Claims for Patent: 9,169,470
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Summary for Patent: 9,169,470
Title: | Methods and compositions for generating bioactive assemblies of increased complexity and uses |
Abstract: | The present invention concerns methods and compositions for making and using bioactive assemblies of defined compositions, which may have multiple functionalities and/or binding specificities. In particular embodiments, the bioactive assembly is formed using dock-and-lock (DNL) methodology, which takes advantage of the specific binding interaction between dimerization and docking domains (DDD) and anchoring domains (AD) to form the assembly. In various embodiments, one or more effectors may be attached to a DDD or AD sequence. Complementary AD or DDD sequences may be attached to an adaptor module that forms the core of the bioactive assembly, allowing formation of the assembly through the specific DDD/AD binding interactions. Such assemblies may be attached to a wide variety of effector moieties for treatment, detection and/or diagnosis of a disease, pathogen infection or other medical or veterinary condition. |
Inventor(s): | Chang; Chien-Hsing (Downingtown, PA), Goldenberg; David M. (Mendham, NJ), McBride; William J. (Boonton, NJ), Rossi; Edmund A. (Woodland Park, NJ) |
Assignee: | IBC Pharmaceuticals, Inc. (Morris Plains, NJ) |
Application Number: | 14/488,921 |
Patent Claims: | 1. A dock and lock (DNL) complex comprising: a) a first fusion protein comprising (i) an anchoring domain (AD) from an A-kinase anchoring protein (AKAP), wherein the amino
acid sequence of the AD moiety is selected from the group consisting of SEQ ID NO:2 and SEQ ID NO:5; and (ii) a first effector protein selected from the group consisting of an antibody and an antigen-binding fragment thereof; and b) a second fusion
protein comprising (iii) a dimerization and docking domain (DDD) moiety, wherein the amino acid sequence of the DDD moiety is selected from the group consisting of residues 1-44 of human protein kinase A (PKA) RII.alpha., residues 1-44 of human PKA
RII.beta. and residues 12-61 of human PKA RI.alpha.; and (iv) a second effector protein that is a toxin, wherein the toxin is selected from the group consisting of ricin, abrin, ribonuclease, ranpirnase, rapLR1, DNase I, Staphylococcal enterotoxin-A,
pokeweed antiviral protein, gelonin, diphtheria toxin, Pseudomonas exotoxin and Pseudomonas endotoxin; wherein two copies of the DDD moiety form a dimer that binds to the AD moiety to form the DNL complex.
2. The DNL complex of claim 1, wherein the antibody is selected from the group consisting of a monoclonal antibody, a chimeric antibody, a humanized antibody, and a human antibody. 3. The DNL complex of claim 1, wherein the antibody fragment is selected from the group consisting of a Fab fragment, a F(ab).sub.2 fragment, a Fab' fragment, a F(ab').sub.2 fragment, a single domain (DAB) antibody fragment, a scFv, a diabody and a triabody. 4. The DNL complex of claim 1, wherein the antibody or antibody fragment binds to an antigen selected from the group consisting of carbonic anhydrase IX, alpha-fetoprotein, CA125, CD1, CD1a, CD3, CD5, CD15, CD16, CD19,CD20, CD21, CD22, CD23, CD25, CD30, CD33, CD38, CD45, CD74, CD79a, CD80,CD138, colon-specific antigen-p (CSAp), CEA (CEACAM5), CEACAM6, EGFR, EGP-1, EGP-2, Flt-1, Flt-3, folate receptor, HLA-DR, human chorionic gonadotropin (HCG), HER2/neu, hypoxia inducible factor (HIF-1), IL-2, IL-6, IL-8,insulin-like growth factor-1 (IGF-1), KS1-4, Le-Y, macrophage inhibition factor (MIF), MAGE, MUC1, MUC2, MUC3, MUC4, MUC16, NCA66, NCA95,placental growth factor, p53, prostatic acid phosphatase, PSA, PSMA, TAG-72, tenascin, TRAIL receptors, Tn antigen, a tumor necrosis antigen, VEGF, and ED-B fibronectin. 5. The DNL complex of claim 1, wherein the antibody is selected from the group consisting of hLL1 (anti-CD74), hLL2 (anti-CD22), hA20 (anti-CD20), L243 (anti-H LA class II), hCC49 (anti-TAG-72), hMN-14 (anti-CEA), hMN-15 (anti-CEA), h679 (anti-H SG), L19 (anti-ED-B fibronectin), hPAM4 (anti-mucin), hRS7 (anti-EGP-1), adalimumab, infliximab, omalizumab and palivizumab. |
Details for Patent 9,169,470
Applicant | Tradename | Biologic Ingredient | Dosage Form | BLA | Approval Date | Patent No. | Expiredate |
---|---|---|---|---|---|---|---|
Ferring Pharmaceuticals Inc. | NOVAREL | chorionic gonadotropin | For Injection | 017016 | 01/15/1974 | ⤷ Try a Trial | 2025-10-19 |
Ferring Pharmaceuticals Inc. | NOVAREL | chorionic gonadotropin | For Injection | 017016 | 12/27/1984 | ⤷ Try a Trial | 2025-10-19 |
Ferring Pharmaceuticals Inc. | NOVAREL | chorionic gonadotropin | For Injection | 017016 | 02/15/1985 | ⤷ Try a Trial | 2025-10-19 |
Ferring Pharmaceuticals Inc. | NOVAREL | chorionic gonadotropin | For Injection | 017016 | 02/16/1990 | ⤷ Try a Trial | 2025-10-19 |
Bel-mar Laboratories, Inc. | CHORIONIC GONADOTROPIN | chorionic gonadotropin | Injection | 017054 | 03/26/1974 | ⤷ Try a Trial | 2025-10-19 |
>Applicant | >Tradename | >Biologic Ingredient | >Dosage Form | >BLA | >Approval Date | >Patent No. | >Expiredate |
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