Entry - #233710 - GRANULOMATOUS DISEASE, CHRONIC, AUTOSOMAL RECESSIVE, 2; CGD2 - OMIM

 
ICD+
# 233710

GRANULOMATOUS DISEASE, CHRONIC, AUTOSOMAL RECESSIVE, 2; CGD2


Alternative titles; symbols

GRANULOMATOUS DISEASE, CHRONIC, AUTOSOMAL RECESSIVE, CYTOCHROME b-POSITIVE, TYPE II
CGD, AUTOSOMAL RECESSIVE CYTOCHROME b-POSITIVE, TYPE II
GRANULOMATOUS DISEASE, CHRONIC, DUE TO NCF2 DEFICIENCY
NEUTROPHIL CYTOSOL FACTOR 2 DEFICIENCY
NCF2 DEFICIENCY
p67-PHOX DEFICIENCY


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
1q25.3 Chronic granulomatous disease 2, autosomal recessive 233710 AR 3 NCF2 608515
Clinical Synopsis
 
Phenotypic Series
 

INHERITANCE
- Autosomal recessive
RESPIRATORY
Lung
- Pneumonia due to immunodeficiency
ABDOMEN
Liver
- Hepatic abscesses due to immunodeficiency
- Hepatomegaly
Spleen
- Splenomegaly
Gastrointestinal
- Perirectal abscesses due to immunodeficiency
SKELETAL
- Osteomyelitis due to immunodeficiency
SKIN, NAILS, & HAIR
Skin
- Dermatitis, infectious, due to immunodeficiency
- Impetigo
- Eczematoid dermatitis
- Discoid lupus in carriers or adults with mild disease
MUSCLE, SOFT TISSUES
- Cellulitis due to immunodeficiency
IMMUNOLOGY
- Bacterial infections, recurrent
- Fungal infections, recurrent
- Absence of bactericidal oxidative 'respiratory burst' in phagocytes
- Abscess formation in any organ
- Lymphadenitis
- Lymphadenopathy
- Aspergillus infections
- Klebsiella infections
- Staphylococcus aureus infections
- E. coli infections
- Burkholderia cepacia infections
- Serratia marcescens infections
- Tissue biopsy shows granulomas
- Biopsy shows lipid-laden macrophages
LABORATORY ABNORMALITIES
- Presence of cytochrome b(-245)
- Deficiency or absence of p67-phox protein (type II)
- Negative nitroblue tetrazolium (NBT) reduction test
- Decreased activity of NADPH oxidase
MISCELLANEOUS
- Onset usually in first decade
- Four types of CGD with basically identical clinical phenotypes
- X-linked recessive cytochrome b-negative CGD (306400)
- Autosomal recessive cytochrome b-negative CGD (233690)
- Autosomal recessive cytochrome b-positive CGD, type I (233700)
- Autosomal recessive cytochrome b-positive CGD, type II
MOLECULAR BASIS
- Caused by mutation in the neutrophil cytosolic factor-2 gene, p67-phox (NCF2, 608515.0001)
▲ Close

TEXT

A number sign (#) is used with this entry because of evidence that autosomal recessive chronic granulomatous disease-2 (CGD2) is caused by homozygous or compound heterozygous mutation in the NCF2 gene (608515), which encodes the p67-phox (phagocyte oxidase) protein, on chromosome 1q25.

For a general phenotypic description and a discussion of genetic heterogeneity of chronic granulomatous disease, see X-linked recessive CGD (CGDX; 306400).

Clinical Features

Nunoi et al. (1995) reported a 19-year-old Japanese with p67-deficient CGD confirmed by mutation in the NCF2 gene (608515.0001). His first episode of infection occurred at age 3 when he had perianal abscess, liver abscess, severe lung abscess, pneumonia with Aspergillus infection, and severe spinal Aspergillus osteomyelitis. Recurrent infections occurred at ages 4, 6, 11, 15, and 19 years. His clinical course was worse than that of 4 other patients with p67-phox deficiency found in Japan. CGD was diagnosed by no reduction of nitroblue tetrazolium in neutrophils. Nunoi et al. (1995) stated that only 5 patients with p67-phox deficiency had been reported in the United States and Europe, whereas in Japan, although such CGD patients are also rare, they accounted for 7 of 90 CGD patients.

