Phase
Condition
Testicular Cancer
Brain Tumor
Neoplasms
Treatment
(C7R)-GD2.CART cells
C7R-GD2.CART cells (IV infusion)
C7R-GD2.CART cells (ICV infusion)
Clinical Study ID
Ages 12-22 All Genders
Study Summary
Eligibility Criteria
Inclusion
Procurement Inclusion Criteria:
Cohort 1:
Histologically confirmed, GD2-expressing newly diagnosed DMG/HGG (including pontine)or confirmation of H3K27 alteration if sufficient tissue for GD2 staining by IHC isnot available. Newly diagnosed is defined as prior to radiographic progression orrecurrence. OR Histologically confirmed, GD2-expressing recurrent, refractory, or progressiveDMG/HGG (except pontine) or confirmation of positive H3K27 alteration if sufficienttissue for GD2 staining by IHC is not available. OR Recurrent, refractory, or progressive high-grade CNS tumor with confirmedGD2-expression. Examples include: medulloblastoma "CNS embryonal tumors, AT/RT,ependymal tumors, diffuse gliomas or glioneuronal tumors. Cohort 2: Recurrent, refractory, or progressive pontine HGG with confirmed GD2-expression orH3K27-altered DMG
Tumors less than 5 cm in maximum dimension at enrollment
Tumors with ≤25% increase in size (on any dimension) on MRI 4-8 weekspost-radiotherapy remain eligible for study
Tumors with >25% increase in size on post-radiation imaging may be reassessedwith repeat MRI in 4-6 weeks, and are eligible if tumor size is subsequently ≤ 25% increased compared with pre-irradiation MRI.
Tumors with sizes between 5 and 5.5 cm are eligible if the tumor was surgicallydebulked
Measurable disease on at least 2 dimensions on MRI
Age 12 months to 22 years
Functional score (Karnofsky/Lansky) ≥ 50 expected at infusion (≥60 for cohort 2)
Exclusion
Procurement Exclusion Criteria:
Patients who are pregnant or breast feeding
Any patient with other risk factors for whom administration of investigational agentis deemed not in the patient's best interest, in the opinion of the investigator.
Treatment Inclusion Criteria
Cohort 1:
Histologically confirmed, GD2-expressing newly diagnosed DMG/HGG (including pontine)or confirmation of H3K27 alteration if sufficient tissue for GD2 staining by IHC isnot available. Newly diagnosed is defined as prior to radiographic progression orrecurrence. OR Histologically confirmed, GD2-expressing recurrent, refractory, or progressiveDMG/HGG (except pontine) or confirmation of positive H3K27 alteration if sufficienttissue for GD2 staining by IHC is not available. OR Recurrent, refractory, or progressive high -grade CNS tumor with confirmedGD2-expression. Examples include: medulloblastoma, CNS embryonal tumors, AT/RT,ependymal tumors, diffuse gliomas, or glioneuronal tumors. Cohort 2: Recurrent, refractory, or progressive pontine HGG with confirmed GD2-expression orH3K27-altered for DMG.
Tumors less than 5 cm in maximum dimension at enrollment
Tumors with ≤25% increase in size (on any dimension) on MRI 4-8 weekspost-radiotherapy remain eligible for study
Tumors with >25% increase in size on post-radiation imaging may be reassessedwith repeat MRI in 4-6 weeks, and are eligible if tumor size is subsequently ≤ 25% increased compared pre-irradiation MRI
Tumors with sizes between 5 and 5.5 cm are eligible if the tumor was surgicallydebulked
Measurable disease on at least 2 dimensions on MRI
Central line (PICC or other) and Ommaya reservoir or VP shunt in place or planned tobe placed
Age 12 months to 22 years
Functional score (Karnofsky/Lansky) ≥ 50 (≥60 for cohort 2)
Patients must have completed radiation therapy at least 4 weeks prior toadministration of investigational agent. Radiation therapy and (If applicable)bevacizumab treatment for radiation necrosis must be completed at least 4 weeksprior to administration of investigational agent.
Stable neurologic exam for 7 days prior to enrollment
Stable or decreasing dose of steroids (max. allowable dose of dexamethasone is 0.1mg/kg/day over the past 7 days prior to infusion of investigational therapy)
Organ function:
ANC > 1000 cells/ul
Platelet count > 100,000 cells/ul
Total bilirubin < 1.5x ULN
ALT and AST < 5x ULN
Serum creatinine or kidney within 2x ULN for age
Treatment Exclusion Criteria
Patients who received any other forms of immunotherapy ≤ 42 days beforeadministration of investigational agent
Patients who received colony-stimulating factors within 14 days prior toadministration of lymphodepletion
Patients receiving any concurrent anti-cancer therapy (it is preferable for patientsto stop any concurrent anti-cancer therapy at least three half-lives prior totreatment)
Patients who are pregnant or breast feeding
Any patient with other risk factors for whom administration of investigational agentis deemed not in the patient's best interest, in the opinion of the investigator.
Study Design
Study Description
Connect with a study center
Texas Children's Hospital
Houston, Texas 77030
United StatesSite Not Available
Texas Children's Hospital
Houston 4699066, Texas 4736286 77030
United StatesActive - Recruiting

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