Cornelia Estaller scite author profile

The nucleotide and complete amino acid sequence for the human beta 2-glycoprotein I (beta 2I) was derived by sequencing the cDNA clone pB2I-1. In addition to the 326 amino acid residues of the mature protein this clone codes for a putative leader peptide and contains sequence representing 5' and 3' untranslated regions. When this amino acid sequence was compared with the previously published primary sequence, three major amino acid substitutions were found, two involving cysteine residues. These substitutions lead to a new alignment of the complement control protein (CCP) repeats present in beta 2I and a prediction of the complete disulphide bond organization. Northern-blot analysis indicates that hepatocytes are a major site of biosynthesis for this protein. A transcription signal of about 1.5 kb was detected by using RNA from HepG2 cells.

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Human complement factor H: two factor H proteins are derived from alternatively spliced transcripts

Estaller

Schwaeble

Dierich

et al. 1991

Eur J Immunol

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The human complement factor H is an important component in the control of the alternative pathway of complement activation. We have previously shown that at least three factor H homologous mRNA species of 4.3 kb, 1.8 kb and 1.4 kb in length are constitutively expressed in human liver. In addition, several factor Hrelated proteins have been detected in human sera using antibodies directed against the classical human factor H glycoprotein of 150 kDa.The structure of the additional polypeptides has not been shown so far. Circumstantial evidence suggests that the 1.8-kb mRNA might encode the 43-kDa factor H-like polypeptide. Here we report the isolation, characterization and eukaryotic expression of the first full-length cDNA representing the major 4.3-kb mRNA and the 1.8-kb mRNA of human factor H. We show that the 4.3-kb transcript encodes the 150-kDa-factor H glycoprotein and the 1.8-kb mRNA the 43-kDa factorH polypeptide. The identity of the two cDNA in a region of 1400 nucleotides suggests that the two factor H-related transcripts are derived from one gene by a process of alternative splicing.

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Human interleukin‐1 receptor antagonist is expressed in liver

Steinkasserer

Estaller²,

Weiß³

et al. 1992

FEBS Letters

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Human Complement Factor H: Molecular Cloning and cDNA Expression Reveals Variability in the Factor H-Related mRNA Species of 1.4 kb

Schwaeble¹,

Feifel²,

Estaller³

et al. 1991

Immunobiology

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Human complement factor B: Functional properties of a recombinant zymogen of the alternative activation pathway convertase

Schwaeble¹,

Lüttig²,

Sokolowski³

et al. 1993

Immunobiology

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