Iobenguane I-131 or Crizotinib and Standard Therapy in Treating Younger Patients With Newly-Diagnosed High-Risk Neuroblastoma or Ganglioneuroblastoma
Status: | Recruiting |
---|---|
Conditions: | Brain Cancer |
Therapuetic Areas: | Oncology |
Healthy: | No |
Age Range: | Any - 30 |
Updated: | 2/24/2019 |
Start Date: | May 9, 2018 |
End Date: | June 30, 2026 |
A Phase 3 Study of 131I-Metaiodobenzylguanidine (131I-MIBG) or Crizotinib Added to Intensive Therapy for Children With Newly Diagnosed High-Risk Neuroblastoma (NBL)
This partially randomized phase III trial studies iobenguane I-131 or crizotinib and standard
therapy in treating younger patients with newly-diagnosed high-risk neuroblastoma or
ganglioneuroblastoma. Radioactive drugs, such as iobenguane I-131, may carry radiation
directly to tumor cells and not harm normal cells. Crizotinib may stop the growth of tumor
cells by blocking some of the enzymes needed for cell growth. Giving iobenguane I-131 or
crizotinib and standard therapy may work better in treating younger patients with
neuroblastoma or ganglioneuroblastoma.
therapy in treating younger patients with newly-diagnosed high-risk neuroblastoma or
ganglioneuroblastoma. Radioactive drugs, such as iobenguane I-131, may carry radiation
directly to tumor cells and not harm normal cells. Crizotinib may stop the growth of tumor
cells by blocking some of the enzymes needed for cell growth. Giving iobenguane I-131 or
crizotinib and standard therapy may work better in treating younger patients with
neuroblastoma or ganglioneuroblastoma.
PRIMARY OBJECTIVES:
I. To determine in the context of a randomized trial whether the event-free survival (EFS) of
patients with newly diagnosed high-risk neuroblastoma (NBL) is improved with the addition of
iobenguane I-131 (131I-MIBG) during induction, prior to tandem autologous stem cell
transplantation (ASCT).
II. To determine whether the addition of crizotinib to intensive multimodality therapy for
patients with high-risk NBL whose tumors harbor activating point mutations in or
amplification of the ALK gene results in superior EFS compared to a contemporaneously treated
cohort of patients whose tumors lack these ALK aberrations.
SECONDARY OBJECTIVES:
I. To describe the toxicities associated with treatment for high-risk NBL with and without
the addition of 131I-MIBG or crizotinib.
II. To compare EFS and toxicity in patients with newly diagnosed high?risk NBL randomized to
treatment with an 131I-MIBG-containing induction prior to either tandem or busulfan/melphalan
(BuMel) ASCT.
III. To describe the overall survival (OS) and response rates (evaluated per International
Neuroblastoma Response Criteria [INRC] criteria prior to ASCT and prior to post-consolidation
therapy) for patients with high-risk neuroblastoma treated with or without 131I-MIBG or
crizotinib.
IV. To prospectively evaluate the relationship of response rate per revised International
Neuroblastoma Response Criteria (INRC) to EFS and OS in patients with high-risk NBL treated
with and without the addition of 131I-MIBG or crizotinib.
TERTIARY OBJECTIVES:
I. To evaluate whole body radiation dose, tumor factors, and host factors as potential
predictors of efficacy and/or toxicity associated with 131I-MIBG therapy and transplant
conditioning.
II. To determine whether the efficacy (end-induction response, EFS, and OS) of crizotinib is
associated with specific ALK mutations or ALK amplification.
III. To characterize changes in tumor markers (circulating tumor deoxyribonucleic acid [DNA],
including ALK and other tumor specific genetic aberrations, and circulating GD2) over time in
response to protocol therapy.
IV. To correlate results of tumor and host profiling with end-induction response and EFS.
V. To prospectively evaluate EFS for patients with MIBG non-avid high-risk NBL compared to
patients with MIBG-avid high-risk NBL who are randomized to treatment without 131I-MIBG.
VI. To correlate Curie scores calculated from 131I-MIBG post-treatment scans with
end-induction response, EFS and OS.
VII. To describe changes in image defined risk factors (IDRFs) over the course of induction
therapy, with correlation to surgical outcomes and local failure rates following primary
tumor resection.
VIII. To define patterns of failure at time of first relapse or progression in patients with
high-risk NBL.
IX. To determine the feasibility of prospectively monitoring adverse events using electronic
health records.
X. To compare local, central, and computer assisted Curie score assignment at baseline and
during therapy in patients with MIBG-avid high-risk NBL.
XI. To compare late toxicities (including impaired organ function and secondary tumor
occurrence) in patients treated with 131I-MIBG or crizotinib to late toxicities in patients
who have not received these therapies.
OUTLINE: Patients are randomized or assigned to 1 of 4 arms.
All patients receive cyclophosphamide intravenously (IV) over 15-30 minutes and topotecan
hydrochloride IV over 30 minutes on days 1-5 during course 1 of induction therapy in the
absence of disease progression or unacceptable toxicity. Patients not assigned to an Arm may
receive an addition course of cyclophosphamide and topotecan.
