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皮质醇对严重烧伤休克患者转录组的调节:一项前瞻性随机试验的辅助分析。

Transcriptome modulation by hydrocortisone in severe burn shock: ancillary analysis of a prospective randomized trial.

机构信息

EA7426, Université Claude Bernard Lyon 1, Hospices Civils de Lyon, bioMérieux ; "Pathophysiology of injury induced immunosuppression (PI3)", hôpital E. Herriot, 5 place d'Arsonval, 69437, Lyon, France.

Hospices Civils de Lyon, Immunology laboratory, hôpital E. Herriot, 5 place d'Arsonval, 69437, Lyon, France.

出版信息

Crit Care. 2017 Jun 16;21(1):158. doi: 10.1186/s13054-017-1743-9.

Abstract

BACKGROUND

Despite shortening vasopressor use in shock, hydrocortisone administration remains controversial, with potential harm to the immune system. Few studies have assessed the impact of hydrocortisone on the transcriptional response in shock, and we are lacking data on burn shock. Our objective was to assess the hydrocortisone-induced transcriptional modulation in severe burn shock, particularly modulation of the immune response.

METHODS

We collected whole blood samples during a randomized controlled trial assessing the efficacy of hydrocortisone administration in burn shock. Using whole genome microarrays, we first compared burn patients (n = 32) from the placebo group to healthy volunteers to describe the transcriptional modulation induced by burn shock over the first week. Then we compared burn patients randomized for either hydrocortisone administration or placebo, to assess hydrocortisone-induced modulation.

RESULTS

Study groups were similar in terms of severity and major outcomes, but shock duration was significantly reduced in the hydrocortisone group. Many genes (n = 1687) were differentially expressed between burn patients and healthy volunteers, with 85% of them exhibiting a profound and persistent modulation over seven days. Interestingly, we showed that hydrocortisone enhanced the shock-associated repression of adaptive, but also innate immunity.

CONCLUSIONS

We found that the initial host response to burn shock encompasses wide and persistent modulation of gene expression, with profound modulation of pathways associated with metabolism and immunity. Importantly, hydrocortisone administration may worsen the immunosuppression associated with severe injury. These data should be taken into account in the risk ratio of hydrocortisone administration in patients with inflammatory shock.

TRIAL REGISTRATION

ClinicalTrials.gov, NCT00149123 . Registered on 6 September 2005.

摘要

背景

尽管在休克中缩短血管加压素的使用时间,但皮质醇的给药仍然存在争议,因为它可能对免疫系统造成损害。很少有研究评估皮质醇对休克中基因转录反应的影响,我们缺乏烧伤休克的数据。我们的目的是评估皮质醇在严重烧伤休克中的诱导转录调节作用,特别是对免疫反应的调节作用。

方法

我们在一项评估皮质醇在烧伤休克中的疗效的随机对照试验中采集了全血样本。使用全基因组微阵列,我们首先将烧伤患者(n=32)与安慰剂组的健康志愿者进行比较,以描述烧伤休克在第一周内引起的基因转录调节。然后,我们将接受皮质醇或安慰剂治疗的烧伤患者进行比较,以评估皮质醇诱导的调节作用。

结果

研究组在严重程度和主要结局方面相似,但皮质醇组的休克持续时间明显缩短。烧伤患者与健康志愿者之间有许多基因(n=1687)存在差异表达,其中 85%的基因在七天内表现出明显和持久的调节。有趣的是,我们发现皮质醇增强了休克相关的适应性免疫和固有免疫的抑制。

结论

我们发现,机体对烧伤休克的初始反应包括广泛和持久的基因表达调节,涉及代谢和免疫途径的显著调节。重要的是,皮质醇给药可能会加重严重损伤相关的免疫抑制。这些数据应在炎症性休克患者使用皮质醇的风险比中加以考虑。

试验注册

ClinicalTrials.gov,NCT00149123。于 2005 年 9 月 6 日注册。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1bbe/5473974/d145635daeef/13054_2017_1743_Fig1_HTML.jpg

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