A bivalent meningococcal B vaccine in adolescents and young adults

Ostergaard, L.; Vesikari, T.; Absalon, J.; Beeslaar, J.; Ward, B. J.; Senders, S.; Eiden, J. J.; Jansen, K. U.; Anderson, A. S.; York, L. J.; Jones, T. R.; Harris, S. L.; O'Neill, R.; Radley, D.; Maansson, R.; Pregaldien, J. -L.; Ginis, J.; Staerke, N. B.; Perez, J. L.; Belle-Isle, J; Elfassi, E; Fredette, P; Garfield, H; Girard, G; Lachance, P; Adamkova, E; Bartonova, E; Drazan, D; Dvorakova, J; Kosina, P; Kyjonkova, A; Ruzkova, R; Vitousova, E; Ahonen, A; Forsten, A; Karppa, T; Kokko, S; Lagerstrom-Tirri, Pm; Simila, Jk; Adelt, T; Behre, U; Schwarz, Tf; Castiglia, P; Esposito, S; Ferrera, G; Icardi, G; Brzostek, J; Hasiec, B; Konior, R; Pejcz, J; Szymanski, H; Witor, A; Faust, Sn; Finn, Ah; Heath, Pt; Pollard, Aj; Altamirano, Dd; Ashley CT Jr,; Bader, Gf; Bauer GH Jr,; Block SL Jr,; Brandon, Dm; Davis, Mg; Devalle, O; Egelhof, Rh; Essink, Bj; Fouch, Bb; Fox, Bp; Franklin, Er; Garscadden, Ag; Goswami, Up; Gregory, Dm; Helman, Ll; Houchin, Vg; Howard, Ce; Johnson, Ad; Johnston WH Jr,; Jordan, Ca; Kimmel, Ma; Klein, Tr; Krilov, Lr; Labarbera, Ap; Labuda JM II,; Latiolais, Tg; Lello, Lg; Lewis, Dh; Ley, Ja; London, Al; Martin, Ms; Mcguire, Mr; Mosteller, Vc; Naccarato, Tr; Nassim, Cg; Rey, Mr; Robbins, Ra; Rouse, Kg; Schear, Mj; Senders, Sd; Shepard, Js; Simpson, Mw; Slandzicki, Aj; Slechta, Sb; Tetrick, Ll; Varman, M; Wadsworth LT III,; Ware, Db; White, Jh; Wisman PP Jr,; Blouin, F; Dionne, M; Dzongowski, P; Heaton, Kj; Langley, Jm; Mfj, O'Mahony; Powell, Cn; Ward, Bj; Ostergaard, Lj; Haapaniemi, Tl; Paassilta, M; Volanen, Ik; Lepich, T; Smukalska, E; Tarczon, I; Tetiurka, Bm; Domingo, Jd; Morato, Av; Riera, Mt; Sanchez, Ca; Jmr, Torrell; Blumenau, J; Campbell, Ng; Cervantes, Ja; Douglas, Wg; Ensz, Dj; Ervin, Je; Fiel, Tc; Fragoso, Vg; Fried, Dl; Gleason, Gp; Green, Sl; Haggag, Az; Johnson, Ct; Khaira, Rs; Kirstein, Jl; Kravitz, Ae; Lederman, Sn; Marcadis, I; Miller, Ve; Moretti, Jm; Pragalos, Aa; Puopolo, Ad; Rubino, J; Seiden, Dj; Sharp, Sc; Sheldon, Ea; Shockey, Gr; Smith, Wb; Stringer, Jc; Strout, Cb; Studdard, He; Tresser, Njl.

doi:10.1056/NEJMoa1614474

BACKGROUND MenB-FHbp is a licensed meningococcal B vaccine targeting factor H-binding protein. Two phase 3 studies assessed the safety of the vaccine and its immunogenicity against diverse strains of group B meningococcus. METHODS We randomly assigned 3596 adolescents (10 to 18 years of age) to receive MenB-FHbp or hepatitis A virus vaccine and saline and assigned 3304 young adults (18 to 25 years of age) to receive MenB-FHbp or saline at baseline, 2 months, and 6 months. Immunogenicity was assessed in serum bactericidal assays that included human complement (hSBAs). We used 14 meningococcal B test strains that expressed vaccine-heterologous factor H-binding proteins representative of meningococcal B epidemiologic diversity; an hSBA titer of at least 1:4 is the accepted correlate of protection. The five primary end points were the proportion of participants who had an increase in their hSBA titer for each of 4 primary strains by a factor of 4 or more and the proportion of those who had an hSBA titer at least as high as the lower limit of quantitation (1:8 or 1:16) for all 4 strains combined after dose 3. We also assessed the hSBA responses to the primary strains after dose 2; hSBA responses to the 10 additional strains after doses 2 and 3 were assessed in a subgroup of participants only. Safety was assessed in participants who received at least one dose. RESULTS In the modified intention-to-treat population, the percentage of adolescents who had an increase in the hSBA titer by a factor of 4 or more against each primary strain ranged from 56.0 to 85.3% after dose 2 and from 78.8 to 90.2% after dose 3; the percentages of young adults ranged from 54.6 to 85.6% and 78.9 to 89.7%, after doses 2 and 3, respectively. Composite responses after doses 2 and 3 in adolescents were 53.7% and 82.7%, respectively, and those in young adults were 63.3% and 84.5%, respectively. Responses to the 4 primary strains were predictive of responses to the 10 additional strains. Most of those who received MenB-FHbp reported mild or moderate pain at the vaccination site. CONCLUSIONS MenB-FHbp elicited bactericidal responses against diverse meningococcal B strains after doses 2 and 3 and was associated with more reactions at the injection site than the hepatitis A virus vaccine and saline. (Funded by Pfizer; ClinicalTrials.gov numbers, NCT01830855 and NCT01352845.).

