US2023021168A1PendingUtilityA1

Methods for preventing or treating certain disorders by inhibiting binding of il-4 and/or il-13 to their respective receptors

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Assignee: PIERIS PHARMACEUTICALS GMBHPriority: Dec 13, 2011Filed: Jun 14, 2022Published: Jan 19, 2023
Est. expiryDec 13, 2031(~5.4 yrs left)· nominal 20-yr term from priority
A61P 29/00A61K 9/0078A61K 9/08A61K 38/1709A61P 11/02A61P 43/00A61P 27/02A61P 35/00A61P 11/16A61P 11/06A61P 11/00A61P 37/08
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Claims

Abstract

The present disclosure relates to methods of treating, ameliorating or preventing a disorder comprising administering a therapeutically effective amount of a composition comprising a protein which inhibits the ligand of Uniprot #P05112 and/or the ligand of Uniprot #P35225 from binding to their respective receptors to a subject in need thereof. In some embodiments, the disorder is preferably associated with an increase of the Th2 immune response. In some embodiments, administration is preferably locally to the lung in order to treat, ameliorate or prevent allergic asthma, rhinitis, conjunctivitis, lung fibrosis, cystic fibrosis, chronic obstructive pulmonary disease, pulmonary alveolar proteinosis or adult respiratory distress syndrome.

Claims

exact text as granted — not AI-modified
1 - 20 . (canceled) 
     
     
         21 . A method of treating or ameliorating a lung disorder, comprising administering to a subject in need thereof a composition comprising a mutein of human tear lipocalin, or a fragment, variant, fusion protein or conjugate thereof, wherein said mutein, or fragment, variant, fusion protein or conjugate thereof, is capable of exhibiting in vivo therapeutic activity in the subject, and wherein said mutein, or fragment or variant thereof has at least 90% identity to an amino acid sequence set forth in SEQ ID NO: 6. 
     
     
         22 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, binds to IL-4 receptor alpha chain. 
     
     
         23 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, is cross-reactive with marmoset IL-4 receptor alpha chain. 
     
     
         24 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, is not cross-reactive with mouse IL-4 receptor alpha chain, cynomolgus IL-4 receptor alpha chain, IL-23 receptor alpha chain, type I cytokine receptor with fibronectin type III domain, IL-6 receptor, or IL-18 receptor alpha chain. 
     
     
         25 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, is capable of inhibiting in vivo human IL-13 induced transcript CCL11 (eotaxin). 
     
     
         26 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, is more potent than an IL-4 mutant (R121D, Y124D) when inhibiting IL-13 induced transcript CCL11 (eotaxin) in vivo. 
     
     
         27 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, is capable of exhibiting a functional activity at a level that is equal to or greater than an anti-IL-4 receptor alpha chain monoclonal antibody having variable light and variable heavy chain sequences as set forth in SEQ ID NOs: 14 and 15, respectively. 
     
     
         28 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, is capable of inhibiting IL-13 induced goblet cell metaplasia at a level that is equal to or greater than an anti-IL-4 receptor alpha chain monoclonal antibody having variable light and variable heavy chain sequences as set forth in SEQ ID NOs: 14 and 15, respectively. 
     
     
         29 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, has the following amino acid residues at amino acid positions corresponding to numbering of amino acid positions of mature human tear lipocalin (SEQ ID NO: 1): Ser at amino acid position 26, Arg at amino acid position 27, Cys at amino acid position 28, Arg at amino acid position 30, Ala at amino acid position 31, Val at amino acid position 32, Tyr at amino acid position 33, Asn at amino acid position 34, Phe at amino acid position 53, Ala at amino acid position 55, Gln at amino acid position 56, Arg at amino acid position 57, Lys at amino acid position 58, Trp at amino acid position 61, Lys at amino acid position 63, Tyr at amino acid position 64, Leu at amino acid position 66, Ser at amino acid position 80, Arg at amino acid position 83, Leu at amino acid position 104, Cys at amino acid position 105, Pro at amino acid position 106, and Gln at amino acid position 108. 
     
     
         30 . The method of  claim 21 , wherein the mutein, or fragment, variant, fusion protein or conjugate thereof, comprises a fragment of the amino acid sequence set forth in SEQ ID NO: 6 that lacks at least one N-terminal and/or C-terminal amino acid residue. 
     
     
         31 . The method of  claim 21 , wherein the mutein, or fragment or variant thereof, has at least 95% identity to an amino acid sequence set forth in SEQ ID NO: 6. 
     
     
         32 . The method of  claim 21 , wherein the mutein has the following amino acid residues at amino acid positions corresponding to numbering of amino acid positions of mature human tear lipocalin (SEQ ID NO: 1): Ser at amino acid position 26, Arg at amino acid position 27, Cys at amino acid position 28, Arg at amino acid position 30, Ala at amino acid position 31, Val at amino acid position 32, Tyr at amino acid position 33, Asn at amino acid position 34, Phe at amino acid position 53, Ala at amino acid position 55, Gln at amino acid position 56, Arg at amino acid position 57, Lys at amino acid position 58, Trp at amino acid position 61, Lys at amino acid position 63, Tyr at amino acid position 64, Leu at amino acid position 66, Ser at amino acid position 80, Arg at amino acid position 83, Leu at amino acid position 104, Cys at amino acid position 105, Pro at amino acid position 106, and Gln at amino acid position 108. 
     
     
         33 . The method of  claim 21 , wherein the fragment of the mutein lacks at least one N-terminal and/or C-terminal amino acid residue of the mutein. 
     
     
         34 . The method of  claim 21 , wherein the composition further comprises a pharmaceutically acceptable formulation. 
     
     
         35 . The method of  claim 21 , wherein the composition is formulated for administration to the lung. 
     
     
         36 . The method of  claim 21 , wherein the composition is formulated for administration via aerosol inhalation. 
     
     
         37 . The method of  claim 21 , wherein the composition is administered to a subject in need thereof at a frequency selected from the group consisting of: up to four times daily, up to three times daily, up to twice daily, up to once daily, up to once every other day, up to once every third day, up to once every week, and up to once every other week. 
     
     
         38 . The method of  claim 21 , wherein said composition is administered to a subject in need thereof at a dosage level between 0.06-600 mg. 
     
     
         39 . The method of  claim 21 , wherein the disorder is selected from the group consisting of asthma, rhinitis, cystic fibrosis, and chronic obstructive pulmonary disease.

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