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多晶型衍生氧化剂对与类风湿因子结合相关的IgG的影响。

Effect of polymorph derived oxidants on IgG in relation to rheumatoid factor binding.

作者信息

Griffiths H R, Lunec J

机构信息

Department of Biochemistry, Selly Oak Hospital, Birmingham, UK.

出版信息

Scand J Rheumatol Suppl. 1988;75:148-56. doi: 10.3109/03009748809096756.

Abstract

UNLABELLED

Immunoglobulin G from rheumatoid patients is denatured around the hinge region. This has been proposed as an explanation for the presence of circulating autoantibodies to IgG in these patients. It has previously been suggested that oxygen radicals (OR) derived from activated polymorphs may play a role in denaturation in vivo. Using sera from rheumatoid patients and age-matched controls in a modified ELISA technique, we have investigated the potential for polyclonal rheumatoid factors (RF) to bind to OR denatured IgG. Three model systems were used to generate OR in vitro: (a) purified PMN s activated by the cell surface stimulant PMA, (b) radiolysis of IgG in solution to generate specifically the superoxide radical and, in a separate system, the hydroxyl radical, (OH.), (c) purified myeloperoxide in the presence of H2O2 and halide ions.

RESULTS

  1. The binding of both IgA and IgM RF s to PMN denatured IgG increased dose dependently for seropositive sera only. 2. The OH. radical but not the superoxide radical significantly increased the binding of IgA and M RF, again only for seropositive sera. 3. The myeloperoxidase enzyme system did not increase RF binding. 4. IgG incubated with elastase was not found to be a better antigen than native IgG. These results indicate that IgG is denatured by OR released from activated PMN, thereby producing an antigen for polyclonal RF s.
摘要

未标记

类风湿患者的免疫球蛋白G在铰链区周围发生变性。这已被提出作为这些患者中存在循环抗IgG自身抗体的一种解释。此前有人提出,活化多形核白细胞产生的氧自由基(OR)可能在体内变性过程中起作用。我们使用改良的酶联免疫吸附测定(ELISA)技术,以类风湿患者和年龄匹配的对照血清,研究了多克隆类风湿因子(RF)与OR变性IgG结合的可能性。使用三种模型系统在体外产生OR:(a)通过细胞表面刺激物佛波酯(PMA)活化的纯化多形核白细胞(PMN);(b)溶液中IgG的辐射分解,专门产生超氧阴离子自由基,在另一个系统中产生羟基自由基(·OH);(c)在过氧化氢和卤离子存在下的纯化髓过氧化物酶。

结果

  1. 仅血清阳性的血清中,IgA和IgM RF与PMN变性IgG的结合呈剂量依赖性增加。2. 羟基自由基而非超氧阴离子自由基显著增加了IgA和IgM RF的结合,同样仅针对血清阳性的血清。3. 髓过氧化物酶系统未增加RF结合。4. 未发现与弹性蛋白酶孵育的IgG比天然IgG是更好的抗原。这些结果表明,IgG被活化PMN释放的OR变性,从而产生多克隆RF的抗原。

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