Artigo
Duplication 9p and their implication to phenotype
Fecha
2014-12-20Registro en:
Bmc Medical Genetics. London: Biomed Central Ltd, v. 15, 8 p., 2014.
1471-2350
WOS000348677600001.pdf
10.1186/s12881-014-0142-1
WOS:000348677600001
Autor
Guilherme, Roberta Santos [UNIFESP]
Meloni, Vera Ayres [UNIFESP]
Perez, Ana Beatriz Alvarez [UNIFESP]
Pilla, Ana Luiza [UNIFESP]
Ramos, Marco Antonio Paula de [UNIFESP]
Dantas, Anelisa Gollo [UNIFESP]
Takero, Sylvia Satomi [UNIFESP]
Kulikowski, Leslie Domenici
Melaragno, Maria Isabel [UNIFESP]
Institución
Resumen
Background: Trisomy 9p is one of the most common partial trisomies found in newborns. We report the clinical features and cytogenomic findings in five patients with different chromosome rearrangements resulting in complete 9p duplication, three of them involving 9p centromere alterations.Methods: the rearrangements in the patients were characterized by G-banding, SNP-array and fluorescent in situ hybridization (FISH) with different probes.Results: Two patients presented de novo dicentric chromosomes: der(9; 15)t(9; 15)(p11.2;p13) and der(9; 21)t(9; 21) (p13.1;p13.1). One patient presented two concomitant rearranged chromosomes: a der(12)t(9; 12)(q21.13;p13.33) and an psu i(9)(p10) which showed FISH centromeric signal smaller than in the normal chromosome 9. Besides the duplication 9p24.3p13.1, array revealed a 7.3 Mb deletion in 9q13q21.13 in this patient. the break in the psu i(9) (p10) probably occurred in the centromere resulting in a smaller centromere and with part of the 9q translocated to the distal 12p with the deletion 9q occurring during this rearrangement. Two patients, brother and sister, present 9p duplication concomitant to 18p deletion due to an inherited der(18)t(9; 18)(p11.2; p11.31) mat.Conclusions: the patients with trisomy 9p present a well-recognizable phenotype due to facial appearance, although the genotype-phenotype correlation can be difficult due to concomitant partial monosomy of other chromosomes. the chromosome 9 is rich in segmental duplication, especially in pericentromeric region, with high degree of sequence identity to sequences in 15p, 18p and 21p, chromosomes involved in our rearrangements. Thus, we suggest that chromosome 9 is prone to illegitimate recombination, either intrachromosomal or interchromosomal, which predisposes it to rearrangements, frequently involving pericentromeric regions.
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