Sars-cov-2 vaccines
US-2024408193-A1 · Dec 12, 2024 · US
MVA-gH/gL-PC vaccine derived antibodies neutralizing human cytomegalovirus infectivity and methods thereof
US11384137B2 · US · B2
| Field | Value |
|---|---|
| Publication number | US-11384137-B2 |
| Application number | US-201916680205-A |
| Country | US |
| Kind code | B2 |
| Filing date | Nov 11, 2019 |
| Priority date | Sep 10, 2015 |
| Publication date | Jul 12, 2022 |
| Grant date | Jul 12, 2022 |
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- Title
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- Abstract
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Abstract
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Vaccine-derived neutralizing antibodies (NAbs) for CMV infections and small peptides which define precise recognition elements of the antigens by the NAbs. The vaccine-derived NAbs may be produced by immunizing a subject with a gH/gL/UL128/UL130/UL131A pentameric glycoprotein complex (gH/gLPC). The vaccine-derived NAbs may have properties similar or identical to those of NAbs induced in a subject naturally infected with CMV. Native and non-native small peptides from UL128 and gH have been defined by mapping epitopes and deriving artificial sequences which are minimal recognition elements of vaccine-derived NAbs. These small peptides can be used to elicit vaccine-derived NAbs that prevent CMV entry into susceptible cell types and protect humans from infection and disease. Multivalent vaccines comprising these small peptides and/or epitopes as well as methods of using the vaccine-derived NAbs and small peptides for treating or preventing CMV infection in a subject are also provided.
First claim
Opening claim text (preview).
What is claimed is: 1. A method of preventing cell-to-cell spread of CMV, syncytia formation in epithelial cells, or both in a subject, comprising administering to the subject an effective amount of a composition comprising a vaccine-derived neutralizing antibody (NAb) against cytomegalovirus (CMV), which the vaccine-derived NAb is selected from the group consisting of: (a) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 3, a CDR2 VH sequence of SEQ ID NO: 4, and a CDR3 VH sequence of SEQ ID NO: 5; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 6, a CDR2 VL sequence of SEQ ID NO: 7, and a CDR3 VL sequence of SEQ ID NO: 8; (b) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 11, a CDR2 VH sequence of SEQ ID NO: 12, and a CDR3 VH sequence of SEQ ID NO: 13; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 14, a CDR2 VL sequence of SEQ ID NO: 15, and a CDR3 VL sequence of SEQ ID NO: 16; (C) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 19, a CDR2 VH sequence of SEQ ID NO: 20, and a CDR3 VH sequence of SEQ ID NO: 21; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 22, a CDR2 VL sequence of SEQ ID NO: 23, and a CDR3 VL sequence of SEQ ID NO: 24; (d) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 27, a CDR2 VH sequence of SEQ ID NO: 28, and a CDR3 VH sequence of SEQ ID NO: 29; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 30, a CDR2 VL sequence of SEQ ID NO: 31, and a CDR3 VL sequence of SEQ ID NO: 32; (e) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 35, a CDR2 VH sequence of SEQ ID NO: 36, and a CDR3 VH sequence of SEQ ID NO: 37; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 38, a CDR2 VL sequence of SEQ ID NO: 39, and a CDR3 VL sequence of SEQ ID NO: 40; (f) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 43, a CDR2 VH sequence of SEQ ID NO: 44, and a CDR3 VH sequence of SEQ ID NO: 45; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 46, a CDR2 VL sequence of SEQ ID NO: 47, and a CDR3 VL sequence of SEQ ID NO: 48; (g) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 51, a CDR2 VH sequence of SEQ ID NO: 52, and a CDR3 VH sequence of SEQ ID NO: 53; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 54, a CDR2 VL sequence of SEQ ID NO: 55, and a CDR3 VL sequence of SEQ ID NO: 56; (h) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 59, a CDR2 VH sequence of SEQ ID NO: 60, and a CDR3 VH sequence of SEQ ID NO: 61; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 62, a CDR2 VL sequence of SEQ ID NO: 63, and a CDR3 VL sequence of SEQ ID NO: 64; (i) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 67, a CDR2 VH sequence of SEQ ID NO: 68, and a CDR3 VH sequence