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Bone sarcoma

      Ahmed Zeeneldin
Associate Professor of Medical
          Oncology
GTNM Staging BS, 2010
• T1: <= 8 cm
• T2: > 8 cm
• T3: Discontinuous tumors in the primary bone site
• No T4 like ovaries

• N1: regional LN (RARE)                     T1    T2    T3    N1    M1a/b
• M1a: lung mets                    LG, GX   IA    IB    IB    IVB   IVA/IVB
• M1b: non-lung distant mets        HG       IIA   IIB   III   IVB   IVA/IVB

• Low grade: G1, 2
• High grade: G3,4
• Grade cannot be assessed: GX
Surgical Staging system 1980
• T1: intracompartmental
• T2: extracompartmental
                                T1    T2    N1    M1
• N1: regional LN (RARE)   LG   IA    IB    III   III

• M1: distant mets         HG   IIA   IIB   III   III




• Low grade: G1, 2
• High grade: G3,4
Incidence
• Rare: 0.2% of all cancers
• Often curable
• Common forms:
   – Osteosarcoma (35%), OS
   – Chondrosarcoma (30%), CS
   – Ewing’s sarcoma (16%), ES
   – Malignant fibrous histiocytoma (MFH) and
     fibrosarcoma (FS) (<1%)
   – Others hemangioendothelioma (HET) and
     hemangiopericytoma (HPC), and chordoma: very rare
CS             OS             ES             MFH         HET        Chor
                                                                  HPC        doma
age      Middle age     Children       Children
         Older adults   Young adults   Young adults
Origin   Cartilage      bone           ?              Fibrous T   vascular   notochord
Multidisciplinary Team
• Core group
   –   Bone pathologist
   –   Musculoskeletal radiologist
   –   Orthopaedic oncologist
   –   Medical/pediatric oncologist
   –   Radiation oncologist
• Specialists critical in certain cases
   –   Thoracic surgeon
   –   Plastic surgeon
   –   Interventional radiologist
   –   Physiatrist
   –   Vascular surgeon
   –   Additional surgical subspecialties
Workup
Workup
• Radiology:
  – Primary site:
     • Plain film, MRI and or CT, bone scan
  – Exclude mets and other lesions:
     • Chest x-ray or CT
     • Bone scan, PET
• Lab:
  – CBC, LDH, Alk Phos, Ca
  – Biopsy: Core needle or surgical (better at treating
    center)
Chondrosarcoma (CS)
CS
• Produce cartilage matrix without bone
• Occur at any age, but more common in older
  adults
• Types:
  – Conventional CS: 85%
     • 1ry or central: from normal bone
     • 2ry or peripheral: from preexisting lesion
  – Other types CS: 10-15%
     • Clear cell
     • Dedifferentiated
     • Myxoid and mesenchymal
CS treatment
Chemotherapy in CS
• Not sensitive to chemo especially
  conventional
• Dedifferentiated and mesenchymal are more
  sensitive
  – Dedifferentiated: treat as OS (cisplatin doxo)
  – Mesenchymal: treat as ES (VACD, VAIA, EVIAI)
Ewing’s sarcoma (ES)
ES
• adolescents and young adults
• All ES are undifferentiated
• Common sites: femur, pelvic bones, and the
  bones of chest wall, but any bone can be
  affected
• Diaphysis is the commonest area
• Symptoms:
  – Pain and swelling
  – Constitutional: fever, weight loss, and fatigue
Xray

On imaging, the
bone appears
mottled.
Periosteal
reaction is
classic and it is
referred to as
“onion skin
Ewing Sarcoma Family of tumors
                 ESFT
•   Ewing’s sarcoma,
•   extraosseous Ewing’s sarcoma
•   Askin’s tumor,
•   Primitive neuroectodermal tumor (PNET),
•   PNET of bone
ES genetics

