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3 research outputs found

Alopecias cicatriciales

Author: Abal Diaz Leandro
Casanova i Seuma Josep M. (Josep Manel)
Soria Xavier
Publication venue: Elsevier
Publication date
Field of study

Las alopecias cicatriciales constituyen un grupo de trastornos que dan lugar a una pérdida permanente de cabello como consecuencia de diversos procesos. En este artículo nos centraremos en las alopecias cicatriciales primarias (ACP), un grupo de enfermedades foliculocéntricas en las que el folículo piloso es la principal diana del proceso inflamatorio. Actualmente se clasifican según la celularidad del infiltrado inflamatorio en linfocíticas, neutrofílicas y mixtas. La patogenia de muchas de ellas sigue siendo desconocida. Algunas presentan similitudes clínicas que dificultan el diagnóstico, lo que hace en muchos casos necesaria la práctica de una o más biopsias cutáneas. En el manejo de estas entidades es necesario un diagnóstico preciso de forma precoz y un tratamiento agresivo en algunos casos, con objeto de evitar la destrucción folicular y el desarrollo de una alopecia cicatricial

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Expression of somatostatin receptors in human melanoma cell lines: effect of two different somatostatin analogues, octreotide and SOM230, on cell proliferation

Author: Abal Diaz Leandro
Baradad Brusau Manuel
Casanova i Seuma Josep M. (Josep Manel)
Dolcet Roca Xavier
Egido Garcia Ramon Maria
Llecha Cano Núria
Martí Laborda Rosa Ma.
Martínez Alonso Montserrat
Matias-Guiu Xavier
Mayorga Mayorga Maritza Elfride
Puig Susana
Sanmartín Novell Verònica
Sorolla Bardají Anabel
Vilella Ramón
Yeramian Hakim Andree
Publication venue: Field House Publishing
Publication date
Field of study

Somatostatin analogues (SAs) are potential anticancer agents. This study was designed to investigate the expression of somatostatin receptors (SSTRs) in melanoma cells and the effect of two SAs on cell proliferation and viability. Eighteen primary and metastatic human cutaneous melanoma cell lines were treated with octreotide and SOM230. Expression of SSTR1, SSTR2, SSTR3 and SSTR5 was assessed by real-time polymerase chain reaction. Proliferation, viability and cell death were assessed using standard assays. Inhibition was modelled by mixed-effect regression. Melanoma cells expressed one or more SSTR. Both SAs inhibited proliferation of most melanoma cell lines, but inhibition was less than 50%. Neither SA affected cell viability or induced cell death. The results suggest that melanoma cell lines express SSTRs. The SAs investigated, under the conditions used in this study, did not, however, significantly inhibit melanoma growth or induce cell death. Novel SAs, combination therapy with SAs and their anti-angiogenic properties should be further investigated

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