Department of Clinical Virology, Institute of Liver and Biliary Sciences, D-1 Vasant Kunj, New Delhi, 110070, India.
Genome Sequencing Laboratory, Institute of Liver and Biliary Sciences, New Delhi, India.
Curr Microbiol. 2024 Aug 8;81(9):301. doi: 10.1007/s00284-024-03786-7.
The limited literature on the clinical course of COVID-19 among patients with underlying liver disease (LD) is available from India. The present study aimed to evaluate the clinical and mutational profile of SARS-CoV-2 among LD cases. This was a retrospective study including admitted LD cases in whom SARS-CoV-2 RT-PCR testing was performed. Complete demographic and clinical details were retrieved from Hospital Information System. Detailed mutational analysis was performed by comparing LD COVID-19 positive study group, i.e. LD-CoV(+) with COVID-19 positive outpatients without any underlying LD as control, i.e. NLD-CoV(+). Out of 232 enrolled LD cases, 137 (59.1%) were LD-CoV(+). LD cases with existing co-morbidities were affected more (P = 0.002) and had 2.29 times (OR 2.29, CI 95%, 1.25-4.29) higher odds of succumbing to COVID-19 (P = 0.006). On multivariate regression analysis, ascites (P = 0.05), severe COVID-19 pneumonia (P = 0.046), and an increased levels of bilirubin (P = 0.005) and alkaline phosphatase (P = 0.003) were found to be associated with adverse outcome in LD-CoV(+).On mutational analysis, we found certain differences between LD- and NLD-CoV(+) infected with Delta [LD- and NLD-CoV (+ /D)] and Omicron [LD- and NLD-CoV(+/O)]. More mutations were shared between LD- and NLD-CoV(+/O) compared to LD- and NLD-CoV(+/D). There were differences in prevalence of indel mutations specific to LD-CoV ( +) for both Delta and Omicron. Moreover, we also reported an interesting genic bias between LD- and NLD-CoV( +) in harbouring deleterious/tolerated mutations. To conclude, LD cases with comorbidities were affected more and had higher odds of mortality due to COVID-19. The definite difference between LD- and NLD-CoV(+) groups with respect to frequency of harboured mutations and an inherent genic bias between them is of noteworthy importance.
关于伴有基础肝病 (LD) 的 COVID-19 患者的临床病程的有限文献可从印度获得。本研究旨在评估 LD 病例中 SARS-CoV-2 的临床和突变特征。这是一项回顾性研究,包括进行了 SARS-CoV-2 RT-PCR 检测的住院 LD 病例。从医院信息系统中检索到完整的人口统计学和临床详细信息。通过比较 LD-COVID-19 阳性研究组,即 LD-CoV(+)与 COVID-19 阳性无任何基础 LD 的门诊患者作为对照,即 NLD-CoV(+),进行详细的突变分析。在纳入的 232 例 LD 病例中,137 例 (59.1%) 为 LD-CoV(+)。伴有现有合并症的 LD 病例受影响更大 (P = 0.002),死于 COVID-19 的几率更高 2.29 倍 (OR 2.29,95%CI,1.25-4.29) (P = 0.006)。多变量回归分析显示,腹水 (P = 0.05)、严重 COVID-19 肺炎 (P = 0.046) 以及胆红素 (P = 0.005) 和碱性磷酸酶 (P = 0.003) 水平升高与 LD-CoV(+)的不良预后相关。在突变分析中,我们发现 LD-和 NLD-CoV(+)感染 Delta [LD-和 NLD-CoV (+ /D)] 和 Omicron [LD-和 NLD-CoV(+/O)] 之间存在某些差异。与 LD-和 NLD-CoV(+/D)相比,LD-和 NLD-CoV(+/O)之间共享更多突变。LD-CoV(+)中存在针对 Delta 和 Omicron 的特定 LD 特异性插入缺失突变的差异。此外,我们还报告了 LD-和 NLD-CoV( +)之间在携带有害/耐受突变方面的有趣基因偏向。总之,伴有合并症的 LD 病例受影响更大,死于 COVID-19 的几率更高。LD-和 NLD-CoV(+) 组之间在携带突变的频率方面存在明确差异,以及它们之间存在内在的基因偏向,这具有重要意义。
