Changes in immature granulocyte levels and their association with disease activation following biologic therapy in patients with ankylosing spondylitis

Burak Okyar , Servet Yüce , İbrahim Halil Bilen , Bekir Torun , İlyas Öztürk , Gözde Yıldırım Çetin
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Abstract

Introduction

AS is a chronic disease with an inflammatory serum microenvironment characterized by increased oxidative stress (OS). Along with OS, reactive oxygen species (ROS) are elevated in patients with AS. Overexpression of ROS causes active inflammatory processes leading to the secretion of pro-inflammatory factors, including tumor necrosis factor-alpha (TNF-α). Immature granulocytes (IG) are essential to the chronic inflammatory process. This may mean that IG can be a parameter used in the follow-up of chronic inflammatory diseases such as AS.

Objective

We aimed to evaluate the change in IG in patients with AS who were on biologic medication for six months after diagnosis and to assess its relationship with disease activity, remission, and BASDAI score.

Methods

This single-center, retrospective study was conducted between January 2020 and January 2022. For the study, 68 patients were included in the patient group and 74 patients in the control group. Demographic and laboratory data were recorded and compared in the groups. Then, the patient group was divided into two groups: pre-biologic drug and post-biologic drug. Hemogram data, IG, ESR, CRP, and BASDAI data were recorded for both groups. Correlation analysis was performed between the results of IG data and hemogram and laboratory data.

Conclusion

In our study, WBC, neutrophil, IG, and IG% ratios were significantly higher in AS patients compared to the control group. Neutrophil, IG, and IG% levels were significantly decreased in the AS group compared to pretreatment and post-treatment comparisons. In addition, IG levels were correlated with WBC, neutrophil, CRP, and ESR levels. This study hypothesized that IG values may be a valuable parameter for monitoring AS disease severity, response to treatment, and disease activation after biological drug use.
强直性脊柱炎患者生物治疗后未成熟粒细胞水平的变化及其与疾病激活的关系
as是一种慢性疾病,其炎症性血清微环境以氧化应激(OS)增加为特征。随着OS的发生,AS患者的活性氧(ROS)升高。ROS的过度表达引起活跃的炎症过程,导致促炎因子的分泌,包括肿瘤坏死因子-α (TNF-α)。未成熟粒细胞(IG)对慢性炎症过程至关重要。这可能意味着IG可以作为慢性炎症性疾病如as的随访参数。目的:我们旨在评估诊断后6个月接受生物药物治疗的AS患者IG的变化,并评估其与疾病活动性、缓解和BASDAI评分的关系。方法本研究于2020年1月至2022年1月进行单中心回顾性研究。在这项研究中,68例患者被纳入患者组,74例患者被纳入对照组。记录并比较各组的人口统计和实验室数据。然后将患者组分为生物前用药组和生物后用药组。记录两组患者血象、IG、ESR、CRP及BASDAI数据。IG数据、血象图结果与实验室数据进行相关性分析。结论在我们的研究中,AS患者的WBC、中性粒细胞、IG和IG%比值明显高于对照组。与治疗前和治疗后比较,AS组的中性粒细胞、IG和IG%水平显著降低。此外,IG水平与WBC、中性粒细胞、CRP和ESR水平相关。本研究假设IG值可能是监测AS疾病严重程度、治疗反应和使用生物药物后疾病激活的有价值参数。
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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