Novel antibodies and combined use of a treg depleting antibody and an immunostimulatory antibody
Abstract
Described is the sequential administration of first a Treg depleting antibody mole-cute selected from antibody molecules, such as an antibody molecule binding specifically to target belonging to the tumour necrosis factor receptor superfamily (TNFRSF), such as a Treg depleting anti-4-1 BB antibody or a Treg depleting OX-40 antibody, and then an immunostimulatory antibody molecule, such as an immunostimulatory anti-4-1 BB anti-body or an immunostimulatory OX-40 antibody, for use in the treatment of cancer. De-scribed are also novel anti-4-1 BB antibodies and novel OX-40 antibodies that may be used in such sequential administration.
Claims
exact text as granted — not AI-modified1 . A method of treating cancer wherein a Treg depleting antibody molecule is administered sequentially with an immunostimulatory antibody molecule with the Treg depleting antibody molecule being administered prior to administration of the immunostimulatory antibody molecule.
2 . A method according to claim 1 , wherein said immunostimulatory antibody molecule is a CD8 activating and/or CD8 boosting antibody molecule.
3 . A method according to claim 1 , wherein the cancer is a solid tumour, such as a solid tumour selected from the group consisting of sarcomas, carcinomas, lymphomas and ovarian cancer and/or a solid tumour selected from the group consisting of squamous cell carcinoma (SCC), thymoma, neuroblastoma or ovarian cancer.
4 . A method according to claim 1 , wherein said Treg depleting antibody molecule and/or said immunostimulatory antibody molecule is selected from the group consisting of a full-size antibody, a Fab, a Fv, an scFv, a Fab′, and a (Fab′) 2 .
5 . A method according to claim 1 , wherein said Treg depleting antibody molecule is a human IgG1 antibody, which optionally may be engineered for improved binding to at least one activatory FcγR.
6 . A method according to claim 1 , wherein said Treg depleting antibody molecule is selected from antibody molecules binding specifically to a target belonging to the tumour necrosis factor receptor superfamily (TNFRSF).
7 . A method according to claim 6 , wherein said Treg depleting antibody molecule is an antibody molecule that binds specifically to a target selected from the group consisting of 4-1BB, OX40, and TNFR2.
8 . A method according to claim 1 , wherein said Treg depleting antibody molecule is an antibody molecule that binds specifically to a target selected from GITR, ICOS, CTLA-4, CD25 and neuropilin-1.
9 . A method according to claim 7 , wherein said Treg depleting antibody molecule is an anti-4-1BB monoclonal antibody molecule.
10 . A method according to claim 9 , wherein the Treg depleting antibody molecule is selected from the group consisting of antibody molecules comprising 1-6 of the CDRs selected from SEQ. ID. NOs: 1-6; 1-6 of the CDRs selected from SEQ. ID. NOs: 9-14; 1-6 of the CDRs selected from SEQ. ID. NOs: 17-22; 1-6 of the CDRs selected from SEQ. ID. NOs: 25-30; 1-6 of the CDRs selected from SEQ. ID. NOs: 33-38; 1-6 of the CDRs selected from SEQ. ID. NOs: 41-46; 1-6 of the CDRs selected from SEQ. ID. NOs: 49-54; 1-6 of the CDRs selected from SEQ. ID. NOs: 57-62; 1-6 of the CDRs selected from SEQ. ID. NOs: 65-70; 1-6 of the CDRs selected from SEQ. ID. NOs: 153-158; and 1-6 of the CDRs selected from SEQ. ID. NOs: 163-168.
11 . A method according to claim 10 , wherein the Treg depleting antibody molecule is selected from the group consisting of antibody molecules comprising a variable heavy chain selected from the group consisting of SEQ. ID. NOs: 7, 15, 23, 31, 39, 47, 55, 63, 71, 159, and 169, and/or a variable light chain selected from the group consisting of SEQ. ID. NOs: 8, 16, 24, 32, 40, 48, 56, 64, 72, 160, and 170.
12 . A method according to claim 10 , wherein the Treg depleting antibody molecule is selected from the group consisting of antibody molecule comprising SEQ. ID. NOs: 7 and 8; SEQ. ID. NOs: 15 and 16; SEQ. ID. NOs: 23 and 24; SEQ. ID. NOs: 31 and 32; SEQ. ID. NOs: 39 and 40; or SEQ. ID. NOs: 47 and 48; SEQ. ID. NOs: 55 and 56; SEQ. ID. NOs: 63 and 64, SEQ. ID. NOs: 71 and 72; SEQ. ID. NOs: 159-160; and SEQ. ID. NOs: 169-170.
13 . A method according to claim 7 , wherein said Treg depleting antibody is a human anti-OX40 monoclonal antibody molecule.
