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HODGKIN LYMPHOMA IN CHILDREN

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HODGKIN LYMPHOMA IN CHILDREN Dr.M.Shamvil Ashraf Children Cancer Hospital, Karachi. Hodgkin Lymphoma One of the most curable cancer in children There are different ... – PowerPoint PPT presentation

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Title: HODGKIN LYMPHOMA IN CHILDREN


1
HODGKIN LYMPHOMA IN CHILDREN
  • Dr.M.Shamvil Ashraf
  • Children Cancer Hospital,
  • Karachi.

2
Hodgkin Lymphoma
  • One of the most curable cancer in children
  • There are different effective treatment
    approaches
  • Can be cured with limited resources

3
Epidemiology
  • Developed Countries
  • 5 - 6 of childhood cancers
  • MaleFemale 3-41 in lt10y
  • MaleFemale 1.31 in gt10y
  • Bimodal age peak- adolescent/young adult, 50yo
  • Uncommon in lt10 yrs
  • Karachi Data
  • 10 of childhood cancers
  • MaleFemale 4.71 in lt10y
  • MaleFemale 1.71 in gt10y
  • gt 5 years 24
  • gt10years 62

4
Biology
  • Inflammatory milieu with rare multinucleated
    giant cells (Reed-Sternberg cells) or large
    mononuclear cell variants (Hodgkins or lacunar
    cells)
  • R-S cell appears to arise from preapoptotic
    germinal center B cells (no Ig production),
    although rarely may arise from T cells

5
RS cells
6
Lacunar Cells
7
Cellular Classification
  • Classical HL (CD15, CD30 , B cell markers )
  • nodular sclerosis (50-60)
  • mixed-cellularity (20-30)
  • lymphocyte rich (lt5)
  • lymphocyte depleted (5-15)
  • Nodular Lymphocyte Predominant HL (5) (CD15 -,
    CD30 /-, B cell markers )

8
Pathological Subtypes Karachi Data
13 (16.2)
2 (2.5)
21 (26)
44 (55)
9
Clinical Presentation
  • Painless adenopathy (80)
  • B symptoms (25-30)
  • fever gt380C x 3 days
  • wt loss gt10 of body wt. over 6 mo
  • drenching night sweats
  • Bulky disease (20)
  • med mass gt1/3 of internal thoracic diameter
  • node/nodal aggregate gt6 cm

10
Clinical Presentation
  • 15 to 20 of patients will have noncontiguous
    extranodal involvement
  • The most common sites of extranodal involvement
    are the lung, liver, bones, and bone marrow

11
Hodgkin vs TB
  • Most common differential especially if limited to
    cervical
  • Often put on ATT without definitive diagnosis
  • Biopsy is essential

12
Diagnosis
  • Excision Biopsy of Node
  • Needle Biopsy of mass if excision not possible
  • FNAC is not recommended in children

13
Staging
  • Ann Arbor staging system I-IV
  • A vs B
  • E- extralymphatic disease resulting from direct
    extension of involved LN region
  • S- splenic disease
  • ideally want pathologic confirmation of
    noncontiguous extralymphatic involvement (Stage
    IV disease)

14
Ann Arbor Staging
  • Stage I Involvement of single lymph node region
    (I) or localized involvement of a single
    extralymphatic organ or site (IE)
  • Stage II Involvement of two or more lymph node
    regions on the same side of the diaphragm (II) or
    localized involvement of a single extralymphatic
    organ or site and its regional lymph node(s) with
    involvement of one or more lymph regions on the
    same side of the diaphragm (IIE)
  • Stage III Involvement of lymph node regions on
    both sides of the diaphragm (III), which may also
    be accompanied by localized involvement of an
    extralymphatic organ or site (IIIE), by
    involvement of the spleen (IIS), or both (III
    ES)
  • Stage IV Disseminated (multifocal) involvement
    of one or more extralymphatic organs or tissues,
    with or without associated lymph node
    involvement, or isolated extralymphatic organ
    involvement with distant (non-regional) nodal
    involvement.

15
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16
Staging Workup
  • Imaging
  • CXR
  • U/Sound
  • CT scan of neck, chest, abdomen and pelvis
  • Gallium
  • PET Scan
  • Other Tests
  • Bone marrow aspirate and trephine only in
  • Patients with stage II B or more
  • Bone scan only in stage III or more
  • Blood tests
  • CBC
  • LDH
  • Urea, Cr, electrolytes, Ca, Mg, LFTs
  • Hepatitis screening

17
Therapy History
  • XRT alone cured early stage disease
  • 1960s- MOPP
  • 1970s- ABVD
  • Combined modality therapy (CMT)? Chemotherapy and
    radiation

18
Therapy History
  • Good results were obtained but at the cost of
    severe late toxicities
  • XRT profound musculoskeletal growth retardation
    and increase the risk for cardiovascular disease
    and secondary solid malignancies in children
  • Chemotherapy induced gonadal injury,cardiovascular
    disease and SMN

