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Garrod's fourth inborn error of metabolism solved by the identification of mutations causing pentosuria.
[cystinuria]
Pentosuria
is
one
of
four
conditions
hypothesized
by
Archibald
Garrod
in
1908
to
be
inborn
errors
of
metabolism
.
Mutations
responsible
for
the
other
three
conditions
(
albinism
,
alkaptonuria
,
and
cystinuria
)
have
been
identified
,
but
the
mutations
responsible
for
pentosuria
remained
unknown
.
Pentosuria
,
which
affects
almost
exclusively
individuals
of
Ashkenazi
Jewish
ancestry
,
is
characterized
by
high
levels
of
the
pentose
sugar
L-
xylulose
in
blood
and
urine
and
deficiency
of
the
enzyme
L-
xylulose
reductase
.
The
condition
is
autosomal-recessive
and
completely
clinically
benign
,
but
in
the
early
and
mid-
20
th
century
attracted
attention
because
it
was
often
confused
with
diabetes
mellitus
and
inappropriately
treated
with
insulin
.
Persons
with
pentosuria
were
identified
from
records
of
Margaret
Lasker
,
who
studied
the
condition
in
the
1930
s
to
1960
s
.
In
the
DCXR
gene
encoding
L-
xylulose
reductase
,
we
identified
two
mutations
,
DCXR
c
.
583
ΔC
and
DCXR
c
.
52
(
+
1
)
G
>
A
,
each
predicted
to
lead
to
loss
of
enzyme
activity
.
Of
nine
unrelated
living
pentosuric
subjects
,
six
were
homozygous
for
DCXR
c
.
583
ΔC
,
one
was
homozygous
for
DCXR
c
.
52
(
+
1
)
G
>
A
,
and
two
were
compound
heterozygous
for
the
two
mutant
alleles
.
L-
xylulose
reductase
was
not
detectable
in
protein
lysates
from
subjects
'
cells
and
high
levels
of
xylulose
were
detected
in
their
sera
,
confirming
the
relationship
between
the
DCXR
genotypes
and
the
pentosuric
phenotype
.
The
combined
frequency
of
the
two
mutant
DCXR
alleles
in
1
,
067
Ashkenazi
Jewish
controls
was
0
.
0173
,
suggesting
a
pentosuria
frequency
of
approximately
one
in
3
,
300
in
this
population
.
Haplotype
analysis
indicated
that
the
DCXR
c
.
52
(
+
1
)
G
>
A
mutation
arose
more
recently
than
the
DCXR
c
.
583
ΔC
mutation
.
Diseases
Validation
Diseases presenting
"high levels"
symptom
22q11.2 deletion syndrome
adrenal incidentaloma
allergic bronchopulmonary aspergillosis
alpha-thalassemia
aromatase deficiency
cadasil
canavan disease
classical phenylketonuria
congenital adrenal hyperplasia
congenital toxoplasmosis
cutaneous mastocytosis
cystinuria
dentin dysplasia
dentinogenesis imperfecta
dracunculiasis
dystrophic epidermolysis bullosa
erythropoietic protoporphyria
gm1 gangliosidosis
hereditary cerebral hemorrhage with amyloidosis
holt-oram syndrome
homocystinuria without methylmalonic aciduria
kabuki syndrome
kallmann syndrome
liposarcoma
papillon-lefèvre syndrome
phenylketonuria
primary effusion lymphoma
primary hyperoxaluria type 1
scrub typhus
severe combined immunodeficiency
systemic capillary leak syndrome
triple a syndrome
von hippel-lindau disease
werner syndrome
wiskott-aldrich syndrome
wolf-hirschhorn syndrome
x-linked adrenoleukodystrophy
zellweger syndrome
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