Immunogenicity and reactogenicity of BNT162b2 booster in ChAdOx1-S-primed participants (CombiVacS): a multicentre, open-label, randomised, controlled, phase 2 trial

Borobia, Alberto M.; Carcas, Antonio J.; Pérez‐Olmeda, Mayte; Castaño, Luís; Bertrán, María Jesús; García-Pérez, Javier; Campins, M.; Portolés, Antonio; González-Pérez, María Alejandra; Morales, María Teresa García; Arana-Arri, Eunate; Aldea, Marta; Díez-Fuertes, Francisco; Fuentes, Inmaculada; Ascaso, Ana; Lora, David; Imaz-Ayo, Natale; Barón-Mira, Lourdes E; Agustí, Antònia; Pérez-Ingidua, Carla; Cámara, Agustı́n Gómez de la; Arribas, José Ramón; Ochando, Jordi; Alcamı́, José; Belda-Iniesta, Cristóbal; Frías, Jesús; Soto, Lucía Martínez de; Mariblanca, Amelia Rodríguez; García, Lucía Díaz; Ramírez, Elena; Meseguer, Enrique Seco; Stewart, Stefan; Candón, Alicia Marín; García, Irene García; Urroz, Mikel; Villatoro, Jaime Monserrat; Rosa, Paula de la; García, Marta Sanz; Crespo, Cristina López; Martínez, Vega Mauleón; Castell, Raquel de Madariaga; Vara, Laura Vitón; Rodríguez, Julio García; Buño, Antonio; Granados, Eduardo López; Cámara, Carmen; Cuevas, Esther Rey; García, Pilar Ayllon; Jiménez-González, María; Rubio, Victoria Hernández; Alapont, Paloma Moraga; Sánchez, Amparo Rodríguez; Prieto, Rocío; Gómez, Silvia Llorente; Roig, Cristina Miragall; Marlasca, Marina Aparicio; Calle, Fernando; Arsuaga, Marta; Duque, B.; Meijide, Susana; Vicuña, Aitor García de; Santorcuato, Ana; Expósito, Iraide; Benito, Sara; Andia, Joseba; Castillo, Cristina; Irurzun, Esther; Camino, Jesús; Temprano, Mikel; Goikoetxea, Josune; Bustinza, Alazne; Larrea, Maialen; Gallego, Mikel; García-Vázquez, Dolores; Hoz, Ana Belén de la; Pérez-Nanclares, Gustavo; Pérez-Guzmán, Estíbaliz; Idoyaga, Eneko; Lamela, Adriana; Oteo, Jesús; Osa, María Castillo de la; Gutiérrez, Lourdes Hernández; Galván, María Elena Andrés; Calonge, Esther; Bermejo, Mercedes; Tarazona, Humberto Erick De La Torre; Cascajero, Almudena; Fedele, Giovanni; Perea, Concepción; Cervera, Isabel; Bodega-Mayor, Irene; Montes-Casado, María; Portolés, Pilar; Baranda, Jana; Granés, Laura; Lazaar, Sulayman; Herranz, Sara; Mellado, María Eugènia; Tortajada, Marta; Malet, Montserrat; Quesada, Sebastiana; Vilella, Anna; Llupià, Anna; Olivé, Victòria; Trilla, Antoni; Gómez, Begoña; González, Elisenda; Romero, Sheila; Gámez, Francisco Javier; Casals, Cristina; Burunat, Laura; Castelló, Juan José; Fernández, Patricia Valcarcél; Bedini, Josep Lluís; Vilà, Jordi; Aguilar, Carla; Altadill, Carmen; Armadans, Lluı́s; Borras-Bermejo, Blanca; Calonge, Julia; Camacho, Lina; Feliu, Anna; Gili, Gisela; Llorente, Cesar A.; Martínez-Gómez, Xavier; Otero‐Romero, Susana; Palacio, Esther; Parés, Oleguer; Pinós, Laia; Plaza, Aitana; Riera, Judith; Rodrigo-Pendás, José Ángel; Sans, Carla; Santos, José Ramón; Torres, Gloria; Torrens, Margarita; Uriona, Sonia; Alins, Elena Ballarin; Esquirol, Eulàlia Pérez; Bosch, Lourdes Vendrell; Laredo, Leonor; López, Diana Uribe; González‐Rojano, Esperanza; Sánchez-Craviotto, Manuel; Paterna, A.; Hernán-Gómez, Teresa Iglesias; Galán, Natalia Rodríguez; Marín, José Antonio Gil; Álvarez-Morales, Verónica; Navalpotro, Ana Belén; Jiménez-Santamaría, M Dolores; Cardós, M Carmen; Hermoso, Elena; García-Arenillas, Mar; Macías, Natalia Pérez; Fernández, Alexandra Domingo; Picado, Amanda López; Quiñones, Jorge Mario; Deidda, Nicoletta; García‐Franco, Ana; Torvisco, José María

doi:10.1016/s0140-6736(21)01420-3

Cited by 334 publications

(359 citation statements)