19
Combination Chemotherapy Regimens Commonly Used
for Children and Young Adults with Hodgkin
Lymphoma
ABVD doxorubicin (Adriamycin), bleomycin, vinblastine, dacarbazine
ABVE doxorubicin (Adriamycin), bleomycin, vincristine, etoposide
VAMP vincristine, doxorubicin (Adriamycin), methotrexate, prednisone
OPPA /- COPP vincristine, prednisone, procarbazine, doxorubicin, cyclophosphamide, vincristine (Oncovin), prednisone, procarbazine
COPP/ABV cyclophosphamide, vincristine (Oncovin), prednisone, procarbazine, doxorubicin (Adriamycin), bleomycin, vinblastine
BEACOPP bleomycin, etoposide, doxorubicin (Adriamycin), cyclophosphamide, vincristine (Oncovin), prednisone, procarbazine
20
Hodgkins Therapy in 90s
  • Prognostic factors and risk grouping concept
    introduced
  • Radiation dose and field were reduced
  • Involved Field Radiotherapy introduced
  • Chemotherapy regimen were manipulated
  • to reduce cumulative dose and avoid long term
    toxicities

21
Determining Risk Assignment
I
22
Chemotherapy Options
23
Current Approaches
  • Current approaches use chemotherapy with or
    without LD-IFRT
  • An exception to this general approach is selected
    patients with stage I, completely resected,
    nodular lymphocyte-predominant Hodgkin lymphoma,
    whose initial treatment may be surgery alone.
  • The number of cycles and intensity of
    chemotherapy may be determined by the rapidity
    and degree of response, as is the radiation dose
    and volume.

24
Approach for Developing Countries
  • Chemotherapy Alone
  • If radiotherapy is not available
  • Pediatric radiotherapy service is not developed
  • Good result (up to 80 survival) can be obtained
    as shown by Indian Experience
  • (Arya et al)

25
Approach for Developing Countries
  • Chemotherapy with Radiotherapy only for bulky
    residual disease
  • Excellent result can be achieved with this
    approach as shown by our experience at Children
    Cancer Hospital

26
CCH Data
  • Retrospective study
  • From Aug 2000 - 2007All the patients with
    histopathological diagnosis of Hodgkin Lymphoma,
    up to 20 years of age were included
  • Mean age 9.9 yrs
  • Pts. included in the study 80

27
Treatment Strategy At CCH
  • Chemotherapy used was alternating courses of
  • ABVD (adriamycin, bleomycin, vincristine and
    dacarbazine)
  • COPDAC (cyclophophamide, vincristine,
    prednisolone and dacarbazine)
  • Radiotherapy was reserved only for the pts. with
    significant residual disease at the end of
    chemotherapy

28
Response Assessment
  • CT scan of all the sites positive on pre
    treatment scan was repeated after 2 cycles
  • Bone marrow or bone scan was repeated only if it
    was positive initially
  • For good responder CT was repeated after 6 cycles
  • PET scan could not be performed because of
    non-availability

29
Response Assessment Criteria
  • CR was taken as complete resolution of all
    measurable disease, clinically and radiologically
  • gt80 response was taken as good response
  • 60 to 80 was taken as partial response
  • lt60 was taken as poor response or stable disease
  • Any increase in the size of an existing lesion or
    appearance of any new lesion during treatment was
    taken as progressive disease

30
Response Adapted Therapy
  • Low risk patients with CR after 2 courses
    received 4 courses
  • All other pts were given 6 8 courses depending
    upon the response (CR 2 courses)
  • 11(13.7) pts received 4 courses
  • Majority of pts 56 (70) received 6 courses

31
Radiation Therapy
  • Radiation therapy was reserved only for the pts
    with residual disease at the end of chemo
  • only 8 (10) needed radiation
  • Stage II A 1 pt
  • Stage II B 1 pt
  • Stage III B 3 pts
  • Stage III BS 1 pt
  • Stage IV 2 pts

32
Results
  • 74 (92) pts achieved first remission (CR) after
    2 courses of chemotherapy
  • Only one pt. died during chemotherapy due to
    meningitis
  • One pt. relapsed on treatment and was switched to
    second line treatment
  • 4 (5) pts relapsed 2 12 months after
    completion of chemotherapy
  • 3 yrs OS 98 and EFS 92

33
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34
Progressive/Relapsed Ds
  • Prognostic factors
  • progressive ds or relapse at lt1y from end of
    treatment
  • B symptoms
  • extranodal ds
  • response to salvage therapy

35
Chemotherapy Options
  • Salvage therapies (with harvest)?
  • ICE, EPIC,mini-BEAM, DHAP, ASHAP,
    bortezomib/ifos/vinorelbine (AHOD 0521)?, GDP
    (PMH)
  • Autologous transplant
  • conditioning CBV, BEAM, VP16/melphalan
  • BEAM plus immunomodulation (AHOD 0121)?- closed

36
Refractory Disease
  • Gemcitabine/Vinorelbine AHOD 0321- closed
  • eligibility gt/ 2 prior regimens
  • beware non-cardiogenic pulmonary edema
  • may require 4-6 cycles to see response
  • Vinblastine, lomustine, VP16
  • New agents/targeted therapies

37
Late Effects
  • Cardiotoxicity and Musculoskeletal problems are
    now rare
  • Endocrine
  • Thyroid Hypothyroidism
  • Fertility
  • Increased risk of ovarian failure in women
  • Oligospermia and sterility in men
  • Second Malignant Neoplasm

38
Conclusion
  • Chemotherapy alone in majority of patients with
    Hodgkin Lymphoma can yield excellent outcome
  • Most of Hodgkin Disease pts can be managed
    without the use of radiotherapy, thereby
    minimizing the adversity associated with
    radiation, specially in young children
  • Hodgkin Lymphoma can be cured within limited
    resources
  • Monitoring for late effects is important
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