Entry - #610181 - AICARDI-GOUTIERES SYNDROME 2; AGS2 - OMIM

 
ICD+
# 610181

AICARDI-GOUTIERES SYNDROME 2; AGS2


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
13q14.3 Aicardi-Goutieres syndrome 2 610181 AR 3 RNASEH2B 610326
Clinical Synopsis
 
Phenotypic Series
 

INHERITANCE
- Autosomal recessive
HEAD & NECK
Head
- Microcephaly (in some patients)
NEUROLOGIC
Central Nervous System
- Normal early development
- Neurologic dysfunction, progressive
- Spastic paraplegia (in some patients)
- Encephalopathy (in some patients)
- Normal cognition (in some patients)
- Dystonia (in some patients)
- Intracranial calcification affecting the basal ganglia (in some patients)
LABORATORY ABNORMALITIES
- Increased interferon-alpha signal
- Lymphocytosis in the cerebrospinal fluid
- No evidence of common prenatal infections
MISCELLANEOUS
- Onset in the first 2 years of life
- Progressive or slowly progressive
- Variable severity
MOLECULAR BASIS
- Caused by mutation in the ribonuclease H2, subunit B gene (RNASEH2B, 610326.0001)
▲ Close

TEXT

A number sign (#) is used with this entry because of evidence that Aicardi-Goutieres syndrome-2 (AGS2) is caused by homozygous or compound heterozygous mutation in the gene encoding subunit B of ribonuclease H2 (RNASEH2B; 610326) on chromosome 13q14.

Description

Aicardi-Goutieres syndrome (AGS) is an autosomal recessive early-onset encephalopathy characterized by calcification of the basal ganglia, chronic cerebrospinal fluid lymphocytosis, and negative serologic investigations for common prenatal infections (summary by Ali et al., 2006). Severe neurologic dysfunction becomes clinically apparent in infancy and manifests as progressive microcephaly, spasticity, dystonic posturing, profound psychomotor retardation, and often death in early childhood (summary by Crow et al., 2006).

For a general phenotypic description and a discussion of genetic heterogeneity of Aicardi-Goutieres syndrome, see AGS1 (225750).

Clinical Features

Ali et al. (2006) reported 17 children from 8 families with progressive neurodegeneration and encephalopathy beginning at birth or in infancy. Six of the families were consanguineous. All of the patients had evidence of intracranial calcification primarily affecting the basal ganglia; several had microcephaly. Laboratory studies showed lymphocytosis of the cerebrospinal fluid (CSF) and increased alpha-interferon in the CSF in most patients. Investigation for common prenatal infections was negative. The families were of multiple ethnic origins, including Algerian, Moroccan, and European.

Clinical Variability

Crow et al. (2014) reported 2 Egyptian sibs and an unrelated patient of North African descent who presented with nonsyndromic spastic paraplegia around age 2 years following normal psychomotor development. Physical examination showed scissoring gait, hypertonia, increased reflexes, ankle and patellar clonus, and extensor plantar responses. All 3 children remained ambulatory between the ages of 5 and 11 years. All had normal head size and normal cognition. Brain imaging of the 2 sibs was normal; the unrelated child had diffuse nonspecific high signal on T2-weighted imaging with some dilatation of the lateral ventricles at age 3. One of the sibs had unilateral optic atrophy, but this may have been unrelated to the primary disorder. None of the patients had increased interferon levels or chilblain skin lesions. Crow et al. (2014) emphasized the phenotypic variability associated with AGS, noting that neurologic dysfunction is not always marked in this disorder.

Tonduti et al. (2019) reported 3 patients with homozygosity for the common RNASEH2B mutation (A177T; 610326.0001) who displayed early clinical and MRI features consistent with AGS2 but showed improvement in neuroimaging including reduction in white matter hyperintensities. Patient 1 was treated with multiple courses of intravenous immunoglobulins and high-dose steroids between the ages of 21 months and 4 years, whereas the other 2 patients did not receive these interventions. Patients 1 and 3 were diagnosed with AGS2, and patient 2 was diagnosed with atypical AGS2 due to lack of cerebral calcifications, CSF lymphocytosis, elevated interferon-alpha concentrations, or a positive interferon signal. Patient 2 was intellectually normal at 4 years of age and had stable spastic diplegia. Patients 1 and 3 had global delays, but did show some developmental progression.


Inheritance

The transmission pattern of AGS2 in the families reported by Ali et al. (2006) was consistent with autosomal recessive inheritance.


Mapping

By genomewide linkage analysis of 10 families with Aicardi-Goutieres syndrome in whom linkage to AGS1 was excluded, Ali et al. (2006) identified a putative disease locus, termed AGS2, on chromosome 13q14-q21 (maximum multipoint lod score of 5.75 at marker D13S768). The AGS2 locus lies within a 4.7-cM region between D13S284 and D13S1309.


Molecular Genetics

In affected members of 18 unrelated families with AGS2, Crow et al. (2006) identified homozygous and compound heterozygous mutations in the RNASEH2B gene (see, e.g., 610326.0001-610326.0002). Most of the families were of European or North African descent.

