An Exploration to Determine if Fab Molecules are Efficacious in Neutralizing Influenza H1 and H3 Subtypes. Nick Poulton June September 2012
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1 An Exploration to Determine if Fab Molecules are Efficacious in Neutralizing Influenza H1 and H3 Subtypes Nick Poulton June September 2012
2 Epidemiology of Influenza Infection Causes between 250,000 and 500,000 deaths worldwide each year [1] Increasing resistance to oseltamivir (TAMIFLU ), a neuraminidase inhibitor [2] With constant mutations to the virus, there is an increasing risk of an influenza pandemic g/diseases/d_influenza.htm&do cid=tedfrg0xr0awnm&imgurl = g/diseases/influenza/6-
3 Influenza Virus Structure/Life Cycle um=10&hl=en&safe=active&tbo=d&biw=1600& bih=671&tbm=isch&tbnid=cmvjosu- Hemagglutinin (HA) is the predominant protein protruding from the viral surface Binds to 2,6 sialic acid receptor on human cells Virus releases its contents into the cell and replicates
4 Hemagglutinin Subtypes bakerinstitute.vet.cornell.edu Thompson et al. (2004)- H3 viruses are important targets in the present Wang et al. (2010)- H1 viruses are also important targets in the present Le et al. (2007)- H5 viruses (avian flu) represent a serious threat of a pandemic Ekiert et al. (2009)- Targeting conserved epitopes on HA will increase the range and duration of efficacy
5 Antibody Therapies for Influenza n/iggdomains/1igt_domains. Monoclonal antibody (Mab) Identical copies of a specific antibody produced by a single B cell clone High specificity for particular antigens Neutralize viruses Fab- Fragment antigen binding has not been tested for neutralization activity
6 Phage Display Technology Phage-display technology intends for Fabs to be produced in the bacteria, purified, and then tested However, there has been some observed disconnect between the activity of mabs and Fabs As a result, the testing of Fabs is often skipped over and Mabs are directly produced Testing with Fabs is much quicker and cheaper Using Fabs would allow for many more antibodies to be tested groups/biomacromolecules/protocols/ eth&docid=pkjvkd4xy_-
7 Research Aim Determine how Fabs neutralize influenza in relation to Mabs Assess the potential of Fabs to be used as an intermediate step in antibody development to increase the number of antibodies tested Assess the potential of Fabs to be used as a prophylactic or therapeutic treatment for Influenza in vivo
8 Methods: Preparation of Fab-Encoding Constructs BlpI + XbaI Digestion Fab Encoding Segment Myc-His Tagged Vector
9 Production of Fabs Transformation of DH5- E. coli bacteria Large scale cultures Maxi-Prep to purify DNA Large scale cultures Electroporation of TGIF- E. coli Analysis of constructs Induction with IPTG to induce Fab production Fab Purification using cobalt resin Analysis of purified Fab via Western Blot and Coomassie Stain Microneutralization Assay Immunofluorescence Assay of Fab Binding
10 Analyses of Purified Fabs Western Blot Coomassie Stain
11 Immunofluorescence Assay Results PA-2 Fab + A/Wisconsin/67/05 UFab-6 + A/Wisconsin/67/05 PA-2 Fab + A/Wyoming/03/2003 UFab-6 + A/Wyoming/03/2003
12 H3 Neutralization Assay Results PA-2 Mab PA-2 Fab Virus Back Titration PBS (No Virus) Uninfected (bottom row) A/Hong Kong/1/1968 (2:6) (H3)
13 H3 Neutralization Assay Results UFab-2 UFab-3 PA-3 Mab UMab-1 UFab-1 UMab-2 Uninfected (bottom row) A/Hong Kong/1/1968 (2:6) (H3)
14 H3 Neutralization Assay Results UFab-6 UFab-7 PBS (no virus) Uninfected A/Hong Kong/1/1968 (2:6) (H3)
15 H1 Neutralization Assay Results UFab-4 UFab-5 UFab-2 Uninfected A/Fort Monmouth/1/1947 (H1)
16 Fabs Show Promise in Neutralization Fab neutralization > Mab neutralization Other Fabs, including UFab-2, showed better neutralization in the Fab form than in the Mab form Fab neutralization = Mab neutralization Certain Fabs, including PA-2 Fab, neutralize similarly in the Mab and Fab form Mab neutralization > Fab neutralization However, UMab- 1 neutralized better in the Mab form than in the Fab form
17 Future Research In order to fully understand the difference between neutralization by Mabs and Fabs a. More antibodies must be tested b. Must be tested against a greater number of subtypes and strains However, these preliminary results suggest that Fabs have great potential to neutralize certain viruses
