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Palliation of Metastases

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Title: Palliation of Metastases


1
Palliation of Metastases
  • Iftekhar Ahmad, MD
  • Wayne State University/KCI
  • July 8thth, 2008

2
Epidemiology
  • Osseous metastases is the most common cause of
    intractable pain in cancer patients
  • Third common site of spread after lung and liver
  • Presentation occurs after primary diagnosis in
    majority of patients
  • But in 23 of patients it is the presenting
    problem which leads to the discovery of disease

3
Pathophysiology
  • Tumor cells primarily gain access to the
    circulation through the capillaries
  • 1). Release of tumor cells from the primary
  • 2). Invasion of vascular or lymphatic channels
  • 3). Dissemination to distant sites
  • 4). Endothelial attachment and invasion of new
    host
  • 5). Growth into a metastatic focus

4
Pathophysiology
  • Skeletal blood flow accounts for only 4-10 of
    total cardiac output
  • Incidence of skeletal metastases appears higher
    than expected
  • Microstructure of marrow renders it vulnerable to
    tumor accumulation and invasion
  • Arteries tend to divide capillaries as they near
    the endosteal margin of bone
  • Capillaries become continuous with venous system
    which has a 6-8 times capacity
  • The circulation comes to a near standstill at
    this point potentially allowing tumor cells more
    time to invade

5
Pathophysiology
  • Tumor angiongenesis factor attracts vessels to a
    small tumor colony
  • Otherwise it would be dependant on local tissue
    circulation and incapable of further invasion
  • The production of this factor is partially
    blocked by immune responses so it may take years
    to have adequate vasculature for invasion

6
Mediators
  • Some tumors produce and secrete humeral mediators
    that stimulate osteoclast activity
  • TGF
  • PDGF
  • TNF
  • Prostaglandins
  • Interleukins

7
Distribution
  • More prevalent in the axial skeleton versus the
    appendicular skeleton
  • But richer blood flow in appendicular skeleton
    would predict higher rates

8
Imaging
  • Plain X-rays are the fastest form of imaging
  • Medulla involved early and cortex late
  • Role for patients with pain and positive bone
    scan to uncover pathologic fractures
  • Sclerotic Prostate, Breast, GI, Bladder
  • Lytic All sites
  • Mixed Breast
  • More than 50 cortical destruction needed to
    detect

9
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11
Imaging
  • Bone scans are more sensitive and also allow
    examination of entire skeleton
  • Most lesions evoke an osteoblastic response
    (increased uptake)
  • Rapidly growing lesions may show decreased uptake
    because rate of destruction exceeds rate of
    formation
  • Non-osteoblastic tumors include myeloma and some
    lymphomas
  • Infection, fractures, and degenerative changes
    may also result in a positive result

12
Imaging
  • CT differentiates between metastases and
    degenerative joint disease
  • DJD can manifest as positive bone scan
  • Muindi and colleagues looked at patients with
    positive bone scans and negative x-rays
  • 50 of patients had mets on CT, 25 had benign
    findings, and 25 had no findings
  • None of the patients with no findings had
    subsequent metastases

13
Imaging
  • MRI is the method of choice for examining the
    spine
  • More sensitive than bone scan for detecting early
    changes (medullary)
  • If cord compression is suspected, thorough exam
    is warranted as 10 of patients may have
    significant disease elsewhere
  • Disadvantages include
  • High cost
  • No metal implants
  • Claustrophobia
  • Still for long period

14
Treatment
  • Primary goal is improvement of QOL
  • Decrease pain and maintain function
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

15
Endocrine Therapy
  • Tamoxifen used for post-menopausal metastatic
    breast cancer in mainly ER patients
  • But 10 of ER- patients respond
  • Median tumor response of 15 months
  • Aromatase inhibitors have challenged tamoxifen as
    first-line therapy for advanced or metastatic
    breast cancer

16
Arimidex vs. Tamoxifen
  • Milla-Santos A et al Am J Clin Oncol. 2003
    Jun26(3)317-22
  • RCT comparing anastrozole with tamoxifen as
    first-line therapy in postmenopausal,
    hormone-dependent, advanced breast cancer
  • Patients were randomized to daily anastrozole (n
    121) or tamoxifen daily (n 117)
  • Median FU of 13.3 months, clinical benefit (CB)
    was achieved in 83 and 56 of anastrozole and
    tamoxifen patients, respectively (p lt 0.001)
  • Median time to disease progression in patients
    was 18.0 months and 7.0 months (p lt 0.01)

