WO2009040562A1 - Dual specificity antibody fusions - Google Patents

Dual specificity antibody fusions Download PDF

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Publication number
WO2009040562A1
WO2009040562A1 PCT/GB2008/003331 GB2008003331W WO2009040562A1 WO 2009040562 A1 WO2009040562 A1 WO 2009040562A1 GB 2008003331 W GB2008003331 W GB 2008003331W WO 2009040562 A1 WO2009040562 A1 WO 2009040562A1
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seq
fab
antibody
single domain
fusion protein
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PCT/GB2008/003331
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English (en)
French (fr)
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David Paul Humphreys
Emma Dave
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UCB SA
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UCB SA
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Priority claimed from GB0718834A external-priority patent/GB0718834D0/en
Priority claimed from GB0718832A external-priority patent/GB0718832D0/en
Priority to CA2700714A priority Critical patent/CA2700714C/en
Priority to JP2010526367A priority patent/JP5592792B2/ja
Application filed by UCB SA filed Critical UCB SA
Priority to US12/679,873 priority patent/US8629246B2/en
Priority to EP08806478.7A priority patent/EP2195341B1/en
Priority to CN200880113719.9A priority patent/CN101842387B/zh
Priority to ES08806478.7T priority patent/ES2622460T3/es
Publication of WO2009040562A1 publication Critical patent/WO2009040562A1/en
Anticipated expiration legal-status Critical
Priority to US14/101,083 priority patent/US9309327B2/en
Priority to US15/058,460 priority patent/US9828438B2/en
Priority to US15/792,373 priority patent/US10100130B2/en
Priority to US16/124,650 priority patent/US11427650B2/en
Ceased legal-status Critical Current

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    • C07K16/00Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies
    • C07K16/46Hybrid immunoglobulins
    • C07K16/468Immunoglobulins having two or more different antigen binding sites, e.g. multifunctional antibodies
    • AHUMAN NECESSITIES
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    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K16/00Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies
    • 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
    • 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
    • C07K16/24Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against cytokines, lymphokines or interferons
    • C07K16/244Interleukins [IL]
    • C07K16/245IL-1
    • 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
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    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K2317/00Immunoglobulins specific features
    • C07K2317/30Immunoglobulins specific features characterized by aspects of specificity or valency
    • C07K2317/31Immunoglobulins specific features characterized by aspects of specificity or valency multispecific
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    • C07K2317/00Immunoglobulins specific features
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    • C07K2317/54F(ab')2
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    • C07K2317/55Fab or Fab'
    • CCHEMISTRY; METALLURGY
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    • 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
    • C07K2317/569Single domain, e.g. dAb, sdAb, VHH, VNAR or nanobody®
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    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K2317/00Immunoglobulins specific features
    • C07K2317/60Immunoglobulins specific features characterized by non-natural combinations of immunoglobulin fragments
    • C07K2317/64Immunoglobulins specific features characterized by non-natural combinations of immunoglobulin fragments comprising a combination of variable region and constant region components
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    • C07ORGANIC CHEMISTRY
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    • 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

Definitions

  • the present invention relates to new dual specificity antibody fusion proteins.
  • Such antibodies comprise a first specificity to an antigen of interest, and a second specificity for a second antigen of interest, for example a serum carrier protein for use in extending their in vivo serum half-life.
  • a serum carrier protein for use in extending their in vivo serum half-life.
  • antibody fragments such as Fv, Fab, Fab' and F(ab') 2 fragments and other antibody fragments.
  • Fv, Fab, Fab' and F(ab') 2 fragments retain the antigen binding activity of whole antibodies and can also exhibit improved tissue penetration and pharmacokinetic properties in comparison to whole immunoglobulin molecules.
  • antibody fragments are proving to be versatile therapeutic agents, as seen by the recent success of products such as ReoPro® and Lucentis®.
  • Antibodies with dual specificity i.e. which bind to two different antigens have been previously described (for reviews, see Segal et al, 1999, Curr. Opin. Immunol. 11:558-562; Pluckthun & Pack, 1997, Immunotechnology, 3:83-105; Fischer and Leger, 2007, Pathobiology, 74, 3-14). Dual specificity antibodies are also described in WO02/02773, US2007065440, US2006257406, US2006106203 and
  • Single variable domain antibodies also known as single domain antibodies or dAbs, correspond to the variable regions of either the heavy (VH) or light (VL) chain of an antibody.
  • Murine single-domain antibodies were described by Ward et al., 1989, Nature, 341, 544-546. Human and 'camelised' human single domain antibodies have also been described (Holt et al, 2003, Trends in Biotechnology, 21 , 484-490). Single domain antibodies have also been obtained from the camelids (camels and llamas) and cartilaginous fish (wobbegong and nurse sharks).
  • VhH high affinity single V-like domains
  • V-NAR high affinity single V-like domains
  • Fc-equivalent constant domain framework an integral and crucial component of their immune system
  • Single domain antibody-enzyme fusions have been described in EP0368684.
  • Single domain-effector group fusions have also been described in WO2004/058820 which comprise a single variable domain.
  • Dual variable domain immunoglobulins have been described in WO2007/024715.
  • Dual specific ligands comprising two single domain antibodies with differing specificities have been described in EP1517921.
  • thyroxine-binding protein thyroxine-binding protein
  • transthyretin ⁇ l-acid glycoprotein
  • transferrin fibrinogen and albumin
  • Serum carrier proteins circulate within the body with half-lives measured in days, for example, 5 days for thyroxine-binding protein or 2 days for transthyretin (Bartalena & Robbins, 1993, Clinics in Lab. Med. 13:583-598), or 65 hours in the second phase of turnover of iodinated ⁇ l-acid glycoprotein (Bree et ah, 1986, Clin. Pharmacokin. 11:336-342).
  • the present invention provides improved dual specificity antibody fusion proteins which can be produced recombinantly and are capable of binding two antigens simultaneously.
  • the present invention provides dual specificity antibody fusion proteins which comprise an immunoglobulin moiety with a first specificity for an antigen of interest, and further comprise a single domain antibody (dAb) with specificity for a second antigen of interest.
  • dAb single domain antibody
  • the present invention also provides dual specificity antibody fusion proteins which comprise an immunoglobulin moiety with a first specificity for an antigen of interest, and further comprise at least one single domain antibody with specificity for a second antigen of interest.
  • a dual specificity antibody fusion of the invention will be capable of selectively binding to two antigens of interest.
  • an antigen of interest bound by the Fab or Fab' fragment may be a cell-associated protein, for example a cell surface protein on cells such as bacterial cells, yeast cells, T-cells, endothelial cells or tumour cells, or it may be a soluble protein.
  • Antigens of interest may also be any medically relevant protein such as those proteins upregulated during disease or infection, for example receptors and/or their corresponding ligands.
  • cell surface proteins include adhesion molecules, for example integrins such as ⁇ l integrins e.g.
  • VLA-4 E- selectin, P selectin or L-selectin
  • CEA carcinoembryonic antigen
  • HMFGl and 2 human milk fat globulin
  • MHC Class I and MHC Class II antigens MHC Class I and MHC Class II antigens
  • VEGF vascular endothelial growth factor
  • Soluble antigens include interleukins such as IL-I, IL-2, IL-3, IL-4, IL-5, IL-6, IL-8, IL-12, IL-16 or IL-17, viral antigens for example respiratory syncytial virus or cytomegalovirus antigens, immunoglobulins, such as IgE, interferons such as interferon ⁇ , interferon ⁇ or interferon ⁇ , tumour necrosis factor- ⁇ , tumor necrosis factor- ⁇ , colony stimulating factors such as G-CSF or GM-CSF, and platelet derived growth factors such as PDGF- ⁇ , and PDGF- ⁇ and where appropriate receptors thereof.
  • interferons such as interferon ⁇ , interferon ⁇ or interferon ⁇
  • tumour necrosis factor- ⁇ such as tumor necrosis factor- ⁇
  • colony stimulating factors such as G-CSF or GM-CSF
  • platelet derived growth factors such as PDGF- ⁇ , and
  • antigens include bacterial cell surface antigens, bacterial toxins, viruses such as influenza, EBV, HepA, B and C, bioterrorism agents, radionuclides and heavy metals, and snake and spider venoms and toxins.
  • the antibody fusion protein of the invention may be used to functionally alter the activity of the antigen of interest.
  • the antibody fusion protein may neutralize, antagonize or agonise the activity of said antigen, directly or indirectly.
