Chimeric antigen receptor T lymphocyte and application thereof to preparation of product for treating solid tumors

A chimeric antigen receptor and cell technology, applied in the field of biomedicine, can solve the problems of no clinical efficacy, inability to truly exert anti-tumor effect, immune escape and other problems

Active Publication Date: 2020-11-03
CARBIOGENE THERAPEUTICS CO LTD
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

The existing targets at this stage, such as Glypican 3 (GPC-3), Claudin18.2, EpCAM, Mesothelin (MSLN), etc., have achieved certain results in preclinical research, but they have not made further progress in clinical efficacy
Although some abnormally high-expressed proteins on the surface of tumor cells can be screened only through omics detection and big data analysis, when immunotherapy products (such as antibody therapy, CAR-T therapy) targeting these protein antigens are released in human When working in vivo, it is often isolated by the immune microenvironment of tumor cells, and cannot really exert its anti-tumor effect
One of the reasons is that in the process of interaction between tumor cells and immune effector cells (such as T cells, macrophages, etc.), the immune checkpoint pathway (such as B7 family protein) of immune cells is often activated, resulting in a decrease in the viability of effector cells. , resulting in immune escape
In addition, the continuous proliferation and insufficient residence time of CAR-T cells in the body also limits the response rate of CAR-T therapy and increases the recurrence rate of CAR-T therapy
More importantly, some solid tumor targets such as HER2, VEGFR, etc. are prone to off-target toxicity due to non-specific expression, and the safety in the actual clinical application process is questionable

Method used

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  • Chimeric antigen receptor T lymphocyte and application thereof to preparation of product for treating solid tumors
  • Chimeric antigen receptor T lymphocyte and application thereof to preparation of product for treating solid tumors
  • Chimeric antigen receptor T lymphocyte and application thereof to preparation of product for treating solid tumors

Examples

Experimental program
Comparison scheme
Effect test

Embodiment 1

[0139] Example 1, Preparation of CAR-T cells

[0140] First, the construction of the reverse transcription viral vector

[0141] 1. Optimization of the full length sequence of wild-type CD27 gene cDNA

[0142] The full-length sequence of the wild-type CD27 gene cDNA is called NCD27. In order to make NCD 27 more suitable for expression in human cells, the NCD27 sequence is optimized on the website http: / / sg.idtdna.com / site in the case of ensuring NCD27 encoded, and obtains OCD27. The nucleotide sequence of OCD27 is shown in Seq ID No. 2719-3501.

[0143] 2, S15-CAR-CD27 gene sequence design and synthesis

[0144] The S15-CAR-CD27 gene sequence includes a coded gene sequence of human CD8 primary peptide, an encoded gene sequence of S15 SCFV, a coded gene sequence of human CD8 hinge transmembrane region, coding gene sequence of human 4-1bb, human CD3ζ Coding gene sequence, P2A peptide (rendered by P2A peptide-1) encoding gene sequence, CSF2RA signal peptide encoding gene sequence, EG...

Embodiment 2

[0184] Example 2, CFSE marker method Detection Car-T cells to tumor cell specific killing

[0185] CFSE (CFDA-SE) is a cell dyeing agent that can fluorescently labeled living cells, which can easily penetrate the cell membrane, covalently bind to intracellular proteins in living cells, and release green fluorescence after hydrolysis. Tumor cells can be labeled and quantified by CFSE labeling living cells, thus detecting killing efficiency of CAR-T cells on tumor target cells. The specific method is: the target cell isometric is divided into two groups, adjusted to the same cell density. The low concentration and high concentration CFSE were dyed, and the high concentration dyed target cells were co-cultured in a certain proportion of the non-stained immunocytes. After incubation for a period of time, high concentration staining target cell tubes (along with immune cells) were mixed with low concentration staining target cell tube. Finally, the killing rate of CAR T cells to target...

Embodiment 3

[0200] Example 3, tumor transplantation model detects tumor killing effect of Car-T cells in an animal

[0201] Experimental materials: 5-6 weeks old, a B-NDG of 18-22 g weight combined with immunodeficiency mice (Bai Oti Gene Biotechnology Co., Ltd.).

[0202] Experimental grouping: randomly divided experimental materials into three experimental groups, 5 mice each group. The method of processing each group is as follows:

[0203] S15 CAR-CD27 T: Temperature of B-NDG Temperamnamotic Mort-NDG U87-Mg Tumor Cell Solution (Solvent is PBS), with a inoculation amount of 0.3 ml (including 2 × 10 6 Tumor cells). After 5 days of inoculation of tumor cells, the S15 CAR-CD27 T cell solution prepared in the tail intravenous injection of Example 1 (PBS), S15 CAR-CD27 T cell injection is 0.2 ml (including 5 × 10 6 S15 CAR-CD27 T cells).

[0204] S15 Car T: Temperature of B-NDG inoculated with immunodeficiency mouse tail intravenous U87-Mg tumor cell solution (solvent is PBS), and inoculate 0.3...

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Abstract

The invention discloses a chimeric antigen receptor T lymphocyte and an application thereof to preparation of a product for treating solid tumors. A chimeric antigen receptor in the chimeric antigen receptor T lymphocyte sequentially comprises a human CD8 lead peptide, an anti-Siglec-15 single-chain antibody, a human CD8 hinge transmembrane region, a human 4-1BB intracellular region, a human CD3 zeta intracellular region, a self-cleavage peptide, a CSF2Ra signal peptide, an EGFRt protein, a self-cleavage peptide and a human CD27. Experiments prove that the chimeric antigen receptor T lymphocyte provided by the invention highly expresses IFN gamma and CD107a, has a strong killing function on Siglec-15 positive tumor cells, and has killing efficiency of more than 80% under the condition thatthe effect-target ratio is 1: 1. A tumor transplantation model experiment shows that the chimeric antigen receptor T lymphocyte also has a strong killing function on Siglec-15 positive tumor cells inan animal body.

Description

Technical field [0001] The present invention relates to the field of biotechnology medicine, in particular to a chimeric T cell antigen receptor and its application in preparing medicine for treating solid tumors in a product, particularly to a Siglec-15-CAR-CD27 chimeric antigen receptor gene modified T lymphocytes and its application in preparing medicine for treating solid tumors in a product. Background technique [0002] With the study of mechanisms of immune responses of T lymphocytes tumor growing emphasis on chimeric antigen receptor T (CAR-T) cell therapy is emerging as a new immunotherapeutic strategies in the field of cancer immunotherapy. Since the T cells recognize the target cell-specific receptor is dependent on T lymphocytes (T Cell Receptor, TCR), and therefore the single chain antibody fragment against tumor cell-associated antigen (scFv) CD3ζ or T cell receptor with FcεRIγ intracellular signaling like the activation motif fused to the chimeric receptor antigen ...

Claims

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Application Information

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Patent Type & Authority Applications(China)
IPC IPC(8): C07K19/00C12N15/62C12N5/10C12N15/867A61K39/00A61P35/00
CPCA61P35/00A61K39/001129A61K2039/80A61K2039/836A61K2039/844A61K2039/86A61K2039/868A61K2039/876A61K2039/892C07K14/7051C07K14/70578C07K16/2803C07K2319/02C07K2319/03C07K2319/33C12N5/0636C12N15/86C12N2510/00C12N2740/10043C12N2740/15043
Inventor 朱建高杨文君
Owner CARBIOGENE THERAPEUTICS CO LTD
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