UMIN-CTR Clinical Trial

Public title

Phase Ib study of 131I-metaiodobenzylguanidine(MIBG) therapy with Valproic Acid(VPA) for high risk or recurrent neuroblastoma

Acronym

Phase Ib study of VPA and 131I-MIBG for recurrent / resistant neuroblastoma

Scientific Title

Phase Ib study of 131I-metaiodobenzylguanidine(MIBG) therapy with Valproic Acid(VPA) for high risk or recurrent neuroblastoma

Scientific Title:Acronym

Phase Ib study of VPA and 131I-MIBG for recurrent / resistant neuroblastoma

Region

Japan

Condition

Intractable neuroblastoma

Classification by specialty

Pediatrics

Classification by malignancy

Malignancy

Genomic information

NO

Narrative objectives1

To investigate whether 131I-MIBG with concurrent VPA, a histon deacerylase (HDAC) inhibitory drug, administration can be completed safely without hematopoetic stem cell rescue

Basic objectives2

Safety

Basic objectives -Others

Trial characteristics_1

Exploratory

Trial characteristics_2

Explanatory

Developmental phase

Phase I

Primary outcomes

Proportion of patients who can recover at normal hematologic status without hematopoetic stem cell rescue

Key secondary outcomes

DLT(profile and incidence)
Adverse events profile
Proportion of patients maintaining target serum concentration of VPA
Clinical benefit rate
Response rate
identification of problem and solution for perform 131I-MIBG therapy

Study type

Interventional

Basic design

Single arm

Randomization

Non-randomized

Randomization unit

Blinding

Open -no one is blinded

Control

Uncontrolled

Stratification

Dynamic allocation

Institution consideration

Blocking

Concealment

No. of arms

1

Purpose of intervention

Treatment

Type of intervention

Medicine

Interventions/Control_1

(1) After enrollment, starting valproic acid (VPA) and adjusting VPA dosing to reach and keep the target concentration (100ug/ml).
(2) Preparing for 131I-MIBG administration by assessing disease status (123I-MIBG, Bone marrow biopsy etc.) and training for staying alone in isolated room
(3) After second admission, 131I-MIBG 12 mCi/kg is infused intravenously, concurrently using KI and perchlorate potassium for protecting thyroid.
(4) outpatient ward management after confirming fall of radiation dose from body.
(5) G-CSF s.c. or reserved stem cell transplantation infusion according patient's hematologic status.

Interventions/Control_2

Interventions/Control_3

Interventions/Control_4

Interventions/Control_5

Interventions/Control_6

Interventions/Control_7

Interventions/Control_8

Interventions/Control_9

Interventions/Control_10

Age-lower limit

3

years-old

<=

Age-upper limit

Not applicable

Gender

Male and Female

Key inclusion criteria

1. histological proven neuroblastoma
2. ability to control urination and body weight = < 18kg
3. PS (Lansky) >= 50%
4. any radiologically confirmed residual disease which are not shrinking or any tumor associated symptoms, despite prior chemotherapies
5. any diseases evaluable by 123I-MIBG scan performed within 8 weeks
6. any non-irradiated disease with 123I-MIBG uptake which compress spinal cord
7. autologous hematopoietic stem cell product available for re-infusion after MIBG treatment whose quantity is more than 1.5*10^6 CD34+ cells/kg or 1.0*10^6 CD34+ cells/kg if the quality is confirmed within 8 weeks.
8. If the last chemotherapy contains one or more drugs with hematologic dose limiting toxicity (DLT),
7 days or more have passed since last use of anti-tumor agents which are administerd protractedly and 14 days or more have passed since last use of anti-tumor agents which are not administered in protracted way
9.7 days or more have passed since the
anti-cancer drug (dosage restriction
toxicity is non-hematologic toxicity)
10. No prior irradiation within 14 days if radiation fields is limited.
No prior irradiation within 3 months if radiation fields contain either whole brain and spine, whole abdomen, whole lung, whole body, or more than 50% of pelvis.
No prior irradiation within 6 weeks if radiation fields contain either less than 50% of pelvis, or 5 or less vertebras.
11. No oral 13-cis-RA within 14 days.
12 Any red blood cell (RCC) transfusion or platlet cell (PC) transfusion history within 7 days from registration or the last RCC or PC transfusion.
13. Normal organ function confirmed by laboratory tests within 14 days
14. No exertional dyspnea and no oxygen supply for everyday life.
15. No need for any anti-epileptics, phycotropics or anti-hypertentsivesexcept VPA during treatment.
16. Written informed consent from patient and/or legal guardian.

Key exclusion criteria

1. active double cancer(synchronous
double cancer and metachronous
double cancer within 5 disease
-free years),excluding carcinoma
In situ(lesions equal to Intraepithelial or intramucosal
Cancer)judged to have been cured
with local treatment
2. active infection requiring
systemic medication
3. abnormality in electrocardiogram
tested within 28 days,requiring
intervention
4. Psychosis which is not appropriate for participating in this study

Target sample size

10

Name of lead principal investigator

1st name	Hiroshi
Middle name
Last name	Kawamoto

Organization

National Cancer Research Center
Hospital

Division name

Division of Pediatric Oncology

Zip code

104-0045

Address

5-1-1 Tsukiji,Chuo-ku,Tokyo

TEL

03-3542-2511

Email

ped-dev@ml.res.ncc.go.jp

Name of contact person

1st name	Hiroshi
Middle name
Last name	Kawamoto

Organization

National Cancer Research Center Hospital

Division name

Division of Pediatric Oncology

Zip code

104-0045

Address

5-1-1 Tsukiji,Chuo-ku,Tokyo

TEL

03-3542-2511

Homepage URL

Email

ped-dev@ml.res.ncc.go.jp

Institute

National Cancer Research Center Hospital

Institute

Department

Personal name

Organization

National Cancer Research Center

Organization

Division

Category of Funding Organization

Self funding

Nationality of Funding Organization

Japan

Co-sponsor

Name of secondary funder(s)

Organization

National Cancer Center

Address

5-1-1 Tsukiji,Chuo-ku,Tokyo

Tel

03-3542-2511

Email

NCC_IRBoffice@ml.res.ncc.go.jp

Secondary IDs

NO

Study ID_1

Org. issuing International ID_1

Study ID_2

Org. issuing International ID_2

IND to MHLW

Institutions

国立がん研究センター中央病院（東京都）

Date of disclosure of the study information

2013

Year

10

Month

14

Day

URL releasing protocol

Publication of results

Unpublished

URL related to results and publications

Number of participants that the trial has enrolled

Results

Results date posted

Results Delayed

Results Delay Reason

Date of the first journal publication of results

Baseline Characteristics

Participant flow

Adverse events

Outcome measures

Plan to share IPD

IPD sharing Plan description

Recruitment status

Completed

Date of protocol fixation

2013

Year

04

Month

01

Day

Date of IRB

2013

Year

09

Month

30

Day

Anticipated trial start date

2013

Year

10

Month

15

Day

Last follow-up date

2015

Year

07

Month

14

Day

Date of closure to data entry

Date trial data considered complete

Date analysis concluded

Other related information

Registered date

2013

Year

10

Month

14

Day

Last modified on

2020

Year

02

Month

04

Day

Link to view the page

Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000014062