ARM A:
INDUCTION THERAPY: Patients receive cyclophosphamide IV over 15-30 minutes and topotecan
hydrochloride IV over 30 minutes on days 1-5 of course 2 and cisplatin IV over 4 hours and
etoposide phosphate IV over 2 hours on days 1-3 of courses 3 and 5. Patients also receive
vincristine sulfate IV over 1 minute on day 1 and dexrazoxane hydrochloride IV over 5-15
minutes, doxorubicin hydrochloride IV over 1-15 minutes, and cyclophosphamide IV over 1-6
hours on days 1-2 of course 4 in the absence of disease progression or unacceptable toxicity.
CONSOLIDATION THERAPY:
HSCT#1: Patients receive thiotepa IV over 2 hours on days -7 to -5 and cyclophosphamide IV
over 1 hour on days -5 to -2 in the absence of disease progression or unacceptable toxicity.
HSCT#2: Patients receive melphalan IV over 15-30 minutes on days -7 to -5, and etoposide
phosphate IV over 24 hours and carboplatin IV over 24 hours on days -7 to -4 in the absence
of disease progression or unacceptable toxicity.
POST-CONSOLIDATION THERAPY: Patients receive sargramostim subcutaneously (SC) on days 1-14,
dinutuximab IV over 10 hours on days 4-7 of courses 1, 3, and 5 and days 8-11 of courses 2
and 4, aldesleukin IV over 96 hours on days 1-4 and 8-11 of courses 2 and 4, and isotretinoin
orally (PO) twice daily (BID) on days 11-24 of courses 1, 3, and 5, and days 15-28 during
courses 2, 4, and 6 in the absence of disease progression or unacceptable toxicity.
ARM B:
INDUCTION THERAPY: Patients receive cyclophosphamide, topotecan hydrochloride, cisplatin, and
etoposide phosphate as in Arm A, iobenguane I-131 IV over 1.5-2 hours on day 1 beginning 3
weeks after the start of course 3, and vincristine sulfate, dexrazoxane hydrochloride,
doxorubicin hydrochloride, and cyclophosphamide as in Arm A beginning no sooner than 35 days
after the infusion of iobenguane I-131.
CONSOLIDATION THERAPY:
HSCT#1: Patients receive thiotepa and cyclophosphamide as in Arm A.
HSCT#2: Patients receive melphalan, etoposide phosphate, and carboplatin as in Arm A.
POST-CONSLIDATION THERAPY: Patients receive sargramostim, dinutuximab, aldesleukin, and
isotretinoin as in Arm A-D.
ARM C:
INDUCTION THERAPY: Patients receive cyclophosphamide, topotecan hydrochloride, cisplatin,
etoposide phosphate, iobenguane I-131, vincristine sulfate, dexrazoxane hydrochloride,
doxorubicin hydrochloride, and cyclophosphamide as in Arm B.
CONSOLIDATION THERAPY: Patients receive busulfan IV over 3 hours on days -6 to -3 and
melphalan IV over 15-30 minutes on day -1 in the absence of disease progression or
unacceptable toxicity.
POST-CONSOLIDATION THERAPY: Patients receive sargramostim, dinutuximab, aldesleukin, and
isotretinoin as in Arm A.
ARM D: Patients receive treatment identical to Arm A.
ARM E:
INDUCTION THERAPY: Patients receive cyclophosphamide, topotecan hydrochloride, cisplatin,
etoposide phosphate, vincristine sulfate, dexrazoxane hydrochloride, doxorubicin
hydrochloride, and cyclophosphamide as in Arm A. Patients also receive crizotinib PO BID on
days 1-21 of courses 2-5 in the absence of disease progression or unacceptable toxicity.
CONSOLIDATION THERAPY:
HSCT#1: Patients receive thiotepa and cyclophosphamide as in Arm A. Patients also receive
crizotinib PO BID until day -7 of HSCT#2 in the absence of disease progression or
unacceptable toxicity.
HSCT#2: Patients receive melphalan, etoposide phosphate, carboplatin, and crizotinib PO BID
on days 1-42 in the absence of disease progression or unacceptable toxicity.
POST-CONSOLIDATION THERAPY: Patients receive sargramostim, dinutuximab, and aldesleukin as in
Arm A-D. Patients also receive isotretinoin PO BID on days 11-24 of courses 1, 3, and 5, and
days 15-28 of courses 2 and 4, and crizotinib PO BID on days 1-24 of courses 1, 3 and 5, and
days 1-28 of courses 2, 4, and 6 in the absence of disease progression or unacceptable
toxicity.
CONTINUATION THERAPY: Patients receive crizotinib PO BID on days 1-28. Courses repeat every
28 days for 1 year in the absence of disease progression or unacceptable toxicity.
After completion of study therapy, patients in Arms A and D are followed up every 3 months
for 18 months, and then every 6 months for 42 months; patients in Arm E are followed up every
3 months for 6 months, and then every 6 months for 42 months.
I. To determine in the context of a randomized trial whether the event-free survival (EFS) of
patients with newly diagnosed high-risk neuroblastoma (NBL) is improved with the addition of
iobenguane I-131 (131I-MIBG) during induction, prior to tandem autologous stem cell
transplantation (ASCT).