of SEQ ID NO: 69; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 70, a CDR2 VL sequence of SEQ ID NO: 71, and a CDR3 VL sequence of SEQ ID NO: 72; (j) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 75, a CDR2 VH sequence of SEQ ID NO: 76, and a CDR3 VH sequence of SEQ ID NO: 77; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 78, a CDR2 VL sequence of SEQ ID NO: 79, and a CDR3 VL sequence of SEQ ID NO: 80; (k) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 83, a CDR2 VH sequence of SEQ ID NO: 84, and a CDR3 VH sequence of SEQ ID NO: 85; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 86, a CDR2 VL sequence of SEQ ID NO: 87, and a CDR3 VL sequence of SEQ ID NO: 88; (l) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 91, a CDR2 VH sequence of SEQ ID NO: 92, and a CDR3 VH sequence of SEQ ID NO: 93; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 94, a CDR2 VL sequence of SEQ ID NO: 95, and a CDR3 VL sequence of SEQ ID NO: 96; (m) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 99, a CDR2 VH sequence of SEQ ID NO: 100, and a CDR3 VH sequence of SEQ ID NO: 101; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 102, a CDR2 VL sequence of SEQ ID NO: 103, and a CDR3 VL sequence of SEQ ID NO: 104; (n) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 107, a CDR2 VH sequence of SEQ ID NO: 108, and a CDR3 VH sequence of SEQ ID NO: 109; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 110, a CDR2 VL sequence of SEQ ID NO: 111, and a CDR3 VL sequence of SEQ ID NO: 112; (o) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 115, a CDR2 VH sequence of SEQ ID NO: 116, and a CDR3 VH sequence of SEQ ID NO: 117; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 118, a CDR2 VL sequence of SEQ ID NO: 119, and a CDR3 VL sequence of SEQ ID NO: 120; (p) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 123, a CDR2 VH sequence of SEQ ID NO: 124, and a CDR3 VH sequence of SEQ ID NO: 125; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 126, a CDR2 VL sequence of SEQ ID NO: 127, and a CDR3 VL sequence of SEQ ID NO: 128; (q) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 131, a CDR2 VH sequence of SEQ ID NO: 132, and a CDR3 VH sequence of SEQ ID NO: 133; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 134, a CDR2 VL sequence of SEQ ID NO: 135, and a CDR3 VL sequence of SEQ ID NO: 136; (r) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 139, a CDR2 VH sequence of SEQ ID NO: 140, and a CDR3 VH sequence of SEQ ID NO: 141; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 142, a CDR2 VL sequence of SEQ ID NO: 143, and a CDR3 VL sequence of SEQ ID NO: 144; (s) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 147, a CDR2 VH sequence of SEQ ID NO: 148, and a CDR3 VH sequence of SEQ ID NO: 149; and a variable light region comprising a CDR1 VL sequence of SEQ ID NO: 150, a CDR2 VL sequence of SEQ ID NO: 151, and a CDR3 VL sequence of SEQ ID NO: 152; (t) an antibody sharing at least 90% identity to the antibody comprising a variable heavy region comprising a CDR1 VH sequence of SEQ ID NO: 155, a CDR2 VH sequence of SEQ ID NO: 156, and a CDR3 VH sequence of SEQ ID NO: 157; and a variable light region compr
Assignees
Inventors
Classifications
Multivalent vaccine · CPC title
Identification of a linear epitope shorter than 20 amino acid residues or of a conformational epitope defined by amino acid residues · CPC title
Cytomegalovirus · CPC title
Herpetoviridae, e.g. cytomegalovirus, Epstein-Barr virus · CPC title
Antagonist effect on antigen, e.g. neutralization or inhibition of binding · CPC title
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- What does patent US11384137B2 cover?
- Vaccine-derived neutralizing antibodies (NAbs) for CMV infections and small peptides which define precise recognition elements of the antigens by the NAbs. The vaccine-derived NAbs may be produced by immunizing a subject with a gH/gL/UL128/UL130/UL131A pentameric glycoprotein complex (gH/gLPC). The vaccine-derived NAbs may have properties similar or identical to those of NAbs induced in a subje…
- Who is the assignee on this patent?
- Hope City
- What technology area does this patent fall under?
- Primary CPC classification A61K39/12. Mapped technology areas include Human Necessities.
- When was this patent published?
- Publication date Tue Jul 12 2022 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).