根据FDA官网公布的药理毒理审评报告,进行简单梳理汇总。具体细节见审评报告全文
| PHARMACOLOGY STUDIES | SAFETY PHARMACOLOGY STUDIES | PHARMACOKINETIC STUDIES(Biodistribution) | TOXICOLOGY STUDIES | |
| KYMRIAH | In Vitro
Studies 1. CD19 mRNA and protein expression in normal human and cynomolgus macaque brain sections by ICH/ISH/RT-PCR [ Study #1, #2] 2. Human membrane protein off-target binding of CD19 scFv [#3] 3. Transduction efficiency and expansion potential in vitro(Lymphocytes from a HD/patient) [#4 #5 #6 #7] In Vivo Studies 1. Efficacy of four CART-19 receptor constructs: αCD19-ζ, αCD19-BB-ζ, αCD19-28-ζ, and αCD19-28-BB-ζ in tumor-bearing XX mouse model [#8 #9] |
None | 1. Evaluation Biodistribution in Human
Immune-reconstituted XX Mice [#11 #12] *conjunction with the toxicology study |
• Toxicology Studies: Evaluation of CART-19 Biotoxicity in Human Immune-reconstituted XX Mice [#11 #12] • Developmental and Reproductive Toxicology Studie: None • Genotoxicity Studies: Lentivirus integration site analysis (ISA) • Carcinogenicity/Tumorigenicity Studies: None • Other Safety/Toxicology Studies: None |
| YESCARTA | In Vitro Studies 1. Characterization of Patient-Derived Anti-CD19 CAR T cells [#3] 2. CD19 Expression on Normal and Malignant B-lineage Cells [#1] 3. Development of a γ-Retroviral Vector Encoding an Anti-CD19 CAR [#2] In Vivo Studies [#4 Publication] 1. Anti-Murine CD19 CAR T-Cell Activity in a Syngeneic Mouse Lymphoma Model,including: • Characterization of T Cells with Different CAR Constructs • Effects on Mice with 38c13 Murine Lymphoma Cells/ Subcutaneous Lymphoma Masses • Effect of Radiation-Induced Lymphodepletion and Supplemental IL-2 • On-target, Off-tumor Effect |
None | No
biodistribution studies with KTE-C19 were conducted. Publication (Study #4) examined the persistence of anti-murine CD19 CAR T cells following administration into immune competent tumor-bearing mice. * detection of CD8+ and CD4+ anti-murine CD19 CAR T cells in the spleen at 8 days after T cell infusion. |
• Toxicology Studies: No toxicology
studies with KTE-C19 were conducted. However, Publication (Study #4), evaluated overall
safety following administration of the anti-murine CD19 CAR T cells into
immune competent tumor-bearing mice. Some mice were followed out to Day 209.
No overt toxicity, but normal B cells were decreased which is consistent with
the clinical trial data for KTE-C19 • Developmental and Reproductive Toxicology Studie: None • Genotoxicity Studies: None • Carcinogenicity/Tumorigenicity Studies: Publications 1. non clinical:Assessment of potential oncogenicity of KTE-C19 due to transformation and clonal expansion was based on published in vivo studies in mice 2. clinical: Carcinogenicity/Tumorigenicity outcomes in subjects administered γ-retroviral vector transduced HSC/T cells • Other Safety/Toxicology Studies: None |
| TECARTUS | In Vitro Studies 1. Characterization of the Activation, Transduction, and Expansion and Functional Characterization of Anti-CD19 CAR T-cell Products [#1 #2] 2. Development of a γ-retroviral Vector Encoding an Anti-CD19 CAR [#3] 3. Undisclosed [#4 #5] In Vivo Studies Same with YESCARTA |
None. | Same with YESCARTA | • Toxicology Studies: Same with YESCARTA • Developmental and Reproductive Toxicology Studie: None • Genotoxicity Studies: Integration Site Analysis • Carcinogenicity/Tumorigenicity Studies: review of the literature regarding the potential for oncogenicity due to transformation and clonal expansion. • Other Safety/Toxicology Studies: None |