II. To determine whether the addition of crizotinib to intensive multimodality therapy for
patients with high-risk NBL whose tumors harbor activating point mutations in or
amplification of the ALK gene results in superior EFS compared to a contemporaneously treated
cohort of patients whose tumors lack these ALK aberrations.
SECONDARY OBJECTIVES:
I. To describe the toxicities associated with treatment for high-risk NBL with and without
the addition of 131I-MIBG or crizotinib.
II. To compare EFS and toxicity in patients with newly diagnosed high?risk NBL randomized to
treatment with an 131I-MIBG-containing induction prior to either tandem or busulfan/melphalan
(BuMel) ASCT.
III. To describe the overall survival (OS) and response rates (evaluated per International
Neuroblastoma Response Criteria [INRC] criteria prior to ASCT and prior to post-consolidation
therapy) for patients with high-risk neuroblastoma treated with or without 131I-MIBG or
crizotinib.
IV. To prospectively evaluate the relationship of response rate per revised International
Neuroblastoma Response Criteria (INRC) to EFS and OS in patients with high-risk NBL treated
with and without the addition of 131I-MIBG or crizotinib.
TERTIARY OBJECTIVES:
I. To evaluate whole body radiation dose, tumor factors, and host factors as potential
predictors of efficacy and/or toxicity associated with 131I-MIBG therapy and transplant
conditioning.
II. To determine whether the efficacy (end-induction response, EFS, and OS) of crizotinib is
associated with specific ALK mutations or ALK amplification.
III. To characterize changes in tumor markers (circulating tumor deoxyribonucleic acid [DNA],
including ALK and other tumor specific genetic aberrations, and circulating GD2) over time in
response to protocol therapy.
IV. To correlate results of tumor and host profiling with end-induction response and EFS.
V. To prospectively evaluate EFS for patients with MIBG non-avid high-risk NBL compared to
patients with MIBG-avid high-risk NBL who are randomized to treatment without 131I-MIBG.
VI. To correlate Curie scores calculated from 131I-MIBG post-treatment scans with
end-induction response, EFS and OS.
VII. To describe changes in image defined risk factors (IDRFs) over the course of induction
therapy, with correlation to surgical outcomes and local failure rates following primary
tumor resection.
VIII. To define patterns of failure at time of first relapse or progression in patients with
high-risk NBL.
IX. To determine the feasibility of prospectively monitoring adverse events using electronic
health records.
X. To compare local, central, and computer assisted Curie score assignment at baseline and
during therapy in patients with MIBG-avid high-risk NBL.
XI. To compare late toxicities (including impaired organ function and secondary tumor
occurrence) in patients treated with 131I-MIBG or crizotinib to late toxicities in patients
who have not received these therapies.
OUTLINE: Patients are randomized or assigned to 1 of 4 arms.
All patients receive cyclophosphamide intravenously (IV) over 15-30 minutes and topotecan
hydrochloride IV over 30 minutes on days 1-5 during course 1 of induction therapy in the
absence of disease progression or unacceptable toxicity. Patients not assigned to an Arm may
receive an addition course of cyclophosphamide and topotecan.
ARM A:
INDUCTION THERAPY: Patients receive cyclophosphamide IV over 15-30 minutes and topotecan
hydrochloride IV over 30 minutes on days 1-5 of course 2 and cisplatin IV over 4 hours and
etoposide phosphate IV over 2 hours on days 1-3 of courses 3 and 5. Patients also receive
vincristine sulfate IV over 1 minute on day 1 and dexrazoxane hydrochloride IV over 5-15
minutes, doxorubicin hydrochloride IV over 1-15 minutes, and cyclophosphamide IV over 1-6
hours on days 1-2 of course 4 in the absence of disease progression or unacceptable toxicity.
CONSOLIDATION THERAPY:
HSCT#1: Patients receive thiotepa IV over 2 hours on days -7 to -5 and cyclophosphamide IV
over 1 hour on days -5 to -2 in the absence of disease progression or unacceptable toxicity.
HSCT#2: Patients receive melphalan IV over 15-30 minutes on days -7 to -5, and etoposide
phosphate IV over 24 hours and carboplatin IV over 24 hours on days -7 to -4 in the absence
of disease progression or unacceptable toxicity.
POST-CONSOLIDATION THERAPY: Patients receive sargramostim subcutaneously (SC) on days 1-14,
dinutuximab IV over 10 hours on days 4-7 of courses 1, 3, and 5 and days 8-11 of courses 2
and 4, aldesleukin IV over 96 hours on days 1-4 and 8-11 of courses 2 and 4, and isotretinoin
orally (PO) twice daily (BID) on days 11-24 of courses 1, 3, and 5, and days 15-28 during
courses 2, 4, and 6 in the absence of disease progression or unacceptable toxicity.
ARM B:
INDUCTION THERAPY: Patients receive cyclophosphamide, topotecan hydrochloride, cisplatin, and
etoposide phosphate as in Arm A, iobenguane I-131 IV over 1.5-2 hours on day 1 beginning 3
weeks after the start of course 3, and vincristine sulfate, dexrazoxane hydrochloride,
doxorubicin hydrochloride, and cyclophosphamide as in Arm A beginning no sooner than 35 days
after the infusion of iobenguane I-131.
