Compositions for treatment of cancer
US-9102761-B2 · Aug 11, 2015 · US
CD20 therapies, CD22 therapies, and combination therapies with a CD19 chimeric antigen receptor (CAR)-expressing cell
US11149076B2 · US · B2
| Field | Value |
|---|---|
| Publication number | US-11149076-B2 |
| Application number | US-201916256731-A |
| Country | US |
| Kind code | B2 |
| Filing date | Jan 24, 2019 |
| Priority date | Apr 8, 2015 |
| Publication date | Oct 19, 2021 |
| Grant date | Oct 19, 2021 |
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- Title
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- Abstract
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Abstract
Official abstract text for this publication.
The invention provides compositions and methods for treating diseases associated with expression of CD19, e.g., by administering a recombinant T cell comprising the CD19 CAR as described herein, in combination with one or more B-cell inhibitors, e.g., inhibitors of one or more of CD10, CD20, CD22, CD34, CD123, FLT-3, ROR1, CD79b, CD179b, or CD79a. The disclosure additionally features novel antigen binding domains and CAR molecules directed to CD20 and CD22, and uses, e.g., as monotherapies or in combination therapies. The invention also provides kits and compositions described herein.
First claim
Opening claim text (preview).
What is claimed is: 1. An isolated nucleic acid molecule encoding a chimeric antigen receptor (CAR) molecule, wherein the CAR molecule comprises a CD22 binding domain, a transmembrane domain, and an intracellular signaling domain, and wherein the CD22 binding domain comprises: i. a light chain complementarity determining region 1 (LC CDR1) of SEQ ID NO: 648, a light chain complementarity determining region 2 (LC CDR2) of SEQ ID NO: 659, and a light chain complementarity determining region 3 (LC CDR3) of SEQ ID NO: 670; and ii. a heavy chain complementarity determining region 1 (HC CDR1) of SEQ ID NO: 498 or SEQ ID NO: 1345, a heavy chain complementarity determining region 2 (HC CDR2) of SEQ ID NO: 509 or SEQ ID NO: 1354, and a heavy chain complementarity determining region 3 (HC CDR3) of SEQ ID NO: 520 or SEQ ID NO: 1363. 2. The isolated nucleic acid molecule of claim 1 , wherein the CD22 binding domain comprises: i. a light chain variable (VL) region with 95-99% sequence identity to SEQ ID NO: 690; and ii. a heavy chain variable (VH) region with 95-99% sequence identity to SEQ ID NO: 680. 3. The isolated nucleic acid molecule of claim 1 , wherein the CD22 binding domain comprises: i. a VL region of SEQ ID NO: 690; and ii. a VH region of SEQ ID NO: 680. 4. The isolated nucleic acid molecule of claim 1 , wherein the CAR molecule further comprises a leader sequence of SEQ ID NO: 13. 5. The isolated nucleic acid molecule of claim 1 , wherein the CAR molecule further comprises a linker of SEQ ID NO: 53. 6. The isolated nucleic acid molecule of claim 1 , wherein the CAR molecule further comprises a CD8 hinge as set forth in SEQ ID NO: 14. 7. The isolated nucleic acid molecule of claim 1 , wherein the transmembrane domain comprises a CD8 transmembrane domain as set forth in SEQ ID NO: 15. 8. The isolated nucleic acid molecule of claim 1 , wherein the intracellular signaling domain comprises a functional signaling domain of 4-1BB, a functional signaling domain of CD3 zeta, or both. 9. The isolated nucleic acid molecule of claim 8 , wherein the functional signaling domain of 4-1BB is as set forth in SEQ ID NO: 16. 10. The isolated nucleic acid molecule of claim 8 , wherein the functional signaling domain of CD3 zeta is as set forth in SEQ ID NO: 43. 11. The isolated nucleic acid molecule of claim 1 , wherein the CAR molecule further comprises a P2A protease cleavage site or a T2A protease cleavage site. 12. The isolated nucleic acid molecule of claim 11 , wherein the P2A protease cleavage site is as set forth in SEQ ID NO: 1329 and the T2A protease cleavage site of SEQ ID NO: 1328. 13. A cell comprising the nucleic acid molecule of claim 1 . 14. A chimeric antigen receptor (CAR) molecule, which comprises a CD22 binding domain, a transmembrane domain, and an intracellular signaling domain, and wherein the CD22 binding domain comprises: i. a LC CDR1 of SEQ ID NO: 648, a LC CDR2 of SEQ ID NO: 659, and a LC CDR3 of SEQ ID NO: 670; and ii. a HC CDR1 of SEQ ID NO: 498 or SEQ ID NO: 1345, a HC CDR2 of SEQ ID NO: 509 or SEQ ID NO: 1354, and a HC CDR3 of SEQ ID NO: 520 or SEQ ID NO: 1363. 15. The CAR molecule of claim 14 , wherein the CD22 binding domain comprises i. a VL region with 95-99% sequence identity to SEQ ID NO: 690; and ii. a VH region with 95-99% sequence identity to SEQ ID NO: 680. 