Novel Flu Vaccines Lots of choices

Novel Flu Vaccines Lots of choices Universal M2 ectodomain (A types, only) Universal HA cleavage site (A and B types) HA made by rdna methods (not eggs or mammalian cells) Vectored delivery of HA genes T cell vaccines to conserved internal proteins Engineered influenza viruses (NS1)

HA Based Vaccines Protein Sciences: HA in insect cells (baculo) Novavax: HA NA M1 VLPs in insect cells VaxInnate: HA globular head fused to flagellin Vical: Formulated plasmid DNA AlphaVax: HA expressed in alphavirus vector Hawaii Biotech: insect cell VLPs Frauenhofer & Medicago: VLPs in tobacco leaves Monoclonal antibody based vaccines

Live virus approaches Green Hills: Live attenuated NS1 mods Vivaldi: Live attenuated NS1 mutants BioDiem: Leningrad 57 Live attenuated Medimmune AZ: Flumist (NIAID) Vaxin: Adenovirus vector, nasal delivery Vaxart: Adenovirus vector capsule delivery of antigen and TLR3 dsrna

M2e Vaccines Merck (M2e plus cleavage site) OMPC, alum, Iscomatrix (QS21) Acambis (M2e x3 on HBcAg, alum, QS21) Dynavax (M2e x8 fused to NSP+CpG) VaxInnate (M2e x4 fused to flagellin)

M2e The ectodomain of M2 presented as a homotetramer ion channel. Note that no true 3D structure has been determined for M2e

Spectrum of M2e Sequences 3 of the recent HIN1 isolates: TEVETPTRSEWECRCSDSSDP TEVETPTRSEWECRCSDSSDP TEVETPTRSEWECRCSDSSDP H1/H2/H3 consensus SLLTEVETPIRNEWGSRSNDSSDP A/New Caledonia/20/99 H1N1 human SLLTEVETPIRNEWGCRCNDSSDP A/Aichi/470/68 H3N1 human SLLTEVETPIRNEWGCRCNDSSDP A/Ann Arbor/6/60 H2N2 human SLLTEVETPIRNEWGCRCNDSSDP A/Berkeley/1/68 H2N2 human SLLTEVETPIRNEWGCRCNDSSDP A/Puerto Rico/8/34 H1N1 human SLLTEVETPIRNEWGCRCNGSSDP A/Wisconsin/3523/88 H1N1 human SLLTEVETPIRNEWGCKCNDSSDP A/Hebei/19/95 H3N2 human SLLTEVETPIRNEWECRCNGSSDP A/Swine/2009 H1N1 human SLLTEVETPTRSEWECRCSDSSDP H5 consensus SLLTEVETPTRNEWESRSSDSSDP A/Viet Nam/1203/2004 H5N1 human SLLTEVETPTRNEWECRCSDSSDP A/Chicken/Nakorn- Patom/Thailand H5N1 avian SLLTEVETPTRNEWECRCSDSSDP A/Thailand/1(KAN-1)/04 H5N1 avian SLLTEVETPTRNEWECRCSDSSDP A/Duck/1525/81 H5N1 avian SLLTEVETPTRNGWECKCSDSSDP A/Hong Kong/156/97 H5N1 human SLLTEVETLTRNGWGCRCSDSSDP A/Chicken/New York/95 H7N2 avian SLLTEVETPTRNGWECKCSDSSDP A/Chicken/Hong Kong/G9/97 H9N2 avian SLLTEVETPTRNGWGCRCSGSSDP A/Hong Kong/1073/99 H9N2 human SLLTEVETLTRNGWECKCRDSSDP

Acambis HBcAg Three copies in tandem presented on HepB core antigen

TLR2, OMPC, Merck M2e peptides chemically conjugated to outer membrane complex from N. meningitidis

TLR5, flagellin, VaxInnate Four copies of the M2e sequence fused to the sequence of flagellin

TLR9, CpG Eight copies of the M2e sequence fused to the NP protein and conjugated to CpG containing oligonucleotide

Bacteriophage Q, Cytos M2e sequence displayed on the phage Qβ

Innate Immune Responses are Mediated by Toll like Receptors Expressed on the Surface of Immune Cells Toll Like Receptors Recognize Pathogen Associated Patterns (PAMPs) 12 VaxInnate s current influenza vaccines incorporate flagellin, a TLR5 ligand, and only well studied protein agonist