CONSOLIDATION THERAPY:
HSCT#1: Patients receive thiotepa and cyclophosphamide as in Arm A.
HSCT#2: Patients receive melphalan, etoposide phosphate, and carboplatin as in Arm A.
POST-CONSLIDATION THERAPY: Patients receive sargramostim, dinutuximab, aldesleukin, and
isotretinoin as in Arm A-D.
ARM C:
INDUCTION THERAPY: Patients receive cyclophosphamide, topotecan hydrochloride, cisplatin,
etoposide phosphate, iobenguane I-131, vincristine sulfate, dexrazoxane hydrochloride,
doxorubicin hydrochloride, and cyclophosphamide as in Arm B.
CONSOLIDATION THERAPY: Patients receive busulfan IV over 3 hours on days -6 to -3 and
melphalan IV over 15-30 minutes on day -1 in the absence of disease progression or
unacceptable toxicity.
POST-CONSOLIDATION THERAPY: Patients receive sargramostim, dinutuximab, aldesleukin, and
isotretinoin as in Arm A.
ARM D: Patients receive treatment identical to Arm A.
ARM E:
INDUCTION THERAPY: Patients receive cyclophosphamide, topotecan hydrochloride, cisplatin,
etoposide phosphate, vincristine sulfate, dexrazoxane hydrochloride, doxorubicin
hydrochloride, and cyclophosphamide as in Arm A. Patients also receive crizotinib PO BID on
days 1-21 of courses 2-5 in the absence of disease progression or unacceptable toxicity.
CONSOLIDATION THERAPY:
HSCT#1: Patients receive thiotepa and cyclophosphamide as in Arm A. Patients also receive
crizotinib PO BID until day -7 of HSCT#2 in the absence of disease progression or
unacceptable toxicity.
HSCT#2: Patients receive melphalan, etoposide phosphate, carboplatin, and crizotinib PO BID
on days 1-42 in the absence of disease progression or unacceptable toxicity.
POST-CONSOLIDATION THERAPY: Patients receive sargramostim, dinutuximab, and aldesleukin as in
Arm A-D. Patients also receive isotretinoin PO BID on days 11-24 of courses 1, 3, and 5, and
days 15-28 of courses 2 and 4, and crizotinib PO BID on days 1-24 of courses 1, 3 and 5, and
days 1-28 of courses 2, 4, and 6 in the absence of disease progression or unacceptable
toxicity.
CONTINUATION THERAPY: Patients receive crizotinib PO BID on days 1-28. Courses repeat every
28 days for 1 year in the absence of disease progression or unacceptable toxicity.
After completion of study therapy, patients in Arms A and D are followed up every 3 months
for 18 months, and then every 6 months for 42 months; patients in Arm E are followed up every
3 months for 6 months, and then every 6 months for 42 months.
Inclusion Criteria:
- Patients must be enrolled on ANBL00B1 or APEC14B1 prior to enrollment on ANBL1531
- Patients must have a diagnosis of neuroblastoma or ganglioneuroblastoma (nodular)
verified by tumor pathology analysis or demonstration of clumps of tumor cells in bone
marrow with elevated urinary catecholamine metabolites; the following disease groups
are eligible:
- Patients with International Neuroblastoma Risk Group (INRG) stage M disease are
eligible if found to have either of the following features:
- MYCN amplification (> 4-fold increase in MYCN signals as compared to
reference signals), regardless of age or additional biologic features; OR
- Age > 547 days regardless of biologic features
- Patients with INRG stage MS disease with MYCN amplification
- Patients with INRG stage L2 disease with MYCN amplification
- Patients > 547 days of age initially diagnosed with INRG stage L1, L2 or MS
disease who progressed to Stage M without prior chemotherapy may enroll within 4
weeks of progression to Stage M
- Patients >= 365 days of age initially diagnosed with MYCN amplified INRG stage L1
disease who progress to Stage M without systemic therapy may enroll within 4
weeks of progression to stage M
- Patients initially recognized to have high-risk disease must have had no prior
systemic therapy (other than topotecan/cyclophosphamide initiated on an emergent basis
and within allowed timing); patients observed or treated with a single cycle of
chemotherapy per a low or intermediate risk neuroblastoma regimen (e.g., as per
ANBL0531, ANBL1232 or similar) for what initially appeared to be non-high risk disease
but subsequently found to meet the criteria will also be eligible; patients who
receive localized emergency radiation to sites of life-threatening or
function-threatening disease prior to or immediately after establishment of the
definitive diagnosis will be eligible
- Creatinine clearance or radioisotope glomerular filtration rate (GFR) >= 70
mL/min/1.73 m^2 or a serum creatinine based on age/sex as follows:
- 1 to < 2 years: male = 0.6; female = 0.6
- 2 to < 6 years: male = 0.8; female = 0.8
- 6 to < 10 years: male = 1; female = 1
- 10 to < 13 years: male = 1.2; female = 1.2
- 13 to < 16 years: male = 1.5; female = 1.4
- >= 16 years: male = 1.7; female = 1.4
- Total bilirubin =< 1.5 x upper limit of normal (ULN) for age, and
- Serum glutamate pyruvate transaminase (SGPT) (alanine aminotransferase [ALT]) < 10 x
ULN; for the purposes of this study, ULN for SGPT (ALT) is 45
- Shortening fraction of >= 27% by echocardiogram, or ejection fraction of > 50% by
echocardiogram or radionuclide angiogram
- No known contraindication to peripheral blood stem cell (PBSC) collection; examples of
contraindications might be a weight or size less than the collecting institution finds
feasible, or a physical condition that would limit the ability of the child to undergo
apheresis catheter placement (if necessary) and/or the apheresis procedure
Exclusion Criteria:
- Patients with INRG stage L2 tumors without amplification of MYCN regardless of tumor
histology (may meet criteria for may meet criteria for high risk classification but
are not eligible for this trial)
- Patients with bone marrow failure syndromes
- Patients for whom targeted radiopharmaceutical therapy would be contraindicated due to
underlying medical disorders
- Female patients who are pregnant; a pregnancy test is required for female patients of
childbearing potential
- Lactating females who plan to breastfeed their infants
- Sexually active patients of reproductive potential who have not agreed to use an
effective contraceptive method for the duration of their study participation
We found this trial at
94
sites
South 34th Street
Philadelphia, Pennsylvania 19104
Philadelphia, Pennsylvania 19104
215-590-1000
Principal Investigator: Rochelle Bagatell
Children's Hospital of Philadelphia Since its start in 1855 as the nation's first hospital devoted...
