癌症成年患者对新冠疫苗接种的全面体液免疫和细胞免疫反应。
Comprehensive humoral and cellular immune responses to COVID-19 vaccination in adults with cancer.
作者信息
Body Amy, Lal Luxi, Srihari Sriganesh, MacIntyre C Raina, Buttery Jim, Ahern Elizabeth Stephanie, Opat Stephen, Leahy Michael Francis, Hamad Nada, Milch Vivienne, Turville Stuart, Smith Corey, Lineburg Katie, Naing Zin, Rawlinson William, Segelov Eva
机构信息
Monash Health, Department of Oncology, Melbourne, VIC, Australia; Monash University, Department of Oncology, School of Clinical Sciences, Melbourne, VIC, Australia.
Monash Health, Department of Oncology, Melbourne, VIC, Australia; Monash University, Department of Oncology, School of Clinical Sciences, Melbourne, VIC, Australia.
出版信息
Vaccine. 2025 Feb 6;46:126547. doi: 10.1016/j.vaccine.2024.126547. Epub 2024 Dec 7.
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.
背景
新冠疫情对癌症患者产生了重大影响。最初的疫苗研究将恶性肿瘤患者排除在外。免疫功能低下的个体仍然易感染新冠病毒,因此有必要详细了解疫苗反应。澳大利亚的新冠疫情流行病学情况为研究极少接触社区新冠病毒的癌症人群提供了独特机会。
方法
SerOzNET前瞻性地研究了之前未接种疫苗的实体瘤和血液系统恶性肿瘤患者,这些患者接受了多达五剂新冠疫苗。通过活病毒中和试验(中和抗体(NAb);阳性滴度≥1:20;研究主要终点)和商业检测法测量抗体反应。通过细胞计数珠阵列测量T细胞反应;阳性定义为对刺突抗原反应时干扰素γ(IFN-γ)≥10 pg/mL。患者和医生报告的不良事件为次要终点。
结果
395名成年人在接受mRNA疫苗(BNT162b2 = 347;mRNA-1273 = 1)或病毒载体疫苗(ChAdOx1-S = 43)进行初始两剂接种疗程之前入组,另外可再接种多达三剂。中位年龄为58岁(范围:20 - 85岁);60%为女性;35%患有血液系统恶性肿瘤,2/395(0.5%)有基线核衣壳抗体阳性,表明既往接触过新冠病毒。总体上,第三剂接种后84%出现NAb反应;实体癌患者中96%出现反应,血液系统癌症患者中64%出现反应(p < 0.001)。无反应的风险因素为血液系统癌症和抗B细胞疗法。一些血液系统癌症患者在第四剂或第五剂接种后首次血清转化。许多缺乏NAb反应的血液系统癌症患者出现了IFN-γ反应。严重不良事件罕见。29%的患者发生了新冠病毒感染,无死亡病例。
解读
新冠疫苗接种可在实体瘤和血液系统癌症患者中引发B细胞和T细胞反应,安全性可接受。相当一部分血液系统癌症患者需要接种超过3剂才能产生NAb,许多患者表现出T细胞反应,这可能是一种免疫保护的替代途径。
Zotero 插件