CD8αα expression on NK cells is associated with different K562 and MOLT4 killing capabilities of PBMC and different involvement CD8pos and CD8neg subsets in anti-viral response

Likars'ka sprava / Ministerstvo okhorony zdorov'ia Ukraïny Pub Date : 2023-03-30 DOI:10.31640/ls-2023-1-04

B. V. Dons’koi, E. I. Dubrovskyi

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Abstract

Introduction. The CD8αα are present in a subset of T cells and NK cells, but its function is mostly unknown, as well as the role of CD8+ and CD8- NK cell subsets in physiological and pathological environments. Methods. We investigated 130 healthy individuals’ blood samples for the NK cell cytotoxicity against K562 and MOLT4 cell lines. We also analyzed patients after SarsCov2 infection and compared to healthy control. The NK cell phenotype and cytotoxicity were studied by the FACScan flow cytometer using BD monoclonal antibodies. Results. We confirmed that MOLT4 is significantly more resistant to the NK cell cytotoxicity compared to the “classical” K562. CD8+ NK cells are more effective at K562 killing compared to CD8- subsets. The correlation of lymphocyte levels with the specific K562 lysis was weaker for CD8- NK cell subsets (r = 0.37) than CD8+ NK cells (r = 0.45) or whole NK cells population (r = 0.46). However, we found that CD8+ NK cells mostly did not participate in the MOLT-4 killing. CD8- NK cells frequency correlates with MOLT4 lysis more significantly (r = 0.49) than CD8+ NK cells lymphocytes levels (r = 0.27) or whole NK cells population (r = 0.44). Also, we showed that HLA-DR and CD158a positive NK cell levels did not correlate with the MOLT4 and K562 killing, while HLA-DR and CD158a negative subsets levels did with the same significance as the whole NK cells population. Decreased of NK lymphocytes after SarsCov2 infection results to decrease NK population owing to CD8+NK decreased but not CD8neg. Conclusion. NK cell numbers determine NK cell cytotoxicity indirectly through the surface phenotype. CD8 expression on the NK cells is associated with the effective cytotoxicity against K562 but at the same time obstructs a response to MOLT4. CD8αα on NK cells might participate in HLA recognition or enhance response to HLA class-I negative target cells.

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NK细胞上CD8αα的表达与PBMC不同的K562和MOLT4杀伤能力以及不同的CD8pos和CD8neg亚群参与抗病毒应答有关

介绍。CD8αα存在于T细胞和NK细胞的一个亚群中，但其功能以及CD8+和CD8- NK细胞亚群在生理和病理环境中的作用大多未知。方法。我们检测了130例健康人血液样本NK细胞对K562和MOLT4细胞系的细胞毒性。我们还分析了感染SarsCov2的患者，并与健康对照进行了比较。采用BD单克隆抗体，流式细胞仪检测NK细胞表型和细胞毒性。结果。我们证实，与“经典”的K562相比，MOLT4对NK细胞毒性的抵抗力明显增强。与CD8-亚群相比，CD8+ NK细胞更有效地杀死K562。淋巴细胞水平与特异性K562裂解的相关性在CD8- NK细胞亚群(r = 0.37)弱于CD8+ NK细胞(r = 0.45)或整个NK细胞群(r = 0.46)。然而，我们发现CD8+ NK细胞大多不参与MOLT-4杀伤。CD8- NK细胞频率与MOLT4溶解的相关性(r = 0.49)高于CD8+ NK细胞淋巴细胞水平(r = 0.27)或整个NK细胞群(r = 0.44)。此外，我们发现HLA-DR和CD158a阳性NK细胞水平与MOLT4和K562的杀伤无关，而HLA-DR和CD158a阴性亚群水平与整个NK细胞群体具有相同的意义。SarsCov2感染后NK淋巴细胞减少，由于CD8+NK减少而非CD8阴性导致NK种群减少。结论。NK细胞数量通过表面表型间接决定NK细胞的细胞毒性。NK细胞上CD8的表达与K562的有效细胞毒性有关，但同时也阻碍了对MOLT4的反应。NK细胞上的CD8αα可能参与HLA识别或增强对HLA - i类阴性靶细胞的应答。

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Likars'ka sprava / Ministerstvo okhorony zdorov'ia Ukraïny

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