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Iatreia

versión impresa ISSN 0121-0793

Resumen

VELASQUEZ MARULANDA, Luz Astrid; ARANGO RINCON, Julián Camilo; ARIAS SIERRA, Andrés Augusto  y  PATINO GRAJALES, Pablo Javier. Gene therapy in chronic granulomatous disease. Iatreia [online]. 2005, vol.18, n.3, pp.308-319. ISSN 0121-0793.

Reactive oxygen species (ROS) production by phagocytes is an important mechanism to kill invading microorganisms. Neutrophils from individuals with chronic granulomatous disease (CGD) do not produce ROS, thereby rendering these individuals more susceptible to infection. CGD results from mutations in the genes encoding essential subunits of respiratory burst NADPH oxidase, the enzyme complex necessary for the production of these reactive molecules. The absence of phagocyte ROS results in recurrent fungal and bacterial infections and inflammatory granulomas, associated with significant morbidity and mortality. Currently, the curative treatment is the allogenic bone marrow transplant (BMT); nevertheless, this therapy has some disadvantages including the HLA incompatibility, the immunosupression due to the myeloablative conditions necessary for the transplant and the high risk to develop graft vs. host disease. As an alternative to BMT the ex vivo gene therapy in hematopoietic stem cells has been intensely studied. Although this option could be the most appropriate treatment, it can give rise to other kinds of adverse effects. The genetic features of CGD have made it a very attractive candidate to be cured with gene therapy. This review summarizes and discusses the current advances about gene therapy and its application to CGD.

Palabras clave : enfermedad granulomatosa crónica; NADPH oxidasa; terapia génica; vectores retrovirales; chonic granulomatous disease; gene therapy; nadph oxidase; retroviral vectors.

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