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新生儿败血症合并硬肿症时的C3、B因子、α1抗胰蛋白酶

C3, factor B, alpha-1-antitrypsin in neonatal septicaemia with sclerema.

作者信息

Pelet B

出版信息

Arch Dis Child. 1980 Oct;55(10):782-8. doi: 10.1136/adc.55.10.782.

Abstract

C3, factor B, and alpha-1-antitrypsin were determined in newborn infants with septicaemia and sclerema, associated with suspected infections, ABO or Rh incompatibility, and hyperbilirubinaemia of unknown origin, during and after treatment with exchange transfusion. Activation products from C3 and factor B, the clearance of the transfused C3, and its synthesis by the recipient were determined also. Infected newborn infants had low levels of C3 and factor B, but a normal amount of alpha-1-antitrypsin. Exchange transfusion lowered the level of alpha-1-antitrypsin and briefly corrected the low level of C3 and factor B. Activation products were formed only exceptionally. As synthesis of C3 is very active, a defective activation of complement pathway linked to an abnormal distribution in extravascular pool is postulated.

摘要

对患有败血症和硬肿症的新生儿进行了检测,这些新生儿伴有疑似感染、ABO或Rh血型不相容以及不明原因的高胆红素血症,检测时间为换血治疗期间及治疗后,检测项目包括C3、B因子和α1-抗胰蛋白酶。同时还测定了C3和B因子的激活产物、输入C3的清除率及其在受者体内的合成情况。感染的新生儿C3和B因子水平较低,但α1-抗胰蛋白酶量正常。换血治疗降低了α1-抗胰蛋白酶水平,并短暂纠正了C3和B因子的低水平。激活产物仅偶尔形成。由于C3的合成非常活跃,推测补体途径的激活缺陷与血管外池的异常分布有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6674/1626890/e106a47b33c3/archdisch00776-0041-a.jpg

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