Entire CD3ε, δ, and γ humanized mouse to evaluate human CD3–mediated therapeutics

Ueda, Otoya; Wada, Naoko; Kinoshita, Yasuko; Hino, Hiroshi; Kakefuda, Mami; Ito, Tsuneo; Fujii, Etsuko; Noguchi, Mitsuho; Sato, Kiyoharu; Morita, Masahiro; Tateishi, Hiromi; Matsumoto, Kaoru; Goto, Chisato; Kawase, Yoshiaki; Kato, Atsuhiko; Hattori, Kunihiro; Nezu, Jun-ichi; Ishiguro, Takahiro; Jishage, Kou-ichi

doi:10.1038/srep45839

Cited by 20 publications

(24 citation statements)

References 32 publications

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“…Even the more elegant models in this research field, in which human CD3E is transgenically expressed in mouse T cells and human TAA are expressed in mouse tumor cell lines under heterologous promoters, fall short, due to artificial expression levels of the CD3 and TAA (21,22). Indeed, the expression levels and frequency of CD3E in these transgenic mouse models are lower than those in wild-type mice (24). Recently, a triple knock-in mouse was reported in which human CD3E, -D, and -G genes replace the mouse homologous genes CD3e, -d, and -g. In this knock-in mouse, T-cell numbers and CD3 expression levels are comparable to those in wild-type mice and treatment with CD3 bsAb binding to human CD3 can representatively be evaluated (23,24).…”

Section: Discussionmentioning

confidence: 99%

“…Indeed, the expression levels and frequency of CD3E in these transgenic mouse models are lower than those in wild-type mice (24). Recently, a triple knock-in mouse was reported in which human CD3E, -D, and -G genes replace the mouse homologous genes CD3e, -d, and -g. In this knock-in mouse, T-cell numbers and CD3 expression levels are comparable to those in wild-type mice and treatment with CD3 bsAb binding to human CD3 can representatively be evaluated (23,24). In our syngeneic mouse model, we report a strong increase of innate immune cells, such as inflammatory macrophages and natural killer cells, and a fast intratumoral activation of CD4 þ and CD8 þ T-cell subsets (Figs.…”

Section: Discussionmentioning

confidence: 99%

“…Recently, transgenic mice that coexpress human CD3e (hCD3e) on their T cells, in addition to mouse CD3e, were exploited in this research field, enabling the use of endogenous T cells in immune-competent mice (21,22). Although hCD3e transgenic mice harbor a relatively normal immune system and allow analysis of immune-tumor cell interaction, they still lack a natural distribution of the selected TAA in mouse tissues, hampering examination of "on-target, off-tumor" effects via target expression in host tissues (21)(22)(23)(24). Moreover, induction of neutralizing anti-human Ig antibodies prevents longterm evaluation in these mouse models.…”

Section: Introductionmentioning

confidence: 99%

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CD3-Bispecific Antibody Therapy Turns Solid Tumors into Inflammatory Sites but Does Not Install Protective Memory

Benonisson

Altıntaş

Sluijter

et al. 2019

Molecular Cancer Therapeutics

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Immunotherapy of cancer with CD3-targeting bispecific antibodies (CD3 bsAb) is a fast developing field, and multiple tumor-associated antigens (TAA) are evaluated for hematologic and solid malignancies. The efficacy of these CD3 bsAb is usually examined in xenograft mouse tumor models with human T cells or in genetically engineered mouse models, where human TAA are introduced. These models often fail to fully recapitulate the natural tumor environment, especially for solid cancers, because of interspecies differences. Here, we investigated the systemic and intratumoral effects of a mouse CD3 bsAb in a fully immune-competent mouse melanoma model. Systemic administration of 0.5 mg/kg antibody induced a brief overall T-cell activation that was selectively sustained in the tumor microenvironment for several days. A fast subsequent influx of inflammatory macrophages into the tumor microenvironment was observed, followed by an increase in the number of CD4 þ and CD8 þ T cells. Although the capacity to directly kill melanoma cells in vitro was very modest, optimal tumor elimination was observed in vivo, even in the absence of CD8 þ T cells, implying a redundancy in T-cell subsets for therapeutic efficacy. Finally, we took advantage of the full immune competence of our mouse model and tested immune memory induction. Despite a strong initial immunity against melanoma, treatment with the CD3 bsAb did not install protective memory responses. The observed mechanisms of action revealed in this immune-competent mouse model might form a rational basis for combinatorial approaches.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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CD3-Bispecific Antibody Therapy Turns Solid Tumors into Inflammatory Sites but Does Not Install Protective Memory

