Interferon response and profiling of interferon response genes in peripheral blood of vaccine-naive COVID-19 patients

未接种疫苗的 COVID-19 患者外周血中的干扰素反应和干扰素反应基因分析

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作者:Baozhen Huang #, Jinghan Huang #, Nim Hang Chiang #, Zigui Chen, Grace Lui, Lowell Ling, Mike Yat Wah Kwan, Joshua Sung Chih Wong, Phoebe Qiaozhen Mak, Janet Wan Hei Ling, Ivan Cheuk San Lam, Rita Wai Yin Ng, Xingyan Wang, Ruonan Gao, David Shu-Cheong Hui, Suk Ling Ma, Paul K S Chan, Nelson Leung Sa

Discussion

As sampling time and age were two major confounders of ISG expression, they may account for contradicting observations among previous studies. On the other hand, the IFN score was not associated with the severity of the disease.

Methods

In this study, we recruited 105 patients with COVID-19 and 30 healthy controls in Hong Kong. Clinical risk factors, disease course, and blood sampling times were recovered. Based on a set of five commonly used ISGs (IFIT1, IFIT2, IFI27, SIGLEC1, IFI44L), the IFN score was determined in blood leukocytes collected within 10 days after onset. The analysis was confined to those blood samples collected within 10 days after disease onset. Additional public datasets of bulk gene and single cell RNA sequencing of blood samples were used for the validation of IFN score

Results

Compared to the healthy controls, we showed that ISGs expression and IFN score were significantly increased during the first 10 days after COVID infection in majority of patients (71%). Among those low IFN responders, they were more commonly asymptomatic patients (71% vs 25%). 22 patients did not mount an overall significant IFN response and were classified as low IFN responders (IFN score < 1). However, early IFN score or ISGs level was not a prognostic biomarker and could not predict subsequent disease severity. Both IFI27 and SIGLEC1 were monocyte-predominant expressing ISGs and IFI27 were activated even among those low IFN responders as defined by IFN score. In

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