WO2008156712A1 - Antibodies to human programmed death receptor pd-1 - Google Patents

Antibodies to human programmed death receptor pd-1 Download PDF

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Publication number
WO2008156712A1
WO2008156712A1 PCT/US2008/007463 US2008007463W WO2008156712A1 WO 2008156712 A1 WO2008156712 A1 WO 2008156712A1 US 2008007463 W US2008007463 W US 2008007463W WO 2008156712 A1 WO2008156712 A1 WO 2008156712A1
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antibody
human
amino acid
seq
variant
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PCT/US2008/007463
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English (en)
French (fr)
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Gregory John Carven
Hans Van Eenennaam
Gradus Johannes Dulos
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N. V. Organon
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Priority to US12/663,950 priority Critical patent/US8354509B2/en
Priority to HK10106898.8A priority patent/HK1140497B/en
Priority to HRP20131167AT priority patent/HRP20131167T1/hr
Priority to ES08768485.8T priority patent/ES2437327T3/es
Priority to BR122017025062A priority patent/BR122017025062B8/pt
Priority to BRPI0812913A priority patent/BRPI0812913B8/pt
Priority to KR1020147030247A priority patent/KR101562580B1/ko
Priority to MEP-2013-545A priority patent/ME02093B/me
Priority to DK08768485.8T priority patent/DK2170959T3/da
Priority to PL08768485T priority patent/PL2170959T3/pl
Priority to RS20130545A priority patent/RS53072B/en
Priority to KR1020157011771A priority patent/KR101586617B1/ko
Priority to JP2010513201A priority patent/JP5191537B2/ja
Priority to CN200880103544.3A priority patent/CN102131828B/zh
Priority to MX2009014199A priority patent/MX2009014199A/es
Priority to CA2691357A priority patent/CA2691357C/en
Priority to NZ582150A priority patent/NZ582150A/xx
Application filed by N. V. Organon filed Critical N. V. Organon
Priority to SI200831125T priority patent/SI2170959T1/sl
Priority to AU2008266951A priority patent/AU2008266951C1/en
Priority to EP08768485.8A priority patent/EP2170959B1/en
Publication of WO2008156712A1 publication Critical patent/WO2008156712A1/en
Priority to IL202813A priority patent/IL202813A/en
Priority to ZA2010/00135A priority patent/ZA201000135B/en
Priority to US13/719,756 priority patent/US8952136B2/en
Priority to US13/719,763 priority patent/US8900587B2/en
Priority to IL225530A priority patent/IL225530A0/en
Priority to US14/576,448 priority patent/US9834605B2/en
Priority to PH12015501524A priority patent/PH12015501524B1/en
Priority to NO2015028C priority patent/NO2015028I1/no
Priority to CY2015058C priority patent/CY2015058I2/el
Priority to NL300788C priority patent/NL300788I2/nl
Priority to LU92936C priority patent/LU92936I2/xx
Priority to LTPA2016001C priority patent/LTC2170959I2/lt
Priority to US15/810,892 priority patent/US11117961B2/en
Priority to US17/469,359 priority patent/US20210403560A1/en
Priority to NO2022040C priority patent/NO2022040I1/no

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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K16/00Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies
    • C07K16/18Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans
    • C07K16/28Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants
    • C07K16/2803Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants against the immunoglobulin superfamily
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P31/00Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P37/00Drugs for immunological or allergic disorders
    • A61P37/02Immunomodulators
    • A61P37/04Immunostimulants
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K16/00Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies
    • C07K16/18Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans
    • C07K16/28Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants
    • C07K16/2803Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants against the immunoglobulin superfamily
    • C07K16/2818Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants against the immunoglobulin superfamily against CD28 or CD152
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N33/00Investigating or analysing materials by specific methods not covered by groups G01N1/00 - G01N31/00
    • G01N33/48Biological material, e.g. blood, urine; Haemocytometers
    • G01N33/50Chemical analysis of biological material, e.g. blood, urine; Testing involving biospecific ligand binding methods; Immunological testing
    • G01N33/53Immunoassay; Biospecific binding assay; Materials therefor
    • G01N33/574Immunoassay; Biospecific binding assay; Materials therefor for cancer
    • G01N33/57484Immunoassay; Biospecific binding assay; Materials therefor for cancer involving compounds serving as markers for tumor, cancer, neoplasia, e.g. cellular determinants, receptors, heat shock/stress proteins, A-protein, oligosaccharides, metabolites
    • G01N33/57488Immunoassay; Biospecific binding assay; Materials therefor for cancer involving compounds serving as markers for tumor, cancer, neoplasia, e.g. cellular determinants, receptors, heat shock/stress proteins, A-protein, oligosaccharides, metabolites involving compounds identifable in body fluids
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N33/00Investigating or analysing materials by specific methods not covered by groups G01N1/00 - G01N31/00
    • G01N33/48Biological material, e.g. blood, urine; Haemocytometers
    • G01N33/50Chemical analysis of biological material, e.g. blood, urine; Testing involving biospecific ligand binding methods; Immunological testing
    • G01N33/68Chemical analysis of biological material, e.g. blood, urine; Testing involving biospecific ligand binding methods; Immunological testing involving proteins, peptides or amino acids
    • G01N33/6863Cytokines, i.e. immune system proteins modifying a biological response such as cell growth proliferation or differentiation, e.g. TNF, CNF, GM-CSF, lymphotoxin, MIF or their receptors
    • G01N33/6869Interleukin
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K2317/00Immunoglobulins specific features
    • C07K2317/20Immunoglobulins specific features characterized by taxonomic origin
    • C07K2317/24Immunoglobulins specific features characterized by taxonomic origin containing regions, domains or residues from different species, e.g. chimeric, humanized or veneered
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K2317/00Immunoglobulins specific features
    • C07K2317/50Immunoglobulins specific features characterized by immunoglobulin fragments
    • C07K2317/56Immunoglobulins specific features characterized by immunoglobulin fragments variable (Fv) region, i.e. VH and/or VL
    • C07K2317/565Complementarity determining region [CDR]
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K2317/00Immunoglobulins specific features
    • C07K2317/70Immunoglobulins specific features characterized by effect upon binding to a cell or to an antigen
    • C07K2317/76Antagonist effect on antigen, e.g. neutralization or inhibition of binding
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K2317/00Immunoglobulins specific features
    • C07K2317/90Immunoglobulins specific features characterized by (pharmaco)kinetic aspects or by stability of the immunoglobulin
    • C07K2317/92Affinity (KD), association rate (Ka), dissociation rate (Kd) or EC50 value
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N2333/00Assays involving biological materials from specific organisms or of a specific nature
    • G01N2333/435Assays involving biological materials from specific organisms or of a specific nature from animals; from humans
    • G01N2333/52Assays involving cytokines
    • G01N2333/54Interleukins [IL]
    • G01N2333/55IL-2
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N2800/00Detection or diagnosis of diseases
    • G01N2800/52Predicting or monitoring the response to treatment, e.g. for selection of therapy based on assay results in personalised medicine; Prognosis

Definitions

  • PD-I Programmed death receptor 1
  • PD-Ll Programmed death receptor 1
  • PD-I (encoded by the gene Pdcdl) is an Immunoglobulin superfamily member related to CD28, and CTLA -4. PD-I has been shown to negatively regulate antigen receptor signaling upon engagement of its ligands (PD-Ll and/or PD-L2) The structure of murine PD-I has been solved as well as the co-crystal structure of mouse PD-I with human PD- Ll (Zhang, X. et al., Immunity 20: 337-347 (2004); Lin et al., Proc. Natl. Acad. ScL USA 105: 3011-6 (2008)).
  • PD-I and like family members are type I transmembrane glycoproteins containing an Ig Variable-type (V-type) domain responsible for ligand binding and a cytoplasmic tail that is responsible for the binding of signaling molecules.
  • the cytoplasmic tail of PD-I contains two tyrosine-based signaling motifs, an ITEvI (immunoreceptor tyrosine-based inhibition motif) and an ITSM (immunoreceptor tyrosine-based switch motif).
  • PD-I recruits the tyrosine phosphatase SHP-2 to the ITSM motif within its cytoplasmic tail, leading to the dephosphorylation of effector molecules such as CD3 zeta, PKC theta and ZAP70 that are involved in the CD3 T cell signaling cascade.
  • effector molecules such as CD3 zeta, PKC theta and ZAP70 that are involved in the CD3 T cell signaling cascade.
  • the mechanism by which PD-I downmodulates T cell responses is similar to, but distinct from that of CTLA-4, as both molecules regulate an overlapping set of signaling proteins (Parry et al., MoI. Cell Biol. 25: 9543-9553.).
  • PD-I was shown to be expressed on activated lymphocytes (peripheral CD4 + and CD8 + T cells, B cells and monocytes) and has also been shown to be expressed during thymic development on CD4 CD8 " (double negative) T cells as well as NK-T cells.
  • the ligands for PD-I are constitutively expressed or can be induced in a variety of cell types, including non-hematopoietic tissues as well as various tumor types.
  • PD-Ll is expressed on B, T, myeloid and dendritic cells (DCs), but also on peripheral cells, like microvascular endothelial cells and non-lymphoid organs like heart, lung etc.
  • DCs myeloid and dendritic cells
  • PD-L2 is only found on macrophages and DCs.
  • the expression pattern of PD-I ligands is suggestive of a role for PD-I in maintaining peripheral tolerance and may serve to regulate self-reactive T- and B-cell responses in the periphery.
  • Both ligands are type I transmembrane receptors containing both IgV- and IgC-like domains in the extracellular region. Both ligands contain short cytoplasmic regions with no known signaling motifs.
  • PD-I tumor microenvironment can protect tumor cells from efficient immune destruction.
  • PD-Ll has recently been shown to be expressed on a number of mouse and human tumors (and is inducible by IFN gamma on the majority of PD-Ll negative tumor cell lines) and is postulated to mediate immune evasion (Iwai Y. et al., Proc. Natl. Acad. Sci. U.S.A. 99: 12293-12297 (2002); Strome S.E. et al., Cancer Res., 63: 6501-6505 (2003).
  • PD-l(on tumor infiltrating lymphocytes) and/or PD-Ll (on tumor cells) has been found in a number of primary tumor biopsies assessed by immunohistochemistry.
  • Such tissues include cancers of the lung, liver, ovary, cervix, skin, colon, glioma, bladder, breast, kidney, esophagus, stomach, oral squamous cell, urothelial cell, and pancreas as well as tumors of the head and neck (Brown J. A. et al., J. Immunol. 170: 1257-1266 (2003); Dong H. et al., Nat. Med.
  • Blockade of the PD-1/PD-Ll interaction could lead to enhanced tumor-specific T-cell immunity and therefore be helpful in clearance of tumor cells by the immune system.
  • T. Nomi et al. ⁇ Clin. Cancer Res. 13: 2151-2157 (2007) demonstrated the therapeutic efficacy of PD-1/PD-Ll blockade.
  • Administration of either PD-I or PD- Ll directed antibody significantly inhibited tumor growth.
  • Antibody blockade effectively promoted tumor reactive CD8 + T cell infiltration into the tumor resulting in the up- regulation of anti-tumor effectors including IFN gamma, granzyme B and perforin.
  • PD-I knockout mice PD-Ll expressing myeloma cells grew only in wild-type animals (resulting in tumor growth and associated animal death), but not in PD-I deficient mice (Iwai Y. et al., Proc. Natl. Acad. Sci. U.S.A. 99: 12293-12297 (2002)).
