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肌肉注射人重组调节激活正常T细胞表达和分泌因子(hrRANTES)可导致小鼠体内肥大细胞募集以及组氨酸脱羧酶转录增加:在基因缺陷的肥大细胞缺陷型W/WV小鼠中无此效应。

Intramuscular injection of hrRANTES causes mast cell recruitment and increased transcription of histidine decarboxylase in mice: lack of effects in genetically mast cell-deficient W/WV mice.

作者信息

Conti P, Reale M, Barbacane R C, Letourneau R, Theoharides T C

机构信息

Immunology Division, University of Chieti School of Medicine, Chieti, Italy.

出版信息

FASEB J. 1998 Dec;12(15):1693-700. doi: 10.1096/fasebj.12.15.1693.

Abstract

RANTES (regulated upon activation, normal T cell expressed and presumably secreted) and other chemoattractant proteins are members of the intercrine or chemokine family of proinflammatory basic polypeptides. RANTES is a prototype of the C-C chemokine subfamily that acts as a selective chemoattractant for human monocytes and CD4-positive lymphocytes and increases the adherence of monocytes to endothelial cells. However, the role of RANTES in white cells is still unclear. We report here that hrRANTES at 20 ng/50 microl in mice causes mast cell recruitment 4 h after intramuscular injection, an effect inhibited by anti-RANTES, as evidenced by 0.1% Toluidine blue, a specific dye for coloring mast cells. Injections of PBS (50 microl) vehicle (negative control) did not produce any appreciable inflammatory response, whereas injection of lipopolysaccharide 20 ng/50 microl (positive control) generated a marked inflammatory state. When RANTES was injected intramuscularly in genetically mast cell-deficient W/Wv mice, the inflammatory effect was not present. The RANTES injection sites were then excised and studied under an optical and electron microscope. A Northern blot analysis was performed using a probe that was prepared to detect mRNA encoding the histidine decarboxylase (HDC) gene on excised muscle tissue. We found that hrRANTES provoked generation of HDC mRNA from muscle tissue after 4 h. These effects were inhibited by an anti-RANTES antibody and were absent in genetically mast cell-deficient mice. The increasing number of mast cells in the RANTES injection sites led to an augmentation of histamine content compared to controls (PBS). The injection of hrRANTES 20 ng/20 microl into the sole of a rat paw confirmed the inflammatory and the mast cell recruitment potential of this chemokine. In these studies, hrRANTES injections in muscle tissue provided direct in vivo evidence that RANTES has a significant effect on mast cell recruitment and HDC mRNA generation.

摘要

调节激活正常T细胞表达和分泌因子(RANTES)及其他趋化蛋白是促炎碱性多肽的白细胞介素或趋化因子家族成员。RANTES是C-C趋化因子亚家族的一个原型,它作为人类单核细胞和CD4阳性淋巴细胞的选择性趋化因子,增加单核细胞与内皮细胞的黏附。然而,RANTES在白细胞中的作用仍不清楚。我们在此报告,小鼠肌肉注射20 ng/50 μl的重组人RANTES(hrRANTES)4小时后可引起肥大细胞募集,抗RANTES可抑制该作用,用0.1%甲苯胺蓝(一种用于染色肥大细胞的特异性染料)可证明这一点。注射PBS(50 μl)载体(阴性对照)未产生任何明显的炎症反应,而注射20 ng/50 μl脂多糖(阳性对照)则产生明显的炎症状态。当在基因缺陷的肥大细胞W/Wv小鼠中肌肉注射RANTES时,未出现炎症效应。然后切除RANTES注射部位,在光学和电子显微镜下进行研究。使用制备的探针进行Northern印迹分析,以检测切除肌肉组织中编码组氨酸脱羧酶(HDC)基因的mRNA。我们发现hrRANTES在4小时后可促使肌肉组织产生HDC mRNA。这些效应被抗RANTES抗体抑制,在基因缺陷的肥大细胞小鼠中未出现。与对照组(PBS)相比,RANTES注射部位肥大细胞数量增加导致组胺含量增加。向大鼠爪垫底部注射20 ng/20 μl的hrRANTES证实了这种趋化因子的炎症和肥大细胞募集潜力。在这些研究中,肌肉组织中注射hrRANTES提供了直接的体内证据,表明RANTES对肥大细胞募集和HDC mRNA产生有显著影响。

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