17
Femara vs. Tamoxifen
  • Mouridsen H et al JCO 2003 Jun 121(11)2101-9
  • 916 patients with locally advanced or metastatic
    ER or unknown tumors (30)
  • Randomized to letrozole 2.5 mg (n 458) or
    tamoxifen 20 mg (n 458) daily until disease
    progression
  • Time to progression (median, 9.4 v 6.0 months,
    respectively p lt.0001) and overall objective
    response rate (32 v 21, respectively p .0002)
    were higher for Femara patients
  • OS at 2 years was 64 for letrozole and 58 for
    tamoxifen (p lt .01)

18
Second Line
  • Patients who fail on aromatase inhibitors may be
    given tamoxifen and vice-versa
  • Other agents include aminoglutethimide and megace
  • Pre-menopausal women may be treated with ovarian
    ablation (surgically or with LHRH agonists)

19
Prostate Cancer
  • Very sensitive to hormones and 80 of patients
    with metastatic disease show some response (or to
    orchiectomy)
  • Flare response is noted in 10-30 of patients on
    LHRH agonist
  • Can be reduced with concurrent use of
    anti-androgens
  • Clinical benefit also seen with the two agent
    therapy (flutamide)

20
Prostate Cancer
  • Crawford ED et al N Engl J Med. 1989 Aug
    17321(7)419-24
  • 603 men received leuprolide in combination with
    either placebo or flutamide
  • As compared with the 300 patients receiving
    leuprolide and placebo, the 303 patients randomly
    assigned to receive leuprolide and flutamide had
    a longer progression-free survival (16.5 vs. 13.9
    months P 0.039) and an increase in the median
    length of survival (35.6 vs. 28.3 months P
    0.035).
  • Differences between the treatments were
    particularly evident for men with minimal disease
    and good performance status
  • Symptomatic improvement was greatest during the
    first 12 weeks of the combined androgen blockade,
    when leuprolide alone often produces a painful
    flare in the disease

21
Treatment
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

22
Biologic Therapy
  • Her-2/neu represents the human EDGF and is
    overexpressed in 20-30 of breast cancer
  • Associated with increased tumor growth rate,
    metastatic rate, and decreased OS
  • Trastuzumab (Herceptin) used in these patients
  • High tumor response correlated with high levels
    of overexpression

23
Herceptin
  • Vogel CL et al J Clin Oncol. 2002 Feb
    120(3)719-26
  • 114 women with HER2-overexpressing metastatic
    breast cancer received first-line treatment with
    trastuzumab
  • Objective response rate was 26 with seven
    complete and 23 partial responses
  • Clinical benefit rates in assessable patients
    with 3 and 2 HER2 overexpression were 48 and
    7, respectively
  • Seventeen (57) of 30 patients with an objective
    response and 22 (51) of 43 patients with
    clinical benefit had not experienced disease
    progression at follow-up at 12 months or later
  • Most common treatment-related adverse events were
    chills (25 of patients), asthenia (23), fever
    (22), pain (18), and nausea (14)

24
Treatment
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

25
Bone Chemotherapy
  • Overall response in bone is poor
  • 0-30
  • Only a partial response with a median duration of
    9-12 months
  • Better response in Small Cell Lung and breast
  • Potentially curative for lymphoma, GC tumors
    (Cytoxan)
  • Myelosuppression may be problematic with
    extensive marrow involvement and XRT treatment

26
Treatment
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

27
Bisphosphonates
  • Inhibition of osteoclast-mediated bone resorption
    (exact mechanism not clear)
  • Direct biochemical effects on osteoclast
  • Prevention of osteoclast attachment to matrix
  • Inhibition of differentiation of osteoclast
    precursors