A bivalent meningococcal B vaccine in adolescents and young adults

Ostergaard L.;Vesikari T.;Absalon J.;Beeslaar J.;Ward B. J.;Senders S.;Eiden J. J.;Jansen K. U.;Anderson A. S.;York L. J.;Jones T. R.;Harris S. L.;O'Neill R.;Radley D.;Maansson R.;Pregaldien J. -L.;Ginis J.;Staerke N. B.;Perez J. L.;Belle-Isle J;Elfassi E;Fredette P;Garfield H;Girard G;Lachance P;Adamkova E;Bartonova E;Drazan D;Dvorakova J;Kosina P;Kyjonkova A;Ruzkova R;Vitousova E;Ahonen A;Forsten A;Karppa T;Kokko S;Lagerstrom-Tirri PM;Simila JK;Adelt T;Behre U;Schwarz TF;Castiglia P;Esposito S;Ferrera G;Icardi G;Brzostek J;Hasiec B;Konior R;Pejcz J;Szymanski H;Witor A;Faust SN;Finn AH;Heath PT;Pollard AJ;Altamirano DD;Ashley CT Jr;Bader GF;Bauer GH Jr;Block SL Jr;Brandon DM;Davis MG;DeValle O;Egelhof RH;Essink BJ;Fouch BB;Fox BP;Franklin ER;Garscadden AG;Goswami UP;Gregory DM;Helman LL;Houchin VG;Howard CE;Johnson AD;Johnston WH Jr;Jordan CA;Kimmel MA;Klein TR;Krilov LR;LaBarbera AP;Labuda JM II;Latiolais TG;Lello LG;Lewis DH;Ley JA;London AL;Martin MS;McGuire MR;Mosteller VC;Naccarato TR;Nassim CG;Rey MR;Robbins RA;Rouse KG;Schear MJ;Senders SD;Shepard JS;Simpson MW;Slandzicki AJ;Slechta SB;Tetrick LL;Varman M;Wadsworth LT III;Ware DB;White JH;Wisman PP Jr;Blouin F;Dionne M;Dzongowski P;Heaton KJ;Langley JM;O'Mahony MFJ;Powell CN;Ward BJ;Ostergaard LJ;Haapaniemi TL;Paassilta M;Volanen IK;Lepich T;Smukalska E;Tarczon I;Tetiurka BM;Domingo JD;Morato AV;Riera MT;Sanchez CA;Torrell JMR;Blumenau J;Campbell NG;Cervantes JA;Douglas WG;Ensz DJ;Ervin JE;Fiel TC;Fragoso VG;Fried DL;Gleason GP;Green SL;Haggag AZ;Johnson CT;Khaira RS;Kirstein JL;Kravitz AE;Lederman SN;Marcadis I;Miller VE;Moretti JM;Pragalos AA;Puopolo AD;Rubino J;Seiden DJ;Sharp SC;Sheldon EA;Shockey GR;Smith WB;Stringer JC;Strout CB;Studdard HE;Tresser NJL.

2017-01-01

Abstract

BACKGROUND MenB-FHbp is a licensed meningococcal B vaccine targeting factor H-binding protein. Two phase 3 studies assessed the safety of the vaccine and its immunogenicity against diverse strains of group B meningococcus. METHODS We randomly assigned 3596 adolescents (10 to 18 years of age) to receive MenB-FHbp or hepatitis A virus vaccine and saline and assigned 3304 young adults (18 to 25 years of age) to receive MenB-FHbp or saline at baseline, 2 months, and 6 months. Immunogenicity was assessed in serum bactericidal assays that included human complement (hSBAs). We used 14 meningococcal B test strains that expressed vaccine-heterologous factor H-binding proteins representative of meningococcal B epidemiologic diversity; an hSBA titer of at least 1:4 is the accepted correlate of protection. The five primary end points were the proportion of participants who had an increase in their hSBA titer for each of 4 primary strains by a factor of 4 or more and the proportion of those who had an hSBA titer at least as high as the lower limit of quantitation (1:8 or 1:16) for all 4 strains combined after dose 3. We also assessed the hSBA responses to the primary strains after dose 2; hSBA responses to the 10 additional strains after doses 2 and 3 were assessed in a subgroup of participants only. Safety was assessed in participants who received at least one dose. RESULTS In the modified intention-to-treat population, the percentage of adolescents who had an increase in the hSBA titer by a factor of 4 or more against each primary strain ranged from 56.0 to 85.3% after dose 2 and from 78.8 to 90.2% after dose 3; the percentages of young adults ranged from 54.6 to 85.6% and 78.9 to 89.7%, after doses 2 and 3, respectively. Composite responses after doses 2 and 3 in adolescents were 53.7% and 82.7%, respectively, and those in young adults were 63.3% and 84.5%, respectively. Responses to the 4 primary strains were predictive of responses to the 10 additional strains. Most of those who received MenB-FHbp reported mild or moderate pain at the vaccination site. CONCLUSIONS MenB-FHbp elicited bactericidal responses against diverse meningococcal B strains after doses 2 and 3 and was associated with more reactions at the injection site than the hepatitis A virus vaccine and saline. (Funded by Pfizer; ClinicalTrials.gov numbers, NCT01830855 and NCT01352845.).