18 Bibliography [1] Thompson WW, et al. (2004) Influenza-associated hospitalizations in the United States. JAMA 292: [2] Le QM, Kiso M, Someya K, Sakai YT, Nguyen TH, et al. (2005) Avian flu: Isolation of drug-resistant H5N1 virus. Nature 437: [3] O Donnell CD, et al. (2012) Antibody pressure by a human monoclonal antibody targeting the 2009 pandemic H1N1 virus hemagglutinin drives the emergence of a virus with increased virulence in mice. mbio 3(3):e doi: /mbio [4] Crowe JE, Jr. (2012) Influenza virus resistance to human neutralizing antibodies. mbio 3(4):e doi: /mbio [5] Wei CJ, et al. (2010) Induction of broadly neutralizing H1N1 influenza antibodies by vaccination. Science (New York, N.Y.) : [6] Whittle JRR, et al. (2011) Broadly neutralizing human antibody that recognizes the receptor-binding pocket of influenza virus hemagglutinin. Proceedings of the National Academy of Sciences of the United States of America (2011) : [7] Ekiert DC, Wilson IA. (2012) Broadly neutralizing antibodies against influenza virus and prospects for universal therapies. Current Opinion in Virology 2.2 (2012) : [8] Samji T. (2009) Influenza A: Understanding the Viral Life Cycle. Yale Journal of Biology and Medicine. 82(4): [9] Kashyap AK, et al. (2008) Combinatorial antibody libraries from survivors of the Turkish H5N1 avian influenza outbreak reveal virus neutralization strategies. Proceedings of the National Academy of Sciences of the United States of America : [10] Simmons CP, Bernasconi NL, Suguitan AL, Mills K, Ward JM, et al. (2007) Prophylactic and therapeutic efficacy of human monoclonal antibodies against H5N1 influenza. PLoS Med 4(5): e178. doi: /journal.pmed [11] Burioni R, et al. (2010) Monoclonal antibodies isolated from human B cells neutralize a broad range of H1 subtype influenza A viruses including swineorigin Influenza virus (S-OIV). Virology 399.1: [12] Ekiert DC, et al. (2009) Antibody recognition of a highly conserved influenza virus epitope. Science : [13] Staneková Z, and Varečková E. (2010) Conserved epitopes of influenza A virus inducing protective immunity and their prospects for universal vaccine development. Virology Journal 7.1: 351. [14] Yoshida R, Igarashi M, Ozaki H, Kishida N, ToMabechi D, et al. (2009) Cross-Protective Potential of a Novel Monoclonal Antibody Directed against Antigenic Site B of the Hemagglutinin of Influenza A Viruses. PLoS Pathog 5(3): e doi: /journal.ppat [15] Grandea AG, Olsen OA, et al. (2010) Human antibodies reveal a protective epitope that is highly conserved among human and nonhuman influenza A viruses. (2010) : n. pag. Print. [16] Wang TT, Tan GS, Hai R, Pica N, Petersen E, et al. (2010) Broadly Protective Monoclonal Antibodies against H3 Influenza Viruses following Sequential Immunization with Different Hemagglutinins. PLoS Pathog 6(2): e doi: /journal.ppat [17] Corti D, et al. (2011) A Neutralizing Antibody Selected from Plasma Cells That Binds to Group 1 and Group 2 Influenza A Hemagglutinins. n. pag. Print. [18] Clementi N, De Marco D, Mancini N, Solforosi L, Moreno GJ, et al. (2011) A Human Monoclonal Antibody with Neutralizing Activity against Highly Divergent Influenza Subtypes. PLoS ONE 6(12): e doi: /journal.pone [19] Sui J, Hwang WC, Perez S, Wei G, et al. (2009) Structural and functional bases for broad-spectrum neutralization of avian and human influenza A viruses. Nature structural & molecular biology 16.3: [20] The Centers for Disease Control. (2006) Influenza : Propagation, Quantification Print. [21] Krammer F, Margine I, Tan GS, Pica N, Krause JC, et al. (2012) A Carboxy-Terminal Trimerization Domain Stabilizes Conformational Epitopes on the Stalk Domain of Soluble Recombinant Hemagglutinin Substrates. PLoS ONE 7(8): e doi: /journal.pone [22] Tan GS, et al. (2012) A pan-h1 anti-hemagglutinin monoclonal antibody with potent broad-spectrum efficacy in vivo. Journal of Virology 86.11: [23] Han T, and Marasco WA. (2011) Structural basis of influenza virus neutralization. Annals Of The New York Academy Of Sciences 1217:
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