- Browse by Author
Browsing by Author "van Leeuwen, Karin"
Now showing 1 - 1 of 1
Results Per Page
Sort Options
Item Two CGD Families with a Hypomorphic Mutation in the Activation Domain of p67(phox)(OMICS Publishing Group, 2014-06-30) Roos, Dirk; van Buul, Jaap D.; Tool, Anton TJ; Matute, Juan D.; Marchal, Christophe M.; Hayee, Bu’Hussain; Köker, M. Yavuz; de Boer, Martin; van Leeuwen, Karin; Segal, Anthony W.; Pick, Edgar; Dinauer, Mary C.; Department of Pediatrics, IU School of MedicineSTUDY BACKGROUND: Chronic granulomatous Disease (CGD) is a rare immunodeficiency caused by a defect in the leukocyte NADPH oxidase. This enzyme generates superoxide, which is needed for the killing of bacteria and fungi by phagocytic leukocytes. Most CGD patients have mutations in CYBB, the X-linked gene that encodes gp91(phox), the catalytic subunit of the leukocyte NADPH oxidase. We report here three autosomal recessive CGD patients from two families with a homozygous mutation in NCF2, the gene that encodes p67(phox), the activator subunit of the NADPH oxidase. METHODS: Leukocyte NADPH oxidase activity, expression of oxidase components and gene sequences were measured with standard methods. The mutation found in the patients' NCF2 gene was expressed as Ala202Val-p67(phox) in K562 cells to measure its effect on NADPH oxidase activity. Translocation of the mutated p67(phox) from the cytosol of the patients' neutrophils to the plasma membrane was measured by confocal microscopy and by Western blotting after membrane purification. RESULTS: The exceptional feature of the A67 CGD patients reported here is that the p.Ala202Val mutation in the activation domain of p67(phox) was clearly hypomorphic: substantial expression of p67(phox) protein was noted and the NADPH oxidase activity in the neutrophils of the patients was 20-70% of normal, dependent on the stimulus used to activate the cells. The extent of Ala202Val-p67(phox) translocation to the plasma membrane during cell activation was also stimulus dependent. Ala202Val-p67(phox) in K562 cells mediated only about 3% of normal oxidase activity compared to cells transfected with the wild-type p67(phox). CONCLUSION: The mutation found in NCF2 is the cause of the decreased NADPH oxidase activity and the (mild) clinical problems of the patients. We propose that the p.Ala202Val mutation has changed the conformation of the activation domain of p67(phox), resulting in reduced activation of gp91(phox).