| Literature DB >> 28792942 |
Silvia Capucci1,2, Edmund G Wee1, Torben Schiffner3, Celia C LaBranche4, Nicola Borthwick1, Albert Cupo5, Jonathan Dodd3, Hansi Dean6, Quentin Sattentau3, David Montefiori4, Per J Klasse5, Rogier W Sanders5,7, John P Moore5, Tomáš Hanke1,8.
Abstract
Rabbits and monkeys immunized with HIV type 1 (HIV-1) native-like BG505 SOSIP.664 (BG505s) glycoprotein trimers are known to induce antibodies that can neutralize the autologous tier-2 virus. Here, we assessed the induction of HIV-1 trimer binding and neutralizing antibody (nAb) titres when BG505s trimers were also delivered by non-replicating simian (chimpanzee) adenovirus and non-replicating poxvirus modified vaccinia virus Ankara (MVA) vaccine vectors. First, we showed that approximately two-thirds and one-third of the trimers secreted from the ChAdOx1.BG505s (C) and MVA.BG505s (M) vaccine-infected cells, respectively, were cleaved and in a native-like conformation. Rabbits were immunized intramuscularly with these vaccine vectors and in some cases boosted with ISCOMATRIX™-adjuvanted BG505s protein trimer (P), using CCC, MMM, PPP, CPP, MPP and CMP vaccine regimens. We found that the peak trimer-binding antibody and tier-1A and autologous tier-2 nAb responses induced by the CC, CM, PPP, CPP, MPP and CMP regimens were comparable, although only PPP induced autologous tier-2 nAbs in all the immunized animals. Three animals developed weak heterologous tier-2 nAbs. These results demonstrate that ChAdOx1 and MVA vectors are useful delivery modalities for not only T-cell, but also antibody vaccine development.Entities:
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Year: 2017 PMID: 28792942 PMCID: PMC5549892 DOI: 10.1371/journal.pone.0181886
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Fig 1Expression of BG505s trimers in tissue culture.
(A) Monolayers of HEK 293T cells were infected with ChAdOx1.BG505s at the indicated MOIs for 48 h. The proteins in the tissue culture supernatants were separated by non-denaturing polyacrylamide gel electrophoresis and transferred onto a nitrocellulose membrane. BG505 Env proteins were detected using the glycan-specific 2G12 mAb as the primary antibody. As a positive control, supernatant from a HEK 293T stable cell line that expresses fully cleaved BG505s trimers was analysed in the first lane. The relative molecular masses of 600 and 450 kDa are indicated. (B) To assess the percentage of correctly folded trimers in the ChAdOx1.BG505s- and MVA.BG505s-infected cell culture supernatants, the ELISA plates were first coated with either 2G12 or PGT151 Env-specific bnAbs and the captured native-like, furin-cleaved trimers were detected using PGT145 as the secondary mAb. To generate the standard curve used for trimer quantification (top), gp140 monomers and trimers purified from stably transfected cells were mixed at different ratios, but at a constant total concentration. The latter values were determined using a different, non-trimer specific capture ELISA (see Methods section). The percentages of native-like BG505s trimer present in the virus-infected cell culture supernatants are shown for the indicated antibody combinations (bottom).
Fig 2Kinetics of BG505s trimer-binding antibody responses induced in rabbits by various immunization regimens.
(A) Groups of 5 rabbits were immunized with ChAdOx1.BG505s (C), MVA.BG505s (P) and ISCOMATRIX™-adjuvanted BG505s protein trimer (P) candidate vaccines, as depicted. The animals were immunized at weeks 0, 8 and 24 (arrows), and bled regularly. (B) Reciprocal endpoint titres of the BG505s trimer-binding antibodies in rabbit sera were determined by capture ELISA. The trimer-binding antibody titres at each time point are shown for individual rabbits, and the median values for group-peak time points are shown above each peak. Note that the time points at which the peak titres were measured differed among the rabbits in each group, and that some rabbits died for protocol-unrelated reasons (S1 Table).
