Missense Mutations in the gp91-phoxGene Encoding Cytochromeb558in Patients With Cytochrome bPositive and Negative X-Linked Chronic Granulomatous Disease

Autor: Kaneda, Mizuho, Sakuraba, Hitoshi, Ohtake, Akira, Nishida, Akira, Kiryu, Chika, Kakinuma, Katsuko
Zdroj: Blood; March 1999, Vol. 93 Issue: 6 p2098-2104, 7p
Abstrakt: Chronic granulomatous disease (CGD) is a disorder of host defense due to genetic defects of the superoxide (O2-) generating NADPH oxidase in phagocytes. A membrane-bound cytochrome b558, a heterodimer consisting of gp91-phoxand p22-phox, is a critical component of the oxidase. The X-linked form of the disease is due to defects in the gp91-phoxgene. We report here biochemical and genetic analyses of patients with typical and atypical X-linked CGD. Immunoblots showed that neutrophils from one patient had small amounts of p22-phoxand gp91-phoxand a low level of O2-forming oxidase activity, in contrast to the complete absence of both subunits in two patients with typical CGD. Using polymerase chain reactions (PCR) on cDNA and genomic DNA, we found novel missense mutations of gp91-phoxin the two typical patients and a point mutation in the variant CGD, a characteristic common to two other patients with similar variant CGD reported previously. Spectrophotometric analysis of the neutrophils from the variant patient provided evidence for the presence of heme of cytochromeb558. Recently, we reported another variant CGD with similar amounts of both subunits, but without oxidase activity or the heme spectrum. A predicted mutation at amino acid 101 in gp91-phoxwas also confirmed in this variant CGD by PCR of the genomic DNA. These results on four patients, including those with two variant CGD, are discussed with respect to the missense mutated sites and the heme binding ligands in gp91-phox.
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