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4900 Mueller Boulevard
Austin, Texas 78723
Austin, Texas 78723
(512) 324-0000
Principal Investigator: Amy C. Fowler
Dell Children's Medical Center of Central Texas Welcome to Dell Children
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1600 7th Avenue
Birmingham, Alabama 35233
Birmingham, Alabama 35233
(205) 638-9100
Principal Investigator: Matthew A. Kutny
Children's Hospital of Alabama Children
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666 Elm Street
Buffalo, New York 14263
Buffalo, New York 14263
(716) 845-2300
Principal Investigator: Clare J. Twist
Phone: 800-767-9355
Roswell Park Cancer Institute Welcome to Roswell Park Cancer Institute (RPCI), America's first cancer center...
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1 South Prospect Street
Burlington, Vermont 05401
Burlington, Vermont 05401
802-656-8990
Principal Investigator: Jessica L. Heath
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3333 Burnet Avenue # Mlc3008
Cincinnati, Ohio 45229
Cincinnati, Ohio 45229
1-513-636-4200
Principal Investigator: Brian D. Weiss
Cincinnati Children's Hospital Medical Center Patients and families from across the region and around the...
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11100 Euclid Avenue
Cleveland, Ohio 44106
Cleveland, Ohio 44106
(216) 844-1000
Principal Investigator: John J. Letterio
Phone: 216-844-5437
Rainbow Babies and Children's Hospital UH Rainbow Babies & Children’s Hospital is a 244-bed, full-service...
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700 Childrens Drive
Columbus, Ohio 43205
Columbus, Ohio 43205
(616) 722-2000
Principal Investigator: Mark A. Ranalli
Nationwide Children's Hospital At Nationwide Children’s, we are creating the future of pediatric health care....
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3533 South Alameda Street
Corpus Christi, Texas 78411
Corpus Christi, Texas 78411
(361) 694-5000
Principal Investigator: Nkechi I. Mba
Driscoll Children's Hospital Driscoll Children's Hospital was built because Clara Driscoll's will requested that a...
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7777 Forest Ln # C840
Dallas, Texas 75230
Dallas, Texas 75230
(972) 566-7000
Principal Investigator: Stanton C. Goldman
Phone: 972-566-5588
Medical City Dallas Hospital If you have concerns for your health, that of a family...
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1200 Pleasant Street
Des Moines, Iowa 50309
Des Moines, Iowa 50309
(515) 241-KIDS
Principal Investigator: Wendy L. Woods-Swafford
Blank Children's Hospital Blank Children's Hospital is completely dedicated to meeting the unique health care...
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100 Michigan Street Northeast
Grand Rapids, Michigan 49503
Grand Rapids, Michigan 49503
616.391.9000
Principal Investigator: Kathleen J. Yost
Helen DeVos Children's Hospital at Spectrum Health Helen DeVos Children's Hospital, located in Grand Rapids,...
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282 Washington St
Hartford, Connecticut 06106
Hartford, Connecticut 06106
(860) 545-9000
Principal Investigator: Michael S. Isakoff
Connecticut Children's Medical Center Connecticut Children’s Medical Center is a nationally recognized, 187-bed not-for-profit children’s...
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524 South Park Street
Kalamazoo, Michigan 49007
Kalamazoo, Michigan 49007
(269) 341-7654
Principal Investigator: Kathleen J. Yost
Phone: 616-391-1230
Bronson Methodist Hospital Our healthcare system serves patients and families throughout southwest Michigan and northern...
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4650 Sunset Blvd
Los Angeles, California 90027
Los Angeles, California 90027
(323) 660-2450
Principal Investigator: Leo Mascarenhas
Childrens Hospital Los Angeles Children's Hospital Los Angeles is a 501(c)(3) nonprofit hospital for pediatric...
