastases is intra- and posttherapeutic follow-up (Gabuniia et al. 1989; Cook and Fogelman 2001). Pinhole scanning is particularly useful in this situation since anatomy and pathology are appreciated in greater detail. This examination efficiently and reliably portrays, first, treatment-naive metastasis (Fig. 17.36a), the flare phenomenon (Fig. 17.36b), and, finally, the cured state (Fig. 17.36c) after adjuvant chemotherapy or external irradiation. The flare is a transient increase in the intensity of bone uptake during treatment, usually chemotherapy, with subsequent recovery. In one recent series, 24.4% of 33 patients who received chemotherapy for non-small cell lung carcinoma showed the flare phenomenon (Lemieux et al. 2002).
17.1.1 Bone Marrow Scintigraphy in Metastasis
Cancer cells are carried to the bone marrow via the bloodstream and are anchored and implanted in the medullary sinusoidal arteries. Surviving tumor cells are facilitated to extravasate into the marrow space because blood flow is sluggish, the endothelium is loose, and the basement membrane is not present. Bone marrow metastases can occur without cortical involvement, for example, in breast carcinoma (Kamby et al. 1987). 99mTc-NCA95 bone marrow scintigraphy can sensitively and accurately detect metastases, which are visualized as photopenic lesions (Fig. 17.37a). This finding sharply contrasts with the photodense (increased uptake) manifestation on 99mTc-MDP scans (Fig. 17.37b). Approximately 90% of bone marrow metastases are blood borne, and, hence it is natural that bone marrow metastases exist in the absence of affected bone (Fig. 17.38). The agents for bone marrow scanning are largely limited, including only 99mTc nanocolloid and 99mTc-labeled anti-nonspecific cross-reacting antigen (anti-NCA) 95.
Immunoscintigraphy has been shown to be a sensitive indicator of the presence and extent of malignant marrow infiltration (Reske et al. 1989; Duncker et al. 1990). It can distinguish malignancy from benignity in patients with an equivocal 99mTc-MDP bone scintigraphic change (Lee et al. 1995). The sensitivity and specificity were 100% and 79%, respectively. False-positives occur in degenerative arthritis of the spine, the marrow of which has been replaced with fat. If a marrow scan defect is found in concordance with a positive bone scan, radiography is mandatory to exclude benign conditions such as red marrow involution (Cooper et al. 1992), focal osteonecrosis (Haubold-Reuter et al. 1993), Paget’s disease, and bone infarction (Yuasa et al. 1991).
Duncker et al. (1990) assessed the usefulness of immunoscintigraphy in patients with breast cancer suspected of having bone metastasis, finding marrow defects in 25 of 32 patients and bone invasion subsequently confirmed in 23 of 25 patients. 99mTc-MDP bone scintigraphy detected metastases in 17 of 32 patients, whereas anti-NCA95 antibody scan detected more metastatic sites in 12 of 17 patients. Other investigators have also reported that bone marrow scintigraphy is superior to bone scintigraphy in diagnosing metastases in patients with carcinomas of the lung, kidney, bladder, and prostate (Widding et al. 1990; Bourgeois et al. 1991) (Fig. 17.38). However, Bourgeois et al. found that the specificity of bone scan was 100% compared to 87% specificity for marrow scan.
17.2 Primary Malignant Bone Tumors
Radiography is the single most efficient imaging method for primary bone tumors, both benign and malignant. Accordingly, bone scintigraphy was once not enthusiastically explored in primary bone tumors. However, with the popularization of refined gamma cameras, bone tumors have been subjected to extensive scintigraphic studies, leading to the accumulation of a volume of knowledge (Kirchner and Simon 1981; McLean and Murray 1984; Gilday et al. 1977). In addition, continued application of the pinhole technique to the diagnosis of bone tumors and tumorous conditions has theoretically and substantially contributed to widening of the horizon of 99mTc-MDP scanning in bone oncology (Baek et al. 1997; Bahk 1996, 1998; Bahk et al. 1995). This section describes the bone scintigraphic features of osteosarcoma, chondrosarcoma, Ewing’s sarcoma, fibrosarcoma, and myelomas.
