成人癌症患者对COVID-19疫苗的全面体液和细胞免疫反应

Vaccine Pub Date : 2025-02-06 Epub Date: 2024-12-07 DOI:10.1016/j.vaccine.2024.126547

Amy Body, Luxi Lal, Sriganesh Srihari, C Raina MacIntyre, Jim Buttery, Elizabeth Stephanie Ahern, Stephen Opat, Michael Francis Leahy, Nada Hamad, Vivienne Milch, Stuart Turville, Corey Smith, Katie Lineburg, Zin Naing, William Rawlinson, Eva Segelov

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引用次数: 0

摘要

背景：2019冠状病毒病大流行对癌症患者产生了重大影响。最初的疫苗研究排除了恶性肿瘤患者。免疫功能低下的个体仍然容易感染SARS-CoV-2，因此需要详细了解疫苗反应。澳大利亚COVID-19的流行病学为研究社区接触SARS-CoV-2最少的癌症人群提供了独特的机会。方法：SerOzNET前瞻性检查了先前未接种过5剂COVID-19疫苗的实体和血液恶性肿瘤患者。抗体反应用活病毒中和试验（中和抗体（NAb））测定；阳性滴度≥1:20；研究主要终点)和商业试验。细胞头阵列法检测T细胞反应；阳性定义为干扰素γ (IFN-γ)≥10 pg/mL。患者和医生报告的不良事件是次要终点。结果：395名成人在接受mRNA疫苗前入组(BNT162b2 = 347；mRNA-1273 = 1)或病毒载体疫苗（ChadOx1-S = 43）用于初始两剂疗程，外加最多三剂。中位年龄58岁（范围：20-85岁）；60%为女性；35%有血液学恶性肿瘤，2/395（0.5%）有基线核衣壳抗体阳性，表明有SARS-CoV-2暴露史。3次剂量后NAb应答率为84%；解释：COVID-19疫苗接种在实体癌和血液学癌患者中引起B细胞和T细胞反应，具有可接受的安全性。相当比例的血液学癌症患者需要>3剂量才能引发NAb，许多患者表现出T细胞反应，这可能是免疫保护的另一种途径。

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Comprehensive humoral and cellular immune responses to COVID-19 vaccination in adults with cancer.

Background: The COVID-19 pandemic has significantly impacted people with cancer. Initial vaccine studies excluded patients with malignancy. Immunocompromised individuals remain vulnerable to SARS-CoV-2, necessitating detailed understanding of vaccine response. The epidemiology of COVID-19 in Australia offered unique opportunities to study cancer populations with minimal community exposure to SARS-CoV-2.

Methods: SerOzNET prospectively examined previously unvaccinated patients with solid and haematological malignancies receiving up to five COVID-19 vaccine doses. Antibody response was measured by live virus neutralisation assay (neutralising antibody (NAb); positive titre ≥1:20; study primary endpoint) and commercial assay. T cell response was measured by cytometric bead array; positive defined as interferon gamma (IFN-γ) ≥10 pg/mL in response to Spike antigen. Patient and physician-reported adverse events were secondary endpoints.

Outcomes: 395 adults were enrolled prior to receiving mRNA vaccine (BNT162b2 = 347; mRNA-1273 = 1) or viral vector vaccine (ChadOx1-S = 43) for initial two-dose course, plus up to three additional doses. Median age was 58 years (range: 20-85); 60 % were female; 35 % had haematological malignancy, 2/395 (0.5 %) had baseline positive nucleocapsid antibody indicating prior SARS-CoV-2 exposure. NAb response post dose three was demonstrated in 84 % overall; 96 % of patients with solid cancers and 64 % with haematological cancer (p < 0·001). Risk factors for non-response were haematological cancer and anti B-cell therapies. Some patients with haematological cancer seroconverted for the first time after the fourth or fifth dose. IFN-γ response was seen in many patients with haematological cancer who lacked NAb response. Serious adverse events were rare. COVID-19 infection occurred in 29 % with no deaths.

Interpretation: COVID-19 vaccination elicits B and T cell responses in patients with solid and haematological cancers, with an acceptable safety profile. A significant proportion of haematological cancer patients require >3 doses to elicit NAb, with many demonstrating T cell response, which may be an alternative pathway of immune protection.

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