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Complement membrane attack complexes in pathologic disc tissues.

机译:病理性椎间盘组织中的补膜攻击复合物。

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STUDY DESIGN: Complement membrane attack complexes were located in lumbar spine disc tissues by immunohistochemistry. Their occurrence was compared in control discs obtained from organ donors (CD), discs showing a normal macroscopic anatomy, samples of intervertebral disc herniations (DH), and intervertebral discs found to be degenerated by discography, but not herniated (DD). OBJECTIVE: To look for a possible role of complement activation, specifically complement membrane attack complexes, an end product of the classic immune complex-mediated complement activation pathway, in disc pathophysiology. SUMMARY OF BACKGROUND DATA: Recent immunohistochemical and biochemical studies suggest a possible role for immune complexes, as observed by immunohistochemical location and biochemical assay of immunoglobulins M and G in intervertebral disc pathophysiology. Immune complexes may trigger complement activation and ultimately cell lysis. There are, however, currently no reports on complement activation in disc tissues, although immune (antigen-antibody) complexes have been demonstrated. Such immune complexes have been reported to occur on or near to disc cells in DH tissues. METHODS: Thin frozen sections of disc tissue from CD (n = 9 discs), DH (n = 58 discs), and DD (n = 11 discs) were cut and then immunostained with a monoclonal antibody to the complement membrane attack complex (C5b-9) using avidin-biotin complex (ABC) immunostaining. The presence or absence of complement membrane attack complex immunoreactivity was compared in the various subtypes of DH and also with preoperative duration of radicular pain. RESULTS: Complement membrane attack complexes could be observed in none of the CDs studied. In contrast, in more than one third of both the DH (21/58, 36.2%) and the DD (4/11, 36.4%), immunoreactivity to complement membrane attack complexes could be observed in disc cells. In DD discs, immunoreactivity to complement membrane attack complexes was most often present in anulus fibrosus samples (5/13, 38.5%). With respect to subtype of DH, complement membrane attack complexes were observed in 19 of 36 sequestrated discs (52.8%), 1 of 16 extrusions (6.3%), and 1 of 6 protrusions (16.7%). Complement membrane attack complexes were more often present with shorter pain duration (P= 0.03), but showed no relation to age. Disc cells often showed a heavy staining pattern for complement membrane attack complexes, suggesting an abundance of these complexes lodged in the membrane of the cells. CONCLUSIONS: The predominant presence of complement membrane attack complexes in sequestrated disc tissue could suggest a role in DH tissue-induced sciatica. Possibly immune (antigen-antibody) complexes, reported in previous studies, trigger the classic pathway of complement activation, with complement membrane attack complexes as the final product. Complement membrane attack complexes also appear to have some as yet undefined role in degenerated nonherniated disc tissue, with a predominant presence in the anulus fibrosus cells of such discs.
机译:研究设计:补体膜攻击复合物通过免疫组织化学位于腰椎间盘组织中。在从器官供体(CD)获得的对照椎间盘,显示正常宏观解剖结构的椎间盘,椎间盘突出症样本(DH)以及发现椎间盘退变但未椎间盘突出(DD)的椎间盘中比较了它们的发生。目的:寻找补体激活的可能作用,特别是补体膜攻击复合物(经典免疫复合物介导的补体激活途径的终产物)在椎间盘病理生理中的作用。背景数据概述:最近的免疫组织化学和生物化学研究表明免疫复合物可能发挥作用,正如免疫组织化学定位和免疫球蛋白M和G在椎间盘病理生理学中的生化测定所观察到的。免疫复合物可能触发补体激活并最终引起细胞裂解。然而,尽管已经证明了免疫(抗原-抗体)复合物,但目前尚无关于椎间盘组织中补体激活的报道。据报道这种免疫复合物在DH组织中的盘细胞上或附近发生。方法:从CD(n = 9片),DH(n = 58片)和DD(n = 11片)中切取椎间盘组织的薄冰冻切片,然后用针对补体膜攻击复合物(C5b)的单克隆抗体进行免疫染色-9)使用抗生物素蛋白-生物素复合物(ABC)进行免疫染色。比较了DH各种亚型中补体膜攻击复合物免疫反应性的存在与否以及术前放射痛的持续时间。结果:在所有研究的CD中均未观察到补体膜攻击复合物。相反,在DH(21 / 58,36.2%)和DD(4 / 11,36.4%)的三分之一以上,可以在椎间盘细胞中观察到与膜攻击复合物互补的免疫反应性。在DD椎间盘中,纤维环样本中最常出现补体膜攻击复合物的免疫反应性(5 / 13,38.5%)。关于DH的亚型,在36个被隔离的椎间盘中观察到补体膜攻击复合物(52.8%),16个突出物中的1个(6.3%)和6个突出物中的1个(16.7%)。补体膜攻击复合物更常见,疼痛持续时间较短(P = 0.03),但与年龄无关。圆盘细胞通常对补体膜攻击复合物表现出较重的染色模式,表明这些复合物大量存在于细胞膜中。结论:在隔离的椎间盘组织中主要存在补体膜攻击复合物,这可能在DH组织诱导的坐骨神经痛中起作用。先前研究中报道的可能的免疫(抗原-抗体)复合物触发补体激活的经典途径,而补体膜攻击复合物为最终产物。补体膜攻击复合物在变性的非突出椎间盘组织中似乎也具有某些尚未定义的作用,主要存在于此类椎间盘的纤维环细胞中。

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