Case report
Alagille syndrome


Alagille syndrome is a highly variable, autosomal dominant multisystem disease
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•Alagille syndrome 1, ALGS1 (MIM # 118450), which is caused by a mutation in the JAG1 gene on
chromosome 20p12, with an incidence of 1:30,000 live births, 98% of patients with ALGS
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•Alagille syndrome 2, ALGS2 (MIM # 610205), which is associated with a mutation in the NOTCH2 gene
on chromosome 1p12 and represents a rarer form of disability (1: 70,000 live births), 1-2% of
patients with ALGS

The basic symptom of the syndrome is a reduction of intrahepatic bile ducts in combination with 5
diagnostic features:
•Cholestasis (jaundice with conjugated hyperbilirubinemia, ↑ GGT, ↑ Chol, ↑ TGL, 10-20% of patients
with rapid progression of liver disease)
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•Congenital heart disease (most often peripheral pulmonary stenosis, Fallot's tetralogy, pulmonary
atresia, atrial or ventricular septal defect)
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•Skeletal abnormalities (most often butterfly vertebrae, vertebral fusion, spina bifida occulta,
hemivertebra, 12th rib anomalies)
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•Eye disorders (most often posterior embryotoxon - prominence of the Schwalbe´s ring at the
interface of the iris and cornea)
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•Characteristic appearance of a triangular face with a wide forehead, deep set eyes, hypertelorism,
lower set ears and a longer onion-shaped nose

•3 of these 5 major characters must be present to confirm the diagnosis
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patient with ALGS, typical face
D:\Dokumenty\ala3.JPG D:\Dokumenty\ala2.JPG
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posterior embryotoxon
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•butterfly vertebrae
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•bile duct paucity
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•
•
•
•
•
•
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•butterfly vertebrae

•About 39% of patients suffer from kidney problems, most often renal dysplasia
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•Growth retardation
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•Pancreatic insufficiency (40%)
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•Hypothyroidism
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•Recurrent infections
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•Mental retardation and learning disabilities usually in patients with deletion 20p12
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•Alagille syndrome is a genetically heterogeneous disorder
•

•
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•We present phenotype of 4 probands with ALGS1, whose involvement was confirmed by molecular
genetic examination
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•
•
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•Method: next generation sequencing technique (MiSeq, Illumina) followed by direct sequencing of
PCR products on a genetic analyzer. At the genomic DNA level, the coding region of the JAG1 gene,
including exon / intron boundaries, was sequenced. The obtained sequences were compared with the
reference sequences of the JAG1 gene NG_007496.1 and NM_000214.2. The analysis of the found
variants was performed on the basis of the reference database
(http://www.ncbi.nlm.nih.gov/projects/SNP).

Phenotype of patients with ALGS1
Table 1 Clinical features present in carriers of JAG1 mutations
Pacient
Diagnosis
Peculiar face
Cholestasis
Liver biopsy

Heart disease
Ocular
Skeletal
Renal
Others


Age






anomalies
anomalies
anomalies


1
16 month
yes
yes
intrahepatic bile duct
peripheral pulmonary
no
butterfly
no
learning disability




paucity

artery stenosis

vertebrae



2
6 years
yes
yes
intrahepatic bile duct
peripheral pulmonary
no
no
no






paucity

artery stenosis





3
7month
yes
yes
intrahepatic bile duct
peripheral pulmonary
no
no
ren
behavioral disorders




paucity

artery stenosis


arcuatus


4
3 month
yes
yes
intrahepatic bile duct
peripheral pulmonary
embryotoxon
rib
cystic
hypothyroidism




paucity

artery stenosis
posterior
anomalies
disease
growth retardation

Results of molecular genetic testing of the JAG1 gene
Table 2 Mutations in JAG1 found in patients with Alagille syndrome




Pacient
identified sequence variants




Mutation
Exon
cDNA
Protein
Mutation









origin



type
1
gene JAG1 (NM_000214.2):c.3189dupG in heterozygous state

not
25
c.3189dupG
p.Asn1064Glufs*45
frameshift

novel mutation, duplication





investigated




2
gene JAG1(NM_000214.2): c.2039delG in heterozygous state


mother
16
c.2039delG
p.Gly680Alafs*63
frameshift

novel mutation, deletion










3
gene  JAG1 (NM_000214.2):c.1913delG in heterozygous state


father
15
c.1913delG
p.Cys638Leufs*105
frameshift

novel mutation, deletion










4
gene  JAG1 (NM_000214.2):c.2230C>T p.(Arg744Ter) in heterozygous state

de novo
18
c.2230C>T
p.Arg744Ter
nonsense

substitution











the c. nomenclature is based on the cDNA sequence NM_000214.2

Family screening
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•The mother of proband No. 2 was monitored at the Department of Gastroenterology for unexplained
hepatitis
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•Molecular - genetic examination also confirmed  ALGS1
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•Cardiac examination revealed aortic valve insufficiency
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•Another sibling - molecular-genetically ALGS1 excluded
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•Importance: diagnosis and genetic counseling in the family

•The care of these patients is multidisciplinary
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•It includes a pediatrician, hepatologist, cardiologist, ophthalmologist, nephrologist,
endocrinologist, nutritional therapist, radiologist, geneticist and, in some cases, a transplant
team.
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•Molecular-genetic examination x classical scoring system
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•Genetic testing in unclear cases