Patino et al. (1999) reported several girls with p67-phox-deficient CGD confirmed by molecular analysis. In an 8-year-old Hispanic girl, the diagnosis of CGD had been made at age 8 months when the patient presented with a right upper lobe pneumonia caused by Serratia marcescens. A 10-year-old girl, born of first-cousin parents native to Jordan, had recurrent abscesses caused by gram-negative bacteria in the first year of life. At the age of 5 years, she had developed inflammatory bowel disease. The diagnosis of CGD was made on the basis of absent NBT reduction and O2(-) production by her PMA-stimulated neutrophils. Deficiency of p67-phox was demonstrated by Western blot analysis. Her sister, aged 2 years, also showed the genetic defect but had not yet developed serious illness or required hospitalization. In a girl with p67-phox-deficient CGD who was 4 years old at the time of her death in Mexico, the diagnosis of CGD was suspected when she presented with skin abscesses containing Enterobacter and Klebsiella and confirmed by a negative NBT test and absent O2(-) production. In her last year of life she was treated successfully for Aspergillus fumigatus pneumonia; however, a few months later, she presented with a severe respiratory infection characterized by necrotizing granulomas and acid-fast bacteria.


Diagnosis

Prenatal Diagnosis

Kenney et al. (1993) reported a 9-year-old girl with CGD due to deficiency of p67-phox who was homozygous for a RFLP disease marker in the NCF2 gene. Her phenotypically normal mother was also homozygous for the marker, whereas the father and 2 brothers were heterozygous. A fetus was shown to be heterozygous as well, showing that it had inherited at least 1 normal NCF2 gene from the father, predicting a normal phenotype. Cord blood samples at birth showed normal oxidative function.


Pathogenesis

Volpp et al. (1988) raised a polyclonal antiserum that recognized the 47-kD and 67-kD proteins and showed that the neutrophils from patients with 2 different forms of autosomal CGD lacked either the 47- or the 67-kD protein. A deficiency of the 47-kD protein is more frequent than that of the 67-kD protein.


Clinical Management

Liese et al. (2000) evaluated the effect of antibiotic and antifungal long-term prophylaxis on the prognosis of CGD in 39 patients with different subtypes, both X-linked and autosomal recessive. Antibiotic prophylaxis with TMP-SMX significantly decreased the incidence of severe infections in patients with complete loss of cytochrome b activity but had no significant effect in patients with the other subtypes. Eight of the patients with complete absence of cytochrome b activity were also given itraconazole, and none developed fungal infections over 15.5 patient-years, whereas patients of all subtypes who received only antibiotics showed an increase in severe fungal infections. The different subtypes were also analyzed for age at diagnosis, age at first infection, and long-term survival.


Inheritance

The transmission pattern of CGD2 in the patients reported by Nunoi et al. (1995) and Patino et al. (1999) was consistent with autosomal recessive inheritance.


Molecular Genetics

In a Japanese patient with p67-phox-deficient CGD, Nunoi et al. (1995) identified a homozygous frameshift mutation in the NCF2 gene (608515.0001).

Patino et al. (1999) reported several girls with p67-phox-deficient CGD confirmed by homozygous or compound heterozygous mutation in the NCF2 gene (see, e.g., 608515.0003-608515.0006).


Genotype/Phenotype Correlations

Clark et al. (1989) concluded that the autosomal form of CGD due to deficiency of NCF1 represents about 33% of all cases of CGD; the autosomal form due to deficiency of NCF2 represents about 5% of cases.


