Safety, Effectiveness and Immunogenicity of heterologous mRNA-1273 Boost after Prime with Ad26.COV2.S among Healthcare Workers in South Africa: the single-arm, open-label, Phase 3 SHERPA Study
Author:
Garrett NigelORCID, Reddy Tarylee, Yende-Zuma NonhlanhlaORCID, Takalani Azwidhwi, Woeber KubashniORCID, Bodenstein Annie, Jonas Phumeza, Engelbrecht ImkeORCID, Jassat Waasila, Moultrie HarryORCID, Bradshaw Debbie, Seocharan Ishen, Odhiambo Jackline, Khuto Kentse, Richardson Simone I., Omondi Millicent A.ORCID, Nesamari Rofhiwa, Keeton Roanne S.ORCID, Riou Catherine, Moyo-Gwete Thandeka, Innes Craig, Zwane Zwelethu, Mngadi Kathy, Brumskine William, Naicker Nivashnee, Potloane Disebo, Badal-Faesen Sharlaa, Innes Steve, Barnabas Shaun, Lombaard Johan, Gill Katherine, Nchabeleng Maphoshane, Snyman Elizma, Petrick Friedrich, Spooner Elizabeth, Naidoo Logashvari, Kalonji Dishiki, Naicker Vimla, Singh Nishanta, Maboa Rebone, Mda Pamela, Malan Daniel, Nana Anusha, Malahleha Mookho, Kotze Philip, Allagappen Jon J., Diacon Andreas H., Kruger Gertruida M., Patel Faeezah, Moore Penny L.ORCID, Burgers Wendy A.ORCID, Anteyi Kate, Leav Brett, Bekker Linda-Gail, Gray Glenda E, Goga AmeenaORCID,
Abstract
AbstractGiven limited data on safety and effectiveness of heterologous COVID-19 vaccine boosting in lower income, high-HIV prevalence settings, we evaluated a mRNA-1273 boost after Ad26.COV2.S priming in South Africa. SHERPA was a single-arm, open-label, phase 3 study nested in the Sisonke implementation trial of 500000 healthcare workers (HCWs). Sisonke participants were offered mRNA-1273 boosters between May and November 2022, a period of circulating Omicron sub-lineages. Adverse events (AE) were self-reported, and co-primary endpoints (SARS-CoV-2 infections and COVID-19 hospitalizations or deaths) were collected through national databases. We used Cox regression models with booster status as time-varying covariate to determine the relative vaccine effectiveness (rVE) of the mRNA-1273 booster among SHERPA versus unboosted Sisonke participants. Of 11248 SHERPA participants in the rVE analysis cohort (79.3% female, median age 41), 45.4% had received one and 54.6% two Ad26.COV2.S doses. Self-reported comorbidities included HIV (18.7%), hypertension (12.9%) and diabetes (4.6%). In multivariable analysis including 413161 unboosted Sisonke participants, rVE of the booster was 59% (95%CI 29-76%) against SARS-CoV-2 infection: 77% (95%CI 9–94%) in the one-Ad26.COV2.S dose group and 52% (95%CI 13-73%) in the two-dose group. Severe COVID-19 was identified in 148 unboosted participants, and only one SHERPA participant with severe HIV-related immunosuppression. Of 11798 participants in the safety analysis, 271 (2.3%) reported a reactogenicity event or unsolicited AE, more among those with prior SARS-CoV-2 infections (adjusted odds ratio [aOR] 2.03, 95%CI 1.59-2.59) and less among people living with HIV (PLWH) (aOR 0.49, 95%CI 0.34-0.69). No related serious AEs were reported. In an immunogenicity sub-study, mRNA-1273 increased antibody functions and T-cell responses 4 weeks after boosting regardless of the number of prior Ad26.COV2.S doses, or HIV status, and generated Omicron spike-specific cross-reactive responses. mRNA-1273 boosters after one or two Ad26.COV2.S doses were well-tolerated, safe and effective against Omicron SARS-CoV-2 infections among HCWs and PLWH.Trial RegistrationThe SHERPA study is registered in the Pan African Clinical Trials Registry (PACTR): PACTR202310615330649 and the South African National Clinical Trial Registry (SANCTR): DOH-27-052022-5778.
Publisher
Cold Spring Harbor Laboratory
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