- fusion of EWS
gene on chr 22q
WITH
ETS gene family
(FLI1) on chr 11
- Found in 85%
of ES
ES IHC
strong expression of cell-surface
glycoprotein MIC2 (CD99)
Prognostic factors
• Good
   – Distal site
   – Absence of mets
   – Normal LDH
• Risk stratification:
   – High risk: mets, high disease volume (< 100 ml)
   – Low/standard risk: no mets, low disease vol(> 100
     ml)
Treatment of ES
Treatment of non-progressive disease
Chemotherapy in ES
• Drugs                        • Metastatic:
  –   V: vincreistine             – VDC
  –   A: dactinomycin             – Others
  –   C: cyclophosphamide      • Nonmetastatic : more
  –   D (A): doxorubicin         intensive
  –   I: fosfamide                – Include etoposide
  –   E: etoposide                – Alternating cycles
• Regimens
  –   VAC vs VACD (IESSI-II)
  –   VACD vs VACD/IE
  –   VAIA vs VACA
  –   VAIA vs EVAIA
VAC vs VACD




           VAC (IESS-I)   VACD (IESS-II)
RFS        24             60%
OS                        Better
toxicity                  More
VACD vs VACD/IE
VACD vs VACDlIE
Non-metastatic disease            Metastatic disease
           VACD   VACD/IE P                   VACD   VACD/IE P
N          ~200   ~200             N          ~120   ~120
5- y EFS   55%    70%     0.005    5- y EFS   22%    22%     0.81
5-y OS     61     72%     0.01     5-y OS     34%    35%     0.43
Figure 1. Event-free Survival According to Study Group   Figure 2. Event-free Survival According to Study Group
and the Presence or Absence of Metastatic Disease.       and Tumor Site among Patients without Metastases
VACD vs VAIA vs EVAIA
VACA vs VAIA vs EVAIA
Standard risk (localized, low volume < 100 ml)   High-risk (metastatic, high volume > 100 ml)
VAIA = VAID, VACA= VACD                          VAIA = VAID

            VAIAà        VAIAà        P                        EVAIA        VAIA         P
            VAIA         VACA
N           79           76                       N            252          242
3- y EFS    74%          73%          NS          3- y EFS     52%          47%          NS
3-y OS      86           90%          NS          3-y OS       62           59           NS
Toxicity    Less         more
Relapsed or Refractory ES
• Good Prognostic factors:
  – Time to Rec => 2years
  – Local recurrence treatable by surgery and
    intensive chemo
  – Lug only mets
  – Non-elevated LDH
Treatment of relapsed or refractory ES
• Relapse => 2years:
  – the same initial therapy can be used
• Relapse < 2 years:
  – Cyclophosphamide and topotecan
  – Temozolomide and irinotecan
  – Ifosfamide and etoposide
  – Ifosfamide, carboplatin and etoposide
  – Docetaxel and gemcitabine
Osteosarcoma (OS)
OS
• Commonest bone malig in children and young
  adults
• Sites of max bone growth (distal femur and
  prox tibia)
• Types:
• Classic: 80%
Prognostic factors
• Tumor site (distal vs prox)
• Tumor size (small vs large)
• Metastases (no vs yes)
• Metastatic site (lung vs non-lung)
• Number of lung mets (few/resectable vs
  many/iresectable)
• Response to chemotherapy ( good vs poor)
• Resection (R0 vs R1)
• LDH (normal vs elevated)
OS plain x ray
• Plain radiographs show
  cortical destruction and
  irregular reactive bone
  formation
Workup in OS
• Imaging:
  – For 1ry:
     • Plain radiograph
     • MRI (BEST) and or CT
     • Bone scan
  – For 2ry:
     • CT chest, bone scan
• Lab: LDH, ALP
Treatment
• Surgery (limb sparing or amputation) AND
• Adjuvant or neoadjuvant chemotherapy
Chemotherapy regimens
•   First line (adj/neoadj/primary)
     –   Cisplatin and doxorubicin
     –   MAP (High-dose methotrexate, cisplatin and doxorubicin)
     –   Doxorubicin, cisplatin, ifosfamide and high-dose methotrexate
     –   Ifosfamide and etoposide
     –   Ifosfamide, cisplatin and epirubicin
•   Second line (relapsed and refractory)
     –   Docetaxel and gemcitabine
     –   Cyclophosphamide and etoposide
     –   Cyclophosphamide and topotecan
     –   Gemcitabine Ifosfamide and etoposide
     –   Ifosfamide, carboplatin and etoposide
     –   High-dose methotrexate, etoposide and ifosfamide
•   Third line
     – Resection
     – RT
     – Samarium
Treatment of OS
Adjuvant CT better than observation
As in the historical experience,
50% of the patients suffered relapse within six months of diagnosis, and
overall, more than 80% developed recurrent disease.
Fewer than 20% of patients treated only with surgery of the primary tumor can be expected to survive free of recurrent disease.
Thus adjuvant chemotherapy should be recommended to all patients with high-grade osteosarcoma of the extremity
Short equal to long CT regimens in operable OS




