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Norepinephrine content in primary and secondary lymphoid organs is altered in rats with adjuvant-induced arthritis.

机译:佐剂诱发的关节炎大鼠的原发性和继发性淋巴器官的去甲肾上腺素含量发生改变。

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Chemical sympathectomy of secondary lymphoid organs with sparing of the hind limbs exacerbates adjuvant-induced arthritis (AA) in Lewis rats supporting a role for noradrenergic (NA) innervation of the immune system in AA pathology. The present study examines sympathetic innervation of lymphoid organs from Lewis rats 32 days after treatment with complete Freund's adjuvant (CFA) or vehicle using fluorescence histochemistry for localization of catecholamines (CA) and high-performance liquid chromatography with electrochemical detection (LCEC) for measurement for norepinephrine. The thymus from AA rats was significantly reduced in size, while secondary lymphoid organs, i.e., spleen and draining lymph nodes (DLN), were significantly enlarged compared with that seen in vehicle-treated controls. Fluorescence histochemistry revealed no apparent differences in the density of NA innervation, or the intensity of staining in sympathetic nerves in any of the secondary lymphoid organs from AA rats compared with thatobserved in control animals. However, there was an apparent increase in the density of NA nerve fibers in the thymus of AA rats. Norepinephrine (NE) concentration (pmol NE per g or mg wet weight), in the thymus from AA rats was significantly increased. Conversely, a significant decrease in splenic and lymph node NE concentration was measured in adjuvant-treated animals compared with that seen in vehicle-treated rats. Total NE content (pmol NE per whole organ weight) in lymphoid organs was not altered, except in popliteal lymph nodes (PLN), where it was increased. Collectively, our findings suggest that changes in NA innervation of lymphoid organs from AA rats result largely from increases or decreases in organ mass. Since NE released from NA nerves acts in a paracrine fashion, changes in lymphoid tissue volume that result from enhanced proliferation, migration, or cell death can make a significant difference in the availability of NE for interaction with immune target cells in these organs, even in the absence of a change in NE metabolism. Decreased thymic weight and increased spleen and lymph node weight should increase and decrease NE availability for interaction with target cells, respectively. Additionally, in PLN (a site where the highest concentration of antigen is encountered) an increase in total NE content suggests compensatory changes in NE metabolism.
机译:继发性淋巴器官的化学交感神经切除术伴有后肢保留,在Lewis大鼠中加重了佐剂诱发的关节炎(AA),从而支持了免疫病理系统中去甲肾上腺素(NA)神经支配的作用。本研究使用荧光组织化学法对儿茶酚胺(CA)进行定位,并用电化学检测的高效液相色谱法(LCEC)检测了用完全弗氏佐剂(CFA)或溶媒处理后32天的Lewis大鼠淋巴器官的交感神经支配。去甲肾上腺素。与用赋形剂处理的对照组相比,AA大鼠的胸腺尺寸明显减小,而次级淋巴器官,即脾脏和引流淋巴结(DLN)明显增大。荧光组织化学显示,与对照动物相比,AA大鼠的任何继发性淋巴器官的NA神经支配密度或交感神经染色强度均无明显差异。但是,AA大鼠胸腺中NA神经纤维的密度明显增加。 AA大鼠胸腺中去甲肾上腺素(NE)的浓度(每摩尔或毫克湿重pmol NE)显着增加。相反,与用赋形剂处理的大鼠相比,在用佐剂处理的动物中测量到脾脏和淋巴结NE浓度显着降低。淋巴器官的总NE含量(每摩尔总pmol NE)没有改变,除了pop淋巴结(PLN)有所增加。总的来说,我们的发现表明来自AA大鼠的淋巴器官的NA神经支配的变化主要是由器官质量的增加或减少引起的。由于从NA神经释放出的NE以旁分泌的方式起作用,因此由增殖,迁移或细胞死亡增强引起的淋巴组织体积变化会大大改变NE与这些器官中免疫靶细胞相互作用的可用性,即使在NE代谢没有变化。胸腺重量减少,脾脏和淋巴结重量增加应分别增加和减少NE与靶细胞相互作用的可用性。另外,在PLN(遇到最高浓度抗原的部位)中,总NE含量的增加表明NE代谢发生补偿性变化。

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