16. The CAR molecule of claim 14 , wherein the CD22 binding domain comprises i. a VL region of SEQ ID NO: 690; and ii. a VH region of SEQ ID NO: 680. 17. The CAR molecule of claim 14 , which further comprises a leader sequence of SEQ ID NO: 13. 18. The CAR molecule of claim 14 , which further comprises a linker of SEQ ID NO: 53. 19. The CAR molecule of claim 14 , which further comprises a CD8 hinge as set forth in SEQ ID NO: 14. 20. The CAR molecule of claim 14 , wherein the transmembrane domain comprises a CD8 transmembrane domain as set forth in SEQ ID NO: 15. 21. The CAR molecule of claim 14 , wherein the intracellular signaling domain comprises a functional signaling domain of 4-1BB, a functional signaling domain of CD3 zeta, or both. 22. The CAR molecule of claim 21 , wherein the functional signaling domain of 4-1BB is as set forth in SEQ ID NO: 16. 23. The CAR molecule of claim 21 , wherein the functional signaling domain of CD3 zeta is as set forth in SEQ ID NO: 43. 24. The CAR molecule of claim 14 , which further comprises a P2A protease cleavage site or a T2A protease cleavage site. 25. A cell comprising the CAR molecule of claim 14 . 26. A chimeric antigen receptor (CAR) molecule that binds to CD22 comprises, from N-terminus to C-terminus: i. a leader sequence of SEQ ID NO: 13; ii. a HC CDR1 of SEQ ID NO: 498 or SEQ ID NO: 1345; iii. a HC CDR2 of SEQ ID NO: 509 or SEQ ID NO: 1354; iv. a HC CDR3 of SEQ ID NO: 520 or SEQ ID NO: 1363; v. a LC CDR1 of SEQ ID NO: 648; vi. a LC CDR2 of SEQ ID NO: 659; vii. a LC CDR3 of SEQ ID NO: 670; viii. a CD8 hinge of SEQ ID NO: 14; ix. a CD8 transmembrane domain of SEQ ID NO: 15; x. a functional signaling domain of 4-1BB of SEQ ID NO: 16; and xi. a functional signaling domain of CD3 zeta of SEQ ID NO: 43. 27. The CAR molecule of claim 26 , which further comprises a VH region of SEQ ID NO: 680 and a VL region of SEQ ID NO: 690. 28. A method of treating a subject having a hematological cancer, comprising administering to the subject an effective number of one or more cells that express a CAR molecule, wherein the CAR molecule comprises a CD22 binding domain, a transmembrane domain, and an intracellular signaling domain, and wherein the CD22 binding domain comprises: i. a LC CDR1 of SEQ ID NO: 648, a LC CDR2 of SEQ ID NO: 659, and a LC CDR3 of SEQ ID NO: 670; and ii. a HC CDR1 of SEQ ID NO: 498 or SEQ ID NO: 1345, a HC CDR2 of SEQ ID NO: 509 or SEQ ID NO: 1354, and a HC CDR3 of SEQ ID NO: 520 or SEQ ID NO: 1363. 29. The method of claim 28 , wherein the hematologic cancer is selected from the group consisting of acute leukemia, T-cell acute lymphoblastic leukemia (TALL), small lymphocytic lymphoma (SLL), acute lymphoblastic leukemia (ALL); chronic leukemia, chronic myelogenous leukemia (CML), chronic lymphocytic leukemia (CLL), non-Hodgkin lymphoma, multiple myeloma, and myeloma. 30. The method of claim 28 , wherein the hematologic cancer is B-cell acute lymphoblastic leukemia (BALL). 31. The method of claim 30 , wherein the hematologic cancer is a pediatric BALL. 32. The method of claim 30 , wherein the hematologic cancer is an adult BALL.
Assignees
Inventors
Classifications
against receptors for cytokines, lymphokines, interferons · CPC title
against the immunoglobulin superfamily · CPC title
fusions for targeting to specific cell types, e.g. tissue specific targeting, targeting of a bacterial subspecies · CPC title
containing a transmembrane segment · CPC title
Single domain, e.g. dAb, sdAb, VHH, VNAR or nanobody® · CPC title
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- What does patent US11149076B2 cover?
- The invention provides compositions and methods for treating diseases associated with expression of CD19, e.g., by administering a recombinant T cell comprising the CD19 CAR as described herein, in combination with one or more B-cell inhibitors, e.g., inhibitors of one or more of CD10, CD20, CD22, CD34, CD123, FLT-3, ROR1, CD79b, CD179b, or CD79a. The disclosure additionally features novel anti…
- Who is the assignee on this patent?
- Novartis Ag, Univ Pennsylvania
- What technology area does this patent fall under?
- Primary CPC classification C07K14/7051. Mapped technology areas include Chemistry & Metallurgy.
- When was this patent published?
- Publication date Tue Oct 19 2021 00:00:00 GMT+0000 (Coordinated Universal Time) (B2). Legal status and post-grant events are not shown on this page.
- What related patents are in patentsdb?
- We list 12 related publications on this page (citations in our corpus or others sharing the same primary CPC).