Chronic Granulomatous Disease: Two Decades of Experience From a Tertiary Care Centre in North West India

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作者
Amit Rawat
Surjit Singh
Deepti Suri
Anju Gupta
Biman Saikia
Ranjana Walker Minz
Shobha Sehgal
Kim Vaiphei
C. Kamae
K. Honma
N. Nakagawa
K. Imai
S. Nonoyama
K. Oshima
N. Mitsuiki
O. Ohara
Koon-Wing Chan
Yu Lung Lau
机构
[1] Postgraduate Institute of Medical Education and Research,Advanced Pediatrics Centre
[2] Postgraduate Institute of Medical Education and Research,Department of Immunopathology
[3] Postgraduate Institute of Medical Education and Research,Department of Histopathology
[4] National Defense Medical College,Department of Pediatrics
[5] Kazusa DNA Research Institute,Department of Pediatrics and Adolescent Medicine, Queen Mary Hospital, LKS Faculty of Medicine
[6] The University of Hong Kong,undefined
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Chronic granulomatous disease; NADPH oxidase; CYBB gene; NCF-1 gene; dihydrorhodamine;
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摘要
Chronic granulomatous disease (CGD) results from an inherited defect in the phagocytic cells of the immune system. It is a genetically heterogenous disease caused by defects in one of the five major subunits of the nicotinamide adenine dinucleotide phosphate (NADPH) oxidase complex. There is a paucity of data from India on CGD. We herein describe the clinical features in 17 children with CGD from a single tertiary referral center in India. A detailed analysis of the clinical features, laboratory investigations and outcome of 17 children 7 with X-linked (XL) and 10 with autosomal recessive (AR) form was performed. Diagnosis of CGD was based on an abnormal granulocyte oxidative burst evaluated by either Nitroblue Tetrazolium (NBT) test or flow cytometry based Dihyrorhodamine 123 assay or both. The molecular diagnosis was confirmed by genetic mutation analysis in 13 cases. The mean age at diagnosis and the age at onset of symptoms was significantly lower in children diagnosed with XL- CGD compared those with AR disease. Mutations were detected in CYBB gene in 6 patients with XL-CGD and NCF-1 gene mutations were observed in 7 cases of AR- CGD. The course and outcome of the disease was much worse in children diagnosed with X-linked form of disease compared to AR forms of the disease; 4/7 (57 %) children with X-CGD were dead at the time of data analysis. This is one of the largest series on chronic granulomatous disease from any developing country.
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页码:58 / 67
页数:9
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