14 . A method according to claim 13 , wherein the Treg depleting antibody molecule is selected from the group consisting of antibody molecule comprising 1-6 of the CDRs selected from SEQ. ID. NOs: 73-78; 1-6 of the CDRs selected from SEQ. ID. NOs: 81-86; 1-6 of the CDRs selected from SEQ. ID. NOs: 89-94; 1-6 of the CDRs selected from SEQ. ID. NOs: 97-102; 1-6 of the CDRs selected from SEQ. ID. NOs: 105-110; 1-6 of the CDRs selected from SEQ. ID. NOs: 113-118; 1-6 of the CDRs selected from SEQ. ID. NOs: 121-126; 1-6 of the CDRs selected from SEQ. ID. NOs: 129-134; 1-6 of the CDRs selected from SEQ. ID. NOs: 137-142; 1-6 of the CDRs selected from SEQ. ID. NOs: 145-150, and 1-6 of the CDRs selected from SEQ. ID. NOs: 171-176.
15 . A method according to claim 14 , wherein the Treg depleting antibody molecule is selected from the group consisting of antibody molecules comprising a variable heavy chain selected from the group consisting of SEQ. ID. NOs: 79, 87, 95, 103, 111, 119, 127, 135, 143, 151, and 177, and/or a variable light chain selected from the group consisting of SEQ. ID. NOs: 80, 88, 96, 104, 112, 120, 128, 136, 144, 152 and 178.
16 . A method according to claim 1 , wherein the immunostimulatory antibody molecule is a human IgG2 antibody or a human IgG4 antibody molecule, which optionally may be engineered for enhanced binding to human FcγRIIB over activatory Fc gamma receptors.
17 . A method according to claim 16 , wherein the immunostimulatory antibody molecule is a human IgG2b antibody molecule, which optionally may be engineered for enhanced binding to human FcγRIIB over activatory Fc gamma receptors.
18 . A method according to claim 1 , wherein the immunostimulatory antibody molecule is an antibody that binds specifically to a target selected from the group consisting of 4-1BB, OX40, ICOS, GITR, CTLA-4, CD25, PD-1 and PDL1.
19 . A method according to claim 18 , wherein the immunostimulatory antibody molecule is an anti-4-1BB antibody molecule.
20 . A method according to claim 19 , wherein the immunostimulatory antibody molecule is selected from the group consisting of antibody molecules comprising 1-6 of the CDRs selected from SEQ. ID. NOs: 1-6; 1-6 of the CDRs selected from SEQ. ID. NOs: 9-14; 1-6 of the CDRs selected from SEQ. ID. NOs: 17-22; 1-6 of the CDRs selected from SEQ. ID. NOs: 25-30; 1-6 of the CDRs selected from SEQ. ID. NOs: 33-38; 1-6 of the CDRs selected from SEQ. ID. NOs: 41-46; 1-6 of the CDRs selected from SEQ. ID. NOs: 49-54; 1-6 of the CDRs selected from SEQ. ID. NOs: 57-62; 1-6 of the CDRs selected from SEQ. ID. NOs: 65-70; 1-6 of the CDRs selected from SEQ. ID. NOs: 153-158; and 1-6 of the CDRs selected from SEQ. ID. NOs: 163-168.
21 . A method according to claim 20 , wherein the immunostimulatory antibody molecule is selected from the group consisting of antibody molecules comprising a variable heavy chain selected from the group consisting of SEQ. ID. NOs: 7, 15, 23, 31, 39, 47, 55, 63, 71, 159 and 169, and/or a variable light chain selected from the group consisting of SEQ. ID. NOs: 8, 16, 24, 32, 40, 48, 56, 64, 72, 160 and 170.
22 . A method according to claim 20 , wherein immunostimulatory antibody molecule is selected from the group consisting of antibody molecule comprising SEQ. ID. NOs: 7 and 8; SEQ. ID. NOs: 15 and 16; SEQ. ID. NOs: 23 and 24; SEQ. ID. NOs: 31 and 32; SEQ. ID. NOs: 39 and 40; and SEQ. ID. NOs: 47 and 48; SEQ. ID. NOs: 55 and 56; SEQ. ID. NOs: 63 and 64, SEQ. ID. NOs: 71 and 72, SEQ. ID. NOs: 159 and 160, and SEQ. ID. NOs: 169 and 170.
23 . A method according to claim 18 , wherein the immunostimulatory antibody molecule is an anti-OX40 antibody molecule.