References 26 publications

(32 reference statements)

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“…In The Lancet , Xinxue Liu and colleagues 2 present results for four of the eight intervention groups of the Com-COV clinical trial, showing that the immunological response of double-dose ChAdOx1 nCoV-19 (AstraZeneca; hereafter referred to as ChAd) is statistically lower than any other schedule including BNT162b2 (Pfizer–BioNTech, hereafter referred to as BNT) and ChAd at 28 days post boost dose, with a 28-day prime–boost interval. In addition, their findings support previous published data from an academic study done by the Instituto de Salud Carlos III, of which I was an investigator and author, 3 suggesting that a heterologous schedule based on the sequential administration of ChAd and BNT could be highly immunogenic, and perhaps more immunogenic than homologous schedules based on ChAd. In addition, Liu and colleagues show that double-dose BNT is more potent in inducing a humoral response than the BNT–ChAd permutation.…”

supporting

confidence: 83%

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Optimising SARS-CoV-2 vaccination schedules

Belda-Iniesta

2021

The Lancet

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supporting

confidence: 83%

“…The Com-COV trial, like the CombiVacS trial, 3 was not able to identify very low-frequency adverse events. Of course, no phase 2 study is able to do so.…”

mentioning

confidence: 99%

Optimising SARS-CoV-2 vaccination schedules

Belda-Iniesta

2021

The Lancet

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“…Our results for the ChAd/BNT schedule build on preliminary data from a Spanish randomised trial, in which 18–60-year-olds received a dose of BNT 2–3 months after priming with ChAd and showed a 37-fold increase in SARS-CoV-2 anti-spike IgG at 14 days post boost, higher than the 22-fold increase at 7 days and 19-fold increase at 28 days post boost in this study. 13 Potential explanations for these differences include the longer prime-boost interval, the different sampling timepoints, and a younger population in the Spanish study. 13 Fold increases in the cellular response were, however, similar (four-fold in the Spanish study versus 3·7-fold in this study).…”

Section: Discussionmentioning

confidence: 99%

“… 13 Potential explanations for these differences include the longer prime-boost interval, the different sampling timepoints, and a younger population in the Spanish study. 13 Fold increases in the cellular response were, however, similar (four-fold in the Spanish study versus 3·7-fold in this study). Early results from a prospective cohort study in Germany, which compared health-care workers immunised with BNT/BNT at a 3-week interval or ChAd/BNT at an 8–12 week interval, showed similar concentrations of binding antibody at 3 weeks post boost and higher cellular responses in the ChAd/BNT recipients.…”

Section: Discussionmentioning

confidence: 99%

“…Nevertheless, preclinical studies support evaluation of this approach, 11 , 12 and results from a randomised study in Spain suggested an increase in binding and neutralising antibody after boosting ChAd-primed participants with BNT, compared with not having a boost dose. 13 Additionally, early results from an observational study in Germany show that humoral responses are similar in the cohort receiving BNT/BNT at a 3-week interval to those receiving ChAd/BNT at a 10-week interval, with cellular responses appearing to be higher in the ChAd/BNT cohort. 14 However, we have previously reported that heterologous schedules incorporating ChAd and BNT are more reactogenic than their homologous schedules.…”

Section: Introductionmentioning

confidence: 99%

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Safety and immunogenicity of heterologous versus homologous prime-boost schedules with an adenoviral vectored and mRNA COVID-19 vaccine (Com-COV): a single-blind, randomised, non-inferiority trial

et al. 2021

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Background Use of heterologous prime-boost COVID-19 vaccine schedules could facilitate mass COVID-19 immunisation. However, we have previously reported that heterologous schedules incorporating an adenoviral vectored vaccine (ChAdOx1 nCoV-19, AstraZeneca; hereafter referred to as ChAd) and an mRNA vaccine (BNT162b2, Pfizer–BioNTech; hereafter referred to as BNT) at a 4-week interval are more reactogenic than homologous schedules. Here, we report the safety and immunogenicity of heterologous schedules with the ChAd and BNT vaccines. Methods Com-COV is a participant-blinded, randomised, non-inferiority trial evaluating vaccine safety, reactogenicity, and immunogenicity. Adults aged 50 years and older with no or well controlled comorbidities and no previous SARS-CoV-2 infection by laboratory confirmation were eligible and were recruited at eight sites across the UK. The majority of eligible participants were enrolled into the general cohort (28-day or 84-day prime-boost intervals), who were randomly assigned (1:1:1:1:1:1:1:1) to receive ChAd/ChAd, ChAd/BNT, BNT/BNT, or BNT/ChAd, administered at either 28-day or 84-day prime-boost intervals. A small subset of eligible participants (n=100) were enrolled into an immunology cohort, who had additional blood tests to evaluate immune responses; these participants were randomly assigned (1:1:1:1) to the four schedules (28-day interval only). Participants were masked to the vaccine received but not to the prime-boost interval. The primary endpoint was the geometric mean ratio (GMR) of serum SARS-CoV-2 anti-spike IgG concentration (measured by ELISA) at 28 days after boost, when comparing ChAd/BNT with ChAd/ChAd, and BNT/ChAd with BNT/BNT. The heterologous schedules were considered non-inferior to the approved homologous schedules if the lower limit of the one-sided 97·5% CI of the GMR of these comparisons was greater than 0·63. The primary analysis was done in the per-protocol population, who were seronegative at baseline. Safety analyses were done among participants receiving at least one dose of a study vaccine. The trial is registered with ISRCTN, 69254139. Findings Between Feb 11 and Feb 26, 2021, 830 participants were enrolled and randomised, including 463 participants with a 28-day prime-boost interval, for whom results are reported here. The mean age of participants was 57·8 years (SD 4·7), with 212 (46%) female participants and 117 (25%) from ethnic minorities. At day 28 post boost, the geometric mean concentration of SARS-CoV-2 anti-spike IgG in ChAd/BNT recipients (12 906 ELU/mL) was non-inferior to that in ChAd/ChAd recipients (1392 ELU/mL), with a GMR of 9·2 (one-sided 97·5% CI 7·5 to ∞). In participants primed with BNT, we did not show non-inferiority of the heterologous schedule (BNT/ChAd, 7133 ELU/mL) against the homologous schedule (BNT/BNT, 14 080 ELU/mL), with a GMR of 0·51 (one-sided 97·5% CI 0·43 to ∞). Four serious adverse events occurred across all groups, none of which were co...