PAMP TLR Endoplasmic Reticulum IL 12 T H 1 Endocytic PRR CD80/86 CD28 Pathogen Phagosome MHC I or II TCR T Cell Dendritic Cell Nucleus T H 2

Influenza Vaccines Importance of Fusion to Flagellin Conventional Adjuvants Ag specific immune response Excessive inflammatory response Non specific immune response Autoimmune response Ag specific immune response Minimal inflammatory response VaxInnate s vaccines = antigen 14 Genetic Fusions of the Vaccine Antigen and TLR Ligand Efficiently Stimulate both the Innate and Adaptive Immune Systems and Mimic Natural Infection.

VAX102: Low Dose & Alternative Routes Longitudinal anti M2e Responses for Doses Spanning 0.03 to 10 mg 3.50 3.00 10 ug 0.3 ug Anti-M2e Geometric Mean Titers ug/ml anti-m2e IgG 2.50 2.00 1.50 1.00 3 ug 1ug 0.1 ug (IM) 0.1 ug (ID) 0.03 ug (IM) 0.03 ug (ID) 0.50 cutoff 0.00 Dy 0 Dy 7 Dy 14 Dy 28 Dy 35 Dy 42 Dy 60 Dy 120 Dy 180 Low doses of VAX102 delivered on days 0 and 28 elicit robust anti M2e titers that remain above the positive cutoff for 6 months 15 Note good prime and especially the boost after the day 28 dose. Boost is not affected by flagellin antibody raised by the prime

Other Conserved Antigens Stalk cleavage site Stalk straight alpha helix Headless stalk Matrix, NP as T cell targets

Influenza Vaccine HA Subunit Vaccine Design HA Globular Head Flagellin HA Trimer HA Monomer Fusion of HA globular head (HA1 2) and S. typhimurium flagellin type 2 (STF2) [a TLR5 ligand] to form STF2.HA1 2 VaxInnate's HA subunit vaccines can be produced in E.coli 17

HA Cleavage Site, Merck Re drawn from Bianchi, et al., ref 26

Peter Palese, Adolfo Garcia Sastre, Mount Sinai

Broadly Neutralizing Monoclonals 2008 2009, Crucell and NIH broadly neutralizing antibodies (both the same germline sequence) binding to stalk (fusion intermediate) Bommakanti, et al (Nehru Crucell Merck) antigen designed from MAb binding site 2011, Corti et al., stalk binding monoclonal FI6 Eikert, et al, Group 2 stalk binding monoclonal

Corti, et al, Science, 2011

How do you turn a MAb into a vaccine? Passive protection, 4 10 mgs/kg reported At catalog price for Synagis (RSV antibody, premature infants) one dose for a 100 kg vaccine developer is $20,000 Use MAb binding site as target antigen Will require full clinical development program since no correlate of protection exists for the target (such as HAI)

Bommakanti et al

What Matters in a Pandemic? TIME! Time to make seed stock Time to build biomass Time to produce antigen Time to harvest purify (doses per unit time) Time to test for release of bulk Time to package and release Time to ship

What Matters? Time to last dose to cover intended population Time to first dose is false comfort Swimming pool analogy (how long to fill?) Garden hose Fire hose It s all about throughput and getting out of eggs, the biological bottleneck!

Virus Like Particles, Tobacco Landry et al. Medicago

Virus Like Particles made in insect cells

Vectored Gene Delivery Vaxin, replication deficient adenovirus vectors expressing HA, delivered intranasally Vaxart, replication deficient adenovirus vectors expressing HA plus dsrna (TLR3), delivered via oral capsule MVA expressing conserved conserved antigens Inovio, electroporation of plasmid DNA Vical, injection of formulated DNA

Engineered Influenza Viruses (Palese Lab, Mt Sinai) Nine segment virus (two different HA genes) Reassortment incompetent viruses NS1 modifications (Palese, AVIR Green Hills) NS1 encodes an inhibitor of poly adenylated RNA Also encodes a viral rnp export protein Interferes with interferon response of infected cell