  • Anti-PD-1 antibodies may also be useful in chronic viral infection.
  • Memory CD8 + T cells generated after an acute viral infection are highly functional and constitute an important component of protective immunity.
  • chronic infections are often characterized by varying degrees of functional impairment (exhaustion) of virus-specific T-cell responses, and this defect is a principal reason for the inability of the host to eliminate the persisting pathogen.
  • functional effector T cells are initially generated during the early stages of infection, they gradually lose function during the course of a chronic infection. Barber et al.
  • mice infected with a laboratory strain of LCMV developed chronic infection resulting in high levels of virus in the blood and other tissues. These mice initially developed a robust T cell response, but eventually succumbed to the infection upon T cell exhaustion.
  • PD-I is highly expressed on T cells from HIV infected individuals and that receptor expression correlates with impaired T cell function and disease progression (Day et al., Nature 443:350-4 (2006).; Trautmann L. et al., Nat. Med. 12: 1198-202 (2006)).
  • blockade of the ligand PD-Ll significantly increased the expansion of HIV-specific, IFN-gamma producing cells in vitro.
  • PD-I knockout mice exhibit better control of adenovirus infection than wild- type mice (Iwai et al., /. Exp. Med. 198:39-50 (2003)). Also, adoptive transfer of HBV- specific T cells into HBV transgenic animals initiated hepatitis (Isogawa M. et al., Immunity 23:53-63 (2005)). The disease state of these animals oscillates as a consequence of antigen recognition in the liver and PD-I upregulation by liver cells.
  • the invention provides isolated antibodies and antibody fragments that bind to human and cyno PD-I.
  • the antibody or antibody fragment blocks binding of human PD-Ll and human PD-L2 to human PD-I.
  • the PD-I antibody or antibody fragment of the invention includes one or more CDRs (antibody Complementarity-- Determining Regions) selected from SEQ ID NOs: 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19 and 20; and in further embodiments, includes one or more heavy chain CDRs of SEQ ID NOs: 12, 13, 14, 18, 19 and 20 and/or the light chain CDRs of SEQ ID NOs: 9, 10, 11, 15, 16 and 17
  • the antibody or antibody fragment is a chime ⁇ c antibody, human antibody, humanized antibody or a fragment thereof
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comp ⁇ sing a light chain comprising CDRs SEQ ID NOs 9, 10 and 11, or va ⁇ ants of any said sequences, and/or a heavy chain comp ⁇ sing CDRs SEQ ED NOs. 12, 13 and 14, or va ⁇ ants of any said sequences.
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comp ⁇ sing a light chain comp ⁇ sing CDRs SEQ ID NOs 15, 16 and 17 or va ⁇ ants of any said sequences; and/or a heavy chain comp ⁇ sing CDRs SEQ ID NOs: 18, 19 and 20, or va ⁇ ants of any said sequences.
  • the invention comp ⁇ ses an anibody or antigen binding fragment comp ⁇ sing a heavy chain va ⁇ able region SEQ ID NO: 5 or a va ⁇ ant thereof; and/or a light chain va ⁇ able region comp ⁇ sing SEQ ID NO: 6 or a va ⁇ ant thereof.
  • the invention comp ⁇ ses an anibody or antigen binding fragment comp ⁇ sing a heavy chain va ⁇ able region SEQ ID NO: 7 or a va ⁇ ant thereof and/or a light chain va ⁇ able region comp ⁇ sing SEQ ID NO: 8 or a va ⁇ ant thereof
  • the invention comp ⁇ ses an anibody or antigen binding fragment comp ⁇ sing a heavy chain va ⁇ able region comp ⁇ sing amino acid residues 20 to 139 of SEQ ID NO: 30 or a variant thereof; and/or a light chain variable region comprising comprising amino acid residues 20 to 130 of SEQ ID NO: 32 or a variant thereof.
  • the invention comprises an anibody or antigen binding fragment comprising a heavy chain variable region comprising amino acid residues 20 to 139 of SEQ ID NO: 30 or a variant thereof; and/or a light chain variable region comprising comprising amino acid residues 20 to 130 of SEQ ID NO: 33 or a variant thereof.
  • the invention comprises an anibody or antigen binding fragment comprising a heavy chain variable region comprising amino acid residues 20 to 139 of SEQ ID NO: 30 or a variant thereof; and/or a light chain variable region comprising comprising amino acid residues 20 to 130 of SEQ ID NO: 34 or a variant thereof.
  • the invention comprises an anibody or antigen binding fragment comprising a heavy chain variable region comprising an amino acid sequence having at least 90% homology to amino acid residues 20 to 139 of SEQ ID NO: 30; and/or a light chain variable region comprising and an amino acid sequence having at least 90% homology to amino acid residues 20 to 130 of SEQ ID NO: 32, 33 or 34.
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comprising: a heavy chain comprising amino acid residues 20 to 466 of SEQ ID NO: 31 or a variant thereof, and/or a light chain comprising amino acid residues 20 to 237 of SEQ ID NO: 36 or a variant thereof.
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comprising: a heavy chain comprising the amino acid residues 20 to 466 of SEQ ID NO: 31 or a variant thereof, and/or a light chain comprising the amino acid residues 20 to 237 of SEQ ID NO: 37 or a variant thereof.
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comprising: a heavy chain comprising amino acid residues 20 to 466 of SEQ ID NO: 31 or a variant thereof, and/or a light chain comprising amino acid residues 20 to 237 of SEQ ID NO: 38 or a variant thereof.
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comprising: a heavy chain comprising amino acid residues 20 to 469 of SEQ ID NO: 35 or a variant thereof, and/or a light chain comprising amino acid residues 20 to 237 of SEQ ED NO: 36 or a variant thereof.
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comprising: a heavy chain comprising amino acid residues 20 to 469 of SEQ ED NO: 35 or a variant thereof, and/or a light chain comprising amino acid residues 20 to 237 of SEQ ED NO: 37 or a variant thereof.
  • the invention provides an isolated antibody or antibody fragment which binds to human PD-I comprising: a heavy chain comprising amino acid residues 20 to 469 of SEQ ED NO: 35 or a variant thereof, and/or a light chain comprising amino acid residues 20 to 237 of SEQ ED NO: 38 or a variant thereof.
  • the variant of the antibody or antibody fragment fragment of the invention may comprise one, two or three conservatively modified amino acid substitutions.
  • the antibody or antibody fragment of the invention may comprise a human heavy chain constant region or a variant thereof, wherein the variant comprises up to 20 conservatively modified amino acid substitutions; and/or a human light chain constant region or a variant thereof, wherein the variant comprises up to 20 conservatively modified amino acid substitutions.
  • the variant may comprise up to 10 conservatively modified amino acid substitutions.
  • the variant may comprise up to 5 conservatively modified amino acid substitutions.
  • the variant may comprise up to 3 conservatively modified amino acid substitutions.
  • the human heavy chain constant region or variant thereof may be of the IgGl or IgG4 isotype.
  • the antibody or antibody fragment of the invention may bind human PD-I with a K D of about 100 pM or lower. In another embodiment, the antibody or antibody fragment may bind human PD-I with a K D of about 30 pM or lower. In another embodiment, the antibody or antibody fragment may bind human PD-I with about the same KD as an antibody having a heavy chain comprising the amino acid sequence of SEQ ID NO: 31 and a light chain comprising the amino acid sequence of SEQ ED NO: 32.
  • the antibody or antibody fragment may bind human PD-I with about the same K D as an antibody having a heavy chain comp ⁇ sing the amino acid sequence of SEQ ID NO: 31 and a light chain comprising the amino acid sequence of SEQ ID NO: 33.
  • the antibody or antibody fragment of the invention may bind human PD-I with a k assoc of about 7.5 x 10 5 I/M s or faster. In one embodiment, the antibody or antibody fragment may bind human PD-I with a k asSoc of about 1 x 10 6 I/M s or faster.
  • the antibody or antibody fragment may bind human PD-I with a kd, SSo c of about 2 x 10 "5 1/s or slower. In one embodiment, the antibody or antibody fragment may bind human PD-I with a k d i ssoc of about 2.7 x 10 ⁇ 5 1/s or slower. In one embodiment, the antibody or antibody fragment may bind human PD-I with a kdissoc of about 3 x 10 "5 1/s or slower.
  • K D , kassoc and kd, SS oc values can be measured using using any available method.
  • the disaaociation constant is measured using bio-light interferometry (for example, the ForteBio Octet method desc ⁇ bed in Example 2).
  • the disassociation constant can be measured using surface plasmon resonance (e.g. Biacore) or Kinexa.
  • the antibody or antibody fragment of the invention may block binding of human PD-Ll or human PD-L2 to human PD-I with an IC 50 of about 1 nM or lower.
  • the blockade of hgand binding can be measured and the IC 50 calculated using any method known in the art, for example, the FACS or FMAT methods desc ⁇ bed in the Examples hereub.
  • the invention also comp ⁇ ses an antibody or antibody fragment which competes for a binding epitope on human PD-I with any of the antibodies desc ⁇ bed above, and which blocks the binding of human PD-Ll or human PD-L2 to human PD-I with an IC 50 of about 1 nM or lower.
  • the invention also comprises an antibody or antibody fragment which competes for a binding epitope on human PD-I with any of the antibodies described above, and which binds human PD-I with a K D of about 100 pM or lower. In one embodiment, the antibody or antibody fragment binds human PD-I with a K D of about 30 pM or lower.
  • the invention also comprises an antibody or antibody fragment which competes for a binding epitope on human PD-I with any of the antibodies described above, and which binds human PD-I with about the same K D as an antibody having a heavy chain comprising the amino acid sequence of SEQ ID NO: 31 and a light chain comprising the amino acid sequence of SEQ ID NO: 32.
  • the invention also comprises an antibody or antibody fragment that competes for a binding epitope on human PD-I with any of the antibodies described above, and which binds human PD-I with about the same K D as an antibody having a heavy chain comprising the amino acid sequence of SEQ ED NO: 31 and a light chain comprising the amino acid sequence of SEQ ID NO: 33.
  • the invention also comprises an antibody or antibody fragment which competes for a binding epitope on human PD-I with any of the antibodies described above, and which binds human PD-I with a k asSoc of about 7.5 x 10 5 I/M s or faster.
  • the antibody or antibody fragment may bind human PD-I with a k asSoc of about 1 x 10 6 1/ M s or faster.
  • the invention also comprises an antibody or antibody fragment which competes for a binding epitope on human PD-I with any of the antibodies described above, and which binds human PD-I with a k d i SS0C of about 2 x 10 "5 1/s or slower.
  • the antibody or antibody fragment may bind human PD-I with a k d i ssoc of about 2.7 x 10 "5 1/s or slower.
  • the antibody or antibody fragment may bind human PD-I with a k d i ssoc of about 3 x 10 ⁇ 5 1/s or slower.
  • the antibody or antibody fragments of the invention are chimeric antibodies or fragments of chimeric antibodies. In some embodiments, the antibody or antibody fragments of the invention are human antibodies or fragments of human antibodies.
  • the antibody or antibody fragments of the invention are humanized antibodies or fragments of humanized antibodies.
  • the antibody fragments of the invention are Fab, Fab', Fab'-SH, Fv, scFv, or F(ab')2 antibody fragments.