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Efficacy and safety of COVID-19 vaccines

Graña

Ghosn

Evrenoglou

et al. 2022

Cochrane Database of Systematic Reviews

180

135

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Background Different forms of vaccines have been developed to prevent the SARS‐CoV‐2 virus and subsequent COVID‐19 disease. Several are in widespread use globally. Objectives To assess the efficacy and safety of COVID‐19 vaccines (as a full primary vaccination series or a booster dose) against SARS‐CoV‐2. Search methods We searched the Cochrane COVID‐19 Study Register and the COVID‐19 L·OVE platform (last search date 5 November 2021). We also searched the WHO International Clinical Trials Registry Platform, regulatory agency websites, and Retraction Watch. Selection criteria We included randomized controlled trials (RCTs) comparing COVID‐19 vaccines to placebo, no vaccine, other active vaccines, or other vaccine schedules. Data collection and analysis We used standard Cochrane methods. We used GRADE to assess the certainty of evidence for all except immunogenicity outcomes. We synthesized data for each vaccine separately and presented summary effect estimates with 95% confidence intervals (CIs). Main results We included and analyzed 41 RCTs assessing 12 different vaccines, including homologous and heterologous vaccine schedules and the effect of booster doses. Thirty‐two RCTs were multicentre and five were multinational. The sample sizes of RCTs were 60 to 44,325 participants. Participants were aged: 18 years or older in 36 RCTs; 12 years or older in one RCT; 12 to 17 years in two RCTs; and three to 17 years in two RCTs. Twenty‐nine RCTs provided results for individuals aged over 60 years, and three RCTs included immunocompromized patients. No trials included pregnant women. Sixteen RCTs had two‐month follow‐up or less, 20 RCTs had two to six months, and five RCTs had greater than six to 12 months or less. Eighteen reports were based on preplanned interim analyses. Overall risk of bias was low for all outcomes in eight RCTs, while 33 had concerns for at least one outcome. We identified 343 registered RCTs with results not yet available. This abstract reports results for the critical outcomes of confirmed symptomatic COVID‐19, severe and critical COVID‐19, and serious adverse events only for the 10 WHO‐approved vaccines. For remaining outcomes and vaccines, see main text. The evidence for mortality was generally sparse and of low or very low certainty for all WHO‐approved vaccines, except AD26.COV2.S (Janssen), which probably reduces the risk of all‐cause mortality (risk ratio (RR) 0.25, 95% CI 0.09 to 0.67; 1 RCT, 43,783 participants; high‐certainty evidence). Confirmed symptomatic COVID‐19 High‐certainty evidence found that BNT162b2 (BioNtech/Fosun Pharma/Pfizer), mRNA‐1273 (ModernaTx), ChAdOx1 (Oxford/AstraZeneca), Ad26.COV2.S, BBIBP‐CorV (Sinopharm‐Beijing), and BBV152 (Bharat Biotect) reduce the incidence of symptomatic COVI...

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Immunogenicity and reactogenicity of BNT162b2 booster in ChAdOx1-S-primed participants (CombiVacS): a multicentre, open-label, randomised, controlled, phase 2 trial

Cited by 334 publications

References 26 publications

Optimising SARS-CoV-2 vaccination schedules

Optimising SARS-CoV-2 vaccination schedules

Safety and immunogenicity of heterologous versus homologous prime-boost schedules with an adenoviral vectored and mRNA COVID-19 vaccine (Com-COV): a single-blind, randomised, non-inferiority trial

Efficacy and safety of COVID-19 vaccines

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