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Recombinational biases in the rearranged C1-inhibitor genes of hereditary angioedema patients
Authors:Dominique Stoppa-Lyonnet  Christiane Duponchel  Tommaso Meo  Jrme Laurent  Philip E Carter  Mario Arala-Chaves  Jacques H M Cohen  Georg Dewald  Joelle Goetz  Georges Hauptmann  Gilbert Lagrue  Philippe Lesavre  Margarita Lopez-Trascasa  Gabriella Misiano  Claude Moraine  Alain Sobel  Pierre J Spth  and Mario Tosi
Affiliation:Unite' d'Immunogénétique et INSERM Unité 276, Institut Pasteur, France.
Abstract:DNA structural changes responsible for hereditary angioedema were sought in the C1-inhibitor gene, which contains unusually dense clusters of Alu repeats in various orientations. Among patients belonging to 45 unrelated families, eight partial C1-inhibitor gene deletions and a partial duplication were found. Four deletions had one of the boundaries within the gene and the other in extragenic regions--in three cases 5' of the gene and in one case 3' of the gene. The boundaries of the partial duplication and of the remaining four deletions mapped instead within a few kilobases of exon 4. The same element--Alu 1--the first of three tandem Alu repeats preceding exon 4, contained one of the breakpoints of each of these five rearrangements. Moreover, these recombination breakpoints spread over the entire length of Alu 1, in contrast with the tight clustering observed near the 5' end of Alu sequences rearranged in other human genes. Thus, two uncommon recombinational biases are observed in the Alu rearrangements of hereditary angioedema patients; one promotes the occurrence of intragenic breakpoints in a single Alu repeat, and the other allows the breaks to be distributed over the entire Alu structure rather than within the hot spot of the left Alu monomer. A region of potential Z-DNA structure, located 1.7 kb upstream of Alu 1, may contribute to both peculiarities.
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