  • a second antigen of interest bound by the single domain antibody or antibodies in the dual specificity antibody fusion proteins of the invention may be a cell-associated protein, for example a cell surface protein on cells such as bacterial cells, yeast cells, T-cells, endothelial cells or tumour cells, or it may be a soluble protein.
  • Antigens of interest may also be any medically relevant protein such as those proteins upregulated during disease or infection, for example receptors and/or their corresponding ligands.
  • Particular examples of cell surface proteins include adhesion molecules, for example integrins such as ⁇ l integrins e.g.
  • Soluble antigens include interleukins such as IL-I, IL-2, IL-3, IL-4, IL-5, IL-6, IL-8, IL- 12, IL- 16 or IL- 17, viral antigens for example respiratory syncytial virus or cytomegalovirus antigens, immunoglobulins, such as IgE, interferons such as interferon ⁇ , interferon ⁇ or interferon ⁇ , tumour necrosis factor- ⁇ , tumor necrosis factor- ⁇ , colony stimulating factors such as G-CSF or GM-CSF, and platelet derived growth factors such as PDGF- ⁇ , and PDGF- ⁇ and where appropriate receptors thereof.
  • Other antigens include bacterial cell surface antigens, bacterial toxins, viruses such as influenza, EBV 5 Hep A, B and C, bio terrorism agents, radionuclides and heavy metals, and snake and spider venoms and toxins.
  • the present invention provides dual specificity antibody fusion proteins which comprise an immunoglobulin moiety with a first specificity for an antigen of interest, and further comprise a single domain antibody with specificity for a second protein, the latter providing the ability to recruit effector functions, such as complement pathway activation and/or effector cell recruitment.
  • fusion proteins of the present invention may be used to chelate radionuclides by virtue of a single domain antibody which binds to a nuclide chelator protein. Such fusion proteins are of use in imaging or radionuclide targeting approaches to therapy.
  • an isolated dual specificity antibody fusion protein comprising an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to at least one dAb which has specificity for a recruitment polypeptide, said dAb providing the ability to recruit cell- mediated effector function(s), directly or indirectly, by binding to said recruitment polypeptide.
  • the recruitment of effector function may be direct in that effector function is associated with a cell, said cell bearing a recruitment molecule on its surface. Indirect recruitment may occur when binding of a dAb to a recruitment molecule causes release of, for example, a factor which in turn may directly or indirectly recruit effector function, or may be via activation of a signalling pathway. Examples include TNF ⁇ , IL2, IL6, IL8, ILl 7, IFN ⁇ , histamine, CIq, opsonin and other members of the classical and alternative complement activation cascades, such as C2, C4, C3- convertase, and C5 to C9.
  • 'a recruitment polypeptide' includes a Fc ⁇ R such as Fc ⁇ RI, Fc ⁇ RII and Fc ⁇ RIII, a complement pathway protein such as, but without limitation, CIq and C3, a CD marker protein (Cluster of Differentiation marker) such as, but without limitation, CD68, CDl 15, CD16, CD80, CD83, CD86, CD56, CD64, CD3, CD4, CD8, CD28, CD45, CD 19, CD20 and CD22.
  • a Fc ⁇ R such as Fc ⁇ RI, Fc ⁇ RII and Fc ⁇ RIII
  • a complement pathway protein such as, but without limitation, CIq and C3
  • CD marker protein Cluster of Differentiation marker
  • CD marker proteins include CDl, CDId, CD2, CD5, CD8, CD9, CDlO, CDIl, CDl Ia, CDl Ib, CDl Ic, CD13, CD14, CD15, CD16, CD18, CD19, CD20,
  • the second protein for which the dAb has specificity is a complement pathway protein, with CIq being particularly preferred.
  • the second protein for which the dAb has specificity is a CD marker protein, with CD68, CD80, CD86, CD64, CD3, CD4, CD8 CD45, CDl 6 and CD35 being particularly preferred.
  • an isolated dual specificity antibody fusion protein comprising an antibody fragment with specificity for an antigen of interest, said fragment being fused to at least one dAb which has specificity for a CD molecule selected from the group consisting of CD68, CD80, CD86, CD64, CD3, CD4, CD8 CD45, CD16 and CD35.
  • the single domain antibody or antibodies provide an extended half-life to the immunoglobulin moiety with the first specificity.
  • a dual specificity antibody fusion protein comprising an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to at least one single domain antibody which has specificity for a serum carrier protein, a circulating immunoglobulin molecule, or CD35/CR1, said single domain antibody providing an extended half-life to the antibody fragment with specificity for said antigen of interest by binding to said serum carrier protein, circulating immunoglobulin molecule or CD35/CR1.
  • an isolated dual specificity antibody fusion protein comprising an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to at least one single domain antibody which has specificity for a serum carrier protein, a circulating immunoglobulin molecule, or CD35/CR1, said single domain antibody providing an extended half-life to the antibody fragment with specificity for said antigen of interest by binding to said serum carrier protein, circulating immunoglobulin molecule or CD35/CR1.
  • 'serum carrier proteins' include thyroxine-binding protein, transthyretin, ⁇ l-acid glycoprotein, transferrin, fibrinogen and albumin, or a fragment of any thereof.
  • a 'circulating immunoglobulin molecule' includes IgGl, IgG2,
  • CD35/CR1 is a protein present on red blood cells which have a half life of 36 days (normal range of 28 to 47 days; Lanaro et al, 1971, Cancer, 28(3):658-661).
  • the second protein for which the dAb has specificity is a serum carrier protein, with a human serum carrier protein being particularly preferred.
  • the serum carrier protein is human serum albumin.
  • a dual specificity antibody fusion protein comprising an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to at least one single domain antibody which has specificity for human serum albumin.
  • the present invention provides an isolated dual specificity antibody fusion protein comprising an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to at least one single domain antibody which has specificity for human serum albumin.
  • the antibody fragment with specificity for an antigen of interest is a Fab fragment. In another embodiment, the antibody fragment with specificity for an antigen of interest is a Fab' fragment.
  • the antibody fusion proteins of the invention are translation fusion proteins, i.e. genetic fusions, the sequence of each of which is encoded by an expression vector.
  • the antibody fusion protein components have been fused using chemical means, i.e. by chemical conjugation or chemical cross-linking. Such chemical means are known in the art.
  • the antibody fragments are Fab' fragments which possess a native or a modified hinge region.
  • the antibody fragment for use in preparing a dual specificity antibody fusion protein of the invention is a Fab' fragment
  • said fragment is generally extended at the C-terminus of the heavy chain by one or more amino acids.
  • an antibody fusion of the invention can comprise a Fab' fragment translation fused (or chemically fused) to a dAb, directly or via a linker.
  • suitable antibody Fab' fragments include those described in WO2005003170 and WO2005003171.
  • an antibody fusion of the invention can comprise a Fab fragment translation fused (or chemically fused) to a linker sequence which in turn is translation fused (or chemically fused) to a dAb.
  • the Fab fragment is a Fab fragment which terminates at the interchain cysteines, as described in WO2005/003169.
  • the antibody Fab or Fab' fragments of use in the present invention can be from any species but are preferably derived from a monoclonal antibody, a human antibody, or are humanised fragments.
  • An antibody fragment for use in the present invention can be derived from any class (e.g. IgG, IgE, IgM, IgD or IgA) or subclass of immunoglobulin molecule and may be obtained from any species including for example mouse, rat, shark, rabbit, pig, hamster, camel, llama, goat or human.
  • the antibody Fab or Fab' fragment is a monoclonal, fully human, humanized or chimeric antibody fragment.
  • the antibody Fab or Fab' fragments are fully human or humanised.
  • Monoclonal antibodies may be prepared by any method known in the art such as the hybridoma technique (Kohler & Milstein, Nature, 1975, 256, 495-497), the trioma technique, the human B-cell hybridoma technique (Kozbor et al, Immunology
  • Antibodies for use in the invention may also be generated using single lymphocyte antibody methods by cloning and expressing immunoglobulin variable region cDNAs generated from single lymphocytes selected for the production of specific antibodies by, for example, the methods described by Babcook, J. et al, Proc. Natl. Acad. ScL USA, 1996, 93(15), 7843-7848, WO 92/02551, WO2004/051268 and WO2004/106377.
  • Humanized antibodies are antibody molecules from non-human species having one or more complementarity determining regions (CDRs) from the non-human species and a framework region from a human immunoglobulin molecule (see, for example, US 5,585,089).
  • the antibodies for use in the present invention can also be generated using various phage display methods known in the art and include those disclosed by Brinkman et al., J. Immunol. Methods, 1995, 182, 41-50; Ames et al., J. Immunol. Methods, 1995, 184, 177-186; Kettleborough et al. Eur. J.
