Method effector cells using anti-CD127 antibodies for applications in cell therapy

What is claimed is: 1. A method for in vitro sorting out T effector cells from a preparation of cells obtained from a biological fluid or tissue wherein the preparation of cells comprises human cells, wherein the method comprises: a. contacting the preparation of cells with an anti-CD127 antibody specifically binding to CD127 on said T effector cells, said anti-CD127 antibody comprising the following CDRs sequences: in a heavy chain, CDRs of a VH3 heavy chain disclosed as sequence of SEQ ID No: 2, with CDRs of VH3-CDR1, VH3-CDR2 and VH3-CDR3 comprising or consisting of sequences of SEQ ID Nos: 14, 16 and 18, respectively and, in a light chain, CDRs of a VL3 or of a VL4 light chain disclosed as sequences of SEQ ID Nos: 4 and 6, respectively, with CDRs VL3-CDR1, VL3/4-CDR2 and VL3/4-CDR3 having the sequences of SEQ ID Nos: 20, 22 and 24 respectively, or with CDRs of VL4-CDR1, VL3/4-CDR2 and VL3/4-CDR3 comprising or consisting of the sequences of SEQ ID Nos: 26, 22 and 24 respectively; b. selecting sorting out said T effector cells bound to said anti-CD127 antibody and recovering the cell preparation enriched in said T effector cells and depleted for at least Treg cells; washing the anti-CD127 antibody from said T effector cells. 2. The method according to claim 1 , wherein the anti-CD127 antibody is selected from anti-CD127 antibodies comprising VH and VL sequences as follows: a. a heavy chain variable domain designated Effi3-VH3 comprising or consisting of sequence of SEQ ID No: 2 or Effi3-VH3 variant comprising or consisting of sequence SEQ ID No: 8 and, for a variant designated Effi3-VH3VL3, either a light chain variable domain designated Effi3-VL3 comprising or consisting of sequence SEQ ID No: 4 or Effi3-VL3 variant comprising or consisting of sequence SEQ ID No: 10, or alternatively b. a heavy chain variable domain designated Effi3-VH3 comprising or consisting of sequence of SEQ ID No: 2 or Effi3-VH3 variant comprising or consisting of sequence SEQ ID No: 8 and, for a variant designated Effi3-VH3VL4, either a light chain variable domain designated Effi3-VL4 comprising or consisting of sequence SEQ ID No: 6 or Effi3-VL4 variant comprising or consisting of sequence SEQ ID No: 12. 3. The method according to claim 1 , wherein the step of sorting out cells is performed using magnetic cell sorting and the anti-CD127 antibody is biotinylated or otherwise marked for staining. 4. The method according to claim 1 , wherein cell sorting is performed until more than 90% of Treg cells are depleted from the preparation of cells. 5. The method of claim 4 wherein more than 99% of Treg cells are depleted from the preparation of cells. 6. The method according to claim 1 , wherein the anti-CD127 antibodies is provided with a composition that comprises polyclonal immunoglobulins suitable for reducing nonspecific interactions of the anti-CD127 antibody with targeted T effector cells. 7. The method according to claim 1 , wherein the cell preparation is a human blood cell preparation. 8. The method according to claim 1 , wherein the cell preparation is a preparation of hematopoietic stem cells for transplantation (HSCT) or T cells for adoptive therapy. 9. The method according to claim 8 wherein the cell preparation includes T cells for adoptive therapy selected from the group consisting of tumor-infiltrating cells (TILs), genetically modified cancer-specific T cells known as Chimeric-Antigen Receptor T cells (CART), or both. 10. The method according to claim 1 , further comprising administering the T effector cells to a human patient to treat a solid or liquid tumor in the human patient or administering the T effector cells to a human patient to treat a chronic infection by a pathogen selected among bacteria, parasites, protozoans, yeasts and viruses. 11. The method according to claim 10 , wherein the anti-CD127 antibody is selected from anti-CD127 antibodies comprising VH and VL sequences as follows: a. a heavy chain variable domain designated Effi3-VH3 comprising or consisting of sequence of SEQ ID No: 2 or Effi3-VH3 variant comprising or consisting of sequence SEQ ID No: 8 and, for a variant designated Effi3-VH3VL3, either a light chain variable domain designated Effi3-VL3 comprising or consisting of sequence SEQ ID No: 4 or Effi3-VL3 variant comprising or consisting of sequence SEQ ID No: 10, or alternatively b. a heavy chain variable domain designated Effi3-VH3 comprising or consisting of sequence of SEQ ID No: 2 or Effi3-VH3 variant comprising or consisting of sequence SEQ ID No: 8 and, for a variant designated Effi3-VH3VL4, either a light chain variable domain designated Effi3-VL4 comprising or consisting of sequence SEQ ID No: 6 or Effi3-VL4 variant comprising or consisting of sequence SEQ ID No: 12. 12. The method according to claim 10 , wherein the step of sorting out cells is performed using magnetic cell sorting and the anti-CD127 antibody is biotinylated or otherwise marked for staining. 13. The method according to claim 10 , wherein cell sorting is performed until more than 90% of Treg cells are depleted from the preparation of cells. 14. The method according to claim 10 , wherein the anti-CD127 antibodies is provided with a composition that comprises polyclonal immunoglobulins suitable for reducing nonspecific interactions of the anti-CD127 antibody with targeted T effector cells. 15. The method according to claim 1 wherein the anti-CD127 antibody is an antibody that does not compete with interleukin-7 for binding to an interleukin-7 (IL-7) receptor.