Gene sequence construct for gene therapy of human immunodeficiency virus infection
US-2024352096-A1 · Oct 24, 2024 · US
Engineered antibody constant domain molecules
US9527903B2 · US · B2
| Field | Value |
|---|---|
| Publication number | US-9527903-B2 |
| Application number | US-201314043366-A |
| Country | US |
| Kind code | B2 |
| Filing date | Oct 1, 2013 |
| Priority date | Jan 31, 2008 |
| Publication date | Dec 27, 2016 |
| Grant date | Dec 27, 2016 |
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Abstract
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Described herein are engineered antibody constant domain molecules, such as CH2 or CH3 domain molecules, comprising at least one mutation, or comprising at least one complementarity determining region (CDR), or a functional fragment thereof, engrafted in a loop region of the CH2 domain. The CH2 domain molecules described herein are small, stable, soluble, exhibit little to no toxicity and are capable of binding antigen.
First claim
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The invention claimed is: 1. An isolated human immunoglobulin CH2 domain of IgG, wherein the CH2 domain comprises an N-terminal truncation of 7 amino acids and a C-terminal truncation of 1 to 4 amino acids, and wherein the CH2 domain has a molecular weight of less than about 15 kD. 2. An isolated human immunoglobulin CH2 domain of IgG, wherein the CH2 domain comprises an N-terminal truncation of 7 amino acids, and further comprises a first amino acid substitution in the N-terminal A strand and a second amino acid substitution in the C-terminal G-strand, wherein the first amino acid substitution is (i)L12 to C12 or (ii)V10 to C10, and the second amino acid substitution is K104 to C104 (numbered with reference to SEQ ID NO:5), and wherein the first and second amino acid substitutions each replace the original residue with a cysteine residue and the cysteine residues form a disulfide bond. 3. The isolated human immunoglobulin CH2 domain of claim 2 , further comprising a C-terminal truncation of 1 to about 4 amino acids. 4. The isolated human immunoglobulin CH2 domain Of claim 2 , further comprising a C-terminal truncation of 4 amino acids. 5. A polypeptide comprising a human immunoglobulin CH2 domain of IgG, wherein the CH2 domain comprises an N-terminal truncation of 7 amino acids, and further comprises a first amino acid substitution in the N-terminal A strand and a second amino acid substitution in the C-terminal G strand, wherein the first amino acid substitution is (i) L12 to C12 or (ii) to V10 to C10, and the second amino acid substitution is K104 to C104 (numbered with reference to SEQ Id No:5), wherein the first and second amino acid substitutions each replace the original residue with a cysteine residue and the cysteine residues form a disulfide bond, and wherein the polypeptide has a molecular weight of less than about 15 kD. 6. The polypeptide of claim 5 , wherein the CH2 domain further comprises a C-terminal truncation of 1 to about 4 amino acids. 7. The polypeptide of claim 5 , wherein the CH2 domain further comprises a C-terminal truncation of 4 amino acids. 8. The isolated immunoglobulin CH2 domain of claim 1 , comprising a C-terminal truncation of 4 amino acids. 9. The isolated human immunoglobulin CH2 domain of claim 1 , wherein the CH2 domain further comprises a first amino acid substitution and a second amino acid substitution, wherein the first and second amino acid substitutions each replace the original residue with a cysteine residue, wherein the cysteine residues form a disulfide bond. 10. The isolated human immunoglobulin CH2 domain, of claim 9 , wherein the first amino acid substitution is in the N-terminal A strand and the second amino acid substitution is in the C-terminal G strand. 11. The isolated CH2 domain of claim 10 , wherein the first amino acid substitution is (i) L12 to C12 or (ii) V10 to C10, and the second amino acid substitution is K104 to C104 (numbered with reference to SEQ ID NO: 5).
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- What does patent US9527903B2 cover?
- Described herein are engineered antibody constant domain molecules, such as CH2 or CH3 domain molecules, comprising at least one mutation, or comprising at least one complementarity determining region (CDR), or a functional fragment thereof, engrafted in a loop region of the CH2 domain. The CH2 domain molecules described herein are small, stable, soluble, exhibit little to no toxicity and are c…
- Who is the assignee on this patent?
- Us Health, The United States Of America As Represent By The Secretary Dept Of Health And Human Services
- What technology area does this patent fall under?
- Primary CPC classification C07K16/1145. Mapped technology areas include Chemistry & Metallurgy.
- When was this patent published?
- Publication date Tue Dec 27 2016 00:00:00 GMT+0000 (Coordinated Universal Time) (B2). Legal status and post-grant events are not shown on this page.
- What related patents are in patentsdb?
- We list 8 related publications on this page (citations in our corpus or others sharing the same primary CPC).