  • transgenic mice or other organisms, including other mammals, may be used to generate humanized antibodies.
  • Fully human antibodies are those antibodies in which the variable regions and the constant regions (where present) of both the heavy and the light chains are all of human origin, or substantially identical to sequences of human origin, not necessarily from the same antibody.
  • Examples of fully human antibodies may include antibodies produced for example by the phage display methods described above and antibodies produced by mice in which the murine immunoglobulin variable and constant region genes have been replaced by their human counterparts eg. as described in general terms in EP0546073 Bl, US 5,545,806, US 5,569,825, US 5,625,126, US 5,633,425, US 5,661,016, US5,770,429, EP 0438474 Bl and EP0463151 Bl.
  • the antibody Fab or Fab' fragment starting material for use in the present invention may be obtained from any whole antibody, especially a whole monoclonal antibody, using any suitable enzymatic cleavage and/or digestion techniques, for example by treatment with pepsin.
  • the antibody starting material may be prepared by the use of recombinant DNA techniques involving the manipulation and re-expression of DNA encoding antibody variable and/or constant regions. Standard molecular biology techniques may be used to modify, add or delete amino acids or domains as desired. Any alterations to the variable or constant regions are still encompassed by the terms 'variable' and 'constant' regions as used herein.
  • the antibody fragment starting material may be obtained from any species including for example mouse, rat, rabbit, hamster, camel, llama, goat or human. Parts of the antibody fragment may be obtained from more than one species, for example the antibody fragments may be chimeric. In one example, the constant regions are from one species and the variable regions from another. The antibody fragment starting material may also be modified. In another example, the variable region of the antibody fragment has been created using recombinant DNA engineering techniques. Such engineered versions include those created for example from natural antibody variable regions by insertions, deletions or changes in or to the amino acid sequences of the natural antibodies.
  • variable region domains containing at least one CDR and, optionally, one or more framework amino acids from one antibody and the remainder of the variable region domain from a second antibody.
  • the methods for creating and manufacturing these antibody fragments are well known in the art (see for example, Boss et al., US 4,816,397; Cabilly et al., US 6,331,415; Shrader et al., WO 92/02551; Ward et al., 1989, Nature, 341, 544; Orlandi et al., 1989, Proc.Natl.Acad.Sci. USA, 86, 3833;
  • each single domain antibody fused to the Fab or Fab' fragment may linked directly or via a linker.
  • linker regions for linking a dAb to a Fab or Fab' include, but are not limited to, flexible linker sequences and rigid linker sequences.
  • Flexible linker sequences include those disclosed in Huston et ⁇ /.,1988, PNAS 85:5879-5883; Wright & Deonarain, MoI. Immunol, 2007, 44(11):2860-2869; Alfthan et al, Prot. Eng., 1995, 8(7):725-731; Luo et ai, J. Biochem., 1995, 118(4):825-831; Tang et al, 1996, J. Biol. Chem. 271(26): 15682- 15686; and Turner et al, 1997, JIMM 205, 42-54 (see Table 1 for representative examples).
  • rigid linkers examples include the peptide sequences GAP AP AAP AP A (SEQ ID NO:34), PPPP (SEQ ID NO:35) and PPP.
  • an antibody hinge sequence or part thereof is used as a linker, eg. the upper hinge sequence.
  • antibody Fab' fragments for use in the present invention possess a native or a modified hinge region.
  • Such hinge regions are used as a natural linker to the dAb moiety.
  • the native hinge region is the hinge region normally associated with the C H I domain of the antibody molecule.
  • a modified hinge region is any hinge that differs in length and/or composition from the native hinge region.
  • Such hinges can include hinge regions from any other species, such as human, mouse, rat, rabbit, hamster, camel, llama or goat hinge regions.
  • Other modified hinge regions may comprise a complete hinge region derived from an antibody of a different class or subclass from that of the C H I domain.
  • a CHI domain of class ⁇ l may be attached to a hinge region of class ⁇ 4.
  • the modified hinge region may comprise part of a natural hinge or a repeating unit in which each unit in the repeat is derived from a natural hinge region.
  • the natural hinge region may be altered by converting one or more cysteine or other residues into neutral residues, such as alanine, or by converting suitably placed residues into cysteine residues.
  • the number of cysteine residues in the hinge region may be increased or decreased.
  • other characteristics of the hinge can be controlled, such as the distance of the hinge cysteine(s) from the light chain interchain cysteine, the distance between the cysteines of the hinge and the composition of other amino acids in the hinge that may affect properties of the hinge such as flexibility e.g. glycines may be incorporated into the hinge to increase rotational flexibility or prolines may be incorporated to reduce flexibility.
  • Alternatively combinations of charged or hydrophobic residues may be incorporated into the hinge to confer multimerisation properties, see for example, Richter et al., 2001, Prot. Eng. 14(10):775-783 for use of charged or ionic tails, e.g., acidic tails as linkers and Kostelny et al, 1992, J. Immunol. 5(1):1547-1553 for leucine zipper sequences.
  • Other modified hinge regions may be entirely synthetic and may be designed to possess desired properties such as length, composition and flexibility.
  • Single variable domains also known as single domain antibodies or dAbs for use in the present invention can be generated using methods known in the art and include those disclosed in WO2005118642, Ward et al, 1989, Nature, 341 , 544-546 and Holt et al., 2003, Trends in Biotechnology, 21, 484-490.
  • a single domain antibody for use in present invention is a heavy chain variable domain (VH) or a light chain domain (VL). Each light chain domain may be either of the kappa or lambda subgroup. Methods for isolating VH and VL domains have been described in the art, see for example EP0368684 and Ward et al., supra. Such domains may be derived from any suitable species or antibody starting material.
  • the single domain antibody may be derived from a rodent, a human or other species.
  • the single domain antibody is humanised.
  • the single domain antibody is derived from a phage display library, using the methods described in for example, WO2005/118642, Jespers et al, 2004, Nature Biotechnology, 22, 1161-1165 and Holt et al, 2003, Trends in Biotechnology, 21, 484-490.
  • Preferably such single domain antibodies are fully human but may also be derived from other species. It will be appreciated that the sequence of the single domain antibody once isolated may be modified to improve the characteristics of the single domain antibody, for example solubility, as described in Holt et al, supra.
  • Li one embodiment the dAb is a human sequence obtained from scFv phage- display or from a transgenic HumouseTM or VelocimouseTM or a humanised rodent.
  • the dAb is obtained from a human or humanised rodent, a camelid or a shark. Such a dAb will preferably be humanised.
  • the single domain antibody is a VHH domain based on camelid immunoglobulins as described in EP0656946.
  • a camel or a llama is immunised with an antigen of interest and blood collected when the titre is appropriate.
  • the gene encoding the dAb may be cloned by single cell PCR, or the B cell(s) encoding the dAb may be immortalised by EBV transformation, or by fusion to an immortal cell line.
  • the present invention provides dual specificity antibody fusion proteins comprising an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to at least one single domain antibody, directly or via a linker, which has specificity for a second antigen of interest.
  • the antibody fragment eg. Fab or Fab' fragment is fused at the N-terminus of the heavy or the light chain variable region to a dAb directly or via a linker.
  • the antibody Fab or Fab' fragment is fused at the C-terminus of the heavy or light chain to a dAb directly or via a linker.
  • the heavy and light chains of the antibody Fab or Fab' fragment are each fused at the C ⁇ terminus to a dAb directly or via a linker.
  • the linkage can be a chemical conjugation but is most preferably a translation fusion, i.e. a genetic fusion where the sequence of each is encoded in sequence by an expression vector.
  • the N-terminus of the single domain antibody will be fused to the C- terminus of the heavy or light chain of the Fab or Fab' fragment, directly or via a linker, and where the single domain antibody is fused to the N-terminus of the Fab or
  • Fab' it will be fused via its C-terminus, optionally via a linker.
  • the present invention provides a dual specificity antibody fusion protein comprising or consisting of an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to a single domain antibody at the N-terminus of the heavy or light chain which has specificity for a second antigen of interest.
  • the present invention provides a dual specificity antibody fusion protein comprising or consisting of an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to a single domain antibody at the C-temrinus of the heavy or light chain which has specificity for a second antigen of interest.
  • the present invention provides a dual specificity antibody fusion protein comprising or consisting of an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to at least one single domain antibody at the C-terminus of the heavy or light chain which has specificity for a second antigen of interest.
  • the present invention provides a dual specificity antibody fusion protein comprising or consisting of an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to two single domain antibodies wherein each single domain antibody is fused in linear sequence to each other, optionally via a linker and the resulting single domain antibody fusion is fused to the C-terminus of the light chain or the heavy chain of the Fab or Fab' fragment.