24 . A method according to claim 23 wherein the immunostimulatory antibody molecule is selected from the group consisting of antibody molecule comprising 1-6 of the CDRs selected from SEQ. ID. NOs: 73-78; 1-6 of the CDRs selected from SEQ. ID. NOs: 81-86; 1-6 of the CDRs selected from SEQ. ID. NOs: 89-94; 1-6 of the CDRs selected from SEQ. ID. NOs: 97-102; 1-6 of the CDRs selected from SEQ. ID. NOs: 105-110; 1-6 of the CDRs selected from SEQ. ID. NOs: 113-118; 1-6 of the CDRs selected from SEQ. ID. NOs: 121-126; 1-6 of the CDRs selected from SEQ. ID. NOs: 129-134; 1-6 of the CDRs selected from SEQ. ID. NOs: 137-142; 1-6 of the CDRs selected from SEQ. ID. NOs: 145-150; and 1-6 of the CDRs selected from SEQ. ID. NOs: 171-176.
25 . A method according to claim 24 , wherein the immunostimulatory antibody molecule is selected from the group consisting of antibody molecules comprising a variable heavy chain selected from the group consisting of SEQ. ID. NOs: 79, 87, 95, 103, 111, 119, 127, 135, 143, 151 and 177, and/or a variable light chain selected from the group consisting of SEQ. ID. NOs: 80, 88, 96, 104, 112, 120, 128, 136, 144, 152 and 178.
26 . A method according to claim 24 , wherein the immunostimulatory antibody molecule is selected from the group consisting of antibody molecules comprising SEQ. ID. NOs: 79 and 80; SEQ. ID. NOs: 87 and 88; SEQ. ID. NOs: 95 and 96; SEQ. ID. NOs: 103 and 104; SEQ. ID. NOs: 111 and 112; SEQ. ID. NOs: 119 and 120; SEQ. ID. NOs: 127 and 128; SEQ. ID. NOs: 135 and 136; SEQ. ID. NOs: 143 and 144; SEQ. ID. NOs: 151 and 152; and SEQ. ID. NOs: 177-178.
27 . A method according to claim 18 , wherein the immunostimulatory antibody molecule is a human anti-PD1 monoclonal antibody molecule, a human anti-PDL1 monoclonal antibody molecule or a human anti-CTLA-4 monoclonal antibody molecule.
28 . A method according to claim 27 , wherein the wherein the immunostimulatory antibody molecule is a human anti-PD1 monoclonal antibody molecule selected from the group consisting of nivolumab and pembrolizumab or the anti-PDL1 antibody atezolizumab or an anti-CTLA-4 antibody selected from the group consisting of ipilimumab and tremilimumab.
29 . An anti-4-1BB antibody molecule selected from the group consisting of antibody molecules comprising 1-6 of the CDRs selected from SEQ. ID. NOs: 1-6; 1-6 of the CDRs selected from SEQ. ID. NOs: 9-14; 1-6 of the CDRs selected from SEQ. ID. NOs: 17-22; 1-6 of the CDRs selected from SEQ. ID. NOs: 25-30; 1-6 of the CDRs selected from SEQ. ID. NOs: 33-38; 1-6 of the CDRs selected from SEQ. ID. NOs: 41-46; 1-6 of the CDRs selected from SEQ. ID. NOs: 49-54; 1-6 of the CDRs selected from SEQ. ID. NOs: 57-62; 1-6 of the CDRs selected from SEQ. ID. NOs: 65-70; 1-6 of the CDRs selected from SEQ. ID. NOs: 153-158; and 1-6 of the CDRs selected from SEQ. ID. NOs: 163-168.
30 - 34 . (canceled)
35 . An anti-OX40 antibody molecule selected from the group consisting of antibody molecule comprising 1-6 of the CDRs selected from SEQ. ID. NOs: 73-78; 1-6 of the CDRs selected from SEQ. ID. NOs: 81-86; 1-6 of the CDRs selected from SEQ. ID. NOs: 89-94; 1-6 of the CDRs selected from SEQ. ID. NOs: 97-102; 1-6 of the CDRs selected from SEQ. ID. NOs: 105-110; 1-6 of the CDRs selected from SEQ. ID. NOs: 113-118; 1-6 of the CDRs selected from SEQ. ID. NOs: 121-126; 1-6 of the CDRs selected from SEQ. ID. NOs: 129-134; 1-6 of the CDRs selected from SEQ. ID. NOs: 137-142; 1-6 of the CDRs selected from SEQ. ID. NOs: 145-150, and 1-6 of the CDRs selected from SEQ. ID. NOs: 171-176.
36 - 39 . (canceled)
40 . An isolated nucleic acid encoding an antibody according to claim 29 .
41 - 81 . (canceled)
82 . An isolated nucleic acid encoding an antibody according to claim 35 .Join the waitlist — get patent alerts
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