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Clr and Cls subcomponents of human complement: two serine proteinases lacking the 'histidine-loop' disulphide bridge.

Abstract

The N-terminal amino acid sequence of human C1s b chain has been extended to 52 residues. The histidine residue involved in the charge-relay system is located at position 38, whereas the histidine-loop disulphide bridge is missing. So far, human complement sub-components C1r and C1s are the only known mammalian serine proteinases lacking this disulphide bridge.

Entities: Chemical Gene Species

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Year: 1981 PMID： 6272901 DOI： 10.1007/bf01114800

Source DB: PubMed Journal: Biosci Rep ISSN： 0144-8463 Impact factor: 3.840

Clr and Cls subcomponents of human complement: two serine proteinases lacking the 'histidine-loop' disulphide bridge.

1. Ancient origin of the complement lectin pathway revealed by molecular cloning of mannan binding protein-associated serine protease from a urochordate, the Japanese ascidian, Halocynthia roretzi.

2. The serine proteinase chain of human complement component C1s. Cyanogen bromide cleavage and N-terminal sequences of the fragments.

3. Amino acid sequence of the Bb fragment from complement Factor B. Sequence of the major cyanogen bromide-cleavage peptide (CB-II) and completion of the sequence of the Bb fragment.