28
Bisphosphonates
  • Zoledronic Acid(Zometaâ), Risedronate(Actonelâ),
    Pamidronate(Arediaâ), Ibandronate(Bonivaâ),
    Etidronate(Didronelâ), Alendronate(Fosamaxâ)
  • Four phase II trials using IV pamidronate for
    sole treatment of osteolytic bone mets from
    breast cancer
  • Relieve bone pain in 50
  • Radiographic evidence of bone healing in 25
  • Decrease incidence of vertebral fractures

29
Zoledronic Acid v Pamidronate
  • Rosen LS et al Cancer 2003 Oct 1598(8)1735-44
  • 1,648 patients with either stage III multiple
    myeloma or metastatic breast cancer (with at
    least one bone
  • Assigned to treatment with zoledronic acid or
    pamidronate
  • After 25 months of follow-up, zoledronic acid
    reduced the overall proportion of patients with
    an skeletal related event (SRE) and reduced the
    skeletal morbidity rate similar to pamidronate
  • Compared with pamidronate, zoledronic acid
    reduced the overall risk of developing skeletal
    complications by an additional 16 (P 0.030)
  • In patients with breast carcinoma, zoledronic
    acid was significantly more effective than
    pamidronate, reducing the risk of SREs by an
    additional 20 (P 0.025) compared with
    pamidronate and by an additional 30 in patients
    receiving hormonal therapy (P 0.009)
  • Zoledronic acid and pamidronate were equally well
    tolerated the most common adverse events were
    bone pain, nausea, fatigue, and fever

30
Treatment
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

31
Analgesics
  • WHO Analgesic Ladder
  • Step I nonopioid /- adjuvant therapy
  • Step II Opioid for moderate pain plus nonopioid
    /- adjuvant therapy
  • Step III Opioid for moderate to severe pain /-
    nonopioid /- adjuvant therapy

32
Step I
  • Nonopioid Analgesics
  • Acetaminophen, Aspirin, NSAIDS
  • Synergistic with opioids
  • Many osseous mets produce PGs involved in
    osteolysis
  • Adjuvant Therapy
  • Massage, Heat, Cold, Acupuncture, Vibration, TENS
  • Anxiolytics, Antidepressants, Antiepileptics
  • Hypnosis, Biofeedback

33
Step II and Step II
  • Step II Opioids
  • Codeine
  • Dihydrocodeine
  • Hydrocodone
  • Oxycodone
  • Propoxyphene
  • Step III Opioids
  • Morphine
  • Hydromorphone
  • Fentanyl

34
Pain Pathway
Points
  • Try to cover multiple steps along the pain
    pathway to maximally treat pain.
  • TCA or Neurontin when pain has neuropathic
    component
  • NSAID with bone involvement
  • Adding nonopioids allows a decreased dose of
    opioid and may improve QOL
  • NV are not allergic reactions to
    opiates/opioids and usually resolve within a week
    when continuing med
  • C-II meds cannot have refills and can only have
    one per prescription form

Pain
Central Processing
Spinal Cord
Peripheral Receptors
35
Treatment
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

36
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37
Surgery
  • Should be considered for patients with pathologic
    or impending fractures
  • Fixation can reduce pain and expedite healing
  • Prophylactic fixation may prevent fracture
    eliminating any functional loss

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40
Surgery
  • Both lytic and blastic lesions alter bone
    elasticity
  • Lytic lesions reduce bone strength more than
    blastic lesions
  • Elongated lesions reduce bone strength more

41
Surgery
  • Guidelines for prophylactic fixation
  • Life expectancy gt3 months
  • Able to tolerate surgery
  • Expectation of expedited mobilization
  • Adequate bone proximal and distal to lesion to
    support fixation device
  • Cortical bone destruction of gt/ 50
  • Pathologic avulsion fracture of lesser trochanter
  • Stress pain persists after radiation

42
Spinal Cord
  • Most common site of skeletal metastases
  • Vertebral body typically affected first
  • Usually asymptomatic
  • 30-50 of vertebral body needs to be destroyed to
    be detected on x-ray
  • Symptoms occur when
  • Enlarging mass breaks through cortex and invades
    paravertebral soft tissue
  • Mass compresses the nerve roots
  • Pathologic fracture occurs
  • Spinal cord compression

43
Spinal Cord Vertebroplasty
  • Patient must be able to undergo sedation or
    anesthesia
  • Indications for surgical intervention
  • Progressive canal impingement or cord compression
  • Bone/soft tissue extruded into canal
  • Progressive spinal deformity
  • Progressive kyphosis
  • Previously treated with radiation

