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孟加拉国为期 1 年的纵向队列研究中 COVID-19 疫苗接种后的抗体持久性和衰减。

Antibody longevity and waning following COVID-19 vaccination in a 1-year longitudinal cohort in Bangladesh.

机构信息

Immunobiology, Nutrition and Toxicology Laboratory, Nutrition Research Division, International Center for Diarrhoeal Disease Research, Bangladesh (icddr, b), Dhaka, 1212, Bangladesh.

UNICEF, Dhaka, 1207, Bangladesh.

出版信息

Sci Rep. 2024 May 20;14(1):11467. doi: 10.1038/s41598-024-61922-6.

Abstract

COVID-19 vaccines have been effective in preventing severe illness, hospitalization and death, however, the effectiveness diminishes with time. Here, we evaluated the longevity of antibodies generated by COIVD-19 vaccines and the risk of (re)infection in Bangladeshi population. Adults receiving two doses of AstraZeneca, Pfizer, Moderna or Sinopharm vaccines were enrolled at 2-4 weeks after second dosing and followed-up at 4-monthly interval for 1 year. Data on COVID-like symptoms, confirmed COVID-19 infection, co-morbidities, and receipt of booster dose were collected; blood was collected for measuring spike (S)- and nucleocapsid (N)-specific antibodies. S-specific antibody titers reduced by ~ 50% at 1st follow-up visit and continued to decline unless re-stimulated by booster vaccine dose or (re)infection. Individuals infected between follow-up visits showed significantly lower S-antibody titers at preceding visits compared to the uninfected individuals. Pre-enrolment infection between primary vaccination dosing exhibited 60% and 50% protection against reinfection at 5 and 9 months, respectively. mRNA vaccines provided highest odds of protection from (re)infection up to 5 months (Odds Ratio (OR) = 0.08), however, protection persisted for 9 months in AstraZeneca vaccine recipients (OR = 0.06). In conclusion, vaccine-mediated protection from (re)infection is partially linked to elevated levels of S-specific antibodies. AstraZeneca vaccine provided the longest protection.

摘要

COVID-19 疫苗在预防重症、住院和死亡方面非常有效,但随着时间的推移,其效果会减弱。在这里,我们评估了 COVID-19 疫苗产生的抗体的持久性以及孟加拉国人群再次感染的风险。在第二次接种后 2-4 周,接受阿斯利康、辉瑞、莫德纳或科兴疫苗两剂接种的成年人被招募,并在接下来的 1 年内每 4 个月随访一次。收集了 COVID 样症状、确诊 COVID-19 感染、合并症和加强剂量接种的数据;采集血液用于测量刺突(S)和核衣壳(N)特异性抗体。S 特异性抗体滴度在第一次随访时降低了约 50%,并继续下降,除非加强疫苗剂量或(再次)感染刺激。在随访期间感染的个体在前一次就诊时的 S 抗体滴度明显低于未感染的个体。初级疫苗接种剂量之间的预登记感染在 5 个月和 9 个月时分别对再次感染提供了 60%和 50%的保护。mRNA 疫苗在 5 个月内提供了最高的免受(再次)感染的保护几率(比值比(OR)=0.08),然而,阿斯利康疫苗的保护作用在 9 个月内持续(OR=0.06)。总之,疫苗介导的免受(再次)感染的保护部分与 S 特异性抗体水平升高有关。阿斯利康疫苗提供的保护时间最长。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8548/11106241/5395bbe2a54c/41598_2024_61922_Fig1_HTML.jpg

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