17.2.1 Osteosarcoma (Osteogenic Sarcoma)
Osteosarcoma is pathologically characterized by its ability to produce neoplastic bone in a fibrous stroma, hence osteogenic sarcoma. This is known as the most common variety of primary malignant bone tumor in the pediatric and adolescent age groups. Boys are affected slightly more frequently than girls. The most commonly affected bones are those of the knee with the proximal humerus the next most commonly affected. The location of tumor may be either central or parosteal in the metadiaphysis of the long bone with, not uncommonly, invasion of the adjacent soft tissue. Multiple primaries have been reported. Pathological fracture is relatively common, deforming the affected bone. Zeifang et al. (2000) surgically treated 30 patients with pathological fracture out of 336 patients with primary malignant bone tumors, reflecting approximately a 9% frequency.
The essential radiographic features of osteosarcomas are osteosclerosis (Fig. 17.39a), osteolysis (Fig. 17.40a), and their combination (Fig. 17.41a). Spicular, sunburst-like, and corona-like bone formation that arises from the lesional bone and periosteum is pathognomonic, especially when the adjacent soft tissues are concomitantly invaded (Fig. 17.42a). Periosteal osteogenesis with elevation and rupture (Codman’s triangle) is another important but not specific sign (Fig. 17.43a). Pathological fractures modify radiographic appearance, manifesting as fracture lines and fragmentation with or without dislocation within a tumor mass, which is the seat of osteolysis and hemorrhage and/or necrosis (Fig. 17.44a).
Contrast angiography provides valuable information on tumor vascularity and blush (Fig. 17.45). Unlike the more common varieties of osteosarcoma, the telangiectatic subtype radiographically presents as an osteolytic tumor strongly resembling aneurysmal bone cyst. Being high-grade osteosarcoma, this subtype produces minimal osteoid with a greater portion of tumor replaced by hemorrhage and/or necrosis (Figs. 17.46a and 17.47a). MRI is an excellent imaging method that can be used for in vivo tumor tissue characterization of the telangiectatic subtype of osteosarcoma (Murphey et al. 2003) (Fig. 17.47).
Scintigraphic manifestations vary according to the histological characteristics of the tumor. In general, the uniformly osteogenic or sclerotic type accumulates tracer extremely intensely (Fig. 17.39b), and the osteolytic type also accumulates tracer (Fig. 17.40b). The mixed type with intratumoral hemorrhage and/or necrosis presents as a mixture of photodense and photopenic areas (Fig. 17.41b). The main body of tumor within a long bone presented as a longitudinally oriented “hot” mass in both sclerotic and lytic types. The mass is fairly well demarcated on scintigraphs (Fig. 17.40b) but becomes distorted with patchy uptake when pathological fracture supervenes (Fig. 17.44c). Interestingly, the larger portion at the center of osteosarcoma with numerous fine tumor vessels and white blush is imaged as photopenia, and conversely the peripheral zone of tumor with lowered vascularity accumulates tracer rather intensely (Fig. 17.45). Fracture is usually indistinct on plain scintigraphs and can be imaged as such only by pinhole scintigraphy (Fig. 17.47). Characteristically, soft-tissue invasion produces the scintigraphic “sunburst” sign (Figs. 17.41b and 17.42b). It is to be emphasized that magnification scanning is extremely helpful for the visualization and analysis of all these pathological changes in detail. Indeed, simple bone distortion and increased uptake seen on ordinary scintigraphs of an osteosarcoma can be resolved into the main bone change with intratumoral hemorrhage or necrosis and more importantly neoplastic osteogenesis in the periostea and the adjacent soft tissues.
As is mentioned above, the telangiectatic osteosarcoma produces minimal osteoid tissues and is replaced by hemorrhage and necrosis. Scintigraphically, the tumor is presented as a large irregular photopenic lesion in the long-bone metadiaphysis (Fig. 17.46b). Occasionally, pathological fracture and viable melted host bone or neoplastic osteoid may accumulate tracer visibly on pinhole scintigraphs (Fig. 17.47b).