  • the antibody fragments of the invention are diabodies.
  • the invention also comprises bispecific antibodies comprising any one of the antibody or antibody fragments described above that bind to human PD-I.
  • the isolated anti-PD-1 antibodies and antibody fragments of the invention increase T cell activation as measured by typical means known to one skilled in the art (including, without limitation, increased immune cell proliferation, increased cytokine secretion or expression of activation markers such as CD25 and/or CD69).
  • the antibody or antibody fragment of the invention may enhance the immune response after stimulation with Staphylococcus Enterotoxin B or Tetanus Toxoid ex vivo or in vivo.
  • the increased immune activation may be determined using methods known to anyone skilled in the art, for example, quantifying proliferation of immune cells (such as T cells) or cytokine production by immune cells (for example production of EFN ⁇ or IL-2 by T cells).
  • the invention also comprises nucleic acids encoding the anti-PD-1 antibodies and antibody fragments of the invention. Included in the invention are nucleic acids encoding any one of the amino acid sequences disclosed in SEQ ID NOS: 5 to 20 and 30-38 (with or without the leader sequences). Also included withn the invention are nucleic acids comprising SEQ ID NOS: 1 to 4 and 21 to 29 (with or without the nucleic acids encoding the leader sequences). The invention also comprises cells and expression vectors comprising nucleic acids encoding the antibodies or antibody fragments of the invention.
  • the invention comprises a method of producing an antibody or antibody fragment of the invention comprising: (a) culturing the host cell comprising a nucleic acid encoding an antibody or antibody fragment of the invention in culture medium under conditions wherein the nucleic acid sequence is expressed, thereby producing polypeptides comprising the light and heavy chain variable regions; and (b) recovering the polypeptides from the host cell or culture medium.
  • compositions comprising an antibody or antibody fragment of the invention in combination with a pharmaceutically acceptable carrier or diluent.
  • the invention also comprises a method of increasing the activity of an immune cell, comprising administering to a subject in need thereof a therapeutically effective amount of an antibody or antibody fragment of the invention.
  • the method may be used to treat cancer.
  • the method may be use to treat an infection or infectious disease.
  • the method may be used as a vaccine adjuvant.
  • the method comprises further administering a second therapeutic agent or treatment modality.
  • the invention comprises a method of increasing the activity of an immune cell, comprising administering to a subject in need thereof a therapeutically effective amount of an antibody or antibody fragment of the invention, and further comprising measuring T cell activation ex vivo in a sample derived from the subject, wherein an increase in T cell activity indicates that the treatment should be continued.
  • the invention comprises a method of increasing the activity of an immune cell, comprising administering to a subject in need thereof a therapeutically effective amount of an antibody or antibody fragment of the invention, and further comprising measuring T cell activation ex vivo in a sample derived from the subject, wherein an increase in T cell activity predicts the likelihood that the treatment will be successful.
  • the increase in T cell activity is determined by: (i) measuring SEB induced production of one or more cytokines selected from the group consisting of: IL-2, TNF ⁇ , IL-17, IFN ⁇ , GM-CSF, RANTES, IL-6, IL-8, IL-5 and EL-13; or (ii) measuring TT induced production of a cytokine selected from the group consisting of: IL-2, TNF ⁇ , IL-17, EFN ⁇ , GM-CSF, RANTES, IL-6, IL-8, IL-5 and IL-13.
  • the invention also comprises the use of an anti-PD-1 antibody or antibody fragment of the invention for the preparation of a medicament to increase immune response.
  • the invention also comprises the use of an anti-PD-1 antibody or antibody fragment of the invention for the preparation of a medicament to treat cancer.
  • the invention also comprises the use of an anti-PD-1 antibody or antibody fragment of the invention as a vaccine adjuvant.
  • the invention also comprises an immunoconjugate comprising an anti-PD-1 antibody or antibody fragment of the invention, linked to a therapeutic agent such as a bacterial toxin or a radiotoxin.
  • a therapeutic agent such as a bacterial toxin or a radiotoxin.
  • cytotoxic agents include taxol, cytochalasin B, mitomycin, etoposide and vincristine or other antimetabolites, alkylating agents, antibiotics and antimitotics.
  • the invention also comprises a method of increasing the activity, or reducing the downmodulation, of an immune cell comprising contacting the immune cell with any one of the antibodies or antibody fragments of the invention.
  • This method could be used to treat cancer or infectious diseases (such as chronic viral infections), or could be used as an adjuvant to a prophylactic or therapeutic vaccine.
  • the invention also comprises a method of increasing an immune response to an antigen, comprising contacting an immune cell with an antigen and an anti-PD-1 antibody or an antibody fragment such that an immune response to the antigen is increased or enhanced.
  • This method could be conducted in vivo (in a subject) or ex vivo.
  • an anti-PD-1 antibody or antibody fragment may be combined with a second therapeutic agent or treatment modality.
  • an anti-PD-1 antibody or antibody fragment may be combined with cancer treatments involving the application of recombinant cytokines or secreted immune factors.
  • Non-limiting examples of combinations include combining anti-PD-1 antibody with recombinant IL-2 or recombinant EFN ⁇ 2 for the treatment of melanoma or renal cell carcinoma.
  • Recombinant IL-2 enhances T cell outgrowth in cancer patients.
  • Recombinant EFN ⁇ 2 inhibits cancer cell growth but also increases expression of the inhibitory ligands for PD-I on cancer cells, antigen-presenting cells and other somatic cells in the treated patients.
  • Anti-PD-1 can be combined with other cytokines that might be considered useful for the treatment of cancer or infectious diseases.
  • anti-PD-1 antibodies or antibody fragments can be combined with a vaccine to prevent or treat cancer or infectious disease.
  • anti-PD-1 could be combined with a protein, peptide or DNA vaccine containing one or more antigens which are relevant to the cancer or infection to be treated, or a vaccine comprising of dendritic cells pulsed with such a) antigen.
  • Another embodiment includes the use of anti-PD-1 with (attenuated) cancer cell or whole virus vaccines.
  • One embodiment involves a combination of anti-PD-1 therapy with a whole cell cancer vaccine that is engineered to secrete GM-CSF.
  • anti-PD-1 antibodies or antibody fragments can be combined with treatment that is considered to be standard of care in cancer or infectious disease. Rationale for such combinations is that concurrent increased immune activation by anti- PD-1 will induce or facilitate initial clinical response to standard of care treatment, induce durable clinical response and long-term immune control of disease.
  • treatment with anti-PD-1 antibodies or antibody fragments may be combined with chemotherapy.
  • Chemotherapy using cytotoxic agents will result in cancer cell death thereby increasing release of tumor antigens.
  • Such increased availability of tumor antigen may result in synergy with anti-PD-1 treatment.
  • a non-limiting example is provided by the use of decarbazine or temozolomide for the treatment of melanoma and gemcitabine for pancreatic cancer.
  • treatment with anti-PD-1 antibodies or antibody fragments may be combined with radiotherapy. Radiotherapy induces cancer cell death and increasing availability of tumor antigens for presentation and activation of immune cells.
  • treatment with an ti -PD-I antibodies or antibody fragments may be combined with surgery to remove cancer cells from a subject.
  • an ti -PD-I antibodies or antibody fragments may be combined with therapies which may result in synergy with PD-I blockade including targeted agents used for hormone deprivation or inhibition of angiogenesis, or targeting proteins active in tumor cells, all resulting in enhanced tumor cell death and availability of immune stimulating tumor antigens.
  • therapies which may result in synergy with PD-I blockade including targeted agents used for hormone deprivation or inhibition of angiogenesis, or targeting proteins active in tumor cells, all resulting in enhanced tumor cell death and availability of immune stimulating tumor antigens.
  • increased T cell activation may result in durable immune control of cancer.
  • an anti-PD-1 antibody or antibody fragment may be comined with another therapeutic antibody useful for the treatment of cancer or infectious disease.
  • a non-limiting example is provided by the combination of anti-PD-1 with an antibody targeting Her2/neu or targeting the EGF receptor.
  • an anti-PD-1 antibody or antibody fragment is combined with treatment targeting VEGF or its receptors.
  • an anti-PD-1 antibody or antibody fragment is combined with anti-CTLA-4.
  • anti-PD-1 is combined with an antibody that targets RSV.
  • Figure IA and IB show the results of experiments demonstrating that antibodies immobilized from hybridoma supernatants are able to reduce IL-2 secretion by Jurkat E6.2.11 cells stimulated with immobilized anti-CD3 and soluble anti-CD28.
  • Figure 2 shows the results of experiments demonstrating that antibodies against human PD-I bind to PD-I.
  • Figure 2A is a graph showing dose dependent binding of anti-PD-1 antibodies to purified PD-l/Fc in a protein ELISA.
  • Figure 2B is a graph showing dose dependent binding of anti PD-I antibodies to PD-I expressed on the surface of CHO cells transfected with hPD-1 in a CELISA.
  • Figure 3 shows results of FMAT experiments demonstrating that the antibodies against PD-I compete for binding of PD-Ll and PD-L2 to CHO cells transfected with human PD- 1.
  • Figure 3A is a graph showing dose dependent inhibition of binding of PD-Ll by hPD- 1.08 A and hPD-1.09A and to a lesser extent by Jl 16.
  • Figure 3B is a graph showing dose dependent inhibition of PD-L2.
  • Figure 4 is a bar graph which shows results of experiments demonstrating that SEB- stimulated EL-2 production by healthy donor blood cells is enhanced in the presence of anti-PD-1, anti PD-Ll or anti-CTLA-4 antibodies. Bars show the average fold increase in EL-2 across donors ( ⁇ SEM). Numbers inside each bar indicate the number of donors represented.
  • Mouse (m)IgGl is the isotype control for anti-PD-1.08A (08A), anti-PD- 1.09A (09A) and anti-PD-Ll.
  • Mouse (m) IgG2a is the isotype control for anti-CTLA-4.
  • Figure 5 shows results of experiments demonstrating that anti-PD-1 antibodies promote T cell proliferation and cytokine secretion (IL-2 and IFN ⁇ ) when stimulated with the recall antigen tetanus toxoid.
  • Figure 5 shows concentration dependent IFN ⁇ secretion.
  • Figure 6 is a graph depicting the k asSoc and k d i ssoc rates for anti-PD-1 antibodies as measured by bio-light interferometry. Diagonal lines indicate theoretical calculated K D values. The antibodies are listed at the right by K D in ascending order.
  • Figure 7 is a bar graph which shows results of experiments demonstrating that SEB- stimulated IL-2 production by healthy donor blood cells is increased in the presence of 25 ug/ml murine (09A) or humanized anti-PD-1 antibodies (M09A11, h409A16 and h409A17). Bars show the average fold increase in.IL-2 across three donors (+ SEM).
  • Mouse (m) IgGl is the isotype control for anti-PD-1.09 A (09A).
  • Human (h) IgG4 is the isotype control for h409Al l, h409A16 and h409A17 antibodies.
  • hPD-1.08A Murine monoclonal anti-hPD-1 antibody
  • hPD-1.09A Murine monoclonal anti-hPD-1 antibody
  • CDR Complementarity determining region in the immunoglobulin variable regions defined using the Kabat numbering system EC50 concentration resulting in 50% efficacy or binding
  • FW Antibody framework region the immunoglobulin variable regions excluding the CDR regions HRP Horseradish peroxidase
  • V region The segment of IgG chains which is variable in sequence between different antibodies. It extends to Kabat residue 109 in the light chain and 113 in the heavy chain.