44
Treatment
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

45
Local Field Radiation Therapy
  • Vast majority of patients managed successfully
    with external beam RT
  • Optimal dose and fractionation continue to be
    debated
  • Results of various studies compounded by use of
    different pain scoring systems, analgesic usage,
    and use of hormone or chemotherapy
  • Treatment technique

46
RTOG 7402 Tong Cancer. 50893 1982
  • RCT of 1016 pts with solitary or multiple mets in
    femur, humerus, pelvis, spine.
  • Pain or narcotic score at least 4
  • Expected survival at least 3-months
  • No previous RT
  • No new CTX

47
RTOG 7402 Study Design
48
RTOG 7402
  • Overall
  • 89 experienced minimal pain relief
  • 83 experienced partial pain relief
  • 54 experienced complete pain relief
  • No significant differences between the treatment
    arms
  • Initial pain score useful predictor of treatment
    response
  • Patients with breast and prostate primaries
    responded best
  • Median duration of complete and partial relief
    was 12 and 20 weeks
  • Median OS
  • 36 weeks for solitary mets
  • 24 weeks for multiple mets

49
Dutch Multicenter Trial
  • 1171 patients with painful bone metastases
    randomly assigned to 8 Gy in a single dose or 24
    Gy in six fractions
  • Excluded melanoma, RCC, or C-spine
  • Palliative benefit was similar in both groups
  • Treatment-related toxicity was similar in both
    groups
  • Retreatment was required by significantly more
    patients treated with a single fraction (25 vs.
    7)

50
British Trial
  • RCT 765 pts painful bone metastases
  • 8 Gy single fraction
  • 20 Gy five fractions
  • 30 Gy 10 fractions
  • At 12 month follow-up
  • No differences in palliation of pain
  • Single fraction twice as likely to require
    reirradiation
  • majority successfully retreated with single
    fraction

51
RTOG 97-14
  • RCT 949 patients with prostate or breast cancer
    painful bone metastases
  • 8 Gy in a single fraction or 30 Gy in 10
    fractions
  • Patients with evidence of cauda equina syndrome
    or epidural spinal cord compression were excluded
  • No significant differences in the rates for
    complete and partial pain relief, the use of
    narcotics, or the incidence of subsequent
    pathologic fractures
  • Patients treated with a single fraction were
    twice as likely to require retreatment (18 vs 9)

52
Meta-Analysis
  • Wu JY et al IJROBP 2003 Mar 155(3)565-7
  • 5455 patients in 16 trials
  • The primary outcomes of interest were complete
    and overall pain relief
  • Included complete and overall response rates from
    studies comparing single-fraction RT (median 8
    Gy, range 8-10 Gy) against multifraction RT
    (median 20 Gy in 5 fractions, range 20 Gy in 5
    fractions to 30 Gy in 10 fractions)
  • Overall response rates were similar for single
    fraction and multifraction RT, at 1011 (72.7) of
    1391 and 958 (72.5) of 1321 (p 0.9)
  • Exploratory analyses by biologic effective dose
    did not reveal any dose-response relationship
    among the fractionation schedules used (single 8
    Gy to 40 Gy in 15 fractions)
  • Only the re-irradiation rates were consistently
    different between the treatment arms (more
    frequent re-irradiation in lower dose arms among
    trials reporting re-irradiation rates)

53
Target Volumes
  • Should be defined after careful review of all
    studies along with thorough patient examination
  • Attention should also be paid to soft tissue
    masses which may contribute or be the cause of
    pain
  • Review of any previous treatment plans
  • Best assessment with CT and MRI
  • Volumes should be kept to a minimum to preserve
    marrow reserves (especially for patients
    undergoing chemotherapy)

54
Radiation Hemibody
  • Rationale
  • Most patients with bone mets have multiple sites
  • Many require additional treatment within 1 year
  • More rapid onset of relief than local-field
  • Draw-backs
  • Similar overall response
  • More side effects
  • Require close monitoring peri-treatment
  • Largely replaced by radioisotope pharmaceuticals

