Hemoglobin:
The hemoglobin genes (and the myoglobin genes of muscle) represent a family of gene. The common ancestor is more than 500 million years old. The ancestor gene duplicated (a number of times), and each duplicated copy mutated, so that the set of resulting genes brought a diversity of various functional genes, and non-functional genes (coding for non functional proteins, they are called pseudogenes). Gene localization:
Each gene is made of 3 exons (coding sequences) separate by 2 introns (non-coding sequences).
The hemoglobin genes split the tasks: some are express by the embryo; others take over in foetus; and finally others in adult. Also, the sequential expression matches the physical distribution of the gene from 5’ to 3’. To be noted that a “foetal” gene can compensate a failing “adult” gene (hereditary persistence of the foetal hemoglobin):
- Hemoglobinopathy: Constitutional anomalies of the Hb structure (qualitative anomaly). - Thalassemia: Constitutional anomalies of the Hb synthesis (quantitative anomaly).
Huret JL, Troussard X
Atlas of Genetics and Cytogenetics in Oncology and Haematology 2008-02-01
Hemoglobin genes; Sickle-cell anemia - Thalassemias
Online version: http://atlasgeneticsoncology.org/teaching/30014/cancer-prone-explorer/favicon/teaching-explorer/