               Short                       Long
Drugs          Doxorubicin 25 mg/m2 D1–3   preoperatively ( 7wks)
               cisplatin 100 mg/m2 D1      vincristine, high-dose methotrexate,
               preoperatively (9wks)       and doxorubicin;
               postoperatively (9 wks)     postoperatively (37 wks) bleomycin,
                                           cyclophosph, dactinomycin,
                                           vincristine, methotrexate, doxorubicin,
                                           cisplatin
Cycles/weeks   6 cycles (18 wks)           44 weeks
Results
PFS the same       OS the same
Two drugs Multiagent
             (Cis-Adria)
Treatment    94%       51%
completion
TOXICITY     Similar   similar
> 90% tumor 29%        29%
necrosis
Ifosfamide/etoposide in met OS
Adding ifosfamide to cisplatin
  Epirubicin in non-met OS
Indirect comparison
               Cisplatin –     Cisplatin –
               adriamycin      epirubicin –
                               ifosfamide
               APx3 àS àAPx3   PEI x 3 àS àPEI x 3
Treatment      94%             84%
complateion

Complete R                     26%
Good R         29%             37%
5-y DFS                        42%
5-y OS                         48%
AP vs PEI
Neoadj CT
High dose CT and SCT
•   Investigational
•   High risk metastatic and relapsed
•   TRM 3%
•   3-y DFS: 12%
•   3-y OS: 21%
Good response (>90% necrosis) to Neoadj chemo is a
good prognostic factor
Bone sarcoma