  • the present invention provides a dual specificity antibody fusion protein comprising or consisting of an antibody Fab or Fab' fragment with specificity for an antigen of interest, said fragment being fused to two single domain antibodies wherein one single domain antibody is fused to the C-terminus of the light chain of the Fab or Fab' fragment and the other single domain antibody is fused to the C-terminus of the heavy chain of the Fab or Fab' fragment, said single domain antibodies having specificity for a second antigen of interest.
  • the heavy and light chains of the Fab or Fab' fragment each comprise a single domain antibody at the C-terminus the two single domain antibodies are identical i.e. have the same binding specificity for the same antigen. In one example, they bind the same epitope on the same antigen.
  • the single domain antibodies may both be the same VH dAb, the same VHH dAb or the same VL dAb.
  • the heavy and light chains of the Fab or Fab' fragment each comprise a single domain antibody at the C-terminus the two single domain antibodies are a complementary VH/VL pair which bind the antigen co-operatively i.e. they are a complementary VH/VL pair which have the same binding specificity.
  • the dual specificity antibody fusion protein of the present invention comprises two single domain antibodies which are a complementary VH/VL pair
  • the VH single domain antibody is fused to the C-terminus of the heavy chain constant region (CHl) and the VL single domain antibody is fused to the C- terminus of the light chain constant region (C kappa or C lambda).
  • the dual specificity antibody fusion protein of the present invention comprises two single domain antibodies which are a complementary VH/VL pair
  • the VL single domain antibody is fused to the C-terminus of the heavy chain constant region (CHl) and the VH single domain antibody is fused to the C- terminus of the light chain constant region (C kappa or C lambda).
  • the single domain antibody or antibodies bind to a second antigen, different from that bound by the Fab or Fab' fragment component.
  • the dAbs for use in the present invention exhibit specificity for a complement pathway protein, a CD marker protein or an Fc ⁇ R.
  • the dAb is preferably specific for a CD molecule.
  • the dAb exhibits specificity for a CD molecule selected from the group consisting of CD68, CD80, CD86, CD64, CD3, CD4, CD8 CD45, CD16 and CD35.
  • the dAbs for use in the present invention exhibit specificity for a serum carrier protein, a circulating immunoglobulin molecule, or CD35/CR1 , the serum carrier protein preferably being a human serum carrier protein such as thyroxine-binding protein, transthyretin, ⁇ l-acid glycoprotein, transferrin, fibrinogen or serum albumin.
  • the dAb exhibits specificity for human serum albumin.
  • a rabbit, mouse, rat, camel or a llama is immunised with a serum carrier protein, a circulating immunoglobulin molecule, or CD35/CR1 (e.g. human serum albumin) and blood collected when the titre is appropriate.
  • the gene encoding the dAb may be cloned by single cell PCR, or the B cell(s) encoding the dAb may be immortalised by EBV transformation, or by fusion to an immortal cell line.
  • the single domain antibody may be obtained by phage display as described herein above.
  • the single domain antibody or antibodies bind human serum albumin. In one embodiment the single domain antibody or antibodies bind human serum albumin, murine serum albumin and rat serum albumin.
  • the single domain antibody which binds serum albumin is a dAb provided in WO2005/118642 (see for example figures 1 c and 1 d) or a VHH provided in WO2004/041862 or a humanised nanobody described in, for example table III of WO2006/122787.
  • a single domain antibody which binds human serum albumin for use in the present invention is a heavy chain VH single domain antibody which comprises at least one of a CDR having the sequence given in Figure 5 (e) SEQ ID NO:56 or Figure 5 (k) SEQ ID NO:62 for CDR-Hl, a CDR having the sequence given in Figure 5(f) SEQ ID NO:57 or Figure 5 (1) SEQ ID NO:63 for CDR-H2 and a CDR having the sequence given in Figure 5 (g) SEQ ID NO:58 or Figure 5 (m) SEQ
  • a single domain antibody which binds human serum albumin for use in the present invention is a heavy chain VH antibody, wherein at least two of CDR-Hl, CDR-H2 and CDR-H3 of the VH domain are selected from the following: the sequence given in SEQ ID NO:56 or SEQ ID NO:62 for CDR-Hl, the sequence given in SEQ ID NO:57 or SEQ ID NO:63 for CDR-H2 and the sequence given in SEQ ID NO.58 or SEQ ID NO.64 for CDR-H3.
  • the single domain antibody may comprise a VH domain wherein CDR-Hl has the sequence given in SEQ ID NO:56 and CDR-H2 has the sequence given in SEQ ID NO:57.
  • the single domain antibody may comprise a VH domain wherein CDR- Hl has the sequence given in SEQ ID NO:56 and CDR-H3 has the sequence given in SEQ ID NO:58.
  • a single domain antibody which binds human serum albumin for use in the present invention is a heavy chain VH single domain antibody, wherein the VH domain comprises the sequence given in SEQ ID NO:56 for CDR- Hl, the sequence given in SEQ ID NO:57 for CDR-H2 and the sequence given in SEQ ID NO:58 for CDR-H3.
  • a single domain antibody which binds human serum albumin for use in the present invention is a heavy chain VH single domain antibody, wherein the VH domain comprises the sequence given in SEQ ID NO:62 for CDR- Hl, the sequence given in SEQ ID NO: 63 for CDR-H2 and the sequence given in SEQ ID NO:64 for CDR-H3.
  • a single domain antibody which binds human serum albumin for use in the present invention is a humanised heavy chain VH single domain antibody, dAbHl, having the sequence given in Figure 5 (a) (SEQ ID NO:52).
  • An example of a suitable CHl -dAbHl fusion comprising a G 4 S linker is given in Figure 6 (SEQ ID NO:68).
  • the single domain antibody which binds human serum albumin for use in the present invention is a humanised heavy chain VH single domain antibody, dAbH2, having the sequence given in Figure 5 (c) (SEQ ID NO: 54).
  • dAbH2 having the sequence given in Figure 5 (c) (SEQ ID NO: 54).
  • An example of a suitable CHl-dAbH2 fusion comprising a G 4 S linker is given in
  • the Kabat residue designations do not always correspond directly with the linear numbering of the amino acid residues.
  • the actual linear amino acid sequence may contain fewer or additional amino acids than in the strict Kabat numbering corresponding to a shortening of, or insertion into, a structural component, whether framework or complementarity determining region (CDR), of the basic variable domain structure.
  • CDR complementarity determining region
  • the correct Kabat numbering of residues may be determined for a given antibody by alignment of residues of homology in the sequence of the antibody with a "standard" Kabat numbered sequence.
  • the CDRs of the heavy chain variable domain are located at residues 31-35 (CDR-Hl), residues 50-65 (CDR-H2) and residues 95-102 (CDR-H3) according to the Kabat numbering system.
  • CDR-Hl residues 31-35
  • CDR-H2 residues 50-65
  • CDR-H3 residues 95-102
  • Chothia Chothia, C. and Lesk, A.M. J. MoI. Biol., 196, 901-917 (1987)
  • the loop equivalent to CDR-Hl extends from residue 26 to residue 32.
  • 'CDR-Hl ' comprises residues 26 to 35, as described by a combination of the Kabat numbering system and Chothia' s topological loop definition.
  • the CDRs of the light chain variable domain are located at residues 24-34 (CDR-Ll), residues 50-56 (CDR-L2) and residues 89-97 (CDR-L3) according to the Kabat numbering system.
  • a single domain antibody which binds human serum albumin for use in the present invention is a light chain VL single domain antibody which comprises at least one of a CDR having the sequence given in Figure 5 (h) SEQ ID NO:59 or Figure 5 (n) SEQ ID NO:65 for CDR-Ll, a CDR having the sequence given in Figure 5(i) SEQ ID NO:60 or Figure 5 (o) SEQ ID NO:66 for CDR-L2 and a CDR having the sequence given in Figure 5 (j) SEQ ID NO:61 or Figure 5 (p) SEQ ID NO:67 for CDR-L3.
  • a single domain antibody which binds human serum albumin for use in the present invention is a light chain VL antibody, wherein at least two of CDR-Ll, CDR-L2 and CDR-L3 of the VL domain are selected from the following: the sequence given in SEQ ID NO:59 or SEQ ID NO:65 for CDR-Ll, the sequence given in SEQ ID NO:60 or SEQ ID NO.66 for CDR-L2 and the sequence given in SEQ ID NO:61 or SEQ ID NO:67 for CDR-L3.