17.2.2 Chondrosarcoma
The exact tissue origin of chondrosarcoma is obscure, but clearly the basic tissue is hyaline cartilage that may be transformed to myxoid, calcified, or ossified tissue. The cell differentiation ranges from almost benign to highly malignant. A chondrosarcoma is primary in nature or metamorphosed from osteochondroma, enchondroma, or exostosis. The incidence of the primary type is over 90% (WHO 2002). This is a malignant tumor of the middle-aged and elderly population and affects men 1.5 times more commonly than women. As with osteosarcoma, intraosseous localization may be central, juxtacortical, or peripheral. The femur, humerus, and axial skeleton are affected in more than 75% of cases and epimetaphysis is the typical site of involvement. Conventional radiography, CT, and MRI (Collins et al. 2003) and bone scanning are used for diagnosis.
Radiographic findings vary from well-defined osteolysis with mild calcification through poorly defined bone destruction with moderate calcification (Fig. 17.48a) to expansive tumefaction with cortical rupture and soft-tissue invasion (Fig. 17.49a). CT scan shows all these features more clearly, distinguishing tumor matrices, calcification, and soft-tissue invasion (Fig. 17.48b), and MRI demonstrates characteristic signal intensity changes of cartilage, myxoid tissue, and calcification (Fig. 17.49). For example, T1-weighted MR images reveal a geographic lesion with low signal intensity that may occasionally contain multiple daughter tumors with increased signal intensity (Fig. 17.49b). Enhanced by contrast agent, the daughter tumors and reactive bone encapsulation become distinctly delineated with bright signal intensity (Fig. 17.49c).
On pinhole scintigraphy, tracer uptake is mild (Fig. 17.48c), moderate, or marked (Fig. 17.49d) according to the degree of calcification.
Visual correlation of the tracer uptake and radiographic change indicates that mild uptake occurs in the tumor matrix with mild calcification, while marked uptake occurs with marked calcification (Fig. 17.48). Conventional angiography in one of our chondrosarcoma cases showed that the grade of neovascularization roughly paralleled the radiopacity of tumor and the intensity of tracer uptake (Fig. 17.48). Radiographically and on CT, lucent tumor matrix with photopenia showed normal vascularity, whereas the matrix with calcification showed hypervascularization. Thus, it appears that tumor vessels are unrelated with tracer uptake in chondrosarcoma as they are in osteosarcoma (Fig. 17.45).
17.2.3 Ewing’s Sarcoma
Ewing’s sarcoma is a highly malignant tumor, consisting of small round cells of unknown tissue origin. The tumor predominantly affects children and young adults, with a strong predilection for males. No bones are immune, but the long bones of the lower extremity and pelvic bones are affected in 60% of patients. Not infrequently the spine and ribs are involved. The tumor tends to metastasize early to the bone and lung.
Radiographic features vary between patients, manifesting any of osteosclerosis, osteolysis, and mixed change and any combination of these. Bone condensation in the sclerotic type is intense, often with periosteal lamellation (Fig. 17.50a). The lamellation may be either single or multiple layered, giving rise to the “onion skin” sign if multilayering. Codman’s triangle may be seen as in other malignant bone tumors. Osteolysis within the marrow space is permeative and poorly demarcated (Fig. 17.51a), and the mixed form shows a mixture of lysis and sclerosis (Fig. 17.51a). Occasional lesions of the irregular bones such as the pelvis and vertebrae may show ballooning (Fig. 17.52a). The ballooning may represent rapidly expanding osteolysis or “pseudoaneurysmal bone cyst.”
Scintigraphic features also vary according to the tumor type. Basically, the osteosclerotic type accumulates tracer intensely (Fig. 17.50b), while the osteolytic type accumulates less tracer (Fig. 17.51b). Understandably, the tracer uptake in the mixed variant is irregular and heterogeneous (Fig. 17.51b). Nuclear angiography is ideal for detecting aneurysmal cystic change of Ewing’s sarcoma or tumor hypervascularity (Fig. 17.52b). Bone scintigraphy has the additional diagnostic advantage of discovering regional and distant metastases in Ewing’s sarcoma as in other malignancies.