Seasonal Vaccines VAX125 Immunogenicity in Man Phase I Clinical Evaluation Prototype (one component) seasonal influenza vaccine, VAX125: Dose response of antibody formulation in adults 18 45 years of age 1000 800 Antibody Titer 600 400 200 0 0 7 14 21 28 35 42 Day 180 3-8 2 1 0.5 0.1-0.3 Placebo Dose (ug) 34 Immunogenicity for doses of 1 µg or above is excellent in healthy adults (18 45 years old)

Whole Virion and Adjuvanted Split Virus Immune Response Immune response to single dose whole virion (WV, Baxter, 7.5 ug) and ASO3 adjuvanted split virus (ASO3, GSK, 3.75 ug) H1N1 CA7/2009 vaccine in different age groups Whole virion ASO3 adjuvanted 18 44 45 64 65 18 44 45 64 65 n=70 n=68 n=34 n=70 n=68 n=37 GMT day 0 7 5 5 7 6 5 GMT day 21 92 24 21 416 116 41 MFR 14 5 4 60 20 8 SP % 71 39 32 94 77 51 SC % 63 36 29 88 74 51 from Nicholson et al. Lancet Infectious Diseases 2010 Adjuvanted vaccine is more immunogenic, but performance in the elderly is modest 35

VAX 125 HAI Response in the Elderly Peak GM HAI response 14 days after VAX125 among subjects 65 years old (left panel). GM HAI titers measured from day 0 to 28 after a single dose of VAX125 ranging from 0.5 to 8 µg among subjects 65 years old (right panel) HAI Titers (GMT+95%CI) 500 400 300 200 100 0 0.5 1 2 3 5 8 Dose (ug) HAI titer (SI) 250 200 150 100 50 0 0 7 14 21 28 35 Day 8 5 3 2 1.5 Elderly adults respond to higher vaccine doses 36

HA Subunit Vaccines Development of Alternative Vaccine Formats D0 D0 D0 D1 D3 D2 D1 D2 D2 D1 C Term = A (Antigen Attached to C terminus) R3 = B (Antigen Replaces D3 Domain) R3.2x = C (2 Antigens Fused to Flagellin) Alternative vaccine formats, which differ in the point of antigen attachment to flagellin were developed, initially, to improve the potency of poorly immunogenic H5 HA vaccines 37

VAX128 02 HAI Response Serum HAI response for VAX128C in VAX128 02 VAX128C dose (µg) 1.25 (n=47) 2.5 (n=50) Total (n=97) GMT 95% C.I. GMT 95% C.I. GMT 95% C.I. GMT Day 0 16 11 23 26 15 43 20 14 28 GMT Day 21 306 187 502 478 290 789 385 272 546 Mean fold resp. 20 12 33 19 11 31 19 13 27 % % % Seroconversion 79 64 89 80 66 90 79 70 87 Seroprotection 89 77 97 94 94 99 92 84 96 38

VAX 128C GMT HAI, SC & SP HAI titers, Seroconversion (SC) and Seroprotection (SP) rates after a single IM dose of VAX128C (CA07) Age group 18 49 50 64 Total Dose (µg) 1.25 2.5 1.25 2.5 n= 36 38 12 12 98 GMT HAI day 0 15 31 16 16 20 GMT HAI day 21 314 574 339 269 393 Mean fold response 21 19 21 17 20 Seroconversion % 81 79 75 83 80 Seroprotection % 89 95 92 91 92 39

VaxInnate s E. Coli Based Manufacturing High Efficiency & Large Capacity Manufacturing Influenza Vaccine for the US Substrate Cost of Recently Built Facilities (without validation) Time to build and Validate New Facility Annual Capacity (TIV) Eggs $150 million > 3 years 100 million Cell Culture $680 million > 3 years 50 Million Baculovirus $40 million > 2 years 100 Million E. coli/vaxinnate $0 (CMO) 0 years 100 400 million* *VaxInnate's capacity is based on performing a single 1,000 liter run for each antigen included in the vaccine. Yields differ by antigen and construct. 40

What s Next? New vaccines will face long and expensive development programs (efficacy based) HA based vaccines have advantage of correlate of protection (HAI) Current low incidence of flu (infant vax?) makes trial size much larger US universal recommendation makes placebo trial impossible, go somewhere else? Major focus on better vaccine for elderly