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Bone sarcoma

  • 1. Bone sarcoma Ahmed Zeeneldin Associate Professor of Medical Oncology
  • 2. GTNM Staging BS, 2010 • T1: <= 8 cm • T2: > 8 cm • T3: Discontinuous tumors in the primary bone site • No T4 like ovaries • N1: regional LN (RARE) T1 T2 T3 N1 M1a/b • M1a: lung mets LG, GX IA IB IB IVB IVA/IVB • M1b: non-lung distant mets HG IIA IIB III IVB IVA/IVB • Low grade: G1, 2 • High grade: G3,4 • Grade cannot be assessed: GX
  • 3. Surgical Staging system 1980 • T1: intracompartmental • T2: extracompartmental T1 T2 N1 M1 • N1: regional LN (RARE) LG IA IB III III • M1: distant mets HG IIA IIB III III • Low grade: G1, 2 • High grade: G3,4
  • 4. Incidence • Rare: 0.2% of all cancers • Often curable • Common forms: – Osteosarcoma (35%), OS – Chondrosarcoma (30%), CS – Ewing’s sarcoma (16%), ES – Malignant fibrous histiocytoma (MFH) and fibrosarcoma (FS) (<1%) – Others hemangioendothelioma (HET) and hemangiopericytoma (HPC), and chordoma: very rare
  • 5. CS OS ES MFH HET Chor HPC doma age Middle age Children Children Older adults Young adults Young adults Origin Cartilage bone ? Fibrous T vascular notochord
  • 6. Multidisciplinary Team • Core group – Bone pathologist – Musculoskeletal radiologist – Orthopaedic oncologist – Medical/pediatric oncologist – Radiation oncologist • Specialists critical in certain cases – Thoracic surgeon – Plastic surgeon – Interventional radiologist – Physiatrist – Vascular surgeon – Additional surgical subspecialties
  • 8. Workup • Radiology: – Primary site: • Plain film, MRI and or CT, bone scan – Exclude mets and other lesions: • Chest x-ray or CT • Bone scan, PET • Lab: – CBC, LDH, Alk Phos, Ca – Biopsy: Core needle or surgical (better at treating center)
  • 10. CS • Produce cartilage matrix without bone • Occur at any age, but more common in older adults • Types: – Conventional CS: 85% • 1ry or central: from normal bone • 2ry or peripheral: from preexisting lesion – Other types CS: 10-15% • Clear cell • Dedifferentiated • Myxoid and mesenchymal
  • 12. Chemotherapy in CS • Not sensitive to chemo especially conventional • Dedifferentiated and mesenchymal are more sensitive – Dedifferentiated: treat as OS (cisplatin doxo) – Mesenchymal: treat as ES (VACD, VAIA, EVIAI)
  • 14. ES • adolescents and young adults • All ES are undifferentiated • Common sites: femur, pelvic bones, and the bones of chest wall, but any bone can be affected • Diaphysis is the commonest area • Symptoms: – Pain and swelling – Constitutional: fever, weight loss, and fatigue
  • 15. Xray On imaging, the bone appears mottled. Periosteal reaction is classic and it is referred to as “onion skin
  • 16. Ewing Sarcoma Family of tumors ESFT • Ewing’s sarcoma, • extraosseous Ewing’s sarcoma • Askin’s tumor, • Primitive neuroectodermal tumor (PNET), • PNET of bone
  • 17. ES genetics - fusion of EWS gene on chr 22q WITH ETS gene family (FLI1) on chr 11 - Found in 85% of ES
  • 18. ES IHC strong expression of cell-surface glycoprotein MIC2 (CD99)
  • 19. Prognostic factors • Good – Distal site – Absence of mets – Normal LDH • Risk stratification: – High risk: mets, high disease volume (< 100 ml) – Low/standard risk: no mets, low disease vol(> 100 ml)
  • 22. Chemotherapy in ES • Drugs • Metastatic: – V: vincreistine – VDC – A: dactinomycin – Others – C: cyclophosphamide • Nonmetastatic : more – D (A): doxorubicin intensive – I: fosfamide – Include etoposide – E: etoposide – Alternating cycles • Regimens – VAC vs VACD (IESSI-II) – VACD vs VACD/IE – VAIA vs VACA – VAIA vs EVAIA
  • 23. VAC vs VACD VAC (IESS-I) VACD (IESS-II) RFS 24 60% OS Better toxicity More
  • 25. VACD vs VACDlIE Non-metastatic disease Metastatic disease VACD VACD/IE P VACD VACD/IE P N ~200 ~200 N ~120 ~120 5- y EFS 55% 70% 0.005 5- y EFS 22% 22% 0.81 5-y OS 61 72% 0.01 5-y OS 34% 35% 0.43
