Ex vivo study on the human blood neutrophil circadian features and effects of alpha1-antitrypsin and lipopolysaccharide

IF 3.5 3区 医学 Q2 PHARMACOLOGY & PHARMACY Vascular pharmacology Pub Date : 2024-06-17 DOI:10.1016/j.vph.2024.107396
Julia Held , Kokilavani Sivaraman , Sabine Wrenger , Wenzhang Si , Tobias Welte , Stephan Immenschuh , Sabina Janciauskiene
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Abstract

Aims

Neutrophils perform various functions in a circadian-dependent manner; therefore, we investigated here whether the effect of alpha1-antitrypsin (AAT), used as augmentation therapy, is dependent on the neutrophil circadian clock. AAT is a vital regulator of neutrophil functions, and its qualitative and/or quantitative defects have significant implications for the development of respiratory diseases.

Methods

Whole blood from 12 healthy women age years, mean (SD) 29.92 (5.48) was collected twice daily, 8 h apart, and incubated for 30 min at 37 °C alone or with additions of 2 mg/ml AAT (Respreeza) and/or 5 μg/ml lipopolysaccharide (LPS) from Escherichia coli. Neutrophils were then isolated to examine gene expression, migration and phagocytosis.

Results

The expression of CD14, CD16, CXCR2 and SELL (encoding CD62L) genes was significantly higher while CDKN1A lower in the afternoon than in the morning neutrophils from untreated blood. Neutrophils isolated in the afternoon had higher migratory and phagocytic activity. Morning neutrophils isolated from AAT-pretreated blood showed higher expression of CXCR2 and SELL than those from untreated morning blood. Pretreatment of blood with AAT enhanced migratory properties of morning but not afternoon neutrophils. Of all genes analysed, only CXCL8 expression was strongly upregulated in morning and afternoon neutrophils isolated from LPS-pretreated blood, whereas CXCR2 expression was downregulated in afternoon neutrophils. The addition of AAT did not reverse the effects of LPS.

Significance

The circadian clock of myeloid cells may affect the effectiveness of various therapies, including AAT therapy used to treat patients with AAT deficiency, and needs further investigation.

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人体血液中性粒细胞昼夜节律特征及α1-抗胰蛋白酶和脂多糖影响的体内外研究。
目的:中性粒细胞以昼夜节律依赖的方式执行各种功能;因此,我们在此研究了作为增强疗法的α1-抗胰蛋白酶(AAT)的作用是否依赖于中性粒细胞的昼夜节律。AAT 是中性粒细胞功能的重要调节因子,其质量和/或数量缺陷对呼吸系统疾病的发展有重要影响:方法:采集 12 名健康女性的全血[年龄,平均(标清)29.92(5.48)岁],每天两次,每次间隔 8 小时,然后在 37 °C 下单独或加入 2 mg/ml AAT(Respreeza)和/或 5 μg/ml 大肠杆菌脂多糖(LPS)培养 30 分钟。然后分离中性粒细胞,检测基因表达、迁移和吞噬能力:结果:从未经处理的血液中分离出的中性粒细胞,其 CD14、CD16、CXCR2 和 SELL(编码 CD62L)基因的表达量在下午明显高于上午,而 CDKN1A 的表达量则低于上午。下午分离的中性粒细胞具有更高的迁移和吞噬活性。与上午未处理的血液相比,上午从 AAT 预处理血液中分离出来的中性粒细胞的 CXCR2 和 SELL 表达更高。用 AAT 预处理血液能增强上午中性粒细胞的迁移特性,但不能增强下午中性粒细胞的迁移特性。在分析的所有基因中,只有 CXCL8 的表达在上午和下午从 LPS 预处理血液中分离出来的中性粒细胞中强烈上调,而 CXCR2 的表达在下午的中性粒细胞中下调。添加 AAT 并不能逆转 LPS 的影响:髓系细胞的昼夜节律可能会影响各种疗法的效果,包括用于治疗AAT缺乏症患者的AAT疗法,因此需要进一步研究。
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来源期刊
Vascular pharmacology
Vascular pharmacology 医学-药学
CiteScore
6.60
自引率
2.50%
发文量
153
审稿时长
31 days
期刊介绍: Vascular Pharmacology publishes papers, which contains results of all aspects of biology and pharmacology of the vascular system. Papers are encouraged in basic, translational and clinical aspects of Vascular Biology and Pharmacology, utilizing approaches ranging from molecular biology to integrative physiology. All papers are in English. The Journal publishes review articles which include vascular aspects of thrombosis, inflammation, cell signalling, atherosclerosis, and lipid metabolism.
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