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1201 W La Veta Ave
Orange, California 92868
Orange, California 92868
(714) 997-3000
Principal Investigator: Elyssa M. Rubin
Children's Hospital of Orange County For more than 45 years, CHOC Children’s has been steadfastly...
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530 Northeast Glen Oak Avenue
Peoria, Illinois 61603
Peoria, Illinois 61603
(309) 624-4945
Principal Investigator: Pedro A. De Alarcon
Phone: 888-226-4343
Saint Jude Midwest Affiliate The Jim and Trudy Maloof St. Jude Midwest Affiliate Clinic was...
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4401 Penn Avenue
Pittsburgh, Pennsylvania 15224
Pittsburgh, Pennsylvania 15224
412-692-5325
Principal Investigator: Jean M. Tersak
Children's Hospital of Pittsburgh of UPMC UPMC is one of the leading nonprofit health systems...
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593 Eddy Street
Providence, Rhode Island 02903
Providence, Rhode Island 02903
401-444-4000
Principal Investigator: Jennifer J. Greene Welch
Phone: 401-444-1488
Rhode Island Hospital Founded in 1863, Rhode Island Hospital in Providence, RI, is a private,...
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7700 Floyd Curl Dr
San Antonio, Texas 78229
San Antonio, Texas 78229
(210) 575-7000
Principal Investigator: Vinod K. Gidvani-Diaz
Methodist Children's Hospital of South Texas Methodist Children
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4502 Medical Drive
San Antonio, Texas 78284
San Antonio, Texas 78284
(210) 567-7000
Principal Investigator: Anne-Marie R. Langevin
Phone: 210-450-3800
University of Texas Health Science Center at San Antonio The University of Texas Health Science...
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1600 Rockland Road
Wilmington, Delaware 19803
Wilmington, Delaware 19803
(302) 651-4200
Principal Investigator: Ramamoorthy Nagasubramanian
Phone: 302-651-6884
Alfred I. duPont Hospital for Children Nemours began more than 70 years ago with the...
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Allentown, Pennsylvania 18103
Principal Investigator: Lydia A. Boateng
Phone: 734-712-3671
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1540 East Hospital Drive
Ann Arbor, Michigan 48109
Ann Arbor, Michigan 48109
(877) 475-6688
Principal Investigator: Rajen Mody
C S Mott Children's Hospital Behind the doors of C.S. Mott Children's Hospital there exist...
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Asheville, North Carolina 28801
Principal Investigator: Douglas J. Scothorn
Phone: 828-213-4150
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Atlanta, Georgia 30322
Principal Investigator: William T. Cash
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13123 E 16th Ave
Aurora, Colorado 80045
Aurora, Colorado 80045
(720) 777-1234
Principal Investigator: Margaret E. Macy
Children's Hospital Colorado At Children's Hospital Colorado, we see more, treat more and heal more...
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2401 W Belvedere Ave
Baltimore, Maryland 21215
Baltimore, Maryland 21215
(410) 601-9000
Principal Investigator: Jason M. Fixler
Phone: 410-601-6120
Sinai Hospital of Baltimore Sinai Hospital of Baltimore provides a broad array of high-quality, cost-effective...
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401 North Broadway
Baltimore, Maryland 21287
Baltimore, Maryland 21287
410-955-5000
Principal Investigator: Allen R. Chen
Phone: 410-955-8804
Johns Hopkins University-Sidney Kimmel Cancer Center The name Johns Hopkins has become synonymous with excellence...
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489 State St
Bangor, Maine 04401
Bangor, Maine 04401
(207) 973-7000
Principal Investigator: Nadine P. SantaCruz
Phone: 207-973-4274
Eastern Maine Medical Center Located in Bangor, Eastern Maine Medical Center (EMMC) serves communities throughout...
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55 Fruit St
Boston, Massachusetts 02114
Boston, Massachusetts 02114
(617) 724-4000
Principal Investigator: Suzanne Shusterman
Phone: 877-726-5130
Massachusetts General Hospital Cancer Center An integral part of one of the world
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450 Brookline Ave
Boston, Massachusetts 2215
Boston, Massachusetts 2215
617-632-3000
Principal Investigator: Suzanne Shusterman
Phone: 877-442-3324
Dana-Farber Cancer Institute Since it’s founding in 1947, Dana-Farber has been committed to providing adults...
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Chapel Hill, North Carolina 27599
Principal Investigator: Stuart H. Gold
Phone: 877-668-0683
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5841 S Maryland Ave
Chicago, Illinois 60637
Chicago, Illinois 60637
1-773-702-6180
Principal Investigator: Susan L. Cohn
Phone: 773-702-8222
University of Chicago Comprehensive Cancer Center The University of Chicago Comprehensive Cancer Center (UCCCC) is...
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Chicago, Illinois 60614
Principal Investigator: Jennifer L. Reichek
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1200 West Harrison Stree
Chicago, Illinois 60607
Chicago, Illinois 60607
(312) 996-4350
Principal Investigator: Mary L. Schmidt
Phone: 312-355-3046
Univ of Illinois A major research university in the heart of one of the world's...
