Understanding fragile X syndrome: insights from animal models

Revisão Revisado por pares

Understanding fragile X syndrome: insights from animal models

2003; Karger Publishers; Volume: 100; Issue: 1-4 Linguagem: Inglês

10.1159/000072845

ISSN

1424-8581

Autores

C.E. Bakker, B.A. Oostra,

Tópico(s)

RNA modifications and cancer

Resumo

The fragile X mental retardation syndrome is caused by large methylated expansions of a CGG repeat in the FMR1 gene leading to the loss of expression of FMRP, an RNA-binding protein. FMRP is proposed to act as a regulator of mRNA transport or translation that plays a role in synaptic maturation and function. To study the physiological function of the FMR1 protein, mouse and Drosophila models have been developed. The loss-of-function mouse model shows slightly enlarged testes, a subtle behavioral phenotype, and discrete anomalies of dendrite spines similar to those observed in brains of patients. Studies in Drosophila indicate that FXMR plays an important role in synaptogenesis and axonal arborization, which may underlie the observed deficits in flight ability and circadian behavior of <i>fxr</i> mutant flies. The relevance of these studies to our understanding of fragile X syndrome is discussed.

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Understanding fragile X syndrome: insights from animal models