Associations of Smoking, Cytomegalovirus Serostatus, and Natural Killer Cell Phenotypes in Smokers With and At Risk for COPD.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Robert M Burkes, Elijah Bailey, Timothy Hwalek, Andrew Osterburg, Laura Lach, Ralph Panos, Stephen N Waggoner, Michael T Borchers
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引用次数: 0

Abstract

Introduction: Chronic obstructive disease (COPD) risk factors, smoking, and chronic infection (cytomegalovirus [CMV]) may mold natural killer (NK) cell populations. What is not known is the magnitude of the effect CMV seropositivity imparts on populations of smokers with and at risk for COPD. We investigate the independent influence of CMV seropositivity on NK cell populations and differential effects when stratifying by COPD and degree of smoking history.

Methods: Descriptive statistics determine the relationship between cytotoxic NK cell populations and demographic and clinical variables. Multivariable linear regression and predictive modeling were performed to determine associations between positive CMV serology and proportions of CD57+ and natural killer group 2C (NKG2C)+ NK cells. We dichotomized our analysis by those with a heavy smoking history and COPD and described the effect size of CMV seropositivity on NK cell populations.

Results: When controlled for age, race, sex, pack-years smoked, body mass index, and lung function, CMV+ serostatus was independently associated with a higher proportion of CD57+, NKG2C+, and NKG2C+CD57+ NK cells. CMV+ serostatus was the sole predictor of larger NKG2C+ and CD57+NKG2C+ populations. Associations are more pronounced in those with COPD and heavy smokers.

Conclusions: Among Veterans who are current and former smokers, CMV+ serostatus was independently associated with larger CD57+ and NKG2C+ populations, with a larger effect in heavy smokers and those with COPD, and was the sole predictor for increased expression of NKG2C+ and CD57+NKG2C+ populations. These findings may be broadened to include the assessment of longitudinal NK cell population change, accrued inflammatory potential, and further identification of pro-inflammatory NK cell population clusters.

吸烟、巨细胞病毒血清状态和自然杀伤细胞表型在慢性阻塞性肺病患者和高危人群中的相关性
慢性阻塞性疾病(COPD)的危险因素,吸烟和慢性感染(巨细胞病毒[CMV])可能会塑造自然杀伤(NK)细胞群。目前尚不清楚的是,巨细胞病毒血清阳性对患有和有COPD风险的吸烟者的影响程度。我们研究了CMV血清阳性对NK细胞群的独立影响,以及在COPD和吸烟史程度分层时的差异效应。方法:描述性统计方法确定细胞毒性NK细胞数量与人口统计学和临床变量之间的关系。通过多变量线性回归和预测建模来确定CMV阳性血清学与CD57+和自然杀伤组2C (NKG2C)+ NK细胞比例之间的关系。我们对重度吸烟史和COPD患者进行了分析,并描述了CMV血清阳性对NK细胞群的影响大小。结果:在控制年龄、种族、性别、吸烟年数、体重指数和肺功能的情况下,CMV+血清状态与CD57+、NKG2C+和NKG2C+CD57+ NK细胞比例较高独立相关。CMV+血清状态是NKG2C+和CD57+NKG2C+人群的唯一预测因子。在慢性阻塞性肺病患者和重度吸烟者中,这种关联更为明显。结论:在当前和以前吸烟的退伍军人中,CMV+血清状态与较大的CD57+和NKG2C+人群独立相关,在重度吸烟者和COPD患者中影响更大,并且是NKG2C+和CD57+NKG2C+人群表达增加的唯一预测因子。这些发现可以扩大到包括纵向NK细胞群变化的评估,累积的炎症潜力,以及进一步鉴定促炎NK细胞群。
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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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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