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    COG CNS Committee

    2003-2007Ian Pollack

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    Identify biological characteristics ofchildhood CNS tumors that influencetreatment response, and initiate risk-adaptedstratification.

    Develop comprehensive treatmentapproaches to improve survival and quality oflife for children with primary CNS tumors.

    Identify effective therapies for CNS tumorsresistant to prior treatments.

    Define and validate strategies for reducingtreatment-related long-term sequelae.

    Scientific Goals

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    Medullo

    PNET

    Infant

    Tumors

    GermCell

    Ependymoma

    Low-Grade

    Glioma

    High-Grade

    Glioma

    Brainstem

    Glioma

    Optimize

    Chemo to

    Reduce

    Sequelae

    AAA999999666111

    ACNS0331

    CCCCCCGGG---

    999999777000333AAACCCNNNSSS---

    000222333222AAACCCNNNSSS---

    000444222111AAA999999555222

    Optimize RT

    DeliveryACNS0331 PPP999999333444

    AAACCCNNNSSS---

    000111222111AAACCCNNNSSS---

    000222222111

    Chemo-RT

    CCCCCCGGG---999999777000111

    AAACCCNNNSSS000333333222

    PPPOOOGGG---999666333111

    AAACCCNNNSSS000333333333 AAACCCNNNSSS---000111222666

    CCCCCCGGG---999777111222

    CCCC

    CCG

    GG-

    --999888000222PPPOOOGGG---999888333666

    AAACCCNNNSSS000111222666

    AAACCCNNNSSS000222222222AAACCCNNNSSS000222222444

    Intensifying

    ChemoCCCCCCGGG---999999777000222

    CCCCCCGGG---

    999999777000333

    AAACCCNNNSSS000333333444

    AAACCCNNNSSS---

    000111222222

    AAACCCNNNSSS---

    000111222111

    AAACCCNNNSSS---

    000222222333

    AAADDDVVVLLL000000111111

    ACNS0423

    AAACCCNNNSSS000222333111

    CNS Committee Cross-Study

    Therapeutic Hypotheses

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    Observation that the use of adjuvantchemotherapy permits CSRT dose reduction

    to 2340 cGy with >75% survival for M0

    medulloblastoma.

    Demonstration that extent of resection is

    associated with outcome for children with

    medulloblastoma,ependymoma, low- and

    high-grade glioma. Initiation of the largest biological study to date

    of high-grade gliomas of childhood, and

    preliminary delineation of prognostic factors.

    Cooperative Group Scientific

    Accomplishments

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    0%

    20%

    40%

    60%

    80%

    100%

    0 2 4 6 8 10

    Survival

    POG-8631/CCG-923 (Reduced

    DoseXRTAlone, N=46)

    CCG-9892 (Reduced

    XRT+ Chemo, N=65)

    POG-8631/CCG-923 (Standard

    Dose XRTAlone, N=42)

    Packer et al. JCO 17: 2127, 1999; Thomas et al. JCO 18: 3004, 2000Years Post Onstudy

    Reduced Dose Radiotherapy Is Feasible in

    Standard-Risk Medulloblastomas If

    Combined with Adjuvant Chemotherapy

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    0%

    20%

    40%

    60%

    80%

    100%

    0 2 4 6 8 10 12

    Years Post Onstudy

    Event-Free

    Sur

    vival

    >90% Resection (N=66)

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    Determination that moderately intensive chemoimproves survival for poor-risk medullo/PNET.

    Identification of molecular factors correlatedwith outcome of infant tumors.

    Documentation that building upon inductionchemo in infant tumors with high-doseconsolidation or focal irradiation improves

    outcome. However, despite improvements in the

    prognosis of some tumor types, others remainresistant and late effects remain a concern.

    Scientific Accomplishments

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    Management of Average-Risk

    Medulloblastomas1) Post fossa location

    2) M0

    3) < 1.5 cm2Residual

    A9961

    2340 cGy CSRT

    5580 cGy Local RT

    CCNU

    CPDDVCR

    CPM

    CPDDVCR N > 400

    Has provided a platform for additional study developmentGoals: 1) Further CSRT dose reduction by modifying chemo

    2) Target volume reduction (boost site) using conformal RT

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    A9961 Progression-Free Survival from Study Entry

    50%

    60%

    70%

    80%

    90%

    100%

    0 1 2 3 4 5 6 7

    Time (Years)

    Per

    centProgression-Free

    RegA RegB

    p=0.49

    86% +/- 2.5%

    84% +/- 3%

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    Accuracy of Staging Strongly Influences

    Effectiveness of Reduced Dose Therapy

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    Overall Survival for A9961 by Anaplasia

    0.00

    0.25

    0.50

    0.75

    1.00

    0 2 4 6 8 10

    Years from study entry

    Prob

    ability

    No Anaplasia (n=300)

    Anaplasia (n=55)

    p=0.04

    Figures 5 and 6 were based on all patients on A9961 with anaplasia information (including those

    ineligible by central review due to dissemination or excess residual).