  • Antibody refers to any form of antibody that exhibits the desired biological activity, such as inhibiting binding of a ligand to its receptor, or by inhibiting ligand-induced signaling of a receptor.
  • antibody is used in the broadest sense and specifically covers, but is not limited to, monoclonal antibodies (including full length monoclonal antibodies), polyclonal antibodies, and multispecific antibodies (e.g., bispecific antibodies).
  • Antibody fragment and “antibody binding fragment” mean antigen-binding fragments and analogues of an antibody, typically including at least a portion of the antigen binding or variable regions (e.g. one or more CDRs) of the parental antibody. An antibody fragment retains at least some of the binding specificity of the parental antibody.
  • an antibody fragment retains at least 10% of the parental binding activity when that activity is expressed on a molar basis. Preferably, an antibody fragment retains at least 20%, 50%, 70%, 80%, 90%, 95% or 100% or more of the parental antibody's binding affinity for the target.
  • antibody fragments include, but are not limited to, Fab, Fab', F(ab') 2 , and Fv fragments; diabodies; linear antibodies; single-chain antibody molecules, e.g., sc-Fv, unibodies (technology from Genmab); nanobodies (technology from Domantis); domain antibodies (technology from Ablynx); and multispecific antibodies formed from antibody fragments. Engineered antibody variants are reviewed in Holliger and Hudson (2005) Nat. Biotechnol. 23:1126-1136.
  • a "Fab fragment” is comprised of one light chain and the C H I and variable regions of one heavy chain.
  • the heavy chain of a Fab molecule cannot form a disulfide bond with another heavy chain molecule.
  • An "Fc" region contains two heavy chain fragments comprising the C H I and C H 2 domains of an antibody.
  • the two heavy chain fragments are held together by two or more disulfide bonds and by hydrophobic interactions of the CH3 domains.
  • a "Fab' fragment” contains one light chain and a portion of one heavy chain that contains the V H domain and the C H I domain and also the region between the C H 1 and C H 2 domains, such that an interchain disulfide bond can be formed between the two heavy chains of two Fab' fragments to form a F(ab') 2 molecule.
  • a “F(ab') 2 fragment” contains two light chains and two heavy chains containing a portion of the constant region between the C H I and C H 2 domains, such that an interchain disulfide bond is formed between the two heavy chains.
  • a F(ab') 2 fragment thus is composed of two Fab 1 fragments that are held together by a disulfide bond between the two heavy chains.
  • the "Fv region” comprises the variable regions from both the heavy and light chains, but lacks the constant regions.
  • a “single-chain Fv antibody” refers to antibody fragments comprising the V H and V L domains of an antibody, wherein these domains are present in a single polypeptide chain.
  • the Fv polypeptide further comprises a polypeptide linker between the V H and V L domains which enables the scFv to form the desired structure for antigen binding.
  • scFv see Pluckthun (1994) THE PHARMACOLOGY OF MONOCLONAL ANTIBODIES, vol. 113, Rosenburg and Moore eds. Springer- Verlag, New York, pp. 269-315. See also, International Patent Application Publication No. WO 88/01649 and U.S. Pat. Nos. 4,946, 778 and 5,260,203.
  • a “diabody” is a small antibody fragment with two antigen-binding sites.
  • the fragments comprises a heavy chain variable domain (V H ) connected to a light chain variable domain (V L ) in the same polypeptide chain (V H -V L or V L -V H ).
  • V H heavy chain variable domain
  • V L light chain variable domain
  • the domains are forced to pair with the complementary domains of another chain and create two antigen-binding sites.
  • Diabodies are described more fully in, e.g., EP 404,097; WO 93/11161; and Holliger et al. (1993) Proc. Natl. Acad. Sci. USA 90: 6444-6448.
  • a “domain antibody fragment” is an immunologically functional immunoglobulin fragment containing only the variable region of a heavy chain or the variable region of a light chain.
  • two or more V H regions are covalently joined with a peptide linker to create a bivalent domain antibody fragment.
  • the two V H regions of a bivalent domain antibody fragment may target the same or different antigens.
  • An antibody fragment of the invention may comprise a sufficient portion of the constant region to permit dimerization (or multimerization) of heavy chains that have reduced disulfide linkage capability, for example where at least one of the hinge cysteines normally involved in inter-heavy chain disulfide linkage is altered as described herein.
  • an antibody fragment for example one that comprises the Fc region, retains at least one of the biological functions normally associated with the Fc region when present in an intact antibody, such as FcRn binding, antibody half life modulation, ADCC function, and/or complement binding (for example, where the antibody has a glycosylation profile necessary for ADCC function or complement binding).
  • chimeric antibody refers to antibodies in which a portion of the heavy and/or light chain is identical with or homologous to corresponding sequences in antibodies derived from a particular species or belonging to a particular antibody class or subclass, while the remainder of the chain(s) is identical with or homologous to corresponding sequences in antibodies derived from another species or belonging to another antibody class or subclass, as well as fragments of such antibodies, so long as they exhibit the desired biological activity (See, for example, U.S. Pat. No. 4,816,567 and Morrison et al., 1984, Proc. Natl. Acad. Sci. USA 81:6851-6855).
  • Humanized forms of non-human (for example, murine) antibodies are chimeric antibodies that contain minimal sequence derived from non-human immunoglobulin.
  • humanized antibodies are human immunoglobulins (recipient antibody) in which residues from a hypervariable region of the recipient are replaced by residues from a hypervariable region of a non-human species (donor antibody) such as mouse, rat, rabbit or nonhuman primate having the desired specificity, affinity, and capacity.
  • donor antibody such as mouse, rat, rabbit or nonhuman primate having the desired specificity, affinity, and capacity.
  • Fv framework region (FR) residues of the human immunoglobulin are replaced by corresponding non-human residues.
  • humanized antibodies may comprise residues that are not found in the recipient antibody or in the donor antibody. These modifications are made to further refine antibody performance.
  • the humanized antibody will comprise substantially all of at least one, and typically two, variable domains, in which all or substantially all of the hypervariable loops correspond to those of a non-human immunoglobulin and all or substantially all of the FR regions are those of a human immunoglobulin sequence.
  • the humanized antibody optionally also will comprise at least a portion of an immunoglobulin constant region (Fc), typically that of a human immunoglobulin.
  • Fc immunoglobulin constant region
  • hypervariable region refers to the amino acid residues of an antibody which are responsible for antigen-binding.
  • the hypervariable region comprises amino acid residues from a "complementarity determining region” or "CDR,” defined by sequence alignment, for example residues 24-34 (Ll), 50-56 (L2) and 89-97 (L3) in the light chain variable domain and 31-35 (Hl), 50-65 (H2) and 95-102 (H3) in the heavy chain variable domain; see Kabat et al., 1991, Sequences of proteins of Immunological Interest, 5th Ed. Public Health Service, National Institutes of Health, Bethesda, Md.
  • HVL hypervariable loop
  • residues 26-32 (Ll), 50-52 (L2) and 91-96 (L3) in the light chain variable domain and 26- 32 (Hl), 53-55 (H2) and 96-101 (H3) in the heavy chain variable domain see Chothia and Leskl, 1987, J. MoI. Biol. 196:901-917.
  • "Framework" or "FR" residues are those variable domain residues other than the hypervariable region residues as herein defined.
  • a "human antibody” is an antibody that possesses an amino acid sequence corresponding to that of an antibody produced by a human and/or has been made using any of the techniques for making human antibodies disclosed herein. This definition specifically excludes a humanized antibody that comprises non-human antigen-binding residues.
  • an “isolated” antibody is one that has been identified and separated and/or recovered from a component of its natural environment. Contaminant components of its natural environment are materials that would interfere with diagnostic or therapeutic uses for the antibody, and may include enzymes, hormones, and other proteinaceous or nonproteinaceous solutes.
  • the antibody will be purified (1) to greater than 95% by weight of antibody as determined by the Lowry method, and most preferably more than 99% by weight, (2) to a degree sufficient to obtain at least 15 residues of N-terminal or internal amino acid sequence by use of a spinning cup sequenator, or (3) to homogeneity by SDS-PAGE under reducing or nonreducing conditions using Coomassie blue or, preferably, silver stain.
  • Isolated antibody includes the antibody in situ within recombinant cells since at least one component of the antibody's natural environment will not be present. Ordinarily, however, isolated antibody will be prepared by at least one purification step.
  • an "isolated" nucleic acid molecule is a nucleic acid molecule that is identified and separated from at least one contaminant nucleic acid molecule with which it is ordinarily associated in the natural source of the antibody nucleic acid.
  • An isolated nucleic acid molecule is other than in the form or setting in which it is found in nature. Isolated nucleic acid molecules therefore are distinguished from the nucleic acid molecule as it exists in natural cells.
  • an isolated nucleic acid molecule includes a nucleic acid molecule contained in cells that ordinarily express the antibody where, for example, the nucleic acid molecule is in a chromosomal location different from that of natural cells.
  • the term "monoclonal antibody” as used herein refers to an antibody obtained from a population of substantially homogeneous antibodies, i.e., the individual antibodies comprising the population are identical except for possible naturally occurring mutations that may be present in minor amounts. Monoclonal antibodies are highly specific, being directed against a single antigenic site. Furthermore, in contrast to conventional (polyclonal) antibody preparations that typically include different antibodies directed against different determinants (epitopes), each monoclonal antibody is directed against a single determinant on the antigen.
  • the modifier "monoclonal” indicates the character of the antibody as being obtained from a substantially homogeneous population of antibodies, and is not to be construed as requiring production of the antibody by any particular method.
  • the monoclonal antibodies to be used in accordance with the present invention may be made by the hybridoma method first described by Kohler et al., 1975, Nature 256:495, or may be made by recombinant DNA methods (see, for example, U.S. Pat. No. 4,816,567).
  • the "monoclonal antibodies” may also be isolated from phage antibody libraries using the techniques described in Clackson et al., 1991, Nature 352:624-628 and Marks et al., 1991, J. MoI. Biol. 222:581-597, for example.
  • the monoclonal antibodies herein specifically include "chimeric" antibodies.
  • Immune cell includes cells that are of hematopoietic origin and that play a role in the immune response.
  • Immune cells include lymphocytes, such as B cells and T cells; natural killer cells; myeloid cells, such as monocytes, macrophages, eosinophils, mast cells, basophils, and granulocytes.
  • an “immunoconjugate” refers to an anti-PD-1 antibody, or a fragment thereof, conjugated to a therapeutic moiety, such as a bacterial toxin, a cytotoxic drug or a radiotoxin.
  • a therapeutic moiety such as a bacterial toxin, a cytotoxic drug or a radiotoxin.
  • Toxic moieties can be conjugated to antibodies of the invention using methods available in the art.
  • a sequence "variant" refers to a sequence that differs from the disclosed sequence at one or more amino acid residues but which retains the biological activity of the resulting molecule.
  • Constantly modified variants or “conservative amino acid substitution” refers to substitutions of amino acids are known to those of skill in this art and may be made generally without altering the biological activity of the resulting molecule. Those of skill in this art recognize that, in general, single amino acid substitutions in non-essential regions of a polypeptide do not substantially alter biological activity ⁇ see, e.g., Watson, et al., Molecular Biology of the Gene, The Benjamin/Cummings Pub. Co., p. 224 (4th Edition 1987)). Such exemplary substitutions are preferably made in accordance with those set forth below as follows:
  • the comparison of sequences and determination of percent identity between two sequences can be accomplished using a mathematical algorithm. For example, the percent identity between two amino acid sequences can be determined using the algorithm of E. Meyers and W. Miller (Comput. Appl.