REFERENCES

  1. Clark, R. A., Malech, H. L., Gallin, J. I., Nunoi, H., Volpp, B. D., Pearson, D. W., Nauseef, W. M., Curnutte, J. T. Genetic variants of chronic granulomatous disease: prevalence of deficiencies of two cytosolic components of the NADPH oxidase system. New Eng. J. Med. 321: 647-652, 1989. [PubMed: 2770793, related citations] [Full Text]

  2. Kenney, R. T., Malech, H. L., Epstein, N. D., Roberts, R. L., Leto, T. L. Characterization of the p67-phox gene: genomic organization and restriction fragment length polymorphism analysis for prenatal diagnosis in chronic granulomatous disease. Blood 82: 3739-3744, 1993. [PubMed: 7903171, related citations]

  3. Liese, J., Kloos, S., Jendrossek, V., Petropoulou, T., Wintergerst, U., Notheis, G., Gahr, M., Belohradsky, B. H. Long-term follow-up and outcome of 39 patients with chronic granulomatous disease. J. Pediat. 137: 687-693, 2000. [PubMed: 11060536, related citations] [Full Text]

  4. Nunoi, H., Iwata, M., Tatsuzawa, S., Onoe, Y., Shimizu, S., Kanegasaki, S., Matsuda, I. AG dinucleotide insertion in a patient with chronic granulomatous disease lacking cytosolic 67-kD protein. Blood 86: 329-333, 1995. [PubMed: 7795241, related citations]

  5. Patino, P. J., Rae, J., Noack, D., Erickson, R., Ding, J., Garcia de Olarte, D., Curnutte, J. T. Molecular characterization of autosomal recessive chronic granulomatous disease caused by a defect of the nicotinamide adenine dinucleotide phosphate (reduced form) oxidase component p67-phox. Blood 94: 2505-2514, 1999. [PubMed: 10498624, related citations]

  6. Volpp, B. D., Nauseef, W. M., Clark, R. A. Two cytosolic neutrophil oxidase components absent in autosomal chronic granulomatous disease. Science 242: 1295-1297, 1988. [PubMed: 2848318, related citations] [Full Text]


Contributors:
Cassandra L. Kniffin - reorganized : 3/12/2004
Cassandra L. Kniffin - updated : 3/11/2004
Victor A. McKusick - updated : 12/14/1999
Victor A. McKusick - updated : 12/7/1999
Creation Date:
Victor A. McKusick : 6/5/1989
Edit History:
carol : 04/16/2024
carol : 07/20/2020
carol : 07/17/2020
carol : 07/07/2020
carol : 07/06/2020
ckniffin : 07/02/2020
carol : 05/27/2016
carol : 3/23/2012
ckniffin : 3/15/2004
terry : 3/15/2004
carol : 3/12/2004
terry : 3/12/2004
ckniffin : 3/12/2004
ckniffin : 3/11/2004
mcapotos : 2/21/2000
yemi : 2/18/2000
mcapotos : 12/17/1999
mcapotos : 12/14/1999
carol : 12/14/1999
mcapotos : 12/13/1999
terry : 12/10/1999
terry : 12/7/1999
dkim : 7/24/1998
mimadm : 2/27/1994
carol : 2/21/1994
carol : 2/18/1993
supermim : 3/16/1992
carol : 12/19/1991
carol : 10/2/1990

# 233710

GRANULOMATOUS DISEASE, CHRONIC, AUTOSOMAL RECESSIVE, 2; CGD2


Alternative titles; symbols

GRANULOMATOUS DISEASE, CHRONIC, AUTOSOMAL RECESSIVE, CYTOCHROME b-POSITIVE, TYPE II
CGD, AUTOSOMAL RECESSIVE CYTOCHROME b-POSITIVE, TYPE II
GRANULOMATOUS DISEASE, CHRONIC, DUE TO NCF2 DEFICIENCY
NEUTROPHIL CYTOSOL FACTOR 2 DEFICIENCY
NCF2 DEFICIENCY
p67-PHOX DEFICIENCY


ORPHA: 379;   DO: 0070191;  


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
1q25.3 Chronic granulomatous disease 2, autosomal recessive 233710 Autosomal recessive 3 NCF2 608515

TEXT

A number sign (#) is used with this entry because of evidence that autosomal recessive chronic granulomatous disease-2 (CGD2) is caused by homozygous or compound heterozygous mutation in the NCF2 gene (608515), which encodes the p67-phox (phagocyte oxidase) protein, on chromosome 1q25.

