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    Por favor, use este identificador para citar o enlazar este ítem:http://uvadoc.uva.es/handle/10324/5940

    Título
    Polymorphisms of the farnesyl diphosphate synthase gene modulate bone changes in response to atorvastatin
    Autor
    Pérez Castrillon, José LuisAutoridad UVA
    Zarrabeitia Cimiano, María Teresa
    Abad Manteca, LauraAutoridad UVA
    Vega, Gemma
    Ruiz Mambrilla, Marta MaríaAutoridad UVA
    González Sagrado, ManuelAutoridad UVA
    Dueñas Laita, AntonioAutoridad UVA
    Riancho Moral, José Antonio
    Año del Documento
    2013
    Editorial
    Springer-Verlag Berlin Heidelberg
    Descripción
    Producción Científica
    Documento Fuente
    Rheumatology International, 2013, p. 1-5
    Abstract
    Although their primary therapeutic indications are different, aminobisphosphonates and statins target enzymes in the mevalonate pathway, which is critical for bone homeostasis. Previous studies have shown that some polymorphisms of the gene encoding farnesyl diphosphate synthase (FDPS), the main target of aminobisphosphonates, modulate the response to these drugs. In this study, we explored whether those single nucleotide polymorphisms (SNPs) also influence the changes in bone mineral density (BMD) following therapy with statins. Sixty-six patients with coronary heart disease were studied at baseline and after 1-year therapy with atorvastatin. BMD was measured by DXA. Three SNPs of the FDPS gene (rs2297480, rs11264359 and rs17367421) were analyzed by using Taqman assays. The results showed that there was no association between the SNPs and basal BMD. However, rs2297480 and rs11264359 alleles, which are in linkage disequilibrium, were associated with changes in hip BMD following atorvastatin therapy. Thus, patients with AA genotype at the rs2297480 locus had a 0.8 ± 0.8 % increase in BMD at the femoral neck, whereas in patients with AC/CC genotypes, BMD showed a 2.3 ± 0.8 % decrease (p = 0.02). Similar results were obtained regarding changes of BMD at the femoral trochanter and when alleles at the rs11264359 locus were analyzed. However, there was no association between BMD and rs17367421 alleles. In conclusion, these results suggest that polymorphisms of the FDPS gene may influence the bone response to various drugs targeting the mevalonate pathway, including not only aminobisphosphonates but also statins.
    Materias (normalizadas)
    Osteoporosis
    ISSN
    0172-8172
    Revisión por pares
    SI
    DOI
    10.1007/s00296-013-2914-x
    Idioma
    eng
    URI
    http://uvadoc.uva.es/handle/10324/5940
    Derechos
    openAccess
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    Universidad de Valladolid

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