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血液血细胞比容水平预测社区心力衰竭发生的作用。

Usefulness of the blood hematocrit level to predict development of heart failure in a community.

机构信息

Framingham Heart Study, Massachusetts, USA.

出版信息

Am J Cardiol. 2012 Jan 15;109(2):241-5. doi: 10.1016/j.amjcard.2011.08.037. Epub 2011 Oct 12.

Abstract

Current data suggest that increases in hemoglobin may decrease nitric oxide and adversely affect vascular function. In the preclinical setting, these changes could precipitate the development of heart failure (HF). We hypothesized that higher hematocrit (HCT) would be associated with an increased incidence of new-onset HF in the community. We evaluated 3,523 participants (59% women) from the Framingham Heart Study who were 50 to 65 years old and free of HF. Participants were followed prospectively until an HF event, death, or the end of 20 years of follow up. HCT was subdivided into 4 gender-specific categories (women: HCT 36.0 to 40.0, 40.1 to 42.0, 42.1 to 45.0, >45.0; men: 39.0 to 44.0, 44.1 to 45.0, 45.1 to 49.0, >49.0). Gender-pooled multivariable Cox proportional hazards models were used to estimate the association of HCT with incident HF, adjusting for clinical risk factors. During the follow-up period (61,417 person-years), 217 participants developed HF (100 events in women). There was a linear increase in risk of HF across the 4 HCT categories (p for trend = 0.002). Hazards ratios for HF in the low-normal, normal, and high HCT categories were 1.27 (95% confidence interval 0.82 to 1.97), 1.47 (1.01 to 2.15), and 1.78 (1.15 to 2.75), respectively, compared to the lowest HCT category (p for trend <0.0001). Adjustment for interim development of other cardiovascular diseases and restriction of the sample to nonsmokers did not alter the results. In conclusion, higher levels of HCT, even within the normal range, were associated with an increased risk of developing HF in this long-term follow-up study.

摘要

目前的数据表明,血红蛋白的增加可能会减少一氧化氮并对血管功能产生不利影响。在临床前环境中,这些变化可能会导致心力衰竭(HF)的发展。我们假设较高的血细胞比容(HCT)与社区中新发 HF 的发生率增加有关。我们评估了来自弗雷明汉心脏研究的 3523 名参与者(59%为女性),年龄在 50 至 65 岁之间,且无 HF。参与者前瞻性随访,直至发生 HF 事件、死亡或随访 20 年结束。HCT 分为 4 个性别特异性类别(女性:HCT 36.0 至 40.0、40.1 至 42.0、42.1 至 45.0、>45.0;男性:39.0 至 44.0、44.1 至 45.0、45.1 至 49.0、>49.0)。使用性别合并多变量 Cox 比例风险模型来估计 HCT 与新发 HF 的相关性,同时调整临床危险因素。在随访期间(61417 人年),217 名参与者发生 HF(女性 100 例)。在 4 个 HCT 类别中,HF 的风险呈线性增加(趋势检验 p 值=0.002)。HCT 低值正常、正常和高值组的 HF 发生风险比分别为 1.27(95%置信区间 0.82 至 1.97)、1.47(1.01 至 2.15)和 1.78(1.15 至 2.75),与最低 HCT 类别相比(趋势检验 p 值<0.0001)。调整中间发生其他心血管疾病以及将样本限制为不吸烟者,并未改变结果。总之,即使在正常范围内,较高的 HCT 水平与长期随访研究中 HF 发生风险增加相关。

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