17.2.4 Fibrosarcoma
Malignant fibrous tumors of bone include the primary and secondary fibrosarcomas and malignant fibrous histiocytoma that has been established as a distinctly independent entity.
The primary form may originate from the medullary space, periostea, or soft tissues, with secondary extension to bone. Pathologically, the tumor cells are spindle shaped, producing no bone, and the differentiation varies from low to highly malignant. This is a tumor of middle age, without gender predilection. Slightly more than 50% of cases are seen in the bones about the knee and in the humerus. Secondary fibrosarcomas are the result of malignant transformation of benign bone disorders such as Paget’s bones, medullary bone infarcts, or irradiated bones.
The characteristic radiographic manifestation of fibrosarcomas of bone is large geographic bone destruction, the contour of which is poorly defined because reactive sclerosis is minimal or absent (Fig. 17.53a). Osteolysis in this tumor is permeative, and accordingly the border shows a moth-eaten appearance. Periosteal invasion is uncommon, but it may cause spiculation, lamellation, or even the Codman’s triangle sign when present. Malignant fibrous histiocytoma also involves bone, forming a single large defect or multiple small defects located centrally or eccentrically in long-bone diaphyses. In occasional cases small lytic areas may coalesce (Capanna et al. 1984), and the tumor becomes expansive showing a bubbly appearance due to septum-like formations (Fig. 17.54).
Pinhole scintigraphy of primary fibrosarcoma shows a large ill-defined photon defect surrounded by an irregular rim of watershed or extended uptake (Fig. 17.53b). The photopenic manifestation of this tumor may be explained on the basis of that fibrous matrix is basically not osteogenic. The nonosteogeny of tumor along with the absence of significant reactive osteosclerosis may be a likely reason for poor scintigraphic demarcation. Infiltrating variants may present as patchy areas of intense tracer uptake intermingled with irregular photopenic areas. The intramedullary spread can be diagnosed by bone scan. The basic scan manifestations of malignant fibrous histiocytoma with bone destruction are essentially the same as those of osteolytic type primary fibrosarcoma except for the expansiveness and multicystic appearance with septation (Fig. 17.54b). The latter finding has a strong resemblance to that in metastatic follicular thyroid carcinoma with septation (Fig. 17.21a).
17.2.5 Myeloma (Plasma Cell Myeloma)
Myeloma is characterized by neoplastic proliferation of abnormal plasma cells in the red bone marrow. Multiple myeloma is not a rare disease, accounting for 1% of all malignant tumors. This is primarily a disease of the elderly, but the range of incidence is wide, between 25 and 80%. One most recent population study performed in the South Thames area of the United Kingdom has shown the age-standardized rate of multiple myeloma to be 3.29 per 100,000 with the median age of those affected being 73 years (Phekoo et al. 2004). When first seen in the clinic, the lesions are either multiple (more than 50%), generalized (15%), or solitary (25%). Solitary myeloma may eventually develop into multiple or generalized lesions. The axial skeleton including the skull, spine, pelvis, sternum, and shoulder bones, as well as the limb bones, are involved (Fig. 17.55). Symptoms include malaise, fatigability, skeletal pain especially in the spine and rib cage, and bone deformity. The solitary form may well pass unnoticed and the generalized form may be disguised as simple osteoporosis. In either form, the first event that brings the patient to hospital may be pathological fractures. Protein electrophoresis may reveal an increase in the globulin fraction, and immunoelectrophoresis can identify different types of globulin such as IgG, IgA, and rarely IgM.
