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成人呼吸窘迫综合征患者的肺泡巨噬细胞表达高水平的热休克蛋白72信使核糖核酸。

Alveolar macrophages of patients with adult respiratory distress syndrome express high levels of heat shock protein 72 mRNA.

作者信息

Kindas-Mügge I, Pohl W R, Zavadova E, Köhn H D, Fitzal S, Kummer F, Micksche M

机构信息

Institute of Tumor Biology/Cancer Research, Vienna University, Austria.

出版信息

Shock. 1996 Mar;5(3):184-9. doi: 10.1097/00024382-199603000-00003.

Abstract

Adult respiratory distress syndrome (ARDS), a multifactorial disease with poor prognosis, is characterized by an accumulation of inflammatory cells within the airspaces of the lungs. There is evidence that alveolar macrophages (AM) are involved in the pathogenesis of this pulmonary disease. It has been demonstrated that AM synthesize heat shock proteins (HSPs) after exposure to certain stress factors. Increasing evidence suggests that HSPs could confer protection against oxidative injury, noxious molecules, and bacterial toxins. In stressed cells HSP 72 appears to be essential for survival during and after exposure to cellular injury. The aim of this study was to evaluate the magnitude of HSP 72 expression by human AM of patients with ARDS and correlate that with respiratory burst activity. Bronchoalveolar lavage was performed in six ARDS patients, 10 patients with high risk for developing ARDS, and two patients who underwent bronchoscopy for other reasons. Spontaneous ex vivo expression of HSP 72 in AM could be demonstrated by immunocytochemistry. Total RNA as well as poly(A)-rich mRNA were extracted from recovered AM and analyzed by Northern blot and slot blot using a human HSP 72-specific probe. Signals of slot blot were analyzed by densitometry and expressed as relative levels of HSP 72 mRNA of stressed (42 degrees C) HT 1080 control cells. Significantly (p < .001) higher levels of HSP 72 mRNA were measured in patients with ARDS (96.2 +/- 9.5 relative levels) in comparison to those not developing this syndrome (46.0 +/- 4.2). With regard to respiratory burst activity of AM in patients with ARDS, there was a negative correlation between HSP 72 expression and reactive oxygen species production. The AM of patients with ARDS with high relative levels of HSP 72 expression showed low respiratory burst activity. A predictive value for disease severity of high level of HSP 72 mRNA in AM in patients at risk for ARDS has to be evaluated by future studies. This demonstration of HSP 72 expression ex vivo suggests a protective role of HSP response against endo/exogenously generated stress factors in AM.

摘要

成人呼吸窘迫综合征(ARDS)是一种预后不良的多因素疾病,其特征是肺内气腔中炎性细胞的积聚。有证据表明肺泡巨噬细胞(AM)参与了这种肺部疾病的发病机制。已经证明,AM在暴露于某些应激因素后会合成热休克蛋白(HSPs)。越来越多的证据表明,HSPs可以提供针对氧化损伤、有害分子和细菌毒素的保护作用。在应激细胞中,HSP 72似乎对于暴露于细胞损伤期间及之后的存活至关重要。本研究的目的是评估ARDS患者的人AM中HSP 72表达的程度,并将其与呼吸爆发活性相关联。对6例ARDS患者、10例有发生ARDS高风险的患者以及2例因其他原因接受支气管镜检查的患者进行了支气管肺泡灌洗。通过免疫细胞化学可以证明AM中HSP 72的自发体外表达。从回收的AM中提取总RNA以及富含多聚腺苷酸的mRNA,并使用人HSP 72特异性探针通过Northern印迹和狭缝印迹进行分析。通过密度测定法分析狭缝印迹的信号,并表示为应激(42℃)HT 1080对照细胞的HSP 72 mRNA的相对水平。与未发生该综合征的患者(46.0±4.2)相比,ARDS患者(96.2±9.5相对水平)中测量到的HSP 72 mRNA水平显著更高(p <.001)。关于ARDS患者AM的呼吸爆发活性,HSP 72表达与活性氧产生之间存在负相关。HSP 72表达相对水平高的ARDS患者的AM显示出低呼吸爆发活性。未来的研究必须评估AM中HSP 72 mRNA高水平对ARDS高危患者疾病严重程度的预测价值。这种体外HSP 72表达的证明表明HSP反应对AM中内源性/外源性产生的应激因素具有保护作用。

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