| BREYANZI | In Vitro Studies 1. Activity/ Cytolytic Activity/ Growth and Viability of JCAR017 [#1 #2 #3 #4 #5] 2. CAR of JCAR017 Intracellular Domain Mechanism of Action [#6] 3. Binder Characterization/Epitope Analysis/ Binding Profile of FMC63(a murine CD19-specific mAb) [#7 #14] 4. CD19-Specific Cytolytic Activity/ Cell Surface Phenotype and Cytokine Production Analysis (GMP) [#8 #9 #10] 5. JCAR017 CD19 Species Cross-Reactivity/CD19 Expression in various species/human tissues [#11 #12 #13 #15] 6. Combination with XX(immunomodulating agents) or Lenalidomide/Epacadostat/ Anti-PD-L1 Antibody (Durvalumab)/ Ibrutinib or Acalabrutinib(BTKi)/ Cetuximab(anti-EGFR antibody) [#16 #17 #18 #19 #20] 7. EGFR expression/ Cetuximab(anti-EGFR antibody) in Mouse Serum/ JCAR017 Cells in Mouse Whole Blood Specimens with Cetuximab [#20 #21 #22] In Vivo Studies 1. Efficacy of JCAR017 in XX Mice Engrafted with Raji [#23] 2. Characterization of CD19-Specific CAR T Cell(Tumor Growth and Survival) [#24] 3. Efficacy Evaluation of JCAR017 in Combination with Ibrutinib or Acalabrutinib(BTKi) /Cetuximab [#25 #26 #27] 4. PK of Erbitux [#28] |
None | None | • Toxicology Studies: None • Developmental and Reproductive Toxicology Studie: An unbiased, genome-wide, assay assessed viral integration events across 54 CAR T cell products derived from 34 patients • Genotoxicity Studies: Genomic Mapping of Lentiviral Integration Sites in JCAR017 Cryopreserved Drug Product [#29] • Carcinogenicity/Tumorigenicity Studies: None • Other Safety/Toxicology Studies: 1. 60-Day In Vitro CAR T Cell Proliferation Study [#30] 2. A Tissue Cross-Reactivity Study of XX in Normal Human Tissues [#31] |
| ABECMA | In Vitro Studies 1. Pharmacologic Activity of bb2121 [#1] 2. BCMA Expression on various tumor cells [#2] 3. Binding profile/Cross-reactivity Study of Anti-BCMA Antibodies [#3 #4] In Vivo Studies 1. Pharmacologic Activity/ Pharmacologic Dose Response of bb2121 in Tumor-bearing Mice [#5 #6 #7 #8 #9] |
None | 1. Pharmacologic Activity, Pharmacokinetics, Pharmacodynamics, Biodistribution and General Safety of bb2121 in Mice with and Without BCMA+ Human Multiple Myeloma Subcutaneous Xenografts [#10] | • Toxicology Studies: None • Developmental and Reproductive Toxicology Studie: None • Genotoxicity Studies: Vector Insertion Site Analysis of 20 Clinical bb2121 [#11] • Carcinogenicity/Tumorigenicity Studies: IL-2 Independent Growth as a Gain of Function Assessment in Clinical and Normal HD bb2121 [#12] • Other Safety/Toxicology Studies: None |
| CARVYKTI | In Vitro Studies 1. Pharmacologic Activity (Characterization/ Cytotoxicity Assay/Cytokine Release) of LCAR-B38M CAR-T [#4 #8 #16] 2. possible off-target evaluation( Cytotoxicity, Binding Profiling) [#7 #10 #13] 3. Binding study of BCMA to LCARB38M CAR [#9] 4. Undisclosed [#1 #2 #3 #5 #6 #11 #14 #17 #18] In Vivo Studies 1. Dose escalating study/ Efficacy Study of LCAR-B38M on XX Engrafted Immune Deficient Mouse [#19 #20] |
None | None | • Toxicology Studies: Pilot Tolerability of LCAR-B38M in Monkeys [#21] • Developmental and Reproductive Toxicology Studie: None • Genotoxicity Studies: Lentivirus Vector ISA Testing • Carcinogenicity/Tumorigenicity Studies: None • Other Safety/Toxicology Studies: Characterization of Cytokine Independent Growth |
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