In 2 Egyptian sibs and an unrelated patient of North African descent who presented with nonsyndromic spastic paraplegia around age 2 years following normal psychomotor development, Crow et al. (2014) identified a homozygous A177T mutation in the RNASEH2B gene (610326.0001). The mutation was found by exome sequencing.


REFERENCES

  1. Ali, M., Highet, L. J., Lacombe, D., Goizet, C., King, M. D., Tacke, U., van der Knapp, M. S., Lagae, L., Rittey, C., Brunner, H. G., van Bokhoven, H., Hamel, B., and 10 others. A second locus for Aicardi-Goutieres syndrome at chromosome 13q14-21. J. Med. Genet. 43: 444-450, 2006. [PubMed: 15908569, images, related citations] [Full Text]

  2. Crow, Y. J., Leitch, A., Hayward, B. E., Garner, A., Parmar, R., Griffith, E., Ali, M., Semple, C., Aicardi, J., Babul-Hirji, R., Baumann, C., Baxter, P., and 33 others. Mutations in genes encoding ribonuclease H2 subunits cause Aicardi-Goutieres syndrome and mimic congenital viral brain infection. Nature Genet. 38: 910-916, 2006. [PubMed: 16845400, related citations] [Full Text]

  3. Crow, Y. J., Zaki, M. S., Abdel-Hamid, M. S., Abdel-Salam, G., Boespflug-Tanguy, O., Cordeiro, N. J. V., Gleeson, J. G., Gowrinathan, N. R., Laugel, V., Renaldo, F., Rodriguez, D., Livingston, J. H., Rice, G. I. Mutations in ADAR1, IFIH1, and RNASEH2B presenting as spastic paraplegia. Neuropediatrics 45: 386-391, 2014. [PubMed: 25243380, related citations] [Full Text]

  4. Tonduti, D., Izzo, G., D'Arrigo, S. Riva, D., Moroni, I., Zorzi, G., Cavallera, V., Pichiecchio, A., Uggetti, C., Veggiotti, P., Orcesi, S., Chiapparini, L., Parazzini, C. Spontaneous MRI improvement and absence of cerebral calcification in Aicardi-Goutieres syndrome: diagnostic and disease-monitoring implications. Molec. Genet. Metab. 126: 489-494, 2019. [PubMed: 30826161, related citations] [Full Text]


Contributors:
Hilary J. Vernon - updated : 11/22/2021
Victor A. McKusick - updated : 8/15/2006
Creation Date:
Cassandra L. Kniffin : 6/12/2006
Edit History:
carol : 12/15/2023
carol : 11/22/2021
carol : 05/26/2017
alopez : 12/18/2014
alopez : 12/18/2014
mcolton : 12/16/2014
ckniffin : 12/15/2014
carol : 1/11/2012
carol : 8/18/2006
ckniffin : 8/17/2006
terry : 8/15/2006
wwang : 6/16/2006
ckniffin : 6/12/2006

# 610181

AICARDI-GOUTIERES SYNDROME 2; AGS2


ORPHA: 51, 689234;   DO: 0050629;  


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
13q14.3 Aicardi-Goutieres syndrome 2 610181 Autosomal recessive 3 RNASEH2B 610326

TEXT

A number sign (#) is used with this entry because of evidence that Aicardi-Goutieres syndrome-2 (AGS2) is caused by homozygous or compound heterozygous mutation in the gene encoding subunit B of ribonuclease H2 (RNASEH2B; 610326) on chromosome 13q14.

Description

Aicardi-Goutieres syndrome (AGS) is an autosomal recessive early-onset encephalopathy characterized by calcification of the basal ganglia, chronic cerebrospinal fluid lymphocytosis, and negative serologic investigations for common prenatal infections (summary by Ali et al., 2006). Severe neurologic dysfunction becomes clinically apparent in infancy and manifests as progressive microcephaly, spasticity, dystonic posturing, profound psychomotor retardation, and often death in early childhood (summary by Crow et al., 2006).

For a general phenotypic description and a discussion of genetic heterogeneity of Aicardi-Goutieres syndrome, see AGS1 (225750).

Clinical Features

Ali et al. (2006) reported 17 children from 8 families with progressive neurodegeneration and encephalopathy beginning at birth or in infancy. Six of the families were consanguineous. All of the patients had evidence of intracranial calcification primarily affecting the basal ganglia; several had microcephaly. Laboratory studies showed lymphocytosis of the cerebrospinal fluid (CSF) and increased alpha-interferon in the CSF in most patients. Investigation for common prenatal infections was negative. The families were of multiple ethnic origins, including Algerian, Moroccan, and European.

Clinical Variability

Crow et al. (2014) reported 2 Egyptian sibs and an unrelated patient of North African descent who presented with nonsyndromic spastic paraplegia around age 2 years following normal psychomotor development. Physical examination showed scissoring gait, hypertonia, increased reflexes, ankle and patellar clonus, and extensor plantar responses. All 3 children remained ambulatory between the ages of 5 and 11 years. All had normal head size and normal cognition. Brain imaging of the 2 sibs was normal; the unrelated child had diffuse nonspecific high signal on T2-weighted imaging with some dilatation of the lateral ventricles at age 3. One of the sibs had unilateral optic atrophy, but this may have been unrelated to the primary disorder. None of the patients had increased interferon levels or chilblain skin lesions. Crow et al. (2014) emphasized the phenotypic variability associated with AGS, noting that neurologic dysfunction is not always marked in this disorder.