  • the percent identity between two amino acid sequences can be determined using the Needleman and Wunsch (J. MoI. Biol. 48:444-453 (1970)) algorithm which has been incorporated into the GAP program in the GCG software package (available at www.gcg.com), using either a Blossum 62 matrix or a PAM250 matrix, and a gap weight of 16, 14, 12, 10, 8, 6, or 4 and a length weight of 1, 2, 3, 4, 5, or 6.
  • the term “about” refers to a value that is within an acceptable error range for the particular value as determined by one of ordinary skill in the art, which will depend ' in part on how the value is measured or determined, i.e., the limitations of the measurement system. For example, “about” can mean within 1 or more than 1 standard deviation per the practice in the art. Alternatively, “about” or “comprising essentially of can mean a range of up to 20%. Furthermore, particularly with respect to biological systems or processes, the terms can mean up to an order of magnitude or up to 5-fold of a value. When particular values are provided in the application and claims, unless otherwise stated, the meaning of "about” or “comprising essentially of should be assumed to be within an acceptable error range for that particular value.
  • Specifically binds, when referring to a ligand/receptor, antibody/antigen, or other binding pair, indicates a binding reaction which is determinative of the presence of the protein, e.g., PD-I, in a heterogeneous population of proteins and/or other biologies.
  • a specified ligand/antigen binds to a particular receptor/antibody and does not bind in a significant amount to other proteins present in the sample.
  • administering refers to contact of an exogenous pharmaceutical, therapeutic, diagnostic agent, or composition to the animal, human, subject, cell, tissue, organ, or biological fluid.
  • administering can refer, e.g., to therapeutic, pharmacokinetic, diagnostic, research, and experimental methods.
  • Treatment of a cell encompasses contact of a reagent to the cell, as well as contact of a reagent to a fluid, where the fluid is in contact with the cell.
  • administering and “treatment” also means in vitro and ex vivo treatments, e.g., of a cell, by a reagent, diagnostic, binding composition, or by another cell.
  • Effective amount encompasses an amount sufficient to ameliorate or prevent a symptom or sign of the medical condition. Effective amount also means an amount sufficient to allow or facilitate diagnosis. An effective amount for a particular subject may vary depending on factors such as the condition being treated, the overall health of the patient, the method route and dose of administration and the severity of side affects. An effective amount can be the maximal dose or dosing protocol that avoids significant side effects or toxic effects.
  • the effect will result in an improvement of a diagnostic measure or parameter by at least 5%, usually by at least 10%, more usually at least 20%, most usually at least 30%, preferably at least 40%, more preferably at least 50%, most preferably at least 60%, ideally at least 70%, more ideally at least 80%, and most ideally at least 90%, where 100% is defined as the diagnostic parameter shown by a normal subject (see, e.g., Maynard, et al. (1996) A Handbook of SOPs for Good Clinical Practice, Interpharm Press, Boca Raton, FL; Dent (2001) Good Laboratory and Good Clinical Practice, Urch Publ., London, UK).
  • Monoclonal antibodies to PD-I can be made according to knowledge and skill in the art of injecting test subjects with PD-I antigen and then isolating hybridomas expressing antibodies having the desired sequence or functional characteristics.
  • DNA encoding the monoclonal antibodies is readily isolated and sequenced using conventional procedures (e.g., by using oligonucleotide probes that are capable of binding specifically to genes encoding the heavy and light chains of the monoclonal antibodies).
  • the hybridoma cells serve as a preferred source of such DNA.
  • the DNA may be placed into expression vectors, which are then transfected into host cells such as E. coli cells, simian COS cells, Chinese hamster ovary (CHO) cells, or myeloma cells that do not otherwise produce immunoglobulin protein, to obtain the synthesis of monoclonal antibodies in the recombinant host cells. Recombinant production of antibodies will be described in more detail below.
  • antibodies or antibody fragments can be isolated from antibody phage libraries generated using the techniques described in McCafferty et al., 1990, Nature, 348:552-554. Clackson et al., 1991, Nature, 352:624-628, and Marks et al., 1991, J. MoI. Biol. 222:581-597 describe the isolation of murine and human antibodies, respectively, using phage libraries.
  • the antibody DNA also may be modified, for example, by substituting the coding sequence for human heavy- and light-chain constant domains in place of the homologous murine sequences (U.S. Pat. No. 4,816,567; Morrison, et al., 1984, Proc. Natl Acad. ScL USA, 81:6851), or by covalently joining to the immunoglobulin coding sequence all or part of the coding sequence for non-immunoglobulin material (e.g., protein domains).
  • non-immunoglobulin material is substituted for the constant domains of an antibody, or is substituted for the variable domains of one antigen-combining site of an antibody to create a chimeric bivalent antibody comprising one antigen-combining site having specificity for an antigen and another antigen-combining site having specificity for a different antigen.
  • a humanized antibody has one or more amino acid residues from a source that is non- human.
  • the non-human amino acid residues are often referred to as "import” residues, and are typically taken from an "import” variable domain.
  • Humanization can be performed generally following the method of Winter and co-workers (Jones et al., 1986, Nature 321:522-525; Riechmann et al., 1988, Nature, 332:323-327; Verhoeyen et al., 1988, Science 239:1534-1536), by substituting rodent CDRs or CDR sequences for the corresponding sequences of a human antibody. Accordingly, such "humanized” antibodies are chimeric antibodies (U.S. Pat. No.
  • humanized antibodies are typically human antibodies in which some CDR residues and possibly some FR residues are substituted by residues from analogous sites in non-human, for example, rodent antibodies.
  • variable domains both light and heavy
  • the choice of human variable domains, both light and heavy, to be used in making the humanized antibodies is very important to reduce antigenicity.
  • the sequence of the variable domain of a rodent antibody is screened against the entire library of known human variable-domain sequences.
  • the human sequence which is closest to that of the rodent is then accepted as the human framework (FR) for the humanized antibody (Sims et al., 1987, J. Immunol. 151:2296; Chothia et al., 1987, J. MoI. Biol. 196:901).
  • Another method uses a particular framework derived from the consensus sequence of all human antibodies of a particular subgroup of light or heavy chains.
  • the same framework may be used for several different humanized antibodies (Carter et al., 1992, Proc. Natl. Acad. Sci. USA 89:4285; Presta et al., 1993, /. Immnol. 151:2623).
  • humanized antibodies are prepared by a process of analysis of the parental sequences and various conceptual humanized products using three-dimensional models of the parental and humanized sequences.
  • Three-dimensional immunoglobulin models are commonly available and are familiar to those skilled in the art.
  • Computer programs are available which illustrate and display probable three-dimensional conformational structures of selected candidate immunoglobulin sequences. Inspection of these displays permits analysis of the likely role of the residues in the functioning of the candidate immunoglobulin sequence, i.e., the analysis of residues that influence the ability of the candidate immunoglobulin to bind its antigen.
  • FR residues can be selected and combined from the recipient and import sequences so that the desired antibody characteristic, such as increased affinity for the target antigen(s), is achieved.
  • the CDR residues are directly and most substantially involved in influencing antigen binding.
  • transgenic animals e.g., mice
  • transgenic animals e.g., mice
  • JH antibody heavy-chain joining region
  • Human antibodies can also be derived from phage- display libraries (Hoogenboom et al., 1991, J. MoI. Biol. 227:381; Marks et al., J. MoI. Biol. 1991, 222:581-597; Vaughan et al., 1996, Nature Biotech 14:309).
  • the antibody can be produced intracellularly, in the periplasmic space, or directly secreted into the medium. If the antibody is produced intracellularly, as a first step, the particulate debris, either host cells or lysed fragments, is removed, for example, by centrifugation or ultrafiltration. Carter et al., 1992, Bio/Technology 10:163-167 describe a procedure for isolating antibodies which are secreted to the periplasmic space of E. coli. Briefly, cell paste is thawed in the presence of sodium acetate (pH 3.5), EDTA, and phenylmethylsulfonylfluoride (PMSF) over about 30 min.
  • sodium acetate pH 3.5
  • EDTA EDTA
  • PMSF phenylmethylsulfonylfluoride
  • supematants from such expression systems are generally first concentrated using a commercially available protein concentration filter, for example, an Amicon or Millipore Pellicon ultrafiltration unit.
  • a protease inhibitor such as PMSF may be included in any of the foregoing steps to inhibit proteolysis and antibiotics may be included to prevent the growth of adventitious contaminants.
  • the antibody composition prepared from the cells can be purified using, for example, hydroxylapatite chromatography, gel electrophoresis, dialysis, and affinity chromatography, with affinity chromatography being the preferred purification technique.
  • affinity chromatography is the preferred purification technique.
  • the suitability of protein A as an affinity ligand depends on the species and isotype of any immunoglobulin Fc region that is present in the antibody. Protein A can be used to purify antibodies that are based on human .gamma.1, .gamma.2, or .gamma.4 heavy chains (Lindmark et al., 1983, J. Immunol. Meth. 62: 1-13).
  • Protein G is recommended for all mouse isotypes and for human .gamma.3 (Guss et al., 1986, EMBO 75:15671575).
  • the matrix to which the affinity ligand is attached is most often agarose, but other matrices are available. Mechanically stable matrices such as controlled pore glass or poly(styrenedivinyl)benzene allow for faster flow rates and shorter processing times than can be achieved with agarose.
  • the antibody comprises a CH3 domain
  • the Bakerbond ABXTM resin J. T. Baker, Phillipsburg, N.J.
  • the glycoprotein may be purified using adsorption onto a lectin substrate (e.g. a lectin affinity column) to remove fucose-containing glycoprotein from the preparation and thereby enrich for fucose-free glycoprotein.
  • a lectin substrate e.g. a lectin affinity column
  • the invention comprises pharmaceutical formulations of a PD-I antibnody or antibody fragment of the invention.
  • a pharmaceutically acceptable carrier or excipient see, e.g., Remington's Pharmaceutical Sciences and U.S. Pharmacopeia: National Formulary, Mack Publishing Company, Easton, PA (1984).
  • Formulations of therapeutic and diagnostic agents may be prepared by mixing with physiologically acceptable carriers, excipients, or stabilizers in the form of, e.g., lyophilized powders, slurries, aqueous solutions or suspensions (see, e.g., Hardman, et al.
  • Toxicity and therapeutic efficacy of the antibody compositions, administered alone or in combination with an immunosuppressive agent can be determined by standard pharmaceutical procedures in cell cultures or experimental animals, e.g., for determining the LD 5O (the dose lethal to 50% of the population) and the ED 50 (the dose therapeutically effective in 50% of the population).
  • the dose ratio between toxic and therapeutic effects is the therapeutic index and it can be expressed as the ratio between LD 50 and ED 50 .
  • the data obtained from these cell culture assays and animal studies can be used in formulating a range of dosage for use in humans.
  • the dosage of such compounds lies preferably within a range of circulating concentrations that include the ED 50 with little or no toxicity.
  • the dosage may vary within this range depending upon the dosage form employed and the route of administration utilized.