For a general phenotypic description and a discussion of genetic heterogeneity of chronic granulomatous disease, see X-linked recessive CGD (CGDX; 306400).

Clinical Features

Nunoi et al. (1995) reported a 19-year-old Japanese with p67-deficient CGD confirmed by mutation in the NCF2 gene (608515.0001). His first episode of infection occurred at age 3 when he had perianal abscess, liver abscess, severe lung abscess, pneumonia with Aspergillus infection, and severe spinal Aspergillus osteomyelitis. Recurrent infections occurred at ages 4, 6, 11, 15, and 19 years. His clinical course was worse than that of 4 other patients with p67-phox deficiency found in Japan. CGD was diagnosed by no reduction of nitroblue tetrazolium in neutrophils. Nunoi et al. (1995) stated that only 5 patients with p67-phox deficiency had been reported in the United States and Europe, whereas in Japan, although such CGD patients are also rare, they accounted for 7 of 90 CGD patients.

Patino et al. (1999) reported several girls with p67-phox-deficient CGD confirmed by molecular analysis. In an 8-year-old Hispanic girl, the diagnosis of CGD had been made at age 8 months when the patient presented with a right upper lobe pneumonia caused by Serratia marcescens. A 10-year-old girl, born of first-cousin parents native to Jordan, had recurrent abscesses caused by gram-negative bacteria in the first year of life. At the age of 5 years, she had developed inflammatory bowel disease. The diagnosis of CGD was made on the basis of absent NBT reduction and O2(-) production by her PMA-stimulated neutrophils. Deficiency of p67-phox was demonstrated by Western blot analysis. Her sister, aged 2 years, also showed the genetic defect but had not yet developed serious illness or required hospitalization. In a girl with p67-phox-deficient CGD who was 4 years old at the time of her death in Mexico, the diagnosis of CGD was suspected when she presented with skin abscesses containing Enterobacter and Klebsiella and confirmed by a negative NBT test and absent O2(-) production. In her last year of life she was treated successfully for Aspergillus fumigatus pneumonia; however, a few months later, she presented with a severe respiratory infection characterized by necrotizing granulomas and acid-fast bacteria.


Diagnosis

Prenatal Diagnosis

Kenney et al. (1993) reported a 9-year-old girl with CGD due to deficiency of p67-phox who was homozygous for a RFLP disease marker in the NCF2 gene. Her phenotypically normal mother was also homozygous for the marker, whereas the father and 2 brothers were heterozygous. A fetus was shown to be heterozygous as well, showing that it had inherited at least 1 normal NCF2 gene from the father, predicting a normal phenotype. Cord blood samples at birth showed normal oxidative function.


Pathogenesis

Volpp et al. (1988) raised a polyclonal antiserum that recognized the 47-kD and 67-kD proteins and showed that the neutrophils from patients with 2 different forms of autosomal CGD lacked either the 47- or the 67-kD protein. A deficiency of the 47-kD protein is more frequent than that of the 67-kD protein.


Clinical Management

Liese et al. (2000) evaluated the effect of antibiotic and antifungal long-term prophylaxis on the prognosis of CGD in 39 patients with different subtypes, both X-linked and autosomal recessive. Antibiotic prophylaxis with TMP-SMX significantly decreased the incidence of severe infections in patients with complete loss of cytochrome b activity but had no significant effect in patients with the other subtypes. Eight of the patients with complete absence of cytochrome b activity were also given itraconazole, and none developed fungal infections over 15.5 patient-years, whereas patients of all subtypes who received only antibiotics showed an increase in severe fungal infections. The different subtypes were also analyzed for age at diagnosis, age at first infection, and long-term survival.


Inheritance

The transmission pattern of CGD2 in the patients reported by Nunoi et al. (1995) and Patino et al. (1999) was consistent with autosomal recessive inheritance.