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    RT Dose Reduction for Average-Risk

    Medulloblastoma (

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    ACNS0331

    Activation 4/04

    RT Dose Reduction for Average-Risk

    Medulloblastoma (>8 yrs)

    2340 cGy CSRT

    w/ VCR

    Conformal tumor

    bed boost (5400 cGy)

    Conformal post fossa

    boost (5400 cGy)

    CCNU, CPDD, VCR

    alt. with CPM, VCR

    Both strata include prospective

    Trk C and erbB2/4 analysis,

    expression profiling, andhistological review to identify ~

    20% of tumors that are notbiologically average risk SPECIMEN SUBMISSION

    STRONGLY ENCOURAGED.

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    High-Risk PNET

    Radiosensitization Study

    Craniospinal (36 Gy) XRT Boost (18 Gy) XRT

    Carbo Carbo Carbo (Carbo) (Carbo) (Carbo)VCR VCR VCR VCR VCR VCR

    week 1 2 3 4 5 6

    CPMVCR

    CDDPCPMVCR(CCG-99701)

    Phase I MTD establishedPhase II completed 12/04

    ACNS0332

    Protocol approved by

    CTEP/PCIRB

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    3 yr OS: 81 5%

    99701 Overall Survival for Metastatic MB

    0.00

    0.25

    0.50

    0.75

    1.00

    0 1 2 3 4 5 6 7

    Years from study entry

    Proba

    bility

    n=58

    3 yr OS: 81 + 5%

    2

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    3 yr OS is 89 5%

    3 yr OS is 64 12%

    0.00

    0.25

    0.50

    0.75

    1.00

    0 1 2 3 4 5 6 7

    Years from study entry

    Probability

    Anaplasia (n=19)

    No Anaplasia (n=39)

    p=0.008

    3 yr OS: 89 5%

    3 yr OS: 64 12%

    Overall Survival by Anaplasia

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    Progressive DiseaseHigh-risk, Unresectable

    < 10 years

    A9952

    Non-NF1

    CarboplatinVCR

    6-thioguanineProcarbazine

    CCNUVCR

    NF1

    Management of Low-Grade Glioma

    N=250

    randomized, 350 total

    New Studies

    Carbo/VCR/TMZ pilot

    ACNS0223 (protocolopened 7/04;

    recently opened

    groupwide - 32 pts)Conformal RT pilot

    ACNS0221

    (recently open)

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    0%

    10%

    20%

    30%

    40%

    50%

    60%

    70%

    80%

    90%

    100%

    0 1 2 3 4

    YEARS

    Event-FreeSurvival

    Regimen A (N=32)

    Regimen B (N=31)

    CCG-9941

    Jennings et al. JCO, 2002

    AA

    Intensive Chemotherapy Followed by

    Irradiation Fails to Alter Prognosis in Newly

    Diagnosed Brainstem Glioma

    Uniformly poor results of all

    recent studies provide for reliable

    natural history control data.

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    Phase I/II Studies of Radiosensitization

    and Chemo-Radiotherapy for Brainstem

    Gliomas

    Temozolomide (ACNS0126)closed 8/05

    accrued at twice rate projected (60/yr)

    standardized BSG stats (SPRT), imaging,response analysis in collaboration with PBTC

    Topotecan (ACNS 0224)protocol opened

    10/10/05

    Gadolinium texaphyrin Phase I completed (CCG-09712)

    Phase II protocol approved by CTEP/PCIRB - in queue to

    open (ACNS0222)

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    Combined Chemoradiotherapy for Non-

    Brainstem High-Grade Glioma(ACNS0126)

    Sequential study design Temozolomide qd w/RT, 5d schedule p-RT - done

    Natural history control (CCG-945 centrally

    reviewed cohort)

    100 pts each, 12-18 months accrual EFS endpoint

    Accrued at twice rate projected

    Preliminary results available

    Temozolomide + anti-angiogenic/signaling

    inhibitor/other chemotherapeutic agent

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    One year (GBM)

    945

    (53)

    126

    (51)

    p-value Stupp

    (287)

    EFS 32% 33% .47 27%

    OS 60% 64% .33 61%

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    Differences in MGMT Expression are

    Noted Among Childhood Malignant

    Gliomas and Correlate with PromoterMethylation

    2

    1 3

    4

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    Overall Survival for HGG by MGMT

    0.00

    0.25

    0.50

    0.75

    1.00

    0.0 0.5 1.0 1.5 2.0 2.5 3.0

    Years from study entry

    Probab

    ility

    No overexpression of MGMT (n=48)

    Overexpression of MGMT (n=22)

    p=0.032

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    Builds upon ADVL0011

    (CCNU/temozolomide) (1CR, 1 near CR, 2 PR,

    3 MR among 27 pts during induction MTD 90 mg/m2CCNU and 160 mg/m2x 5 TMD

    q6wk

    ACNS0423, opened 3/21/05has accrued 58

    pts

    A third study (ACNS0622) is under

    development (TMZ/irinotecan)

    Combined Chemoradiotherapy for Non-

    Brainstem High-Grade Glioma (ACNS0423)

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    Management of Germinomas(ACNS 0232)Approved by CTEP/CIRB

