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单克隆类风湿因子-IgG免疫复合物。尽管补体激活有效,但调理素C4和C3的固定较差。

Monoclonal rheumatoid factor-IgG immune complexes. Poor fixation of opsonic C4 and C3 despite efficient complement activation.

作者信息

Ng Y C, Peters D K, Walport M J

机构信息

Rheumatology Unit, Royal Postgraduate Medical School, Hammersmith Hospital, London, UK.

出版信息

Arthritis Rheum. 1988 Jan;31(1):99-107. doi: 10.1002/art.1780310114.

Abstract

Monoclonal IgM rheumatoid factor forms complexes with IgG in essential mixed cryoglobulinemia. We demonstrate that such complexes fix C3 and C4 poorly, although efficient fluid-phase C3 conversion can occur. Fixation of small amounts of C4 may be sufficient to generate a C3 convertase, but may prevent subsequent fixation of C3 by competing for binding sites on the complex. These complexes bind inefficiently to normal erythrocyte complement receptor type 1 (CR1) in vitro, and are undetectable on erythrocytes of patients with essential mixed cryoglobulinemia in vivo. Clearance of such phlogistic complexes from tissues by CR1-bearing cells may be inefficient.

摘要

在原发性混合性冷球蛋白血症中,单克隆IgM类风湿因子与IgG形成复合物。我们证明,尽管可以发生有效的液相C3转化,但此类复合物补体C3和C4的固定效果较差。少量C4的固定可能足以产生C3转化酶,但可能会通过竞争复合物上的结合位点而阻止随后C3的固定。这些复合物在体外与正常红细胞补体受体1型(CR1)的结合效率低下,并且在原发性混合性冷球蛋白血症患者的红细胞上,在体内无法检测到。携带CR1的细胞从组织中清除此类炎性复合物的效率可能较低。

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