内毒素激活培养新生大鼠心肌细胞表达功能性表面相关白细胞介素-1 α。

Elena Westphal, Li Chen, Claudia Pilowski, Susanne Koch, Henning Ebelt, Ursula Müller-Werdan, Karl Werdan, Harald Loppnow
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引用次数: 10

摘要

白细胞介素-1 (IL-1)是心血管增殖、凋亡、收缩或炎症介质产生的有效调节剂。因此,我们研究了内毒素刺激下培养的新生大鼠心脏细胞中IL-1的表达和功能。我们发现培养的新生大鼠心肌细胞表达il -1 α和il -1 β mRNA。这些细胞表达了功能性细胞相关的IL-1活性,一种特异性抗IL-1 α抗体抑制了这种活性。共培养实验表明,具有生物活性的il -1 α存在于心肌细胞表面。免疫组化示新生儿心肌细胞il -1 α染色。虽然细胞也表达il -1 β mRNA,但我们没有通过ELISA或免疫组织化学染色在培养的心肌细胞上清中检测到il -1 β。此外,新生儿和成年大鼠心脏组织表达il -1 α mRNA,而胎儿(而非成人)心脏组织表达可检测到的il -1 α mRNA。相比之下,il -1 β mRNA存在于大鼠和人胎儿和成人样本中。此外,在扩张型或缺血性心肌病患者中,我们测量了il -1 β,而不是il -1 α mRNA。这些结果为新生大鼠心肌细胞表面存在功能活跃的il -1 α提供了证据,并可能提示il -1 α在大鼠和人类心脏细胞发育、衰老和疾病过程中调节细胞功能的不同作用。
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Endotoxin-activated cultured neonatal rat cardiomyocytes express functional surface-associated interleukin-1alpha.

Interleukin-1 (IL-1) is a potent regulator of cardiovascular proliferation, apoptosis, contraction or production of inflammatory mediators. Thus, we investigated expression and function of IL-1 in cultured neonatal rat heart cells upon endotoxin stimulation. We show that cultured neonatal rat cardiomyocytes expressed IL-1alpha and IL-1beta mRNA. The cells expressed functional cell-associated IL-1 activity and a specific anti-IL-1alpha-antibody inhibited the activity. Biologically active IL-1alpha was present at the cell surface of the cardiomyocytes, as indicated in co-culture experiments. Immunohistochemistry showed IL-1alpha-staining of the neonatal cardiomyocytes. Although the cells also expressed IL-1beta mRNA, we did not detect IL-1beta in the supernatants of cultured cardiomyocytes by ELISA or in immunohistochemical staining. Furthermore, neonatal and adult rat heart tissues expressed IL-1alpha mRNA, whereas fetal, but not adult, human cardiac tissues expressed detectable IL-1alpha mRNA. In contrast, IL-1beta mRNA was present in rat and human fetal and adult samples. Furthermore, in patients with dilated or ischemic cardiomyopathy, we measured IL-1beta, but not IL-1alpha, mRNA. These results provide evidence for the presence of functionally active IL-1alpha on the cell surface of neonatal rat cardiomyocytes and may suggest a differential role of IL-1alpha in regulation of cellular functions during development, aging and disease in rat and human heart cells.

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