    Endpoints:EFS, QOL, Neuropsych

    Biopsy Confirmation-Markers

    Std RT (45Gy)

    21Gy Whole ventricular24 Gy boost to 1osite

    (30Gy CSR/15Gy 1ofor disseminated)

    < CR

    40.5 Gy to 1

    o

    site(24 Gy CSR/16.5 Gy 1ofor disseminated)

    CR

    30 Gy to 1

    o

    site(21Gy CSR/9 Gy 1ofor disseminated)

    Chemotherapy(Carbo/etoposide)

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    Management Paradigm for

    NGGCTs (ACNS0122)Tissue Diagnosis

    (Open/Stereo Bx)

    + Markers

    Induction ChemoCarbo/VP alt with

    Ifos/VP x 3

    CR(60%)

    < CR(40%)

    RT36 Gy CS Axis

    54 Gy Tumor Bed

    PBSC Harvest

    High Dose

    ChemoThiotepa/VP16

    Second LookSurgery

    Activation 1/04

    46 pts accrued

    E d M t S h

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    Ependymoma Management SchemaACNS0121 (Opened 8/25/03)

    Ependymoma

    Central Pathology Review

    Observation

    Extent of Resection: GTR 1

    Differentiated Histology

    Supratentorial

    Extent of Resection: STR

    Any Histology

    Any Location

    Chemotherapy

    Carboplatin/Vincristine

    Cyclophosphamide/EtoposideDuration: 7 weeks

    Response Evaluation

    (PD/SD/PR/CR)

    Conformal Radiation Therapy

    Total Dose: 59.4 Gy

    Clinical Target Volume: 1.0 cm

    Unresectable

    Conformal Radiation Therapy

    Total Dose: 59.4 Gy

    Clinical Target Volume: 1.0 cm

    Second Surgery

    Surgery Endpoint 1: Resectability

    Surgery Endpoint 2: Morbidity

    Resectable

    Extent of Resection: NTR/GTR 2

    Any Histology

    Any Location

    Extent of Resection: GTR 1

    Anaplastic Histology Supratentorial

    Any Histology Infratentorial

    Conformal Radiation Therapy

    Total Dose: 59.4 GyClinical Target Volume: 1.0 cm

    Novel Features

    1) Observation arm

    2) Histo-based stratification

    3) Chemo to increase rate of

    GTR via 2nd-look surgery

    4) Group-wide conformal RT

    (270 pts accrued, twicero ected rate5/62/76/127

    CCG 99 03 Ph I/II S d f I i

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    CCG-99703: Phase I/II Study of Intensive

    Consolidation Chemo with PBSC Support

    In fant B rain Tumors

    Completed: Results Pending

    Surgery

    Induction Chemotherapy(9921 Regimen A)

    PBSC harvesting

    ConsolidationCBDCA/Thio/VCR x 3 courses

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    Event-Free Survival

    0.00

    0.25

    0.50

    0.75

    1.00

    0 1 2 3 4 5 6 7 8

    Years from study entry

    Probabi

    lity CCG-99703 (n=92)

    CCG-9921 (n=284)

    Logrank p=0.025

    Event-Free Survival 99703 v 9921

    01/16/06

    BIOLOGICAL STRATIFICATION OF INFANT

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    0%

    20%

    40%

    60%

    80%

    100%

    0 1 2 3 4 5 6

    Years Post Onstudy

    Survival

    Rhabdoid (N=16)

    Non-Rhabdoid PNET (N=94)

    CCG-9921

    p=0.02

    BIOLOGICAL STRATIFICATION OF INFANT

    TUMORS: AT/RTs are prognostically distinct

    from PNETs and warrant distinct therapy

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    Histologicdiagnosis:PNET

    FISH:Deletion 22

    INI1 mutation analysis:Single base pair change

    Molecular Evaluation (FISH and Mutation

    Analysis) Will Be Included for Stratification on

    All Infant Malignant Tumor Studies

    Biegel et al. Cancer Res 59: 74, 1999; Cancer Res 62: 328, 2002

    M t f M0 I f t

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    Management of M0 Infant

    Medulloblastomas (P9934)

    Resection

    Staging8-36 months

    Induction

    Chemotherapy4 4-wk cycles

    Focal conformal RT(Age & response-adjusted)

    Maintenance

    Chemotherapy

    Second

    Surgery

    Endpoints:Survival vs. P8633/9233

    Neuropsych and endocrine outcome

    Safety of 2nd-look surgery

    Separate studies for M+

    medullo (ACNS0334 (in queue

    to open)) and AT/RT(ACNS0333 (Protocol to

    CTEP ))SPECIMEN SUBMISSION

    MANDATORY

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    Biologically based concepts for high-

    risk/refractory malignant brain tumors

    Examples:

    Disruption of growth factor-mediated signal

    transduction R115777 (ACNS0226) - 97

    Tarceva (ADVL0214) - 46

    Cilengitide (ACNS0621)in development

    Tarceva/Avastin (ADVL0526)in development

    Induction of maturation (e.g., 13-cis-RA)

    medullo (ACNS0332)in queue to open


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