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Licensed Unlicensed Requires Authentication Published by De Gruyter June 1, 2005

The analysis of the complement activation product SC5 b-9 is applicable in neonates in spite of their profound C9 deficiency

  • Anne K. M. Høgåsen , Inger Øverlie , Thor W. R. Hansen , Tore G. Abrahamsen , Per H. Finne and Kolbjørn Høgåsen

Abstract

Native complement factors and complement activation products were measured in healthy neonates (n = 72) and in a group of infants with premature prolonged rupture of the membranes (PPROM) without sepsis (n = 10). Vitronectin concentration in normal cord blood was not correlated with gestational age, and the median value was 86.0% of adult values. This was markedly higher than other native complement factors studied (factor B: 35.9% , C4: 45.1% , C3: 56.2% ). The concentration of C9 showed a positive correlation with gestational age and was very low, 10.8% of normal adult values in cord blood and 8.3% in the patients. Fifteen percent of the neonates had C9 levels lower than 2% of adult values. The complement activation products Bb and SC5 b-9 were significantly elevated in the patients (159% and 130% of control values, respectively), indicating alternative and terminal pathway activation. In contrast, C4 bc and C3 bc levels were not increased. The maximum amount of SC5 b-9 which could be generated in the neonatal sera by cobra venom factor was highly correlated with C9 concentration (rs= 0.86, p = 0.0001) The profound C9 deficiency found in neonates is correlated with gestational age, limits the capacity to form bacteriolytic C5 b-9 (m) and may predispose for severe invasive bacterial infection. The plasma level of SC5 b-9 under normal conditions was very low, only 0.3% (0.1%–3.0 %) of the values obtained after CVF activation of the same samples. Therefore, we suggest that the analysis of SC5 b-9 is applicable also in neonates, in spite of their extremely low C9 levels.

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Published Online: 2005-06-01
Published in Print: 2000-01-10

Copyright (c)2000 by Walter de Gruyter GmbH & Co. KG

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