55
RTOG 8206
  • Poulter CA et al IJROBP 1992 23(1)207-14
  • RCT of 499 patients who received HBI or were
    observed following local field RT (3 Gy x 10
    followed in 8 Gy of HBI)
  • Improvement was seen in time-to-disease
    progression at one year, 35 for local HBI
    versus 46 on the local-only control arm
  • At one year, 50 of patients on the local HBI
    arm showed new disease compared to 68 on the
    local-only arm
  • At one year, 76 of the local only group had been
    retreated versus 60 in the local HBI arm
  • There were no fatalities and no radiation
    pneumonitis was seen in the local HBI arm (lung
    blocks limited dose to 7 Gy)
  • The occurrence of severe hematopoetic toxicities
    were significantly different in the local HBI
    arm one life-threatening thrombocytopenia
    occurred
  • But ultimate progression rates have been shown to
    not significantly different

56
Treatment
  • Modalities include
  • Pharmacologic therapy
  • Endocrine therapy
  • Biologic therapy
  • Chemotherapy
  • Bisphosphonates
  • Analgesics
  • Surgery
  • Radiotherapy
  • External beam
  • Radionuclide therapy

57
Radionuclide Therapy
  • Can be considered in the following situations
  • Patients with widely metastatic disease as an
    adjuvant to RT
  • First-line therapy in patients without a
    predominantly painful site
  • When external beam RT has been used and normal
    tissue tolerance reached
  • Life expectancy of less than 3 months
  • No evidence of cord compression, fracture, or
    mechanical instability
  • Good marrow reserve (WBC gt2400 Plt gt100,000)

58
Strontium 89
  • Decays by beta emission to yttrium 89 with a T1/2
    of 50.6 days
  • Maximum energy of 1.46 MeV
  • Quickly taken up by bone matrix
  • Fraction taken up is proportional to tumor burden
    (20-80)
  • Localizes to areas of osteoblastic activity
  • Remains deposited for as long as 100 days
  • Normal bones take up only a small amount
  • Eliminated through the kidneys

59
Strontium 89
  • Porter AT et al IJROBP 1993 Apr 225(5)805-13
  • 126 patients with metastatic hormone refractory
    prostate cancer
  • Received local field radiotherapy and either
    strontium-89 as a single injection of 10.8 mCi or
    placebo
  • No significant differences in survival or in
    relief of pain at the index site
  • Decreased intake of analgesics in strontium 89
    arm
  • Progression of pain as measured by sites of new
    pain or the requirement for radiotherapy showed
    statistically significant differences between the
    arms in favor of strontium-89
  • PSA, acid phosphatase, and alkaline phosphatase
    were also reduced in patients receiving
    strontium-89
  • QOL analysis demonstrated an overall superiority
    of strontium-89 with alleviation of pain and
    improvement in physical activity being
    statistically significant
  • Toxicity was evaluated and demonstrated increased
    hematological toxicity in the group receiving
    strontium-89

60
Strontium 89
  • Quilty PM et al Radiother Oncol. 1994
    Apr31(1)33-40
  • 284 patients with prostate cancer and painful
    bone metastases were treated with either
    radiotherapy or strontium-89
  • After 4, 8 and 12 weeks pain sites were mapped,
    toxicity monitored, and all additional palliative
    treatments recorded
  • There was no significant difference in median
    survival 33 weeks following strontium-89 and 28
    weeks following radiotherapy (p 0.1)
  • All treatments provided effective pain relief
    improvement was sustained to 3 months in 61
    after local radiotherapy compared with 65.9 in
    the comparable strontium-89 group
  • Fewer patients reported new pain sites after
    strontium-89 than after local or hemibody
    radiotherapy (p lt 0.05)
  • Radiotherapy to a new site was required by 12
    patients in the local radiotherapy group compared
    with 2 after strontium-89 (p lt 0.01)
  • Platelets and leukocytes fell by an average
    30-40 after strontium-89 but sequelae were
    uncommon, and other symptoms rare

61
Samarium 153
  • Man made radionuclide that emits beta particles
    and gamma photons
  • T1/2 of 46.3 hours
  • Maximum energy of 0.81 MeV
  • Once chelated to a phosphatate it becomes a bone
    seeking complex
  • About 50 of administered stays within the bone