Tonduti et al. (2019) reported 3 patients with homozygosity for the common RNASEH2B mutation (A177T; 610326.0001) who displayed early clinical and MRI features consistent with AGS2 but showed improvement in neuroimaging including reduction in white matter hyperintensities. Patient 1 was treated with multiple courses of intravenous immunoglobulins and high-dose steroids between the ages of 21 months and 4 years, whereas the other 2 patients did not receive these interventions. Patients 1 and 3 were diagnosed with AGS2, and patient 2 was diagnosed with atypical AGS2 due to lack of cerebral calcifications, CSF lymphocytosis, elevated interferon-alpha concentrations, or a positive interferon signal. Patient 2 was intellectually normal at 4 years of age and had stable spastic diplegia. Patients 1 and 3 had global delays, but did show some developmental progression.


Inheritance

The transmission pattern of AGS2 in the families reported by Ali et al. (2006) was consistent with autosomal recessive inheritance.


Mapping

By genomewide linkage analysis of 10 families with Aicardi-Goutieres syndrome in whom linkage to AGS1 was excluded, Ali et al. (2006) identified a putative disease locus, termed AGS2, on chromosome 13q14-q21 (maximum multipoint lod score of 5.75 at marker D13S768). The AGS2 locus lies within a 4.7-cM region between D13S284 and D13S1309.


Molecular Genetics

In affected members of 18 unrelated families with AGS2, Crow et al. (2006) identified homozygous and compound heterozygous mutations in the RNASEH2B gene (see, e.g., 610326.0001-610326.0002). Most of the families were of European or North African descent.

In 2 Egyptian sibs and an unrelated patient of North African descent who presented with nonsyndromic spastic paraplegia around age 2 years following normal psychomotor development, Crow et al. (2014) identified a homozygous A177T mutation in the RNASEH2B gene (610326.0001). The mutation was found by exome sequencing.


REFERENCES

  1. Ali, M., Highet, L. J., Lacombe, D., Goizet, C., King, M. D., Tacke, U., van der Knapp, M. S., Lagae, L., Rittey, C., Brunner, H. G., van Bokhoven, H., Hamel, B., and 10 others. A second locus for Aicardi-Goutieres syndrome at chromosome 13q14-21. J. Med. Genet. 43: 444-450, 2006. [PubMed: 15908569] [Full Text: https://doi.org/10.1136/jmg.2005.031880]

  2. Crow, Y. J., Leitch, A., Hayward, B. E., Garner, A., Parmar, R., Griffith, E., Ali, M., Semple, C., Aicardi, J., Babul-Hirji, R., Baumann, C., Baxter, P., and 33 others. Mutations in genes encoding ribonuclease H2 subunits cause Aicardi-Goutieres syndrome and mimic congenital viral brain infection. Nature Genet. 38: 910-916, 2006. [PubMed: 16845400] [Full Text: https://doi.org/10.1038/ng1842]

  3. Crow, Y. J., Zaki, M. S., Abdel-Hamid, M. S., Abdel-Salam, G., Boespflug-Tanguy, O., Cordeiro, N. J. V., Gleeson, J. G., Gowrinathan, N. R., Laugel, V., Renaldo, F., Rodriguez, D., Livingston, J. H., Rice, G. I. Mutations in ADAR1, IFIH1, and RNASEH2B presenting as spastic paraplegia. Neuropediatrics 45: 386-391, 2014. [PubMed: 25243380] [Full Text: https://doi.org/10.1055/s-0034-1389161]

  4. Tonduti, D., Izzo, G., D'Arrigo, S. Riva, D., Moroni, I., Zorzi, G., Cavallera, V., Pichiecchio, A., Uggetti, C., Veggiotti, P., Orcesi, S., Chiapparini, L., Parazzini, C. Spontaneous MRI improvement and absence of cerebral calcification in Aicardi-Goutieres syndrome: diagnostic and disease-monitoring implications. Molec. Genet. Metab. 126: 489-494, 2019. [PubMed: 30826161] [Full Text: https://doi.org/10.1016/j.ymgme.2019.02.006]


Contributors:
Hilary J. Vernon - updated : 11/22/2021
Victor A. McKusick - updated : 8/15/2006

Creation Date:
Cassandra L. Kniffin : 6/12/2006

Edit History:
carol : 12/15/2023
carol : 11/22/2021
carol : 05/26/2017
alopez : 12/18/2014
alopez : 12/18/2014
mcolton : 12/16/2014
ckniffin : 12/15/2014
carol : 1/11/2012
carol : 8/18/2006
ckniffin : 8/17/2006
terry : 8/15/2006
wwang : 6/16/2006
ckniffin : 6/12/2006



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® 1966-2025 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® 1966-2025 Johns Hopkins University.
Printed: March 5, 2025