The radiographic features include multiple or diffusely spread bone destructive changes or solitary lysis. Characteristically, lesions in the skull are well defined and discrete and give rise to a “punched-out” or “bubbly” appearance (Fig. 17.56). If generalized, however, the individual lesions imperceptibly blend into advanced senile osteoporosis (Fig. 17.57). Myelomatous bones are fragile and prone to pathological fracture, but the fractures are radiographically undetectable in most cases because of severe osteoporosis. An interesting radiographic sign of multiple myeloma is endosteal scalloping caused by the physical effect of proliferative plasma cells that are expansive (Fig. 17.58). With gradual increase in volume, myelomas in small bones such as the sternum and ribs may become expansive, eventually breaking the cortex (Fig. 17.59a). On occasion, such lesions are permeant and expansive and induce a periosteal reaction (Fig. 17.60).
99mTc- MDP bone scintigraphy was once held to be of limited value since the plasma cells of myeloma do not accumulate tracer regardless of the disease type (Wahner et al. 1980; Waxman et al. 1981). However, the extended application of whole-body and pinhole scans to the diagnosis of myelomas has indicated that bone scintigraphy is not only useful but also even indispensable in certain clinical settings. The first and most important situation is probably pathological fractures that are common in myelomatosis. Radiographic diagnosis of such fractures is notably difficult and even harder when advanced myelomatosis is superimposed on severe porosis (Fig. 17.57). Fortunately, fractures intensely accumulate tracer regardless of the porosis in host bones. The second advantageous situation is solitary myelomas in the long tubular bones and small bones such as the ribs and sternum (Fig. 17.59a). A sizeable lesion may be missed radiographically in these bones, but pinhole scintigraphy can reveal signs that strongly suggest or indicate the diagnosis. Myeloma in the sternum presents as an expansive photon defect visualized as broken eggshell-like uptake in the ruptured cortex (Fig. 17.59a). CT scan is an excellent alternative (Fig. 17.59b). Pinhole scintigraphy is far more informative in studying solitary myeloma in the long bones because it can distinguish permeative bone invasion from simple expansion (Fig. 17.60b). The tracer uptake in simple expansion or scalloping is negligible or very subtle at most, but that in actively invaded or ruptured cortex is obvious. The third advantage is scintigraphic detection of radiographically invisible myelomas, but this is rare.
On the other hand, 99mTc-tin colloid bone marrow scintigraphy is a useful adjunct to the diagnosis of myelomas (Feggi et al. 1988) and the myelomas, metastases, lymphoma, and leukemia that are rooted in the red bone marrow (Lentle et al. 1987). Bone marrow scanning using radiocolloids relies on the phagocytosis of reticuloendothelial cells. Accordingly, once the bone marrow has been replaced with myeloma cells, they become photopenic on colloid scintigraphs (Fig. 17.58). 18F-FDG PET is a useful adjunct to the diagnosis of multiple myeloma. The sensitivity and specificity in detecting multiple myeloma lesions have been reported to be 85 and 92%, respectively (Bredella et al. 2005). The superiority of 18F-FDG PET is based on the fact that 18F-FDG PET can directly visualize denatured plasma cells that avidly consume glucose, while 99mTc-MDP bone scintigraphy can image indirect bone change that occurs secondarily (Fig. 17.61). In passing, it is worth mentioning that pinhole scintigraphy can conveniently and reliably evaluate and archive the results of adjuvant chemotherapy, external irradiation, or bone marrow replacement (Fig. 17.62).
17.3 Leukemias and Lymphomas
Leukemias and lymphomas, respectively, comprise myeloproliferative neoplasms and lymphoreticular tumors of the reticuloendothelial system. Clinically, leukemias are classified into the acute form and the chronic form. Acute leukemia affects both children and adults and chronic leukemia middle-aged adults. Lymphomas arise from the lymphocytic cells, reticulum cells, or primitive precursor cells, and they are pathologically classified as non-Hodgkin’s lymphoma, Hodgkin’s lymphoma, Burkitt’s lymphoma, and mycosis fungoides.