  • 26. Figure 1. Event-free Survival According to Study Group Figure 2. Event-free Survival According to Study Group and the Presence or Absence of Metastatic Disease. and Tumor Site among Patients without Metastases
  • 27. VACD vs VAIA vs EVAIA
  • 28. VACA vs VAIA vs EVAIA Standard risk (localized, low volume < 100 ml) High-risk (metastatic, high volume > 100 ml) VAIA = VAID, VACA= VACD VAIA = VAID VAIAà VAIAà P EVAIA VAIA P VAIA VACA N 79 76 N 252 242 3- y EFS 74% 73% NS 3- y EFS 52% 47% NS 3-y OS 86 90% NS 3-y OS 62 59 NS Toxicity Less more
  • 29. Relapsed or Refractory ES • Good Prognostic factors: – Time to Rec => 2years – Local recurrence treatable by surgery and intensive chemo – Lug only mets – Non-elevated LDH
  • 30. Treatment of relapsed or refractory ES • Relapse => 2years: – the same initial therapy can be used • Relapse < 2 years: – Cyclophosphamide and topotecan – Temozolomide and irinotecan – Ifosfamide and etoposide – Ifosfamide, carboplatin and etoposide – Docetaxel and gemcitabine
  • 32. OS • Commonest bone malig in children and young adults • Sites of max bone growth (distal femur and prox tibia) • Types: • Classic: 80%
  • 33. Prognostic factors • Tumor site (distal vs prox) • Tumor size (small vs large) • Metastases (no vs yes) • Metastatic site (lung vs non-lung) • Number of lung mets (few/resectable vs many/iresectable) • Response to chemotherapy ( good vs poor) • Resection (R0 vs R1) • LDH (normal vs elevated)
  • 34. OS plain x ray • Plain radiographs show cortical destruction and irregular reactive bone formation
  • 35. Workup in OS • Imaging: – For 1ry: • Plain radiograph • MRI (BEST) and or CT • Bone scan – For 2ry: • CT chest, bone scan • Lab: LDH, ALP
  • 36. Treatment • Surgery (limb sparing or amputation) AND • Adjuvant or neoadjuvant chemotherapy
  • 37. Chemotherapy regimens • First line (adj/neoadj/primary) – Cisplatin and doxorubicin – MAP (High-dose methotrexate, cisplatin and doxorubicin) – Doxorubicin, cisplatin, ifosfamide and high-dose methotrexate – Ifosfamide and etoposide – Ifosfamide, cisplatin and epirubicin • Second line (relapsed and refractory) – Docetaxel and gemcitabine – Cyclophosphamide and etoposide – Cyclophosphamide and topotecan – Gemcitabine Ifosfamide and etoposide – Ifosfamide, carboplatin and etoposide – High-dose methotrexate, etoposide and ifosfamide • Third line – Resection – RT – Samarium
  • 39. Adjuvant CT better than observation
  • 40. As in the historical experience, 50% of the patients suffered relapse within six months of diagnosis, and overall, more than 80% developed recurrent disease. Fewer than 20% of patients treated only with surgery of the primary tumor can be expected to survive free of recurrent disease. Thus adjuvant chemotherapy should be recommended to all patients with high-grade osteosarcoma of the extremity
  • 41. Short equal to long CT regimens in operable OS Short Long Drugs Doxorubicin 25 mg/m2 D1–3 preoperatively ( 7wks) cisplatin 100 mg/m2 D1 vincristine, high-dose methotrexate, preoperatively (9wks) and doxorubicin; postoperatively (9 wks) postoperatively (37 wks) bleomycin, cyclophosph, dactinomycin, vincristine, methotrexate, doxorubicin, cisplatin Cycles/weeks 6 cycles (18 wks) 44 weeks
  • 42. Results PFS the same OS the same
  • 43. Two drugs Multiagent (Cis-Adria) Treatment 94% 51% completion TOXICITY Similar similar > 90% tumor 29% 29% necrosis
  • 45.
  • 46. Adding ifosfamide to cisplatin Epirubicin in non-met OS
  • 47. Indirect comparison Cisplatin – Cisplatin – adriamycin epirubicin – ifosfamide APx3 àS àAPx3 PEI x 3 àS àPEI x 3 Treatment 94% 84% complateion Complete R 26% Good R 29% 37% 5-y DFS 42% 5-y OS 48%
  • 49.
  • 51. High dose CT and SCT • Investigational • High risk metastatic and relapsed • TRM 3% • 3-y DFS: 12% • 3-y OS: 21%
  • 52.
  • 53. Good response (>90% necrosis) to Neoadj chemo is a good prognostic factor