Cancer-Related Bone Pain



Cancer-Related Bone Pain


Edgar Ross

Lalitha Sundararaman

Mary Alice Vijjeswarapu



Epidemiology Review

Bone pain due to cancer is caused by primary bone tumors and those malignant diseases that commonly metastasize to the bones. Bone is the third most common site of metastasis after lung and liver.1 Metastatic bone pain most commonly results from cancers of the breast, prostate, and lung.2 Other malignancies involving bone are renal cell carcinoma, thyroid cancer, lymphoma, and multiple myeloma.3 The longer these malignancies persist, the higher the probability of finding bone metastases. Current therapies have increased survival time of patients suffering from many of these malignancies. This has resulted in an increasing prevalence of metastatic bone disease. Li et al.4 estimated that 279,679 (95% confidence interval: 274,579 to 284,780) US adults alive on December 31, 2008, had evidence of metastatic bone disease in the previous 5 years (Table 46.1). Breast, prostate, and lung cancers accounted for 68% of these cases.

Prostate cancer is very likely to metastasize to bone rather than other organs. Because patients are living longer than other patients with metastatic diseases, prostate cancer patients are at increased risk of having prolonged periods of pain secondary to bony invasion.5

Vertebral involvement is the most common site of bony metastases. The incidence ranges from 30% to 70%.6 Most patients with metastatic disease of the vertebrae experience back pain.7

Bony metastases compromise both the bone’s integrity and strength. In the vertebrae, this leads to the increased risk of a pathologic fracture, found most commonly in the elderly. Compression fractures affect between 8% and 30% of cancer patients with vertebral body involvement.8,9 In many cases, the fracture occurs without an initial traumatic event suggesting that vertebral load is an independent factor in the etiology of a pathologic fracture.10 Other factors that can lead to pathologic fractures include iatrogenic causes such as steroids, malnutrition-induced osteoporosis, bone mineral loss as a result of inactivity, and destruction of bone secondary to radiation therapy.11

Complications from vertebral fracture include a redistribution of load across affected vertebral bodies creating the increased risk of fractures at adjacent levels, increased risk of embolic phenomena as a result of inactivity and pain, kyphosis-induced restriction of vital capacity,12 predisposition to atelectasis, and early satiety-induced anorexia.13 Because of this, bony metastases contribute significantly morbidity and decreased life span.3,14








TABLE 46.1 Estimated Number of Prevalent Cases of Metastatic Bone Disease in the National Commercially Insured Population Aged 18-64 Years, The National Fee-for-Service Medicare Population Aged ≥65 Years, and the US Adult Population on December 31, 2008, All Cancers and by Specific Cancer Types







































Cancer Type


Commercially Insured, Ages 18-64 years (n = 120,694,145)


Fee-for-Service Medicare, Ages ≥65 years (n = 25,950,760)


US adult populationa (n = 230,118,000)


All cancers


60,411 (59,134-61,689)


128,540 (125,485-131,595)


279,679 (274,579-284,780)


Female breast


25,754 (24,911-26,596)


35,960 (34,341-37,579)


90,904 (88,095-93,714)


Prostate


4,969 (4,609-5,329)


37,240 (35,593-38,887)


62,841 (60,253-65,429)


Lung


7,879 (7,421-8,337)


15,900 (14,823-16,977)


35,222 (33,415-37,030)


Other


21,809 (21,046-22,573)


39,440 (37,745-41,135)


90,712 (87,843-93,580)


NOTES: Data presented as estimated number of patients with metastatic bone disease (95% confidence interval).


a US Census 2008.


From Li S, Peng Y, Weinhandl ED, et al. Estimated number of prevalent cases of metastatic bone disease in the US adult population. Clin Epidemiol 2012;4(1):87-93. Reproduced with permission of Dove Medical Press in the format Republish in a book via Copyright Clearance Center.




EVALUATION OF THE PATIENT WITH BONE CANCER

The two most important imaging modalities in the evaluation of malignancy of the bone are plain radiography and radioisotope bone scans.


Radiography

Radiographic studies should be ordered first in the evaluation of patients with complaints of bone pain in the context of malignancy. Radiographic patterns fall into osteolytic, osteoblastic, or mixed presentation. Osteoblastic lesions appear opaque and sclerotic. Osteolytic lesions appear more radiolucent compared to surrounding bone. Risk of fracture is greatest if more than 50% of long bone is involved.7,29


Bone Scan

Radioisotope bone scans are very good at identification of multifocal lesions.30 Radioisotopes accumulate in areas of new bone growth and are diminished in areas of metastasis secondary to decreased blood flow to the area. Cancers such as melanoma and multiple myeloma may have false negatives when reviewed on bone scan secondary due to their lack of reactive bone activity.


Computed Tomography

Computed tomography (CT) offers improved spatial resolution in the evaluation of cortical bone destruction.31 CT is beneficial in evaluation of the three-dimensional characteristics of diseased bone identified by plain radiographs and isotope scans. CT scan evaluations are optimal to study the pelvic and shoulder girdles and spinal lesions. Additionally, CT-guided needle biopsies can be used to identify cell types.


18F-FDG-PET-CT

The visualization of glucose metabolism by positron-emission tomography with 18F-fluorodeoxyglucose, coupled with a simultaneously obtained CT (18F-FDG-PET-CT), is now a standard diagnostic technique in oncology. In patients with highly metabolically active cancers such as lung cancer or malignant melanoma, PET-CT with FDG has replaced other techniques for the detection of bone metastases. In highly active tumors, bony metastases can be detected with high sensitivity and specificity.32


Magnetic Resonance Imaging

Magnetic resonance imaging (MRI) provides better contrast resolution in defining soft tissue and marrow involvement. Also, it can define vascular relationships without contrast enhancement.31 MRI is very beneficial in the evaluation of tumor infiltration of muscle and bone marrow, spinal cord compression, and lesions which are otherwise insufficiently imaged by the previously listed approaches.




CYCLOOXYGENASE-2-SPECIFIC INHIBITORS

COX-2-specific inhibitors (coxibs) have demonstrated efficacy in the treatment of chronic and acute pain comparable to traditional (nonselective) NSAIDs without the severity of GI complication during short-term use or platelet inhibition effects.34 The superior safety profile of coxibs in conjunction with similar efficacy of conventional NSAIDs supports their use in analgesic regimens for bone cancer. Many tumors express the COX-2 isoenzyme, which is involved in the synthesis of prostaglandins.35 In the murine sarcoma model, acute administration of a selective COX-2 inhibitor attenuated both ongoing and movementevoked bone cancer pain, whereas chronic inhibition of COX-2 significantly reduced ongoing and movement-evoked pain behaviors and reduced tumor burden, osteoclastogenesis, and bone destruction by >50%. COX-2 is expressed in 40% of human invasive breast cancers, and bone is the primary site of metastasis in cases of breast cancer.36,37 COX-2 inhibition also inhibited bone metastasis in both a prevention and treatment regimen. This suggests COX-2 produced in breast cancer cells are significant in supporting progression of osteolytic bone metastases in patients with breast cancer, and that COX-2 inhibition may halt this process. Furthermore, COX-2 inhibition may benefit iatrogenically caused tumor progression.38 COX-2 inhibitors, such as celecoxib, have also been shown to increase apoptosis and decreased progression of osteosarcoma cell lines.39

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Sep 21, 2020 | Posted by in PAIN MEDICINE | Comments Off on Cancer-Related Bone Pain

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