Peak reciprocal anti-trimer Ab end-point titres in rabbit sera, ranked by immunization group.
| Rank | Regimen | Median | Range | n |
|---|---|---|---|---|
| 1 | CMP | 161300 | 58900–179400 | 4 |
| 2 | CPP | 158700 | 88400–285600 | 4 |
| 3 | CM | 141900 | 23700–287500 | 5 |
| 4 | CP | 90200 | 40300–133600 | 4 |
| 5 | MPP | 87000 | 21600–210200 | 4 |
| 6 | PPP | 69400 | 52300–287500 | 5 |
| 7 | PP | 63600 | 41600–98500 | 5 |
| 8 | MP | 22800 | 10500–49600 | 4 |
| 9 | CC | 16000 | 9200–16700 | 4 |
| 10 | C | 6300 | 1600–17300 | 13 |
| 11 | CCC | 4200 | 400–9400 | 4 |
| 12 | MM | 3400 | 100–6400 | 4 |
| 13 | MMM | 3300 | 100–7000 | 3 |
| 14 | P | 3100 | 1100–7000 | 5 |
| 15 | M | 100 | 0–1000 | 9 |
Neutralization of tier-1 and tier-2 viruses in TZM-bl cell assay.
| Tier 1A | Tier 2 | ||||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Clade B | Clade C | Clade A | Clade C | Clade B | CRF07 BC | Clade B | Clade C | Clade AC | CRF07 BC | Clade A | CRF01 AB | ||||
| Regimen | Animal ID | Bleed Week | Negative Control | MN.3 | MW965.26 | BG505ΔCT/T332N | 25710–2.43 | TRO.11 | BJOX002000.03.2 | X1632-S2-B10 | Ce1176 A3 | 246-F3 C10 2 | CH119.10 | Ce703010217 B6 | CNE55 |
| M17 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| M19 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| M23 | 10 | 34 | 40 | 32 | 32 | 28 | 35 | 28 | 35 | 40 | 27 | 24 | |||
| F2 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| F21 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||
| M17 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||
| M19 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||
| M23 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||
| F2 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| M8 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |
| F20 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||
| F31 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||
| M10 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| M12 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| M27 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| F4 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||||
| F13 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||
| M7 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| F5 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||||
| F6 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| F22 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||
| M9 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| M15 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| M18 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||||
| F29 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||
| M11 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| F1 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| F3 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| F26 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| M16 | 10 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||
| M11 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||
| F1 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| F3 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| F26 | 26 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | ||||
| median | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | <20 | |||||
a—Values are the serum dilution at which relative luminescence units (RLUs) were reduced 50% compared to virus control wells (no test sample). Highlighted bold values are considered positive for neutralization based on the criterion of signal ≤3x the signal of that sample against the MLV-pseudotyped negative-control virus.
Antibody recognition of glycan holes.
| Regimen | Animal ID | Bleed Week | BG505ΔCT T332N | BG505ΔCT T332N.S241N | BG505ΔCT T332N.P291T | BG505ΔCT T332N.S241N.P291T |
|---|---|---|---|---|---|---|
| M17 | 26 | nd | nd | nd | nd | |
| M19 | 26 | <20 | nd | nd | nd | |
| M23 | 26 | <20 | <20 | <20 | <20 | |
| F2 | 26 | <20 | <20 | <20 | <20 | |
| M8 | 26 | <20 | <20 | <20 | <20 | |
| F20 | 26 | <20 | <20 | <20 | <20 | |
| F31 | 26 | |||||
| M10 | 26 | <20 | <20 | <20 | ||
| M12 | 26 | |||||
| M27 | 26 | <20 | <20 | <20 | <20 | |
| F4 | 26 | <20 | <20 | |||
| F13 | 26 | <20 | <20 | <20 | <20 | |
| M7 | 26 | <20 | nd | nd | nd | |
| F5 | 26 | |||||
| F6 | 26 | |||||
| F22 | 26 | <20 | <20 | <20 | <20 | |
| M9 | 26 | |||||
| M15 | 26 | <20 | <20 | <20 | <20 | |
| M18 | 26 | <20 | <20 | <20 | ||
| F29 | 26 | |||||
| M11 | 26 | <20 | <20 | <20 | <20 | |
| F1 | 26 | <20 | <20 | <20 | <20 | |
| F3 | 26 | |||||
| F26 | 26 | <20 | <20 | <20 |
a—Values are the serum dilution at which relative luminescence units (RLUs) were reduced 50% compared to virus control wells (no test sample). Highlighted bold values are considered positive for neutralization based on the criterium of signal ≤3x the signal of that sample against the MLV-pseudotyped negative-control virus;
b—animals neutralized 2 to 3 tier-2 viruses (Table 2); nd—not done due to lack of sample.