  • the domain antibody may comprise a VL domain wherein CDR-Ll has the sequence given in SEQ ID NO:59 and CDR-L2 has the sequence given in SEQ ID NO:60.
  • the domain antibody may comprise a VL domain wherein CDR-Ll has the sequence given in SEQ ID NO:59 and CDR-L3 has the sequence given in SEQ ID NO:61.
  • CDR-Ll has the sequence given in SEQ ID NO:59
  • CDR-L3 has the sequence given in SEQ ID NO:61.
  • a single domain antibody which binds human serum albumin for use in the present invention is a light chain VL domain antibody, wherein the VL domain comprises the sequence given in SEQ ID NO: 59 for CDR-Ll, the sequence given in SEQ ID NO:60 for CDR-L2 and the sequence given in SEQ ID NO:61 for CDR-L3.
  • a single domain antibody which binds human serum albumin for use in the present invention is a light chain VL domain antibody, wherein the VL domain comprises the sequence given in SEQ ID NO.65 for CDR-Ll, the sequence given in SEQ ID NO:66 for CDR-L2 and the sequence given in SEQ ID NO:67 for CDR-L3.
  • a single domain antibody which binds human serum albumin for use in the present invention is a humanised light chain VL single domain antibody, dAbLl, having the sequence given in Figure 5 (b) (SEQ ID NO:53).
  • dAbLl humanised light chain VL single domain antibody
  • An example of a suitable CHl-dAbLl fusion and a Ckl-dAbLl fusion both comprising a G 4 S linker is given in Figure 6 (SEQ ID NO:70 and SEQ ID NO:72).
  • a single domain antibody which binds human serum albumin for use in the present invention is a humanised light chain VL single domain antibody, dAbL2, having the sequence given in Figure 5 (d) (SEQ ID NO:55).
  • dAbL2 humanised light chain VL single domain antibody
  • An example of a suitable CHl-dAbL2 fusion and a Ckl-dAbL2 fusion both comprising a G 4 S linker is given in Figure 6 (SEQ ID NO.71 and SEQ ID NO:73).
  • the heavy and light chains of the Fab or Fab' fragment each comprise a single domain antibody at the C-terminus and the two single domain antibodies are a complementary VH/VL pair which bind the antigen co-operatively as described herein above
  • the VH dAb is dAbHl (SEQ ID NO:52) and the VL dAb is dAbLl (SEQ ID NO:53).
  • the heavy and light chains of the Fab or Fab' fragment each comprise a single domain antibody at the C-terminus the two single domain antibodies are a complementary VH/VL pair which bind the antigen cooperatively as described herein above, the VH dAb is dAbH2 (SEQ ID NO: 54) and the VL dAb is dAbL2 (SEQ ID NO:55).
  • the present invention provides albumin binding antibodies or fragments thereof containing one or more of the CDRs provided herein above and in Figure 5 (e-p).
  • Said CDRs may be incorporated into any suitable antibody framework and into any suitable antibody format.
  • Such antibodies include whole antibodies and functionally active fragments or derivatives thereof which may be, but are not limited to, monoclonal, humanised, fully human or chimeric antibodies.
  • albumin binding antibodies may comprise a complete antibody molecule having full length heavy and light chains or a fragment thereof and may be, but are not limited to Fab, modified Fab, Fab', F(ab') 2 , Fv, single domain antibodies, scFv, bi, tri or tetra-valent antibodies, Bis-scFv, diabodies, triabodies, tetrabodies and epitope-binding fragments of any of the above (see for example Holliger and Hudson, 2005, Nature Biotech. 23(9): 1126-1136; Adair and Lawson, 2005, Drug Design Reviews - Online 2(3), 209-217).
  • Multi-valent antibodies may comprise multiple specificities or may be monospecific (see for example WO 92/22853 and WO05/113605). It will be appreciated that this aspect of the invention also extends to variants of these albumin binding antibodies.
  • albumin binding antibodies in particular single domain antibodies may be conjugated to any other antibody or protein or other molecule, as desired or used in any other suitable context.
  • the single domain antibodies dAbHl, dAbLl, dAbH2, dAbL2 as described above and shown in Figure 5 (a-d) may be incorporated into any suitable antibody format or used as single domain antibodies in any suitable context, such as a fusion or conjugate.
  • antibodies of this aspect of the invention comprise the sequence given in Figure 5(e) for CDR-Hl, the sequence given in Figure 5(f) for CDR-H2 and the sequence given in Figure 5(g) for CDR-H3.
  • antibodies of this aspect of the invention comprise the sequence given in Figure 5(k) for CDR-Hl, the sequence given in Figure 5(1) for CDR-H2 and the sequence given in Figure 5(m) for CDR-H3.
  • antibodies of this aspect of the invention comprise the sequence given in Figure 5(h) for CDR-Ll, the sequence given in Figure 5(i) for CDR-L2 and the sequence given in Figure 5(j) for CDR-L3.
  • antibodies of this aspect of the invention comprise the sequence given in Figure 5(n) for CDR-Ll, the sequence given in Figure 5(o) for CDR- L2 and the sequence given in Figure 5(p) for CDR-L3.
  • the binding affinity of the single domain antibody for albumin will be sufficient to extend the half-life of the Fab or Fab' in vivo. It has been reported that an affinity for albumin of less than or equal to 2.5 ⁇ M affinity will extend half-life in vivo (Nguyen, A. et al (2006) Protein Engineering, Design & Selection, 19(7), 291-297).
  • the single domain antibody molecules of the present invention preferably have a binding affinity suited to their purpose and the antigen to which they bind.
  • the single domain antibodies have a high binding affinity, for example picomolar.
  • the single domain antibodies have a binding affinity for antigen which is nanomolar or micromolar. Affinity may be measured using any suitable method known in the art, including BIAcore as described in the Examples herein using natural or recombinant antigen.
  • the single domain antibody molecules of the present invention which bind albumin have a binding affinity of about 2 ⁇ M or better. In one embodiment the single domain antibody molecule of the present invention has a binding affinity of about l ⁇ M or better. In one embodiment the single domain antibody molecule of the present invention has a binding affinity of about 50OnM or better. In one embodiment the single domain antibody molecule of the present invention has a binding affinity of about 20OnM or better. In one embodiment the domain antibody molecule of the present invention has a binding affinity of about InM or better. It will be appreciated that the affinity of single domain antibodies provided by the present invention and known in the art may be altered using any suitable method known in the art.
  • the present invention therefore also relates to variants of the domain antibody molecules of the present invention, which have an improved affinity for albumin.
  • variants can be obtained by a number of affinity maturation protocols including mutating the CDRs (Yang et al, J. MoI. Biol., 254, 392-403, 1995), chain shuffling (Marks et al, Bio/Technology, 10, 779-783, 1992), use of mutator strains of E. coli (Low et al, J. MoI. Biol., 250, 359-368, 1996), DNA shuffling (Patten et al, Curr. Opin. BiotechnoL, 8, 724-733, 1997), phage display (Thompson et al, J. MoI. Biol, 256, 77-88, 1996) and sexual PCR (Crameri et al, Nature, 391, 288-291, 1998). Vaughan et al ⁇ supra) discusses these methods of affinity matur
  • the present invention also provides an isolated DNA sequence encoding a dual specificity antibody fusion protein of the present invention.
  • the DNA sequences of the present invention may comprise synthetic DNA, for instance produced by chemical processing, cDNA, genomic DNA or any combination thereof.
  • DNA sequences which encode the dual specificity antibody fusion protein of the present invention can be obtained by methods well known to those skilled in the art. For example, DNA sequences coding for part or all of the antibody fragments, linkers and/or dAbs may be synthesised as desired from the determined DNA sequences or on the basis of the corresponding amino acid sequences.
  • Standard techniques of molecular biology may be used to prepare DNA sequences coding for the dual specificity antibody fusion protein of the present invention. Desired DNA sequences may be synthesised completely or in part using oligonucleotide synthesis techniques. Site-directed mutagenesis and polymerase chain reaction (PCR) techniques may be used as appropriate.
  • PCR polymerase chain reaction
  • the present invention further relates to a cloning or expression vector comprising one or more DNA sequences of the present invention. Accordingly, provided is a cloning or expression vector comprising one or more DNA sequences encoding a dual specificity antibody fusion protein of the present invention.
  • the cloning or expression vector comprises a single DNA sequence encoding the entire dual specificity antibody fusion protein.
  • the cloning or expression vector comprises DNA encoded transcription units in sequence such that a translation fusion protein is produced.