  • Suitable routes of administration include parenteral administration, such as intramuscular, intravenous, or subcutaneous administration and oral administration.
  • Administration of antibody used in the pharmaceutical composition or to practice the method of the present invention can be carried out in a variety of conventional ways, such as oral ingestion, inhalation, topical application or cutaneous, subcutaneous, intraperitoneal, parenteral, intraarterial or intravenous injection.
  • the binding compound of the invention is administered intravenously.
  • the binding compound of the invention is administered subcutaneously.
  • one may administer the antibody in a local rather than systemic manner for example, via injection of the antibody directly into the site of action, often in a depot or sustained release formulation.
  • Determination of the appropriate dose is made by the clinician, e.g., using parameters or factors known or suspected in the art to affect treatment or predicted to affect treatment. Generally, the dose begins with an amount somewhat less than the optimum dose and it is increased by small increments thereafter until the desired or optimum effect is achieved relative to any negative side effects.
  • Important diagnostic measures include those of symptoms of, e.g., the inflammation or level of inflammatory cytokines produced.
  • Antibodies, antibody fragments, and cytokines can be provided by continuous infusion, or by doses at intervals of, e.g., one day, one week, or 1-7 times per week. Doses may be provided intravenously, subcutaneously, intraperitoneally, cutaneously, topically, orally, nasally, rectally, intramuscular, intracerebrally, intraspinally, or by inhalation.
  • a preferred dose protocol is one involving the maximal dose or dose frequency that avoids significant undesirable side effects.
  • a total weekly dose is generally at least 0.05 ⁇ g/kg body weight, more generally at least 0.2 ⁇ g/kg, most generally at least 0.5 ⁇ g/kg, typically at least 1 ⁇ g/kg, more typically at least 10 ⁇ g/kg, most typically at least 100 ⁇ g/kg, preferably at least 0.2 mg/kg, more preferably at least 1.0 mg/kg, most preferably at least 2.0 mg/kg, optimally at least 10 mg/kg, more optimally at least 25 mg/kg, and most optimally at least 50 mg/kg (see, e.g., Yang, et al. (2003) New Engl J. Med. 349:427-434; Herold, et al. (2002) New Engl. J. Med.
  • a small molecule therapeutic e.g., a peptide mimetic, natural product, or organic chemical, is about the same as for an antibody or polypeptide, on a moles/kg basis.
  • inhibit or “treat” or “treatment” includes a postponement of development of the symptoms associated with disease and/or a reduction in the severity of such symptoms that will or are expected to develop with said disease.
  • the terms further include ameliorating existing symptoms, preventing additional symptoms, and ameliorating or preventing the underlying causes of such symptoms.
  • the terms denote that a beneficial result has been conferred on a vertebrate subject with a disease.
  • the term "therapeutically effective amount” or “effective amount” refers to an amount of an anti-PD-1 antibody or fragment thereof, that when administered alone or in combination with an additional therapeutic agent to a cell, tissue, or subject is effective to prevent or ameliorate the disease or condition to be treated.
  • a therapeutically effective dose further refers to that amount of the compound sufficient to result in amelioration of symptoms, e.g., treatment, healing, prevention or amelioration of the relevant medical condition, or an increase in rate of treatment, healing, prevention or amelioration of such conditions.
  • a therapeutically effective dose refers to that ingredient alone.
  • a therapeutically effective dose refers to combined amounts of the active ingredients that result in the therapeutic effect, whether administered in combination, serially or simultaneously.
  • An effective amount of therapeutic will decrease the symptoms typically by at least 10%; usually by at least 20%; preferably at least about 30%; more preferably at least 40%, and most preferably by at least 50%.
  • the pharmaceutical composition of the invention may also contain other agent, including but not limited to a cytotoxic, cytostatic, anti-angiogenic or antimetabolite agent, a tumor targeted agent, an immune stimulating or immune modulating agent or an antibody conjugated to a cytotoxic, cytostatic, or otherwise toxic agent.
  • agent including but not limited to a cytotoxic, cytostatic, anti-angiogenic or antimetabolite agent, a tumor targeted agent, an immune stimulating or immune modulating agent or an antibody conjugated to a cytotoxic, cytostatic, or otherwise toxic agent.
  • the pharmaceutical composition can also be employed with other therapeutic modalities such as surgery, chemotherapy and radiation.
  • Typical veterinary, experimental, or research subjects include monkeys, dogs, cats, rats, mice, rabbits, guinea pigs, horses, and humans.
  • the antibody or antigen binding fragments of the invention which specifically bind to human PD-I, can be used to increase, enhance, stimulate or up-regulate an immune response.
  • the antibodies and antibody fragments of the invention are particularly suitable for treating subjects having a disorder that can be treated by increasing the T-cell mediated immune response.
  • Preferred subjects include human patients in need of enhancement of an immune response.
  • the antibody or antigen binding fragments of the invention can be used to treat cancer (i.e., to inhibit the growth or survival of tumor cells).
  • Preferred cancers whose growth may be inhibited using the antibodies of the invention include cancers typically responsive to immunotherapy, but also cancers that have not hitherto been associated with immunotherapy.
  • Non-limiting examples of preferred cancers for treatment include melanoma (e.g., metastatic malignant melanoma), renal cancer (e.g. clear cell carcinoma), prostate cancer (e.g. hormone refractory prostate adenocarcinoma), pancreatic adenocarcinoma, breast cancer, colon cancer, lung cancer (e.g.
  • non-small cell lung cancer non-small cell lung cancer
  • esophageal cancer squamous cell carcinoma of the head and neck
  • liver cancer ovarian cancer
  • cervical cancer thyroid cancer
  • glioblastoma glioma
  • leukemia lymphoma
  • other neoplastic malignancies include refractory or recurrent malignancies whose growth may be inhibited using the antibodies of the invention.
  • the antibody or antibody fragments of the invention can be used alone or in combination with: other anti-neoplastic agents or immunogenic agents (for example, attenuated cancerous cells, tumor antigens (including recombinant proteins, peptides, and carbohydrate molecules), antigen presenting cells such as dendritic cells pulsed with tumor derived antigen or nucleic acids, immune stimulating cytokines (for example, JL-2, IFNa2, GM-CSF_), and cells transfected with genes encoding immune stimulating cytokines such as but not limited to GM-CSF); standard cancer treatments (for example, chemotherapy, radiotherapy or power); or other antibodies (including but not limited to antibodies to VEGF, EGFR, Her2/neu, VEGF receptors, other growth factor receptors, CD20, CD40, CTLA-4, OX-40, 4- IBB, and ICOS).
  • other anti-neoplastic agents or immunogenic agents for example, attenuated cancerous cells, tumor antigens (including recombinant proteins
  • the antibody or antibody fragments of the invention can also be used to prevent or treat infections and infectious disease.
  • the antibody or antibody fragments can be used alone, or in combination with vaccines, to stimulate the immune response to pathogens, toxins, and self-antigens.
  • the antibodies or antigen-binding fragment thereof can be used to stimulate immune response to viruses infectious to humans, such as, but not limited to, human immunodeficiency viruses, hepatitis viruses class A, B and C, Eppstein Barr virus, hyman cytomegalovirus, human papilloma viruses, herpes viruses.
  • the antibodies or antigen-binding fragment thereof can be used to stimulate immune response to infection with bacterial or fungal parasites, and other pathogens.
  • the antibody or antibody fragments of the invention can be used in conjunction with other recombinant proteins and/or peptides (such as tumor antigens or cancer cells) in order to increase an immune response to these proteins (i.e., in a vaccination protocol).
  • other recombinant proteins and/or peptides such as tumor antigens or cancer cells
  • anti-PD-1 antibodies and antibody fragments thereof may be used to stimulate antigen-specific immune responses by coadministration of an anti-PD-1 antibody with an antigen of interest (e.g., a vaccine).
  • an antigen of interest e.g., a vaccine
  • the invention provides a method of enhancing an immune response to an antigen in a subject, comprising administering to the subject: (i) the antigen; and (ii) an anti-PD-1 antibody of the invention or antigen-binding portion thereof, such that an immune response to the antigen in the subject is enhanced.
  • the antigen can be, for example, a tumor antigen, a viral antigen, a bacterial antigen or an antigen from a pathogen.
  • Non-limiting examples of such antigens include, without limitation, tumor antigens, or antigens from the viruses, bacteria or other pathogens.
  • Anti-PD-1 antibodies and antibody fragments of the invention can also be used to treat Th2 mediated diseases, such as asthma and allergy. This is based on the finding that the antibodies of the invention can help induce a ThI response. Thus, the antibodies of the invention can be used to in Th2 mediated diseases to generate a mofre balanced immune response.
  • the antibodies and antigen fragments of the invention can also be used for the ex vivo activation and expansion of antigen specific T cells and adoptive transfer of these cells into recipients in order to increase antigen-specific T cells against tumor. These methods may also be used to activate T cell responses to infectious agents such as CMV. Ex vivo activation in the presence of anti-PD-1 antibodies may be expected to increase the frequency and activity of the adoptively transferred T cells.
  • anti-PD-1 antibodies of the invention can be coadministered with one or other more therapeutic agents, e.g., a cytotoxic agent, a radiotoxic agent or an immunosuppressive agent.
  • the antibody can be linked to the agent (as an immunocomplex) or can be administered separately from the agent. In the latter case (separate administration), the antibody can be administered before, after or concurrently with the agent or can be co-administered with other known therapies.
  • Antibodies and antigen binding fragments of the invention can also be used to increase the effectiveness of donor engrafted tumor specific T cells.
  • the antibody of the invention may be used as an affinity purification agent.
  • the antibody may also be useful in diagnostic assays, e.g., for detecting expression of PD- 1 in specific cells, tissues, or serum.
  • the antibody typically will be labeled (either directly or indirectly) with a detectable moiety.
  • Numerous labels are available which can be generally grouped into the following categories: biotin, fluorochromes, radionucleotides, enzymes, iodine, and biosynthetic labels.
  • the antibody of the present invention may be employed in any known assay method, such as competitive binding assays, direct and indirect sandwich assays, and immunoprecipitation assays. Zola, Monoclonal Antibodies. A Manual of Techniques, pp.147-158 (CRC Press, Inc. 1987).
  • the antibody may also be used for in vivo diagnostic assays.
  • the antibody is labeled with a radionuclide (such as 111 In, 99 Tc, 4 C, 3 II, 125 1, 3 H, 32 P 35 S or 18 F) so that the antigen or cells expressing it can be localized using immunoscintiography or positron emission tomography.
  • a radionuclide such as 111 In, 99 Tc, 4 C, 3 II, 125 1, 3 H, 32 P 35 S or 18 F
  • DNA constructs encoding the variable regions of the heavy and light chains of the humanized antibodies h409All, h409A16 and h409A17 have been deposited with the American Type Culture Collection Patent Depository (10801 University Boulevard., Manassas, VA).
  • the plasmid containing the DNA encoding the heavy chain of h409A-l 1, h409A-16 and h409A-17 was deposited on June 9, 2008 and identified as 081469_SPD-H.
  • the plasmid containing the DNA encoding the light chain of h409Al 1 was deposited on June 9, 2008 and identified as 0801470_SPD-L-l 1.
  • the plasmid containing the DNA encoding the light chain of h409A16 was deposited on June 9, 2008 and identified as 0801471_SPD-L-16.
  • the plasmid containing the DNA encoding the light chain of h409A17 was deposited on June 9, 2008 and was designated 0801472_SPD-L-17.
