Some Aspects of Mast Cells Carboxypeptidase A3 Participation in the Pathogenesis of COVID-19

被引:0
作者
Budnevsky, Andrey V. [1 ]
Avdeev, Sergey N. [2 ]
Ovsyannikov, Evgeniy S. [1 ]
Alekseeva, Nadezhda G. [1 ]
Shishkina, Victoria V. [1 ,3 ]
Savushkina, Inessa A. [1 ]
Perveeva, Inna M. [4 ]
Feigelman, Sofia N. [1 ]
Kitoyan, Avag G. [1 ]
Drobysheva, Valeria R. [1 ]
机构
[1] Voronezh State Med Univ, Voronezh, Russia
[2] I M Sechenov First Moscow State Med Univ Sechenov, Moscow, Russia
[3] Voronezh State Med Univ, Res Inst Expt Biol & Med, Voronezh, Russia
[4] Voronezh Reg Clin Hosp 1, Voronezh, Russia
关键词
COVID-19; SARS-CoV-2; carboxypeptidase A3; mast cells;
D O I
10.21103/Article13(4)_OA11
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
Background: This study aimed to determine the involvement of carboxypeptidase A3 (CPA3) in developing lung damage in patients with COVID-19. Methods and Results: The study included samples of autopsy material from the lungs of patients who died as a result of severe COVID-19 (the main group [MG] and persons who died from external causes (the control group [CG]). Immunohistochemical staining for CPA3 was carried out. A quantitative study of CPA3-positive mast cells (MCs) and the degree of their degranulation was carried out using a x40 objective lens with an analysis of >= 50 fields of view with further conversion to 1 mm(2). Significant representation of CPA3-positive MCs per 1 mm(2) of CPA3-positive MCs, CPA3-positive MCs with signs of degranulation (SD), and co-adjacent MCs was found in the MG compared to the CG (P=0.01 in all cases). In the main group, positive correlations were identified between the total number of CPA3-positive MCs, CPA3-positive MCs with SD and the blood hemoglobin level shortly before death (r=0.491 [P=0.008] and r=0.521 [P=0.004], respectively). Co-adjacent CPA3-positive MCs were negatively correlated with blood eosinophils at the beginning of hospitalization (r=-0.420 [P=0.023]). Also, the number of separately lying, CPA3-positive MCs negatively correlated with the blood monocyte shortly before death (r=-0.384 [P=0.044]). A positive correlation was established between the total number of CPA3-positive MCs, CPA3-positive MCs with SD, and adjacent CPA3-positive MCs with total blood protein in patients at the beginning of hospitalization (r=0.431 [P=0.020], r=0.449 [P=0.015] and r=0.456 [P=0.013], respectively). In addition, the study demonstrated a positive correlation between CPA3-positive MCs with SD and the total number of CPA3-positive MCs with blood aPTT levels (r=0.304 [P=0.045] and r=0.375 [P=0.045], respectively). A negative correlation was also found between the total number of CPA3-positive MCs and the blood INR level (r=-0.812 [P=0.050]). Finally, in patients at the beginning of hospitalization, a negative correlation was found between CPA3-positive MCs with SD, CPA3-positive MCs without SD, separately located CPA3-positive MCs, adjacent CPA3-positive MCs, and the total number of CPA3-positive MCs with blood amylase (r=-0.550 [P=0.002], r=-0.452 [P=0.045], r=-0.485 [P=0.030], r=-0.622 [P=0.008], and r=-0.590 [P=0.006], respectively). Conclusion: Our study identifies the potential involvement of CPA3 in the pathogenesis of severe COVID-19. However, many aspects of its participation remain unclear and require further study.
引用
收藏
页码:301 / 305
页数:5
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