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2049 E 100th St
Cleveland, Ohio 44106
Cleveland, Ohio 44106
(216) 444-2200
Principal Investigator: Aron Flagg
Phone: 866-223-8100
Cleveland Clinic Foundation The Cleveland Clinic (formally known as The Cleveland Clinic Foundation) is a...
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5 Richland Medical Park Dr
Columbia, South Carolina 29203
Columbia, South Carolina 29203
(803) 434-7000
Principal Investigator: Stuart L. Cramer
Phone: 803-434-3680
Palmetto Health Richland Palmetto Health Richland, originally founded in 1892 as Columbia Hospital, has a...
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Dallas, Texas 75390
Principal Investigator: Tanya C. Watt
Phone: 214-648-7097
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Fort Myers, Florida 33908
Principal Investigator: Emad K. Salman
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801 7th Avenue
Fort Worth, Texas 76104
Fort Worth, Texas 76104
(682) 885-4000
Principal Investigator: Mary Meaghan P. Granger
Cook Children's Medical Center Cook Children's Health Care System is a not-for-profit, nationally recognized pediatric...
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1600 Southwest Archer Road
Gainesville, Florida 32610
Gainesville, Florida 32610
Principal Investigator: William B. Slayton
Phone: 352-273-8010
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30 Prospect Ave
Hackensack, New Jersey 07601
Hackensack, New Jersey 07601
(201) 996-2000
Principal Investigator: Katharine Offer
Phone: 201-996-2879
Hackensack University Medical Center Hackensack University Medical Center, part of the Hackensack University Health Network,...
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Hollywood, Florida 33021
Principal Investigator: Iftikhar Hanif
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1319 Punahou St
Honolulu, Hawaii 96826
Honolulu, Hawaii 96826
(808) 983-6000
Principal Investigator: Wade T. Kyono
Phone: 808-983-6090
Kapiolani Medical Center for Women and Children Hawai‘i Pacific Health is an integrated health care...
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Houston, Texas 77030
Principal Investigator: Jennifer H. Foster
Phone: 713-798-1354
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705 Riley Hospital Dr
Indianapolis, Indiana 46202
Indianapolis, Indiana 46202
(317) 944-5000
Principal Investigator: Kamnesh R. Pradhan
Phone: 800-248-1199
Riley Hospital for Children Riley Hospital for Children at IU Health is a place of...
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Iowa City, Iowa 52242
Principal Investigator: Mariko Sato
Phone: 800-237-1225
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Jacksonville, Florida 32207
Principal Investigator: Ramamoorthy Nagasubramanian
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Kansas City, Missouri 64108
Principal Investigator: Keith J. August
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2018 W Clinch Ave
Knoxville, Tennessee 37916
Knoxville, Tennessee 37916
(865) 541-8000
Principal Investigator: Ray C. Pais
Phone: 865-541-8266
East Tennessee Children's Hospital East Tennessee Children's Hospital is a not-for-profit, private, independent pediatric medical...
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Las Vegas, Nevada 89135
Principal Investigator: Alan K. Ikeda
Phone: 702-384-0013
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1 Medical Center Dr
Lebanon, New Hampshire 03756
Lebanon, New Hampshire 03756
(603) 650-5000
Principal Investigator: Julie Kim
Phone: 800-639-6918
Dartmouth Hitchcock Medical Center Dartmouth-Hitchcock is a national leader in patient-centered health care and building...
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Lexington, Kentucky
Principal Investigator: Vlad C. Radulescu
Phone: 859-257-3379
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1 Children's Way
Little Rock, Arkansas 72202
Little Rock, Arkansas 72202
(501) 364-1100
Principal Investigator: David L. Becton
Arkansas Children's Hospital Arkansas Children's Hospital (ACH) is the only pediatric medical center in Arkansas...
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11234 Anderson St
Loma Linda, California 92354
Loma Linda, California 92354
(909) 558-4000
Principal Investigator: Albert Kheradpour
Phone: 909-558-3375
Loma Linda University Medical Center An outgrowth of the original Sanitarium on the hill in...
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600 Highland Ave
Madison, Wisconsin 53792
Madison, Wisconsin 53792
(608) 263-6400
Principal Investigator: Kenneth B. De Santes
Phone: 800-622-8922
University of Wisconsin Hospital and Clinics UW Health strives to meet the health needs of...
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Marshfield, Wisconsin 54449
Principal Investigator: Michelle A. Manalang
Phone: 800-782-8581
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Miami, Florida 33136
Principal Investigator: Julio C. Barredo
Phone: 305-243-2647
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9000 W Wisconsin Ave #270
Milwaukee, Wisconsin 53226
Milwaukee, Wisconsin 53226
(414) 266-2000
Principal Investigator: Meghen B. Browning
Phone: 414-955-4727
Children's Hospital of Wisconsin Nothing matters more than our children. At Children's Hospital of Wisconsin,...
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259 1st Street
Mineola, New York 11501
Mineola, New York 11501
Principal Investigator: Mark E. Weinblatt
Phone: 866-946-8476
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Minneapolis, Minnesota 55455
Principal Investigator: Emily G. Greengard
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2525 Chicago Ave
Minneapolis, Minnesota 55404
Minneapolis, Minnesota 55404
(612) 813-6000
Principal Investigator: Michael K. Richards
Children's Hospitals and Clinics of Minnesota - Minneapolis Children's Hospitals and Clinics of Minnesota is...