  • a fusion protein of the invention can have the dAb at the N-terminus or the C-terminus and thus, the dAb DNA encoded transcription unit will be first or last, respectively, within the DNA sequence encoding the translation fusion.
  • a translation fusion may comprise an N-terminal dAb and a C-terminal Fab or Fab'.
  • a translation fusion may comprise an N- terminal Fab or Fab' and a C-terminal dAb.
  • one vector may comprise a translation fusion comprising a Fab or Fab' heavy chain and a C-terminal dAb and another vector may comprise a translation fusion comprising a Fab or Fab' light chain and a C-terminal dAb.
  • the vector will comprise DNA transcription units in sequence order; a DNA transcription unit encoding the dAb moiety, optionally a DNA transcription unit encoding a linker sequence, and a DNA transcription unit encoding an antibody fragment.
  • the vector will comprise DNA transcription units in sequence order; a DNA transcription unit encoding an antibody fragment, optionally a DNA transcription unit encoding a linker sequence, and a DNA transcription unit encoding dAb moiety with specificity for a serum carrier protein, a circulating immunoglobulin molecule, or CD35/CR1, for example, human serum albumin.
  • a translation fusion of the invention can be in different configurations including, for example but without limitation, dAb-linker-Fab, Fab-linker-dAb, dAb- Fab, Fab-dAb, Fab'-dAb, dAb-Fab', dAb-linker Fab', Fab'-linker-dAb.
  • the first may comprise the heavy chain of a Fab or Fab' fused to a dAb and the second may comprise the light chain of a Fab or Fab' fused to a dAb.
  • DNA code for an antibody fragment comprised within a translation fusion of the invention can be incorporated into a vector as a transcription unit in configurations as known to the person skilled in the art, for example a transcription unit can comprise code for the light chain followed by the heavy chain code, or vice versa; see, in particular, Humphreys et ah, 2002, Protein Expression and Purification, 26:309-320.
  • a vector according to the present invention comprises an appropriate leader sequence, such as an antibody leader sequence.
  • leader sequences are well known in the art.
  • a host cell comprising one or more cloning or expression vectors comprising one or more DNA sequences encoding a dual specificity antibody fusion protein of the present invention.
  • Any suitable host cell/vector system may be used for expression of the DNA sequences encoding the dual specificity antibody fusion protein.
  • Bacterial, for example E. coli, and other microbial systems may be used or eukaryotic, for example mammalian, host cell expression systems may also be used.
  • Suitable mammalian host cells include NSO, CHO, myeloma or hybridoma cells. Accordingly in one embodiment the fusion protein of the present invention is expressed in E. coli. In another embodiment the fusion protein of the present invention is expressed in mammalian cells.
  • the present invention also provides a process for the production of a dual specificity antibody fusion protein comprising culturing a host cell comprising a vector of the present invention under conditions suitable for the expression of protein from the DNA sequence encoding said dual specificity antibody fusion protein.
  • the invention further provides methods for isolating the dual specificity antibody fusion protein.
  • a dual specificity antibody fusion protein of the present invention may be purified, where necessary, using any suitable method known in the art. For example, but without limitation, chromatographic techniques such as ion exchange, size exclusion, protein G or hydrophobic interaction chromatography may be used.
  • the size of a dual specificity antibody fusion protein may be confirmed by conventional methods known in the art such as size exclusion chromatography and non-reducing SDS-PAGE.
  • Dual specificity antibody fusion proteins of the invention are useful in the treatment of diseases or disorders including inflammatory diseases and disorders, immune disease and disorders, fibrotic disorders and cancers.
  • inflammatory disease or "disorder” and “immune disease or disorder” includes rheumatoid arthritis, psoriatic arthritis, still's disease, Muckle Wells disease, psoriasis, Crohn's disease, ulcerative colitis, SLE (Systemic Lupus Erythematosus), asthma, allergic rhinitis, atopic dermatitis, multiple sclerosis, vasculitis, Type I diabetes mellitus, transplantation and graft-versus-host disease.
  • fibrotic disorder includes idiopathic pulmonary fibrosis (IPF), systemic sclerosis (or scleroderma), kidney fibrosis, diabetic nephropathy, IgA nephropathy, hypertension, end-stage renal disease, peritoneal fibrosis (continuous ambulatory peritoneal dialysis), liver cirrhosis, age-related macular degeneration (ARMD), retinopathy, cardiac reactive fibrosis, scarring, keloids, burns, skin ulcers, angioplasty, coronary bypass surgery, arthroplasty and cataract surgery.
  • IPF idiopathic pulmonary fibrosis
  • systemic sclerosis or scleroderma
  • kidney fibrosis diabetic nephropathy
  • IgA nephropathy IgA nephropathy
  • hypertension end-stage renal disease
  • peritoneal fibrosis continuous ambulatory peritoneal dialysis
  • liver cirrhosis liver cirrhos
  • cancer includes a malignant new growth that arises from epithelium, found in skin or, more commonly, the lining of body organs, for example: breast, ovary, prostate, lung, kidney, pancreas, stomach, bladder or bowel. Cancers tend to infiltrate into adjacent tissue and spread (metastasise) to distant organs, for example: to bone, liver, lung or the brain.
  • compositions which comprises an antibody fusion of the invention in association with one or more pharmaceutically acceptable carriers, excipients or diluents.
  • an antibody fusion protein of the invention for the manufacture of a medicament for the treatment of a disease or disorder.
  • the disease or disorder is an inflammatory disease or disorder.
  • Pharmaceutical compositions according to the invention may take a form suitable for oral, buccal, parenteral, subcutaneous, nasal, topical, ophthalmic or rectal administration, or a form suitable for administration by inhalation or insufflation.
  • the pharmaceutical compositions may take the form of, for example, tablets, lozenges or capsules prepared by conventional means with pharmaceutically acceptable excipients such as binding agents (e.g. pregelatinised maize starch, polyvinylpyrrolidone or hydroxypropyl methyl cellulose); fillers (e.g. lactose, microcrystalline cellulose or calcium hydrogenphosphate); lubricants (e.g. magnesium stearate, talc or silica); disintegrants (e.g.
  • binding agents e.g. pregelatinised maize starch, polyvinylpyrrolidone or hydroxypropyl methyl cellulose
  • fillers e.g. lactose, microcrystalline cellulose or calcium hydrogenphosphate
  • lubricants e.g. magnesium stearate, talc or silica
  • disintegrants e.g.
  • Liquid preparations for oral administration may take the form of, for example, solutions, syrups or suspensions, or they may be presented as a dry product for constitution with water or other suitable vehicle before use. Such liquid preparations may be prepared by conventional means with pharmaceutically acceptable additives such as suspending agents, emulsifying agents, non-aqueous vehicles or preservatives. The preparations may also contain buffer salts, flavouring agents, colouring agents or sweetening agents, as appropriate. Preparations for oral administration may be suitably formulated to give controlled release of the active compound.
  • compositions may take the form of tablets or lozenges formulated in conventional manner.
  • the bispecific antibodies of the invention may be formulated for parenteral administration by injection, e.g. by bolus injection or infusion.
  • Formulations for injection may be presented in unit dosage form, e.g. in glass ampoules or multi-dose containers, e.g. glass vials.
  • the compositions for injection may take such forms as suspensions, solutions or emulsions in oily or aqueous vehicles, and may contain formulatory agents such as suspending, stabilising, preserving and/or dispersing agents.
  • the active ingredient may be in powder form for constitution with a suitable vehicle, e.g. sterile pyrogen- free water, before use.
  • the bispecific antibodies of the invention may also be formulated as a depot preparation.
  • Such long-acting formulations may be administered by implantation or by intramuscular injection.
  • the compounds according to the present invention may be conveniently delivered in the form of an aerosol spray presentation for pressurised packs or a nebuliser, with the use of a suitable propellant, e.g. dichlorodifluoromethane, fluorotrichloromethane, dichlorotetrafluoroethane, carbon dioxide or other suitable gas or mixture of gases.
  • a suitable propellant e.g. dichlorodifluoromethane, fluorotrichloromethane, dichlorotetrafluoroethane, carbon dioxide or other suitable gas or mixture of gases.
  • compositions may, if desired, be presented in a pack or dispenser device which may contain one or more unit dosage forms containing the active ingredient.
  • the pack or dispensing device may be accompanied by instructions for administration.
  • the compounds according to the present invention may be conveniently formulated in a suitable ointment containing the active component suspended or dissolved in one or more pharmaceutically acceptable carriers.
  • Particular carriers include, for example, mineral oil, liquid petroleum, propylene glycol, polyoxyethylene, polyoxypropylene, emulsifying wax and water.