The radiographic changes of bone and bone marrow in acute leukemias are basically not dissimilar to those of multiple myeloma. Thus, radiographic features include diffuse osteopenia, irregular osteolysis and osteosclerosis, lucent metaphyseal band, and periosteal reaction (Fig. 17.63a). Chronic leukemia also manifests as osteopenia and occasional osteolysis that is discrete. On the other hand, lymphomas, both the non-Hodgkin’s type and the Hodgkin’s type, typically affect the axial bones including the skull, the facial bones, the spine, the pelvis, the ribs, and the femurs. The spread of lymphomas to bone occurs either directly from contiguous lymph nodes or through blood flow. Osteolysis is geographic in appearance with poorly defined borders in large flat or irregular bones such as the sacrum (Fig. 17.64a) or segmental with cortical rupture in small bones such as the ribs (Fig. 17.65a). Endosteal scalloping and periosteal or soft-tissue invasion may occasionally be seen as in myeloma.
99mTc-MDP bone scintigraphy of acute leukemia in children manifests as band-like uptake in the long-bone metaphyses with small segmental uptake in the diaphyses (Fig. 17.63b). Generally, the scintigraphic features of lymphoma are similar to those of other osteolytic tumors (Fig. 17.64b). Tracer uptake becomes markedly intensified when the affected bone is fractured (Fig. 17.65b). Lymphocytic leukemia in adults characteristically accumulates tracer in scalloped endosteums of the long bones reflecting bone marrow involvement (Fig. 17.66).
17.4 Chordoma
Chordoma is a slow-growing, low-grade malignancy that arises from primitive notochordal mucoid intercellular material. The tumor is strongly inclined to involve both the caudal sacral region and the clivus near the spheno-occipital synchondrosis. The incidence ranges from 1 to 4% and is nearly twice as common in men as in women, with the vast majority of cases occurring between the fourth and seventh decades of life. Sacrococcygeal lesions are more common in women than in men, whereas the spheno-occipital lesions have an equal sex distribution. Clinical manifestations relate to the location of the tumor. In the early stages the symptoms are mild and nonspecific. Sacrococcygeal invasion causes progressive perineal pain, constipation, urinary difficulties, and bleeding, whereas chordomas at the cranial base lead to increased intracranial pressure and compression of the adjacent structures causing headaches, blurred vision, memory loss, and emotional instability. When vertebrae are involved, tumors invade the spinal cord and nerve roots with pain, numbness, motor weakness, and paralysis.
Radiography shows an expansive, osteolytic mass with a lobular or geographic appearance. Typically, the tumors are located in the midline in the caudal sacrum or the skull base. Sacral chordoma produces an anteriorly protruding mass that contains irregular bony shards when seen on lateral radiographs. Rarely, the entire tumor mass may be located within the sacrum. Not infrequently, the sacral mass is overshaded by the intestinal contents and gas. A CT scan is ideal for revealing the lobular mass with osteolysis and irregular fragmentations (Fig. 17.67a).
Pinhole scintigraphy is valuable for the mapping of large, expansile, intraosseous photonic tumor, which is characteristically situated in the midline of the caudal sacrum. The tumor can be outlined by irregular, interconnected, spotty “hot” areas of reactive or destroyed bones around it (Fig. 17.67b).
17.5 Periosteal Leiomyosarcoma
Leiomyomas and leiomyosarcomas outside the uterus and gastrointestinal tract are extremely rare. Conklin et al. (1981) reported a case of leiomyoma that occurred in the tibia. Their case showed mild but diffusely increased tracer uptake. Recently, we came across a case of exophytic leiomyosarcoma arising from the sub-periosteal layer of the juxtaspinal portion of the right ninth rib in a 40-year-old man (Fig. 17.68a,b). The tumor was photopenic with faint tracer uptake in the periphery where a bone fragment was detached from the rib that was widely destroyed (Fig. 17.68c). Moderately intense uptake was noted in the host bone as well as the suprajacent rib that was compressed by the tumor. Histologically, the tumor was necrotic with hemorrhage.
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Bahk, YW., Bahk, WJ. (2017). Malignant Tumors of Bone. In: Combined Scintigraphic and Radiographic Diagnosis of Bone and Joint Diseases. Springer, Singapore. https://doi.org/10.1007/978-981-10-2759-8_17
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