  • the deposits were made under the provisions of the Budapest Treaty on the International Recognition of the Deposit of Microorganisms for the Purpose of Patent Procedure and the Regulations thereunder (Budapest Treaty).
  • a cDNA encoding the open reading frame of the hPD-1 receptor was obtained by PCR and subcloned into vector pcDNA3.1 (Invitrogen, Carlsbad, CA).
  • pcDNA3.1 Invitrogen, Carlsbad, CA.
  • CHO-Kl cells were stably transfected with hPD-1, and expression was monitored using flow cytometry.
  • CHO-Kl clones were isolated expressing human PD-I on their membranes and named CHO-hPDl.
  • mice were immunized by gene gun immunization using a Helios gene gun (BioRad) and DNA coated gold bullets (BioRad) following manufacturers instructions. Briefly, 1 ⁇ m gold particles were coated with hPD-1 cDNA (cloned into pcDNA3.1) and, where indicated, commercial expression vectors for mouse Flt3L and mouse GM-CSF in a 2: 1 : 1 ratio (both from Aldevron, Fargo ND). A total of 1 ⁇ g of plasmid DNA was used to coat 500 ⁇ g of gold bullets.
  • mice 7-8 week-old female BALB/C mice were immunized on the ear by gene gun receiving 2, 3, or 4 cycles of a shot on both ears (see Table I).
  • One mouse received a final booster with 5 x 10 6 CHO-hPDl cells in the peritoneal cavity.
  • a 1 :1000 anti-hPD-1 titers was detectable in mouse serum after two DNA immunizations by cell ELISA using CHO-hPD-1 versus CHO-Kl parental cells.
  • mice Four days after the final immunization, mice were sacrificed, and erythrocyte-depleted spleen cell populations were prepared as described previously (Steenbakkers et al., 1992, J. Immunol. Meth. 152:69-77; Steenbakkers et al., 1994, MoI. Biol. Rep. 19:125-134) and frozen at -140°C.
  • mice 730, 731 and 738 were pooled for a B-cell culture.
  • Spleen cells were incubated in DMEM/HAM's F12/10% Calf Serum (Hyclone, Logan, UT, USA) for one hour at 37°C in a plastic culture flask to remove monocytes.
  • Non-adherent cells were submitted to one round of negative panning on CHO-Kl cells, followed by positive panning on CHO-hPDl cells.
  • B-cells were cultured and immortalized as described in Steenbakkers et al., 1994, MoI. Biol. Rep. 19: 125-134. Briefly, selected B cells were mixed with 7.5% (v/v) T-cell supernatant and 50,000 irradiated (2,500 RAD) EL-4 B5 nursing cells in a final volume of 200 ⁇ L DMEM/HAM's F12/10% Bovine Calf Serum, in 96-well flat-bottomed tissue culture plates. On day eight, supernatants were screened for their anti-hPD-1 reactivity by CHO-hPD-1 cell ELISA using the following procedure.
  • CHO-Kl and CHO-hPDl cells were cultured to confluency in flatbottom 96-well plates in 50 ⁇ L DMEM/HAM'S F12, 10% FBS. Next, 50 ⁇ L of immunoglobulin-containing supernatant was added for 1 hr at 37°C. After three washes with PBS-Tween, 100 ⁇ L (1: 1000 diluted) goat-anti -mouse- horseradish peroxidase (HRP, Southern, Birmingham, AL, USA) in DMEM/HAM'S F12/10% FBS was added for 1 hour at 37 0 C. After three washes with PBS-Tween, immobilized immunoglobulins were visualized with UPO/TMB (Biomerieux, Boxtel, Netherlands).
  • UPO/TMB Biomerieux, Boxtel, Netherlands
  • B-cells From this B-cell culture, 13 hPD-1 reactive supernatants were identified and shown to inhibit Jurkat T cell activation when immobilized on plastic, and B-cell clones from positive wells were immortalized by mini-electrofusion following published procedures (Steenbakkers et al., 1992, J. Immunol. Meth. 152:69-77; Steenbakkers et al., 1994, MoI. Biol. Rep. 19:125-134). Specifically, B-cells were mixed with 10 6 NS-I myeloma cells, and serum was removed by washing with DMEM/HAM's F12. Next, cells were treated with pronase solution for three minutes and subsequently washed with fusion medium.
  • Electrofusion was performed in a 50 ⁇ L fusion chamber by an alternating electric field of 30 s, 2 MHz, 400 V/cm followed by a square, high field pulse of 10 ⁇ s, 3 kV/cm and again an alternating electric field of 30 s, 2 MHz, 400 V/cm. Finally, the content of the fusion chamber was transferred to hybridoma selection medium and plated into a 96-well plate under limiting dilution conditions. On day 14 after fusion, the cultures were examined for hybridoma growth and screened for the presence of antibody reactivity to hPD-1.
  • Jurkat E6.1 cells (American Type Culture Collection) were subcloned by limiting dilution using standard methodology and subclones were tested for enhanced capacity to produce IL-2 upon cross-linking of CD3 and CD28.
  • a high IL-2 producing subclone was obtained and subsequently named Jurkat E6.2.11and used in further assays.
  • Costar 3370 96-well assay plates were coated overnight at 4°C with 5 ⁇ g/mL Sheep Anti-Mouse Ig (SAM). Excess of SAM was removed and plates were blocked for 1 hr at room temperature with 200 ⁇ L/well PBS/10% Fetal Bovine Serum.
  • hPD-Ll/Fc recombinant human B7-Hl/Fc chimera, R&D systems
  • mouse IgGl kappa from Sigma
  • Stable hybridoma cells were then cultured under serum-free conditions using CELLine bioreactors (Integra-biosciences) for six to eight days. Cells were seeded in the inner chamber in serum-free media at a density of 3 x 10 6 c/mL in 15 mL and expanded to approximately 4 x 10 7 c/mL over eight days. The outer chamber was filled with media supplemented with up to 10% BCS (bovine calf serum). On day six to eight, the inner chamber culture was harvested, washed with 15 mL SF media and re-innoculated with hybridoma cells.
  • BCS bovine calf serum
  • Bioreactor supernatant and wash were combined and clarified by centrifugation. The resulting supernatant was filtered through a 0.22 ⁇ M filter membrane.
  • Anti- PD-I antibody clone Jl 16 (#14-9989) was purchased from eBioscience.
  • Anti-CTLA-4 clone 14D3 (mAb 16-1529) was purchased from eBioscience.
  • Anti-PD-1 clone 192106 (mAblO86) was purchased from R&D systems (#mAblO86).
  • Isotype control antibody mlgGl, kappa, clone MOPC21 was purchased from Sigma (#M9269).
  • Isotype controls mlgGl kappa (mAb 16-4714) and IgG2a kappa (mAb 16-4724) were purchased from eBioscience.
  • a protein ELISA was used for determination of the relative binding of antibodies to human PD-l/Fc.
  • hPD-l/Fc (R & D Systems) was immobilized onto Maxisorp 96-well plates (Nunc) by incubation for 4 h at room temperature (or overnight at 4°C). Nonspecific binding sites were blocked by incubation with 3% BSA in PBST for one hour at room temperature. After coating, the plates were washed three times with PBST. Dilutions of anti-PD-1 antibodies were prepared in binding buffer (PBS containing 0.1% Tween 20 and 0.3% BSA) and incubated with the immobilized fusion protein for one hour at 25°C.
  • binding buffer PBS containing 0.1% Tween 20 and 0.3% BSA
  • CHO-hPD-1 cells were cultured to 80 to 100 percent confluency in 50 ⁇ L culture medium (DMEM/HAM'S F12, 10% FBS).
  • This assay was. performed by coupling PD-I-Fc fusion protein (R&D Systems) to amine-reactive biosensors (Fortebio) using standard amine chemistry.
  • biosensors were then activated using a 0.1M NHS / 0.4M EDC mixture for 5 minutes.
  • PD-l/Fc fusion protein R & D systems
  • the biosensor surface was quenched using a solution of IM ethanolamine for 5 minutes.
  • Biosensors were equilibrated in PBS for 5 minutes. Association of anti-PD-1 mAbs was observed by placing the biosensors in wells containing various antibody concentrations (10-80 nM purified antibody >99% by SDS- PAGE in PBS) and monitoring interferometry for 30 minutes.
  • CHO cells expressing human PD-I were dissociated from adherent culture flasks and mixed with varying concentrations of anti-PD-1 antibody and a constant concentration (600ng/mL) of unlabeled hPD-Ll/Fc or recombinant human PD-L2/Fc fusion protein (both from R&D Systems) in a 96- well plate.
  • the mixture was equilibrated for 30 minutes on ice, washed three times with FACS buffer (PBS containing 1% BCS and 0.1% sodium azide), and incubated with FITC labeled goat anti-human Fc for a further 15 minutes on ice
  • FACS buffer PBS containing 1% BCS and 0.1% sodium azide
  • FITC labeled goat anti-human Fc for a further 15 minutes on ice
  • the cells were washed again with FACS buffer and analyzed by flow cytometry Data were analyzed with P ⁇ sm (GraphPad Software, San Diego, CA) using non-linear regression, and IC50 values were calculated.
  • Ligand blockade was confirmed using a homogeneous competition assay and detection using fluorometric microvolume assay technology (FMAT). Briefly, CHO.hPD-1 were dissociated from adherent culture flasks, mixed with varying concentrations of anti-PD-1 antibody and a constant concentration (600ng/mL) of hPD-Ll/Fc or hPD-L2/Fc fusion protein (both from R&D Systems), labeled with a fluorescent dye (AlexaFluor 647, Invitrogen) in a 96-well plate. The mixture was equilibrated for 90 minutes at 37°C and read using an AB8200 Cellular Detection Analyzer (Applied Biosystems, Foster City, CA).
  • FMAT fluorometric microvolume assay technology
  • FIG. 1 shows results of a dose- response experiment indicating that the magnitude of ligand blockade is determined by antibody concentration. Binding of both hPD-Ll/Fc and hPD-L2/Fc to CHO-hPD-1 cells can be completely inhibited by hPD-1.08A, hPD-1.09A and (to a lesser extent) by Jl 16 in a dose-dependent fashion. Calculated IC 50 data are summarized in Table II. Confirming the results obtained using flow cytometry, the high affinity antibodies hPD-1.08A and hPD-1.09A inhibited PD-Ll binding with IC 50 values below 1 nM.
  • the mouse and cynomolgus macaque PD-I receptors were cloned by PCR and stably transfected CHO-Kl cells were generated.
  • the antibodies were tested for binding to the cynomolgus receptor using a CELISA.
  • Commercial antibody Jl 16, hPD-1.08A and hPD-1.09A were found to bind with equal affinity to human and cynomolgus PD-I and block binding of hPD-Ll/Fc and hPD- L2/Fc to cynomolgous PD-I with similar efficacy as compared to human PD-I.
  • anti-PD-1 monoclonal antibodies were purified and characterized, which were isolated based on their ability to modulate Jurkat function. These antibodies bound tightly to PD-I (with dissociation constants in the 20 pM to 3 nM range) and were capable of blocking the interaction with both PD-Ll and PD-L2 with varying IC50 values.
  • PD-I dissociation constants in the 20 pM to 3 nM range
  • Four of these anti-hPD-1 mAbs were considerably better than the best available commercial anti- PD-1 mAbs.
