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Properdin- and nephritic factor-dependent C3 convertases: requirement of native C3 for enzyme formation and the function of bound C3b as properdin receptor

机译:备解素和肾病因子依赖性C3转化酶:天然C3对酶形成的要求以及结合的C3b作为备解素受体的功能

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摘要

Two complex enzymes were assembled that both converted C3 to C3b, one consisting of activated properdin (P), native C3, proactivator (PA) and proactivator convertase (PAase), and the other of nephritic factor (NF) and the same three cofactors. By maintaining a critical concentration of PAase, the P-C3 convertase and the NF-C3 convertase were shown to function efficiently without formation of the C3b-feedback enzyme. The former two enzymes are distinct from the C3b-dependent C3 convertase in that they utilize native C3 instead of C3b and PA in an apparently uncleaved form. The P- and NF-C3 convertase express maximal activity within approximately 10 min at 37 degrees C and decay with a half-life of 35 min at 37 degrees C, which is in contradistinction to the reported lability of the C3b-feedback enzyme. P- and NF-C3 convertases are inhibited by their product C3b, which may constitute a heretofore unknown control of the alternative pathway. A direct physical interaction of P with native C3 and C3b was demonstrated by agglutination of C3b-bearing erythrocytes and by agglutination inhibition. Bound C3b thus constitutes the only known receptor of P and may fulfill an important localizing function for P and the P-C3 convertase in vivo. Although P and NF form functionally similar enzymes, they act independently of each other and are apparently immunochemically unrelated proteins.
机译:组装了两种复杂的酶,它们都将C3转化为C3b,一种由活化的备解素(P),天然C3,促活化剂(PA)和促活化剂转化酶(PAase)组成,另一种由肾病因子(NF)和相同的三个辅因子组成。通过维持临界浓度的PAase,P-C3转化酶和NF-C3转化酶可有效发挥功能,而不会形成C3b反馈酶。前两种酶与C3b依赖型C3转化酶的不同之处在于,它们以天然的C3代替了显然未切割的C3b和PA。 P-和NF-C3转化酶在37摄氏度下约10分钟内表达最大活性,并在37摄氏度下衰变,具有35分钟的半衰期,这与C3b反馈酶的报道的稳定性相矛盾。 P-和NF-C3转化酶受到其产物C3b的抑制,其产物可能构成该替代途径迄今未知的控制。 P与天然C3和C3b的直接物理相互作用通过含C3b的红细胞的凝集和凝集抑制来证明。因此,结合的C3b构成了P的唯一已知受体,并且可以在体内对P和P-C3转化酶履行重要的定位功能。尽管P和NF形成功能相似的酶,但它们彼此独立发挥作用,并且显然是免疫化学无关的蛋白质。

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  • 年度 1975
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