Immunomodulation in COVID-19

Sirshendu Pal, Rupsha Dutta
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Abstract

Immunology forms the basis for effective treatment strategies and production of vaccines. In COVID 19 immune insufficiency may increase viral replication while uncontrolled immunity may result in tissue damage. The angiotensin converting enzyme receptors on alveolar type 2 cells of lungs act as target cells are the sites of Corona virus attack. These cells through cytokines or interferons initiate an early local response which may control the infection. However, in COVID-19 this interferon response can be subdued or lagging which may allow the COVID virus to escape detection by the innate immunity or depress the downstream reaction leading to unchecked SARS-COV-2 replication. The suppression of host responses leads to increase in pro-inflammatory cytokines and the resulting inflammatory damage leads to a release of suppressive cytokines as a counter regulatory response. This is the cytokine storm. Thus, immuneregulatory treatments that may succeed are the ones that are in real time tuned to the subject's immunophenotype, where immunosuppression may be helpful at some points while immune-stimulation in others.
COVID-19的免疫调节
免疫学是有效治疗策略和生产疫苗的基础。在COVID - 19中,免疫功能不全可能增加病毒复制,而不受控制的免疫可能导致组织损伤。肺肺泡2型细胞上的血管紧张素转换酶受体是冠状病毒攻击的靶细胞。这些细胞通过细胞因子或干扰素启动可能控制感染的早期局部反应。然而,在COVID-19中,这种干扰素反应可能被抑制或滞后,这可能使COVID病毒逃脱先天免疫的检测或抑制下游反应,导致不受控制的SARS-COV-2复制。对宿主反应的抑制导致促炎细胞因子的增加,由此产生的炎症损伤导致抑制细胞因子的释放,作为一种反调节反应。这是细胞因子风暴。因此,可能成功的免疫调节治疗是那些实时调整到受试者的免疫表型的治疗,免疫抑制在某些点可能有用,而免疫刺激在其他点可能有用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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