  • Each of the antibodies when added in solution acted as receptor antagonists, ultimately enhancing T cell responses (see Example 3).
  • Anti-PD-1 antibodies were tested for their capacity to enhance T cell activity in vitro using blood cells from healthy volunteers.
  • One assay used to characterize the functional consequence of blocking human PD-I receptor utilized Staphylococcus enterotoxin B (SEB) to engage and activate all T cells expressing the Y ⁇ 3 and V ⁇ 8 T cell receptor chain.
  • SEB Staphylococcus enterotoxin B
  • Healthy human donor blood was obtained and diluted 1:10 into culture medium. Diluted whole blood was plated (150 ⁇ l per well) in 96-well round-bottom plates and pre- incubated for 30-60 min with mAb and varying concentrations. SEB was then added at various concentrations ranging from 10 ng/mL to 10 ⁇ g/mL.
  • IL-2 Supernatants were collected after 2 to 4 days of culture and the amount of IL-2 produced was quantified using ELISA (described in Example 1) or using standard multiplex technology (Luminex platform - Biosource cytokine detection kits). Titration of SEB from 100 ng/mL up to 10 ⁇ g/mL significantly stimulated IL-2 production by whole-blood cells. Usually, depending on the donor, 100 to 1000 pg/mL IL-2 was detectable by ELISA 2-4 days after stimulation with 1 ⁇ g/mL of SEB. Addition of hPD-1.08A and hPD-1.09A enhanced IL-2 production over control mouse IgGl, on average 2 to 4 fold at the highest antibody concentration tested (25 ⁇ g/mL).
  • Anti-PD-Ll monoclonal antibody (clone MIH5, Ebiosciences #16-5982) and anti-CTLA-4 (clone 14D3, eBiosciences #16-1529) also induced an increase in IL-2 production under similar conditions, a finding that further validated the use of the SEB stimulation assay to quantify T cell activity after manipulation of costimulatory pathways ( Figure 4).
  • the enhanced IL-2 production by anti-PD-1 antibodies was found to be dose- dependent.
  • Luminex technology levels of TNF ⁇ , IL-17, JL-I, IL-6 and EFN ⁇ were also found to be significantly modulated by hPD-1.08A and hPD-1.09A. The results of these experiments indicate that hPD-1.08A and hPD-1.09 can be used to stimulate human T cell responses.
  • Anti-PD-1 antibody hPD-1.09A
  • hPD-1.09A was further tested for its capacity to enhance T cell activity in vitro using blood cells derived from cancer patients. Blood from patients with advanced melanoma (1 patient) or prostate cancer (3 patients) was tested following the above protocol. Results of the cytokine quantitation are presented in Table III as fold increase of cytokine produced when cells are stimulated in the presence of 25 ug/mL hPD- 1.09 A compared to SEB stimulation in the absence of antibody. In summary, hPD-1.09A was found to increase the SEB induced IL-2 production 2 to 3.5 fold for each of the 4 patients. Similarly production of TNF ⁇ , IL-17 and EFN ⁇ was enhanced, and production of IL-5 and IL- 13 was decreased. These experiments indicate that hPD-1.09A has the ability to stimulate T cell responses in cancer patients. Further, these experiments suggest a preference towards ThI responses.
  • TT tetanus toxoid
  • Cytokine concentrations were determined by ELISA (IL-2 and EFN- ⁇ ELISA detection antibody pair sets from eBioscience) and multiplex analysis (Luminex platform - Biosource cytokine detection kits). Blockade of PD-I enhanced proliferation and significantly enhanced cytokine production (Figure 5) including EFN ⁇ and EL-2 compared to antigen alone. Luminex analysis revealed that production of the cytokines GM-CSF, RANTES, and IL-6 are increased upon PD-I blockage.
  • SEB-stimulated blood cells demonstrated enhanced expression of PD-I by flow cytometry, these cells were used to determine if hPD-1.09A could detect PD-I in formalin-fixed paraffin embedded tissue for histological use.
  • Human donor peripheral blood mononuclear cells were stimulated with 0.1 ⁇ g/mL SEB for 3 days, after which the non-adherent cells (mainly lymphocytes) were collected, washed twice with PBS and centrifuged (1100 rpm for 5 min.). The cells were fixed for 10 min in 4% formaldehyde, the cell-pellet was embedded in agarose, dehydrated in ethanol (subsequently 70%, 80%, 96% and 100%) and xylene, and thereafter embedded in paraffin.
  • Sections (4 ⁇ m) were mounted onto glass slides and hydrated (xylene, ethanol 100%, 96%, 80%, 70%, PBS buffer), after which antigen retrieval in heated citrate buffer was performed using standard methodology. Peroxidase activity was blocked using 100% methanol including 0.3% H 2 O 2 and slides were rinsed in water and PBS, Tween 0.1%. Sections were incubated with hPD- 1.09A for 1.5 hours at room temperature, rinsed with PBS-T ween, followed by standard detection methods. Slides were counterstained with hematoxylin for 30 seconds at room temperature, dehydrated with xylene, and mounted for microscopical examination.
  • lymphocytes derived from SEB stimulated PBMC cultures stained strongly (when compared to the isotype control) with hPD-1.09A, as opposed to unstimulated PBMC cultures, indicating that hPD-1.09A is useful as a diagnostic reagent.
  • the DNA sequences encoding the variable regions of the mouse antibodies expressed by hybridomas hPD-1.08A and hPD-1.09A were determined. Briefly, gene specific cDNAs for the heavy and light chains were generated using the iScript Select cDNA synthesis kit (Biorad # 1708896) according to the manufacturer's instructions. PCR primers used were based on the Ig-primer set (Novagen # 69831-3). Degenerate PCR reactions were carried out using Taq polymerase according to the Novagen primer set protocol. PCR products were analyzed by agarose gel electrophoresis. The expected amplicon size for both the heavy and light chain variable region is about 500 base pairs.
  • Clones were sequenced in both directions using universal primers M13 forward, M13 reverse, T3 and T7. Results of each sequencing reaction for each clone were analyzed using Seqman. Consensus sequences were searched against databases of germline and rearranged Ig Variable region sequences using NCBI Ig-Blast
  • Blast results for hPD-1.08A identified a productively (in-frame) rearranged heavy chain with no stop codons introduced.
  • Light chain clones were identified which encode two different sequences; one is a productively (in-frame) rearranged light chain with no stop codons introduced, the other is a non- productively rearranged sequence containing a frame-shift leading to a stop codon in the FR4 region.
  • the non-productive sterile transcript observed likely originates from the myeloma fusion partner (Carroll W. L. et al., MoI. Immunol. 25:991-995 (1988) and was ruled out.
  • CDR and framework regions are annotated according to Kabat E. A., et al., 1991, Sequences of proteins of Immunological interest, In: NIH Publication No. 91-3242, US Department of Health and Human Services, Bethesda, MD.
  • Chimeric light and heavy chains were constructed by linking the PCR-cloned cDNAs of mouse hPD-1.09A VL and VH regions to human kappa and IgGl constant regions, respecitvely.
  • the 5' and 3' ends of the mouse cDNA sequences were modified using PCR primers designed to add a suitable leader sequence to each chain, and restriction sites to enable cloning into existing recombinant antibody expression vectors.
  • COS-7 cells (0.7 mL at 10 7 /mL) were electroporated with lO ⁇ g of each of the chimeric heavy and light chain expression plasmids. These cells were then cultured in 8 mL growth medium for three days. A sandwich ELISA was used to measure the antibody concentrations in the supernatants from the COS-7 transfections. This showed that the transfected COS-7 cells secreted about 295 ng/mL of the chimeric IgGi -kappa antibody in three separate transfections. Binding of the chimeric antibody produced by the transfected COS-7 cells was measured using PD-I binding ELISA and CELISA (see Example 2) and was shown to bind to PD-I with comparable affinity to that of the murine antibody.
  • the hPD-1.09A antibody was humanized by MRCT (Cambridge UK) using CDR grafting technology (see, e.g., U.S. Patent No. 5,225,539). Briefly, the variable chain sequences of the murine antibody hPD-1.09A were compared to those available in the Research Collaboratory for Structural Bioinformatics (RCSB) protein databank. A homology model of hPD-1.09A was generated based on the nearest VH and VK structures. Human sequences with highest identity to hPD-1.09A were identified and analyzed. (Foote and Winter, J. MoI. Biol. 224:487-499 (1992); Morea V.
  • the framework encoded by genbank accession # AB063829 was determined to be the most appropriate. Analysis of the hPD-1.09A VK sequence shows that its CDRl length (15 residues) is not found in any human VK. For this reason, frameworks of three different CDRl lengths (11, 16 and 17 residues) were analyzed in order to test which CDRl length would reproduce the behavior of hPD-1.09A VK. The human VK sequences with highest identity to hPD-1.09A VK at selected residues important in the structure and with CDRl lengths 11, 16 and 17 were identified. The framework of genbank accession # M29469 was selected on which to base K109A-L-11. The framework from genbank accession # AB064135 was selected on which to base K09A-L-16 and the framework from genbank accession # X72431 was chosen on which to base K09 A-L- 17.
  • Humanized antibodies h409Al 1, h409A16 and h409A17 were produced by transient transfection of CHO - S cells. Cells were grown in CD-CHO (Gibco) and C5467 media (Sigma) for 8 days in shaker flasks. Antibodies were purified from cell supernatants by Protein A chromatography, washed, eluted using 1 M acetic acid and neutralized using 3 M Tris. Finally, the buffer was exchanged for 100 mM acetic acid which had been adjusted to pH 5.5 with 1 M Tris base.
  • Protein-based and cell-based ELISAs to determine apparent binding affinities were performed as described in Example 2.
  • the humanized anti-PD-1 antibodies each bound to PD-l/Fc and cellularly expressed PD-I with comparable EC50 values to the murine parent antibody (Table V).
  • the ability of the humanized antibodies to block the binding of PD-Ll and PD-L2 to PD-I was measured using a homogeneous competition assay and detection using an FMAT competition assay as described in Example 2.
  • Binding of both hPD-Ll/Fc and hPD-L2/Fc to CHO-hPD-1 cells can be completely inhibited in a dose-dependent fashion by any of the humanized antibodies tested. Calculated IC 50 data are summarized in Table V. Similarly to the parent murine antibody hPD-1.09A, each of the humanized mAbs, h409Al l, h409A16 and h409A17 inhibited PD-Ll and PD-L2 binding with IC 50 values below 1 nM.
  • the humanized anti-PD-1 antibodies h409Al l, h409A16 and h409A17 demonstrated inhibition of ligand binding to cynomolgous PD-I with calculated IC 5O values under about 1 nM.
  • Humanized anti-PD-1 antibodies were tested for their capacity to enhance T cell activity in vitro using blood cells from healthy volunteers as described in Example 3. Supernatants were collected after 4 days of culture and the amount of IL-2 produced was quantified using ELISA The humanized PD-I antibodies demonstrated the capacity to increase IL-2 production stimulated by SEB ( Figure 7). Additionally, the humanized PD-I antibodies increased SEB induced EL-2 production in cancer patient blood, similar to what is described in Example 3. In summary, the humanized mAbs h409Al 1, h409A16, and h409A17 retained all functional activity during the humanization process. The h409Al l and h409A16 mAbs fully retained the affinity of the mouse parental antibody hPD109A upon humanization.

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