Raglow Zoe, Surie Diya, Chappell James D, Zhu Yuwei, Martin Emily T, Kwon Jennie H, Frosch Anne E, Mohamed Amira, Gilbert Julie, Bendall Emily E, Bahr Auden, Halasa Natasha, Talbot H Keipp, Grijalva Carlos G, Baughman Adrienne, Womack Kelsey N, Johnson Cassandra, Swan Sydney A, Koumans Emilia, McMorrow Meredith L, Harcourt Jennifer L, Atherton Lydia J, Burroughs Ashley, Thornburg Natalie J, Self Wesley H, Lauring Adam S
Department of Internal Medicine, University of Michigan, Ann Arbor, MI, USA.
National Center for Immunization and Respiratory Diseases, Centers for Disease Control and Prevention, Atlanta, GA, USA.
Lancet Microbe. 2024 Mar;5(3):e235-e246. doi: 10.1016/S2666-5247(23)00336-1. Epub 2024 Jan 26.
Prolonged SARS-CoV-2 infections in people who are immunocompromised might predict or source the emergence of highly mutated variants. The types of immunosuppression placing patients at highest risk for prolonged infection have not been systematically investigated. We aimed to assess risk factors for prolonged SARS-CoV-2 infection and associated intrahost evolution.
In this multicentre, prospective analysis, participants were enrolled at five US medical centres. Eligible patients were aged 18 years or older, were SARS-CoV-2-positive in the previous 14 days, and had a moderately or severely immunocompromising condition or treatment. Nasal specimens were tested by real-time RT-PCR every 2-4 weeks until negative in consecutive specimens. Positive specimens underwent viral culture and whole genome sequencing. A Cox proportional hazards model was used to assess factors associated with duration of infection.
From April 11, 2022, to Oct 1, 2022, 156 patients began the enrolment process, of whom 150 were enrolled and included in the analyses. Participants had B-cell malignancy or anti-B-cell therapy (n=18), solid organ transplantation or haematopoietic stem-cell transplantation (HSCT; n=59), AIDS (n=5), non-B-cell malignancy (n=23), and autoimmune or autoinflammatory conditions (n=45). 38 (25%) participants were real-time RT-PCR-positive and 12 (8%) were culture-positive 21 days or longer after initial SARS-CoV-2 detection or illness onset. Compared with the group with autoimmune or autoinflammatory conditions, patients with B-cell dysfunction (adjusted hazard ratio 0·32 [95% CI 0·15-0·64]), solid organ transplantation or HSCT (0·60 [0·38-0·94]), and AIDS (0·28 [0·08-1·00]) had longer duration of infection, defined as time to last positive real-time RT-PCR test. There was no significant difference in the non-B-cell malignancy group (0·58 [0·31-1·09]). Consensus de novo spike mutations were identified in five individuals who were real-time RT-PCR-positive longer than 56 days; 14 (61%) of 23 were in the receptor-binding domain. Mutations shared by multiple individuals were rare (<5%) in global circulation.
In this cohort, prolonged replication-competent omicron SARS-CoV-2 infections were uncommon. Within-host evolutionary rates were similar across patients, but individuals with infections lasting longer than 56 days accumulated spike mutations, which were distinct from those seen globally. Populations at high risk should be targeted for repeated testing and treatment and monitored for the emergence of antiviral resistance.
US Centers for Disease Control and Prevention.
免疫功能低下人群中SARS-CoV-2感染持续时间延长可能预示或引发高度变异毒株的出现。尚未对使患者面临最长感染风险的免疫抑制类型进行系统研究。我们旨在评估SARS-CoV-2感染持续时间延长及相关病毒宿主内进化的风险因素。
在这项多中心前瞻性分析中,参与者在美国的五个医疗中心入组。符合条件的患者年龄在18岁及以上,在过去14天内SARS-CoV-2检测呈阳性,且患有中度或重度免疫功能低下疾病或正在接受相关治疗。每2-4周采集鼻拭子样本进行实时逆转录聚合酶链反应(RT-PCR)检测,直至连续样本呈阴性。对阳性样本进行病毒培养和全基因组测序。采用Cox比例风险模型评估与感染持续时间相关的因素。
从2022年4月11日至2022年10月1日,156名患者开始入组流程,其中150名患者入组并纳入分析。参与者包括B细胞恶性肿瘤或接受抗B细胞治疗者(n=18)、实体器官移植或造血干细胞移植(HSCT)者(n=59)、艾滋病患者(n=5)、非B细胞恶性肿瘤患者(n=23)以及自身免疫或自身炎症性疾病患者(n=45)。38名(25%)参与者在首次SARS-CoV-2检测或发病后21天或更长时间实时RT-PCR检测呈阳性,12名(8%)培养检测呈阳性。与自身免疫或自身炎症性疾病组相比,B细胞功能障碍患者(调整后风险比0.32 [95%置信区间0.15-0.64])、实体器官移植或HSCT患者(0.60 [0.38-0.94])以及艾滋病患者(0.28 [0.08-1.00])的感染持续时间更长,感染持续时间定义为最后一次实时RT-PCR检测呈阳性的时间。非B细胞恶性肿瘤组无显著差异(0.58 [0.31-1.09])。在5名实时RT-PCR检测阳性超过56天的个体中鉴定出一致性新发刺突突变;23名中的14名(61%)位于受体结合域。多个个体共有的突变在全球流行毒株中很少见(<5%)。
在该队列中,具有复制能力的奥密克戎SARS-CoV-2感染持续时间延长的情况并不常见。患者体内病毒进化率相似,但感染持续时间超过56天的个体积累了刺突突变,这些突变与全球所见不同。应针对高危人群进行重复检测和治疗,并监测抗病毒耐药性的出现。
美国疾病控制与预防中心。