  • the compounds according to the present invention may be formulated in a suitable lotion containing the active component suspended or dissolved in one or more pharmaceutically acceptable carriers.
  • Particular carriers include, for example, mineral oil, sorbitan monostearate, polysorbate 60, cetyl esters wax, cetearyl alcohol, benzyl alcohol, 2-octyldodecanol and water.
  • the compounds according to the present invention may be conveniently formulated as microionized suspensions in isotonic, pH-adjusted sterile saline, either with or without a preservative such as a bactericidal or fungicidal agent, for example phenylmercuric nitrate, benzylalkonium chloride or chlorhexidine acetate.
  • a bactericidal or fungicidal agent for example phenylmercuric nitrate, benzylalkonium chloride or chlorhexidine acetate.
  • compounds may be formulated in an ointment such as petrolatum.
  • the compounds according to the present invention may be conveniently formulated as suppositories. These can be prepared by mixing the active component with a suitable non-irritating excipient which is solid at room temperature but liquid at rectal temperature and so will melt in the rectum to release the active component.
  • suitable non-irritating excipient include, for example, cocoa butter, beeswax and polyethylene glycols.
  • daily dosages may range from around 10 ng/kg to 1000 mg/kg, typically from 100 ng/kg to 100 mg/kg, e.g. around 0.01 mg/kg to 40 mg/kg body weight for oral or buccal administration, from around 10 ng/kg to 50 mg/kg body weight for parenteral administration, and from around 0.05 mg to around 1000 mg, e.g. from around 0.5 mg to around 1000 mg, for nasal administration or administration by inhalation or insufflation.
  • Figure 1 Diagrammatic representation of Fab-dAbs where the dAb is at the C- terminus
  • Figure 2 Diagrammatic representation of Fab-didAbs
  • FIG. 3 SDS PAGE analysis of FabA-dAbL3 (CK-SG 4 SE) (1) and FabA-dAbL3 (CK-G[APAPA] 2 ) (2).
  • FIG. 4 Western blot analysis of FabA-dAbL3 (CK-SG 4 SE) (1) and FabA-dAbL3
  • Lane 5 FabB-didAb, -dAbL2 (CK-G 4 Sx2) & dAbH2 (CHl-G 4 Sx2)
  • Figure 5 Sequences of domain antibodies dAbHl, dAbH2, dAbLl and dAbL2 and the CDRs derived from each of those antibodies.
  • Figure 6 FabB-dAb constructs comprising FabB heavy or light chain variable domain fused to a domain antibody.
  • An in-frame DNA encoded transcription unit encoding a dAb with specificity for human serum albumin was produced using recombinant DNA technology.
  • an in-frame DNA encoded transcription unit encoding a dAb with specificity for a recruitment protein can be produced using recombinant DNA technology.
  • Example 2 Production of antibody fragment For fusion of a dAb to the C-terminus of the light chain, DNA was synthesised encoding a human kappa light chain constant region (with the Km3 allotype of the kappa constant region), a peptide linker and a dAb and cloned as a SacI-PvuII restriction fragment into the UCB-Celltech in-house expression vector pTTOD(Fab) (a derivative of pTTO-1, described in Popplewell et ah, Methods MoL Biol. 2005; 308: 17-30) which contains DNA encoding the human gamma-1 CHl constant region.
  • pTTOD(Fab) a derivative of pTTO-1, described in Popplewell et ah, Methods MoL Biol. 2005; 308: 17-30
  • DNA was synthesised encoding a human CHl fragment (of the ⁇ l isotype) followed by a linker encoding sequence and a dAb. This was sublcloned as an Apal-EcoRI restriction fragment into the UCB-Celltech in-house expression vector pTTOD(Fab) (a derivative of pTTO-1, described in Popplewell et ah, above) which contains DNA encoding the human gamma-1 CHl constant region.
  • pTTOD(Fab) a derivative of pTTO-1, described in Popplewell et ah, above
  • the antibody chain to which the dAb is fused is denoted either as CK or LC for the cKappa light chain and as CHl or HC for the heavy chain constant domain, CHl.
  • Fab-dAb fusion proteins were constructed by fusing dAbL3 or dAbH4 to the C- terrninus of the constant region of either the light or heavy chain of Fab A.
  • a flexible (SGGGGSE (SEQ ID NO: I)) or a rigid (G(APAPA) 2 (SEQ ID NO: 34)) linker was used to link the dAb to the cKappa region (SEQ ID NO: 75) whereas the linker DKTHTS (SEQ ID NO:2) was used to link the dAb to the CHI region (SEQ ID NO:76).
  • the DNA sequence coding for the constant region-dAb fusion was manufactured synthetically as fragments to enable sub-cloning into the FabA sequence of the in-house pTTOD vector.
  • Light chain-dAb fusions were constructed by sub-cloning the Sacl-Apal fragment of the synthesized genes, encoding a C-terminal cKappa fused to either dAbL3 or dAbH4 via either a (SGGGGSE (SEQ ID NO: I)) or a rigid (G(APAPA) 2 (SEQ ID NO: 34)) linker, into the corresponding sites of a plasmid capable of expressing FabA.
  • Heavy chain-dAb fusions were constructed by sub-cloning the Apal-EcoRl fragment of the synthesised genes, encoding a C-terminal CHI fused to either dAbL3 or dAbH4 via a DKTHTS linker, into the corresponding sites of a plasmid capable of expressing FabA.
  • Fab' A is derived from an IL-I beta binding antibody, the heavy and light chain sequences of which are provided in SEQ ID NOs:74 and 75 respectively as shown in Figure 7.
  • the hinge of the heavy chain was altered to DKTHTS even where no dAb is attached to the heavy chain (SEQ ID NO:76).
  • FabA comprises the same light chain sequence (SEQ ID NO:75) and a truncated heavy chain sequence which terminates at the interchain cysteine (SEQ ID NO:77).
  • dAbL3 and dAbH4 are light and heavy chain domain antibodies respectively which bind human serum albumin.
  • FabA-didAb fusion plasm ⁇ ds for expression in E.coli FabA-didAb with dAbL3 or dAbH4 on both light and heavy chains were constructed by sub-cloning the Apal-EcoRl fragment coding for CHl-dAb fusions into the existing Fab-dAb plasmids where the dAb is fused to the light chain via the flexible linker.
  • FabB-dAbs FabB-dAbHl (CHl-G 4 Sx2), FabB-dAbH2 (CHl-G 4 Sx2), FabB- dAbLl (CHl-G 4 Sx2), FabB-dAbL2 (CHl-G 4 Sx2) were all assembled by PCR then cloned into a mammalian expression vector under the control of the HCMV-MIE promoter and SV40E polyA sequence. These were paired with a similar vector containing the FabB light chain for expression in mammalian cells (see below).
  • FabB is derived from an antibody which bids a cell surface co-stimulatory molecule.
  • dAbHl, dAbH2, dAbLl and dAbL2 were obtained as described in Example 3.
  • FabB-dAbs The FabB-dAbs, FabB-dAbHl (CHl-G 4 Sx2), FabB-dAbH2 (CHl-G 4 Sx2), FabB- dAbLl (CK-G 4 Sx2), FabB-dAbL2 (CK-G 4 Sx2) were all assembled by PCR then cloned into a mammalian expression vector under the control of the HCMV-MIE promoter and SV40E polyA sequence.
  • HEK293 cells were transfected with the heavy and light chain plasmids using Invitrogen's 293fectin transfection reagent according to the manufacturer's instructions. Briefly, 2 ⁇ g heavy chain plasmid + 2 ⁇ g light chain plasmid was incubated with 1 O ⁇ l 293fectin + 340 ⁇ l Optimem media for 20mins at RT. The mixture was then added to 5x10 6 HEK293 cells in suspension and incubated for 4 days with shaking at 37°C. Biacore
  • Binding affinities and kinetic parameters for the interactions of Fab-dAb constructs were determined by surface plasmon resonance (SPR) conducted on a Biacore TlOO using CM5 sensor chips and HBS-EP (1OmM HEPES ( ⁇ H7.4), 15OmM NaCl, 3mM EDTA, 0.05% v/v surfactant P20) running buffer.
  • Fab-dAb samples were captured to the sensor chip surface using either a human F(ab') 2 -specific goat Fab (Jackson ImmunoResearch, 109-006-097) or an in-house generated anti human CHl monoclonal antibody. Covalent immobilisation of the capture antibody was achieved by standard amine coupling chemistry.
