M. J. Hobart scite author profile

The terminal components of the complement system (C6-C9) are related proteins, differing in size and complexity. They seem to be typical mosaic proteins, composed of modules which are homologous with parts of other proteins. Individual elements in a mosaic protein are often bounded by introns in the gene, and where they are duplicated within a polypeptide, partial gene duplication within the gene is responsible. It is often found in such genes that the intron/exon boundaries are of the class 1 type. We have examined the boundaries of 17 of the 18 exons of C6 and five of C7. When considered with published data for C9, only one of the protein elements appears to follow the conventional pattern. These data suggest a more complex evolutionary history for the genes of the terminal complement components than had been anticipated and challenge the notions both that discovery of a recognized protein module is of predictive value in relation to gene structure and that these genes evolved from the simple to the complex.

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Genetic polymorphism of human plasminogen

Hobart

1979

Annals of Human Genetics

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M. J. Hobart

Inherited Structural Variation and Linkage Relationships of C7

Polymorphism of Human C6

Haemolytic diffusion plate assays for factors B and D of the alternative pathway of complement activation

Structure of the human C6 gene

Genetic polymorphism of human plasminogen

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