Benonisson

Altıntaş

Sluijter

et al. 2019

Molecular Cancer Therapeutics

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“…In the cocitation network, CD3D, CD3E, and CD3G, which are compositions of CD3 complex of TCR, interacted with each other to affect the assembly of TCR membrane complex and disturb T-cell responsiveness [ 27 ], especially CD3E [ 28 ]. After TCR engagement, the phosphorylation of CD3 immunoreceptor tyrosine-based activation motifs of CD3E in CD3 complex is combined with activated LCK, which is also called Src kinase lymphocyte kinase [ 29 ].…”

Section: Discussionmentioning

confidence: 99%

LCK as a Potential Therapeutic Target for Acute Rejection after Kidney Transplantation: A Bioinformatics Clue

Jia

et al. 2018

Journal of Immunology Research

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Objectives We aim to identify the key biomarker of acute rejection (AR) after kidney transplantation via bioinformatics methods. Methods The gene expression data GSE75693 of 30 samples with stable kidney transplantation recipients and 15 AR samples were downloaded and analyzed by the limma package to identify differentially expressed genes (DEGs). Then, Gene Ontology (GO) functional enrichment analysis and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway analysis were done to explore the biological functions and potential important pathways of DEGs. Finally, protein-protein interactions (PPIs) and literature mining were applied to construct the cocitation network and to select the hub protein. Results A total of 437 upregulated genes and 353 downregulated genes were selected according to P < 0.01 and |log2(fold change)| > 1.0. DEGs of AR are mainly located on membranes and impact the activation of receptors in immune responses. In the PPI network, Src kinase, lymphocyte kinase (LCK), CD3G, B2M, interferon-γ, CD3D, tumor necrosis factor, VAV1, and CD3E in the T cell receptor signaling pathway were selected as important factors, and LCK was identified as the hub protein. Conclusion LCK, via acting on T-cell receptor, might be a potential therapeutic target for AR after kidney transplantation.

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“…Expression vectors transfected into FreeStyle293 cells were expressed as recombinant IgGs, which were then purified from culture supernatants using rProtein A-Sepharose (GE Healthcare). GPRC5D TRABs were generated by Fab-arm exchange as described previously (16).…”

Section: Generation Of Gprc5d-specific Recombinant Mabsmentioning

confidence: 99%

Anti-GPRC5D/CD3 Bispecific T-Cell–Redirecting Antibody for the Treatment of Multiple Myeloma

Kodama

Kochi

Nakai³

et al. 2019

Molecular Cancer Therapeutics

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Although treatment advances over recent decades have significantly improved survival of patients with multiple myeloma, there is still an unmet medical need for more effective treatments. In this study, we identified G-protein-coupled receptor family C group 5 member D (GPRC5D) expression on the surface of malignant cells involved in multiple myeloma, but except for plasma cells and B cells, not at appreciable levels on normal hematopoietic cells and bone marrow progenitors , including hematopoietic stem cells. In addition, we constructed IgG-based anti-GPRC5D/CD3 bispecific T-cell-redirecting antibodies (GPRC5D TRAB), which suppressed the tumor growth of GPRC5D-positive myeloma cells through the activation of T cells in vitro and in vivo in xenograft models. Collectively, these findings suggest that GPRC5D is an antigen specific to multiple myeloma and a potential target of TRAB therapy.

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Entire CD3ε, δ, and γ humanized mouse to evaluate human CD3–mediated therapeutics

Cited by 20 publications

References 32 publications

CD3-Bispecific Antibody Therapy Turns Solid Tumors into Inflammatory Sites but Does Not Install Protective Memory

CD3-Bispecific Antibody Therapy Turns Solid Tumors into Inflammatory Sites but Does Not Install Protective Memory

LCK as a Potential Therapeutic Target for Acute Rejection after Kidney Transplantation: A Bioinformatics Clue

Anti-GPRC5D/CD3 Bispecific T-Cell–Redirecting Antibody for the Treatment of Multiple Myeloma

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