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Morgantown, West Virginia 26505
Principal Investigator: Stephan R. Paul
Phone: 304-293-7374
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Nashville, Tennessee 37232
Principal Investigator: Carrie L. Kitko
Phone: 800-811-8480
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New Haven, Connecticut 6520
(203) 432-4771
Principal Investigator: Nina S. Kadan-Lottick
Phone: 203-785-5702
Yale University Yale's roots can be traced back to the 1640s, when colonial clergymen led...
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New York, New York 10032
Principal Investigator: Alice Lee
Phone: 212-305-6361
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Oakland, California 94611
Principal Investigator: Laura A. Campbell
Phone: 877-642-4691
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940 NE 13th St
Oklahoma City, Oklahoma 73190
Oklahoma City, Oklahoma 73190
(405) 271-6458
Principal Investigator: Rene Y. McNall-Knapp
Phone: 405-271-8777
University of Oklahoma Health Sciences Center The OU Health Sciences Center is composed of seven...
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8200 Dodge St
Omaha, Nebraska 68114
Omaha, Nebraska 68114
(402) 955-5400
Principal Investigator: Minnie Abromowitch
Children's Hospital and Medical Center of Omaha Children's Hospital & Medical Center has a rich...
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Emile St
Omaha, Nebraska 68198
Omaha, Nebraska 68198
(402) 559-4000
Principal Investigator: Minnie Abromowitch
Phone: 402-559-6941
Univ of Nebraska Med Ctr A vital enterprise in the nation’s heartland, the University of...
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13535 Nemours Parkway
Orlando, Florida 32827
Orlando, Florida 32827
(407) 567-4000
Principal Investigator: Ramamoorthy Nagasubramanian
Nemours Children's Hospital Nemours Children's Hospital in Orlando brings pediatric specialty care never before offered...
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Park Ridge, Illinois 60068
Principal Investigator: Caroline Y. Hu
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Royal Oak, Michigan 48073
Principal Investigator: Laura K. Gowans
Phone: 248-551-0360
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Saint Louis, Missouri 63141
Principal Investigator: Robin D. Hanson
Phone: 314-251-6770
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660 S Euclid Ave
Saint Louis, Missouri 63110
Saint Louis, Missouri 63110
(314) 362-5000
Principal Investigator: Shalini Shenoy
Phone: 800-600-3606
Washington University School of Medicine Washington University Physicians is the clinical practice of the School...
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Saint Petersburg, Florida 33701
Principal Investigator: Nanette H. Grana
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San Antonio, Texas 78207
Principal Investigator: Timothy C. Griffin
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San Francisco, California 94158
Principal Investigator: Kieuhoa T. Vo
Phone: 877-827-3222
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4700 Waters Ave
Savannah, Georgia 31404
Savannah, Georgia 31404
(912) 350-8000
Principal Investigator: Andrew L. Pendleton
Phone: 912-350-7887
Memorial Health University Medical Center Memorial University Medical Center (MUMC) is a nonprofit, 622-bed tertiary...
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4800 Sand Point Way NE
Seattle, Washington 98105
Seattle, Washington 98105
(206) 987-2000
Principal Investigator: Douglas S. Hawkins
Seattle Children's Hospital Seattle Children’s Hospital specializes in meeting the unique physical, emotional and developmental...
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101 W 8th Ave
Spokane, Washington 99204
Spokane, Washington 99204
(509) 474-3131
Principal Investigator: Judy L. Felgenhauer
Providence Sacred Heart Medical Center & Children's Hospital When Mother Joseph and the Sisters of...
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9040 Jackson Ave
Tacoma, Washington 98431
Tacoma, Washington 98431
(253) 968-1110
Principal Investigator: Melissa A. Forouhar
Phone: 253-968-0129
Madigan Army Medical Center Located on Joint Base Lewis-McChord, Madigan Army Medical Center comprises a...
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2142 N Cove Blvd
Toledo, Ohio 43606
Toledo, Ohio 43606
(419) 291-5437
Principal Investigator: Jamie L. Dargart
Phone: 419-824-1842
The Toledo Hospital/Toledo Children's Hospital ProMedica's Mission is to improve your health and well-being. And...
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111 Michigan Ave NW
Washington, District of Columbia
Washington, District of Columbia
(202) 476-5000
Principal Investigator: Jeffrey S. Dome
Childrens National Medical Center As the nation’s children’s hospital, the mission of Children’s National Medical...
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901 45th St
West Palm Beach, Florida 33407
West Palm Beach, Florida 33407
(561) 844-6300
Principal Investigator: Narayana Gowda
Saint Mary's Hospital Our team of dedicated physicians, nurses and staff offer a broad spectrum...
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1 Medical Center Blvd
Winston-Salem, North Carolina 27157
Winston-Salem, North Carolina 27157
336-716-2011
Principal Investigator: Thomas B. Russell
Phone: 336-713-6771
Wake Forest University Health Sciences Welcome to Wake Forest Baptist Medical Center, a fully integrated...
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