Research School of Biology, Australian National University, Canberra, Australia.
John Curtin School of Medical Research, Australian National University, Canberra, Australia.
Asia Pac J Clin Oncol. 2024 Jun;20(3):379-385. doi: 10.1111/ajco.14047. Epub 2024 Jan 14.
Cancer patients have increased morbidity and mortality from COVID-19, but may respond poorly to vaccination. The Evaluation of COVID-19 Vaccination Efficacy and Rare Events in Solid Tumors (EVEREST) study, comparing seropositivity between cancer patients and healthy controls in a low SARS-CoV-2 community-transmission setting, allows determination of vaccine response with minimal interference from infection.
Solid tumor patients from The Canberra Hospital, Canberra, Australia, and healthy controls who received COVID-19 vaccination between March 2021 and January 2022 were included. Blood samples were collected at baseline, pre-second vaccine dose and at 1, 3 (primary endpoint), and 6 months post-second dose. SARS-CoV-2 anti-spike-RBD (S-RBD) and anti-nucleocapsid IgG antibodies were measured.
Ninety-six solid tumor patients and 20 healthy controls were enrolled, with median age 62 years, and 60% were female. Participants received either AZD1222 (65%) or BNT162b2 (35%) COVID-19 vaccines. Seropositivity 3 months post vaccination was 87% (76/87) in patients and 100% (20/20) in controls (p = .12). Seropositivity was observed in 84% of patients on chemotherapy, 80% on immunotherapy, and 96% on targeted therapy (differences not satistically significant). Seropositivity in cancer patients increased from 40% (6/15) after first dose, to 95% (35/37) 1 month after second dose, then dropped to 87% (76/87) 3 months after second dose.
Most patients and all controls became seropositive after two vaccine doses. Antibody concentrations and seropositivity showed a decrease between 1 and 3 months post vaccination, highlighting need for booster vaccinations. SARS-CoV-2 infection amplifies S-RBD antibody responses; however, cannot be adequately identified using nucleocapsid serology. This underlines the value of our COVID-naïve population in studying vaccine immunogenicity.
癌症患者 COVID-19 的发病率和死亡率增加,但对疫苗的反应可能较差。在 SARS-CoV-2 社区传播水平较低的情况下,比较癌症患者和健康对照者的血清阳性率的评估 COVID-19 疫苗功效和实体瘤罕见事件(EVEREST)研究,可在最小的感染干扰下确定疫苗反应。
纳入 2021 年 3 月至 2022 年 1 月期间在澳大利亚堪培拉医院接受 COVID-19 疫苗接种的实体瘤患者和健康对照者。在基线、第二次疫苗剂量前和第一次(主要终点)、第三次和第六次疫苗剂量后 1 个月采集血样。测量 SARS-CoV-2 抗刺突-RBD(S-RBD)和抗核衣壳 IgG 抗体。
纳入 96 例实体瘤患者和 20 例健康对照者,中位年龄 62 岁,60%为女性。参与者接种了 AZD1222(65%)或 BNT162b2(35%)COVID-19 疫苗。接种后 3 个月,患者的血清阳性率为 87%(76/87),对照组为 100%(20/20)(p=0.12)。化疗患者的血清阳性率为 84%,免疫治疗患者为 80%,靶向治疗患者为 96%(差异无统计学意义)。第一剂后,血清阳性率从 40%(15/37)增加到第二剂后 1 个月的 95%(35/37),然后在第二剂后 3 个月下降到 87%(76/87)。
大多数患者和所有对照组在两次疫苗接种后均呈血清阳性。接种后 1 至 3 个月,抗体浓度和血清阳性率下降,强调需要加强接种。SARS-CoV-2 感染可增强 S-RBD 抗体反应;然而,核衣壳血清学无法充分识别。这突出了我们 COVID-19 未感染人群在研究疫苗免疫原性方面的价值。
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