  • Each assay cycle consisted of firstly capturing the Fab-dAb using a 1 min injection, before an association phase consisting of a 3 min injection of antigen, after which dissociation was monitored for 5 min. After each cycle, the capture surface was regenerated with 2 x 1 min injections of 4OmM HCl followed by 30s of 5mM NaOH. The flow rates used were lO ⁇ l/min for capture, 30 ⁇ l/min for association and dissociation phases, and 1 O ⁇ l/min for regeneration.
  • a titration of antigen for human serum albumin typically 62.5nM- 2 ⁇ M, for IL- l ⁇ 1.25-4OnM was performed, a blank flow-cell was used for reference subtraction and buffer-blank injections were included to subtract instrument noise and drift.
  • E.coli pellets containing the Fab-dAbs within the periplasm were re-suspended in original culture volume with 10OmM Tris/HCl, 1OmM EDTA pH 7.4. These suspensions were then incubated at 4 0 C for 16 hours at 250rpm. The re-suspended pellets were centrifuged at lOOOOxg for 1 hour at 4 0 C. The supernatants were removed and 0.45 ⁇ m filtered.
  • Protein-G capture The Fab-dAbs were captured from the filtered supernatant by Protein-G chromatography. Briefly the supernatants were applied, with a 20 minute residence time, to a Gammabind Plus Sepharose (GE Healthcare) column equilibrated in 2OmM phosphate, 15OmM NaCl pH7.1. The column was washed with 2OmM phosphate,
  • the pH adjusted elutions were concentrated and diafiltered into 5OmM sodium acetate pH4.5 using a 10k MWCO membrane.
  • the Fab-dAbs were further purified by cation exchange chromatography at pH4.5 with a NaCl elution gradient. Briefly the diafiltered Protein-G eluates were applied to a Sourcel5S (GE Healthcare) column equilibrated in 5OmM sodium acetate pH4.5.
  • the column was washed with 5OmM sodium acetate pH4.5 and the bound material eluted with a 20 column volume linear gradient from 0 to IM NaCl in 5OmM sodium acetate pH4.5. Third column volume fractions were collected through out the gradient. The fractions were analysed by A280 and SDS-PAGE and relevant fractions pooled.
  • the Fab-dAbs were further purified by gel filtration. Briefly the Fab A- dAbL3 (CK-SG 4 SE) pooled ion exchange elution fractions were applied to a Superdex200 (GE Healthcare) column equilibrated in 5OmM sodium acetate, 125mM
  • fractions were analysed by A280 and SDS-PAGE and relevant fractions pooled.
  • the pooled ion exchange elution fractions were concentrated and diafiltered into 5OmM sodium acetate, 125mM NaCl pH 5.0 using a 10k MWCO membrane.
  • the PVDF membrane was block for lhr with 2% MarvelTM in
  • HRP-rabbit anti-human kappa light chains 1/5000 dilution in blocking buffer for lhr. anti-heavy chain mouse anti-human heavy chain, 1/7000 dilution in blocking buffer for lhr.
  • HRP-goat anti-mouse 1/2000 dilution in blocking buffer for lhr.
  • HRP-goat anti-rabbit IgG 1/1000 dilution in blocking buffer for lhr.
  • the yields of Fab-dAb were measured using a sandwich ELISA. Briefly, the Fab- dAb was captured with an anti-CHI antibody then revealed with an anti-kappa-HRP.
  • a lop rabbits were immunised with recombinant chromapure human serum albumin (purchased from Jackson). Rabbits received 3 immunisations of lOOug HSA protein sub cutaneously, the first immunisation in complete Freunds adjuvant and subsequent immunisations in incomplete Freunds.
  • Antibodies 1 and 2 which bind human, mouse and rat serum albumin were isolated using the methods described in WO04/051268. Genes for the heavy chain variable domain (VH) and light chain variable domain (VL) of antibodies 1 and 2 were isolated and sequenced following cloning via reverse transcription PCR.
  • the light chain grafted sequences were sub-cloned into the rabbit light chain expression vector pVRbcK which contains the DNA encoding the rabbit C-Kappa constant region.
  • the heavy chain grafted sequences were sub-cloned into the rabbit heavy chain expression vector pVRbHFab, which contains the DNA encoding the rabbit Fab' heavy chain constant region. Plasmids were co-transfected into CHO cells and the antibodies produced screened for albumin binding and affinity (Table 1). Transfections of CHO cells were performed using the LipofectamineTM 2000 procedure according to manufacturer's instructions (InVitrogen, catalogue No. 11668).
  • Humanised VL and VH regions were designed using human V-region acceptor frameworks and donor residues in the framework regions.
  • One grafted VL region (Ll (SEQ ID NO:53) and L2 (SEQ ID NO:55)) and one VH region (Hl (SEQ ID NO:52) and H2 (SEQ ID NO:54)) were designed for each of antibodies 1 and 2 and genes were built by oligonucleotide assembly and PCR mutagenesis.
  • the grafted domain antibodies and their CDRs are shown in Figure 5.
  • FabB-dAb constructs were produced as described in the methods and the supernatants from the tranfected HEK293 cells containing the FabB-dAbs were tested directly in BIAcore.
  • FabB-didAb constructs were produced as described in the methods and the supernatants from the tranfected HEK293 cells containing the didAbs tested directly in BIAcore. Further analysis was performed using didAb constructs in which single dAbs were fused to both heavy and light C-termini of Fab. Constructs in which the didAb was derived from a natural heavy and light variable domain pairing showed a marked improvement in affinity compared to the single dAb alone (table 2 and 3). The didAb fusion consisting of two identical dAbLls showed no improvement in affinity over that seen for the single dAbLl (data not shown). Table 3
  • CK-G[APAPA] 2 in E.coli were constructed as described in the methods.
  • the Fab- dAbs were expressed into the periplasm of the E.coli and purified to homogeneity as described in the methods. The purity of the Fab-dAbs were assessed by high temperature reverse phase HPLC, SDS-PAGE and Western blotting. The Fab-dAbs were also assessed for antigen binding by Biacore.
  • High temperature reverse phase HPLC High temperature reverse phase HPLC as performed as described in the methods gave quantitative analysis of all species contained in FabA-dAbL3 (CK-SG 4 SE) and Fab A- dAbL3 (CK-G[APAPA] 2 ). The percentage of each species present is shown in table
  • Fab-dAb samples were prepared under non-reduced and reduced conditions and run on a gel as described in the methods. The gel was Coomassie stained. The banding profile of both Fab-dAb samples, Fab'A-dAbL3 (CK-SG 4 SE) and Fab'A-dAbL3 (CK-G[APAPA] 2 ), corresponds well to the profile observed by high temperature reverse phase HPLC (figure 3).
  • Fab-dAbs are capable of simultaneous binding to both IL- l ⁇ and human serum albumin, and that binding of either IL- l ⁇ or human serum albumin does not inhibit the interaction of the other.
  • the original Fab A bound only to IL-I ⁇ , with negligible binding to human serum albumin.
  • the table above shows the binding response (RU) seen for each construct after separate injections of HSA or IL- l ⁇ , or injection of premixed HSA and IL-l ⁇ . In each case the final concentration was 5 ⁇ M for HSA and 10OnM for IL-l ⁇ . The sum of the individual HSA and IL-l ⁇ responses is shown in parentheses.
  • FabA-dAbs and FabA-didAb fusions terminating with a C-terminal HIS6 tag were expressed in Escherichia coli. After periplasmic extraction, dAb fusion proteins were purified via the C-terminal His ⁇ tag. Fab expression was analysed by Western blotting of a non-reduced gel with anti-CHI and anti-cKappa antibodies. FabA-dAb and FabA-didAb were expressed as full-length proteins and were shown to react to both antibody detection reagents.
  • Binding assays were performed on a variety of constructs in which dAbL3 or dAbH4 fused to either the light or heavy chain of the Fab A (see Table 8 for details of the constructs and summary of the binding data).

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US20180118853A1 (en) 2018-05-03
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CA2700714C (en) 2018-09-11
US10100130B2 (en) 2018-10-16
US20160311930A1 (en) 2016-10-27
US20190127489A1 (en) 2019-05-02
US20140194596A1 (en) 2014-07-10
US9309327B2 (en) 2016-04-12
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EP2535351A2 (en) 2012-12-19
ES2667729T3 (es) 2018-05-14
EP2535350A1 (en) 2012-12-19
ES2622460T3 (es) 2017-07-06
CN104004088B (zh) 2017-11-07
CN101842387A (zh) 2010-09-22
US11427650B2 (en) 2022-08-30
US9828438B2 (en) 2017-11-28
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US20100239582A1 (en) 2010-09-23
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US8629246B2 (en) 2014-01-14
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