Dept of Anaesthesia and Intensive Care Medicine, St James Hospital, James Street, Dublin 08, Ireland.
Crit Care. 2011 Jun 28;15(3):R158. doi: 10.1186/cc10293.
Lymphocyte homeostasis is dependent on the γc cytokines. We hypothesised that sepsis in humans is associated with differential gene expression of the γc cytokines and their associated apoptosis mediators.
The study population consisted of a total of 60 patients with severe sepsis, 15 with gram negative bacteraemia, 10 healthy controls and 60 patients undergoing elective lung resection surgery. Pneumonia was diagnosed by CDC NNIC criteria. Gene expression in peripheral blood leukocytes (PBLs) of interleukin (IL)-2, 7, 15 and interferon (IFN)-γ, Bax, Bim, Bcl-2 was determined by qRT-PCR and IL-2 and IL-7 serum protein levels by ELISA. Gene expression of IL-2, 7 and IFN-γ was measured in peripheral blood leukocytes (PBL), cultured in the presence of lipopolysaccharide (LPS) and CD3 binding antibody (CD3ab)
IL-2 gene expression was lower in the bacteraemia group compared with controls, and lower still in the sepsis group (P < 0.0001). IL-7 gene expression was similar in controls and bacteraemia, but lower in sepsis (P < 0.0001). IL-15 gene expression was similar in the three groups. Bcl-2 gene expression was less (P < 0.0001) and Bim gene expression was greater (P = 0.0003) in severe sepsis compared to bacteraemic and healthy controls. Bax gene expression was similar in the three groups.In lung resection surgery patients, post-operative pneumonia was associated with a perioperative decrease in IL-2 mRNA (P < 0.0001) and IL-7 mRNA (P = 0.003). IL-2 protein levels were reduced in sepsis and bacteraemia compared to controls (P = 0.02) but similar in pneumonia and non-pneumonia groups. IL-7 protein levels were similar in all groups.In cultured PBLs, IFN-γ gene expression was decreased in response to LPS and increased in response to CD3ab with sepsis: IL-7 gene expression increased in response to LPS in controls and to CD3ab with sepsis; Bcl-2 gene expression decreased in response to combined CD3ab and IL-2 with sepsis.
Patients with infection and sepsis have deficient IL-2 and IL-7 gene expression in PBLs. Aberrant cytokine gene expression may precede the onset of infection.
淋巴细胞稳态依赖于 γc 细胞因子。我们假设,人类脓毒症与 γc 细胞因子及其相关凋亡介质的差异基因表达有关。
研究人群包括 60 例严重脓毒症患者、15 例革兰氏阴性菌血症患者、10 例健康对照者和 60 例择期行肺切除术患者。肺炎的诊断采用 CDC NNIC 标准。通过 qRT-PCR 测定白细胞介素 (IL)-2、7、15 和干扰素 (IFN)-γ、Bax、Bim、Bcl-2 的外周血白细胞 (PBL) 中的基因表达,并通过 ELISA 测定血清 IL-2 和 IL-7 蛋白水平。在脂多糖 (LPS) 和 CD3 结合抗体 (CD3ab) 的存在下,测量 PBL 中 IL-2、7 和 IFN-γ 的基因表达。
与对照组相比,菌血症组的 IL-2 基因表达较低,脓毒症组的 IL-2 基因表达更低 (P < 0.0001)。对照组和菌血症组的 IL-7 基因表达相似,但脓毒症组的 IL-7 基因表达较低 (P < 0.0001)。三组的 IL-15 基因表达相似。与菌血症和健康对照组相比,严重脓毒症患者的 Bcl-2 基因表达减少 (P < 0.0001),Bim 基因表达增加 (P = 0.0003)。三组 Bax 基因表达相似。在肺切除术患者中,术后肺炎与围手术期 IL-2 mRNA 减少相关 (P < 0.0001),与 IL-7 mRNA 减少相关 (P = 0.003)。与对照组相比,脓毒症和菌血症患者的 IL-2 蛋白水平降低 (P = 0.02),但肺炎组和非肺炎组的 IL-2 蛋白水平相似。所有组的 IL-7 蛋白水平相似。在培养的 PBL 中,IL-2 和 LPS 反应时 IFN-γ 基因表达减少,CD3ab 反应时 IFN-γ 基因表达增加;与对照组相比,LPS 反应时 IL-7 基因表达增加,与脓毒症时 CD3ab 反应时 IL-7 基因表达增加;与脓毒症时联合 CD3ab 和 IL-2 反应时 Bcl-2 基因表达减少。
感染和脓毒症患者的 PBL 中 IL-2 和 IL-7 基因表达不足。细胞因子基因表达异常可能先于感染的发生。
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