溶血磷脂酸种类与慢性阻塞性肺疾病恶化有关。
Lysophosphatidic acid species are associated with exacerbation in chronic obstructive pulmonary disease.
机构信息
Department of Microchemistry, Proteomics and Lipidomics, Genentech, Inc., South San Francisco, CA, USA.
Department of Biomarker Discovery OMNI, Genentech, Inc., South San Francisco, CA, USA.
出版信息
BMC Pulm Med. 2021 Sep 23;21(1):301. doi: 10.1186/s12890-021-01670-9.
BACKGROUND
Chronic obstructive pulmonary disease (COPD) exacerbations are heterogenous and profoundly impact the disease trajectory. Bioactive lipid lysophosphatidic acid (LPA) has been implicated in airway inflammation but the significance of LPA in COPD exacerbation is not known. The aim of the study was to investigate the utility of serum LPA species (LPA16:0, 18:0, 18:1, 18:2, 20:4) as biomarkers of COPD exacerbation.
PATIENTS AND METHODS
LPA species were measured in the baseline placebo sera of a COPD randomized controlled trial. Tertile levels of each LPA were used to assign patients into biomarker high, medium, and low subgroups. Exacerbation rate and risk were compared among the LPA subgroups.
RESULTS
The levels of LPA species were intercorrelated (rho 0.29-0.91). Patients with low and medium levels of LPA (LPA16:0, 20:4) had significantly higher exacerbation rate compared to the respective LPA-high patients [estimated rate per patient per year (95% CI)]: LPA16:0-low = 1.2 (0.8-1.9) (p = 0.019), LPA16:0-medium = 1.3 (0.8-2.0) (p = 0.013), LPA16:0-high = 0.5 (0.2-0.9); LPA20:4-low = 1.4 (0.9-2.1) (p = 0.0033), LPA20:4-medium = 1.2 (0.8-1.8) (p = 0.0089), LPA20:4-high = 0.4 (0.2-0.8). These patients also had earlier time to first exacerbation (hazard ratio (95% CI): LPA16:0-low = 2.6 (1.1-6.0) (p = 0.028), LPA16:0-medium = 2.7 (1.2-6.3) (p = 0.020); LPA20.4-low = 2.8 (1.2-6.6) (p = 0.017), LPA20:4-medium = 2.7 (1.2-6.4) (p = 0.021). Accordingly, these patients had a significant increased exacerbation risk compared to the respective LPA-high subgroups [odd ratio (95% CI)]: LPA16:0-low = 3.1 (1.1-8.8) (p = 0.030), LPA16:0-medium = 3.0 (1.1-8.3) (p = 0.031); LPA20:4-low = 3.8 (1.3-10.9) (p = 0.012), LPA20:4-medium = 3.3 (1.2-9.5) (p = 0.025). For the other LPA species (LPA18:0, 18:1, 18:2), the results were mixed; patients with low and medium levels of LPA18:0 and 18:2 had increased exacerbation rate, but only LPA18:0-low patients had significant increase in exacerbation risk and earlier time to first exacerbation compared to the LPA18:0-high subgroup.
CONCLUSIONS
The study provided evidence of association between systemic LPA levels and exacerbation in COPD. Patients with low and medium levels of specific LPA species (LPA16:0, 20:4) had increased exacerbation rate, risk, and earlier time to first exacerbation. These non-invasive biomarkers may aid in identifying high risk patients with dysregulated LPA pathway to inform risk management and drug development.
背景
慢性阻塞性肺疾病(COPD)加重是异质的,对疾病轨迹有深远影响。生物活性脂质溶血磷脂酸(LPA)已被牵连到气道炎症中,但 LPA 在 COPD 加重中的意义尚不清楚。本研究旨在探讨血清 LPA 种类(LPA16:0、18:0、18:1、18:2、20:4)作为 COPD 加重的生物标志物的效用。
患者和方法
在 COPD 随机对照试验的安慰剂基线血清中测量了 LPA 种类。每个 LPA 的三分位数水平用于将患者分配到高、中、低生物标志物亚组。比较了 LPA 亚组之间的加重率和风险。
结果
LPA 种类之间存在相关性(rho 0.29-0.91)。低和中水平 LPA(LPA16:0、20:4)的患者与各自的 LPA 高患者相比,加重率显著更高[估计每位患者每年的发生率(95%CI)]:LPA16:0-低=1.2(0.8-1.9)(p=0.019),LPA16:0-中=1.3(0.8-2.0)(p=0.013),LPA16:0-高=0.5(0.2-0.9);LPA20:4-低=1.4(0.9-2.1)(p=0.0033),LPA20:4-中=1.2(0.8-1.8)(p=0.0089),LPA20:4-高=0.4(0.2-0.8)。这些患者也更早地出现首次加重(风险比(95%CI):LPA16:0-低=2.6(1.1-6.0)(p=0.028),LPA16:0-中=2.7(1.2-6.3)(p=0.020);LPA20:4-低=2.8(1.2-6.6)(p=0.017),LPA20:4-中=2.7(1.2-6.4)(p=0.021)。因此,与各自的 LPA 高亚组相比,这些患者的加重风险显著增加[比值比(95%CI)]:LPA16:0-低=3.1(1.1-8.8)(p=0.030),LPA16:0-中=3.0(1.1-8.3)(p=0.031);LPA20:4-低=3.8(1.3-10.9)(p=0.012),LPA20:4-中=3.3(1.2-9.5)(p=0.025)。对于其他 LPA 种类(LPA18:0、18:1、18:2),结果不一;低和中水平 LPA18:0 和 18:2 的患者加重率增加,但只有 LPA18:0-低的患者与 LPA18:0-高亚组相比,首次加重的风险和时间更早。
结论
该研究提供了血清 LPA 水平与 COPD 加重之间关联的证据。特定 LPA 种类(LPA16:0、20:4)低和中水平的患者加重率、风险和首次加重时间更早。这些非侵入性生物标志物可能有助于识别失调的 LPA 途径的高危患者,以告知风险管理和药物开发。
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