62
Samarium 153
  • 118 patients w/ painful bone metastases
  • All tumor types (68 prostate)
  • 1.0mCi/kg 153Sm, 0.5mCi/kg 153Sm, or placebo
  • If no relief in 4-weeks placebo patients
    eligible for crossover
  • 72 higher dose patients had pain relief
  • Significant benefit compared to placebo
  • No survival difference
  • Mild decrease in WBC and platelets

63
Spinal Cord Compression
  • Occurs in 5 of all patients with malignant
    disease and 20 of patients with vertebral
    metastases
  • More than 95 due to extra-medullary malignancy
  • Most commonly secondary to involvement of
    vertebral column anterior to the cord

64
Signs and Symptoms
  • Common symptoms pain, motor loss, autonomic
    dysfunction, and sensory loss
  • Pain is initial symptom in 96
  • Often radicular present for weeks-months before
    neurologic symptoms
  • Weakness usually precedes sensory loss
  • Incontinence, paraplegia, and paralysis are late
    effects

65
Cord Compression Diagnosis
  • Carefull HP (for specific symptoms as well as
    timeline of symptoms)
  • MRI is study of choice
  • CT myelogram (if patients cannot have MRI)
  • Dianosis/treatment often delayed
  • About 10 of patients will have multiple sites
    involved
  • Imaging of entire spine recommended

66
MRI of the same patient
L-4 comp Fx (Breast CA)
67
Treatment
  • Initially 10-20 mg of Decadron IV followed with 4
    mg q 6 hours
  • Start on PPI and monitor blood sugar
  • Careful taper of steroids necessary toward the
    end of palliative RT

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69
Decompression /- RT
  • 101 patients with metastatic disease
  • Lymphoma primary spine tumor excluded
  • Treatment
  • Direct circumferential surgical decompression
    followed by RT (30Gy/Gy w/in 14 days)
  • RT alone (30Gy/Gy)
  • Surgery RT improved
  • Ambulatory rate (84 vs 57)
  • Retained the ability to walk (median 122 vs 13
    days)
  • Decreased doses of steroids and analgesics

70
Dosing and Outcome
  • 3 Gy x 10 and 4 Gy x 5 are typical
  • Longer life expectancy can be treated with 2.5 Gy
    x 15
  • Outcome dependent on pretreatment function
  • 80 ambulatory will remain ambulatory
  • 16 non-ambulatory will become ambulatory
  • Worse response with greater degree of compression
    fracture at the level of compression

71
Radiation Doses Rades JCO 2005
Retrospective analysis 1304pts treated from
1992-8003
72
Brain Metastases
  • Incidence of brain mets is 20-40 of all patients
    diagnosed with cancer
  • Lung, breast, colon, and melanoma most common
  • Multiple sites much more common than single
  • 80 in cerebral hemispheres
  • 15 in cerebellum
  • 5 in brainstem
  • Contrast enhanced MRI is study of choice

73
Treatment
  • WBRT is treatment of choice for most patients
  • Goal is to limit tumor progression
  • Clinical dosing varies from 20 Gy in 5 fractions
    to 40 Gy in 20 fractions
  • Side Effects
  • Short-term alopecia, scalp irritation, transient
    worsening of symptoms, otitis
  • Long-term memory loss, decreased concentration

74
Single Metastases
  • Three RCTs have been done comparing WBRT to
    surgeryWBRT
  • Relatively small studies
  • Two showed median survival advantage (one
    significant-Patchell)

75
Stereotactic Radiosurgery (SRS)
  • Competing modality to surgery
  • Without the disadvantage of a craniotomy
  • Size limited to lesions lt3-4 cm
  • RTOG 9805 randomized patients to WBRT (167) vs.
    WBRTSRS (167) All with 1-3 lesions
  • Survival advantage in the WBRTSRS group for
    patients with a single metastasis (median
    survival 6.5 vs 4.9 months, p0.0393)
  • SRS group more stable or improved Karnofsky
    Performance Status (KPS) score at 6 months' F/U
    (43 vs 27, respectively p0.03)
  • By multivariate analysis, survival improved in
    patients with an RPA class 1 (plt0.0001)
  • OS improved in patients with an RPA class 1
    (plt0.0001)
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