Your search keyword '"previous infection"' showing total 3 results

1. Long-Term Dynamic Changes in Hybrid Immunity over Six Months after Inactivated and Adenoviral Vector Vaccination in Individuals with Previous SARS-CoV-2 Infection.

Author

Suntronwong, Nungruthai, Kanokudom, Sitthichai, Auphimai, Chompoonut, Thongmee, Thanunrat, Assawakosri, Suvichada, Vichaiwattana, Preeyaporn, Yorsaeng, Ritthideach, Duangchinda, Thaneeya, Chantima, Warangkana, Pakchotanon, Pattarakul, Nilyanimit, Pornjarim, Srimuan, Donchida, Thatsanathorn, Thaksaporn, Sudhinaraset, Natthinee, Wanlapakorn, Nasamon, and Poovorawan, Yong

Subjects

SARS-CoV-2 Omicron variant, VACCINATION, SARS-CoV-2, IMMUNITY, COVID-19 vaccines

Abstract

Numerous studies have largely focused on short-term immunogenicity in recovered individuals post mRNA vaccination. However, understanding the long-term durability, particularly in inactivated and adenoviral vectored vaccines, remains limited. We evaluated antibody responses, omicron variant neutralization, and IFN-γ responses in 119 previously infected individuals vaccinated with CoronaVac or ChAdOx1 up to six months post-vaccination. Both vaccines elicited robust immune responses in recovered individuals, surpassing those who were infection-naïve, and these persisted above pre-vaccination levels for six months. However, antibody levels declined over time (geometric mean ratio (GMR) = 0.52 for both vaccines). Notably, neutralizing activities against omicron declined faster in ChAdOx1 (GMR = 0.6) compared to CoronaVac recipients (GMR = 1.03). While the first dose of ChAdOx1 adequately induced immune responses in recovered individuals, a second dose demonstrated advantages in omicron variant neutralization and slower decline. Although both vaccines induced T cell responses, the median IFN-γ level at six months returned to pre-vaccination levels. However, more individuals exhibited reactive T cell responses. Extending the interval (13–15 months) between infection and vaccination could enhance antibody levels and broaden neutralization. Together, these findings demonstrate a robust humoral and cellular response that was sustained for at least six months after vaccination, thus guiding optimal vaccination strategies based on prior infection and vaccine platforms. [ABSTRACT FROM AUTHOR]

Published

2024

2. Role of previous infection with SARS-CoV-2 in protecting against omicron reinfections and severe complications of COVID-19 compared to pre-omicron variants: a systematic review.

Author

Arabi, Maryam, Al-Najjar, Yousef, Sharma, Omna, Kamal, Ibtihal, Javed, Aimen, Gohil, Harsh S., Paul, Pradipta, Al-Khalifa, Aljazi M., Laws, Sa'ad, and Zakaria, Dalia

Subjects

*SARS-CoV-2 Omicron variant, *SARS-CoV-2 Delta variant, *SARS-CoV-2, *COVID-19, *BREAKTHROUGH infections

Abstract

Background: The SARS-CoV-2 virus elicited a major public concern worldwide since December 2019 due to the high number of infections and deaths caused by COVID-19. The Omicron variant was detected in October 2021 which evolved from the wild-type SARS-CoV-2 and was found to possess many mutations. Omicron exhibited high transmissibility and immune evasion as well as reduced severity when compared to the earlier variants. Although vaccinated individuals were largely protected against infections in previous waves, the high prevalence of both reinfections and breakthrough infections with Omicron was observed. The aim of this review is to understand the effectiveness of previous infection on subsequent reinfection, given its significance in driving public health policy, including vaccination prioritization and lockdown requirements. Methods: A comprehensive literature search was conducted using several databases to target studies reporting data related to the effectiveness of the previous infection with SARS-CoV-2 in protecting against the Omicron variant. Screening of the studies, quality assessment and data extraction were conducted by two reviewers for each study. Results: Only 27 studies met our inclusion criteria. It was observed that previous infection was less effective in preventing reinfections with the Omicron variant compared to the Delta variant irrespective of vaccination status. Furthermore, being fully vaccinated with a booster dose provided additional protection from the Omicron variant. Additionally, most infections caused by Omicron were asymptomatic or mild and rarely resulted in hospitalizations or death in comparison to the Delta wave. Conclusion: A majority of the studies reached a consensus that although previous infection provides some degree of immunity against Omicron reinfection, it is much lower in comparison to Delta. Full vaccination with two doses was more protective against Delta than Omicron. Receiving a booster dose provided additional protection against Omicron. It is therefore clear that neither vaccination nor previous infection alone provide optimal protection; hybrid immunity has shown the best results in terms of protecting against either Omicron or Delta variants. However, additional research is needed to quantify how long immunity from vaccination versus previous infection lasts and whether individuals will benefit from variant-specific vaccinations to enhance protection from infection. [ABSTRACT FROM AUTHOR]

Published

2023

3. Efficacy of vaccination and previous infection against the Omicron BA.1 variant in Syrian hamsters.

Author

Halfmann, Peter J., Kuroda, Makoto, Maemura, Tadashi, Chiba, Shiho, Armbrust, Tammy, Wright, Ryan, Balaram, Ariane, Florek, Kelsey R., Bateman, Allen C., and Kawaoka, Yoshihiro

Abstract

The emergence of the SARS-CoV-2 Omicron (B.1.1.529) variant with a surprising number of spike mutations raises concerns about reduced sensitivity of this virus to antibody neutralization and subsequent vaccine breakthrough infections. Here, we infect Moderna mRNA-vaccinated or previously infected hamsters with the Omicron BA.1 variant. While the Moderna mRNA vaccine reduces viral loads in the respiratory tissues upon challenge with an early S-614G isolate, the vaccine efficacy is not as pronounced after infection with the Omicron variant. Previous infection with the early SARS-CoV-2 isolate prevents replication after rechallenge with either virus in the lungs of previously infected hamsters, but the Omicron variant replicates efficiently in nasal turbinate tissue. These results experimentally demonstrate in an animal model that the antigenic changes in the Omicron variant are responsible for vaccine breakthrough and re-infection. [Display omitted] • Moderna-vaccinated hamsters are more susceptible to BA.1 than to an early isolate • BA.1 replicates less efficiently than an early isolate in the lungs of hamsters • Prior infection does not prevent BA.1 replication in the nasal turbinates of hamsters • Prior infection does prevent BA.1 replication in the lungs of hamsters Halfmann et al. report that while the Moderna mRNA vaccine reduces BA.1 replication in vaccinated hamsters, the vaccine efficacy is not as pronounced as that against an early prototypical SARS-CoV-2 isolate. Previously infected hamsters are better protected than vaccinated hamsters against re-infection with the BA.1 variant. [ABSTRACT FROM AUTHOR]

Published

2022