Molecular Genetics

In a Japanese patient with p67-phox-deficient CGD, Nunoi et al. (1995) identified a homozygous frameshift mutation in the NCF2 gene (608515.0001).

Patino et al. (1999) reported several girls with p67-phox-deficient CGD confirmed by homozygous or compound heterozygous mutation in the NCF2 gene (see, e.g., 608515.0003-608515.0006).


Genotype/Phenotype Correlations

Clark et al. (1989) concluded that the autosomal form of CGD due to deficiency of NCF1 represents about 33% of all cases of CGD; the autosomal form due to deficiency of NCF2 represents about 5% of cases.


REFERENCES

  1. Clark, R. A., Malech, H. L., Gallin, J. I., Nunoi, H., Volpp, B. D., Pearson, D. W., Nauseef, W. M., Curnutte, J. T. Genetic variants of chronic granulomatous disease: prevalence of deficiencies of two cytosolic components of the NADPH oxidase system. New Eng. J. Med. 321: 647-652, 1989. [PubMed: 2770793] [Full Text: https://doi.org/10.1056/NEJM198909073211005]

  2. Kenney, R. T., Malech, H. L., Epstein, N. D., Roberts, R. L., Leto, T. L. Characterization of the p67-phox gene: genomic organization and restriction fragment length polymorphism analysis for prenatal diagnosis in chronic granulomatous disease. Blood 82: 3739-3744, 1993. [PubMed: 7903171]

  3. Liese, J., Kloos, S., Jendrossek, V., Petropoulou, T., Wintergerst, U., Notheis, G., Gahr, M., Belohradsky, B. H. Long-term follow-up and outcome of 39 patients with chronic granulomatous disease. J. Pediat. 137: 687-693, 2000. [PubMed: 11060536] [Full Text: https://doi.org/10.1067/mpd.2000.109112]

  4. Nunoi, H., Iwata, M., Tatsuzawa, S., Onoe, Y., Shimizu, S., Kanegasaki, S., Matsuda, I. AG dinucleotide insertion in a patient with chronic granulomatous disease lacking cytosolic 67-kD protein. Blood 86: 329-333, 1995. [PubMed: 7795241]

  5. Patino, P. J., Rae, J., Noack, D., Erickson, R., Ding, J., Garcia de Olarte, D., Curnutte, J. T. Molecular characterization of autosomal recessive chronic granulomatous disease caused by a defect of the nicotinamide adenine dinucleotide phosphate (reduced form) oxidase component p67-phox. Blood 94: 2505-2514, 1999. [PubMed: 10498624]

  6. Volpp, B. D., Nauseef, W. M., Clark, R. A. Two cytosolic neutrophil oxidase components absent in autosomal chronic granulomatous disease. Science 242: 1295-1297, 1988. [PubMed: 2848318] [Full Text: https://doi.org/10.1126/science.2848318]


Contributors:
Cassandra L. Kniffin - reorganized : 3/12/2004
Cassandra L. Kniffin - updated : 3/11/2004
Victor A. McKusick - updated : 12/14/1999
Victor A. McKusick - updated : 12/7/1999

Creation Date:
Victor A. McKusick : 6/5/1989

Edit History:
carol : 04/16/2024
carol : 07/20/2020
carol : 07/17/2020
carol : 07/07/2020
carol : 07/06/2020
ckniffin : 07/02/2020
carol : 05/27/2016
carol : 3/23/2012
ckniffin : 3/15/2004
terry : 3/15/2004
carol : 3/12/2004
terry : 3/12/2004
ckniffin : 3/12/2004
ckniffin : 3/11/2004
mcapotos : 2/21/2000
yemi : 2/18/2000
mcapotos : 12/17/1999
mcapotos : 12/14/1999
carol : 12/14/1999
mcapotos : 12/13/1999
terry : 12/10/1999
terry : 12/7/1999
dkim : 7/24/1998
mimadm : 2/27/1994
carol : 2/21/1994
carol : 2/18/1993
supermim : 3/16/1992
carol : 12/19/1991
carol : 10/2/1990



NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.

NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.
Printed: April 29, 2024