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Cellular evidence for selfish spermatogonial selection in aged human testes.
[achondroplasia]
Owing
to
a
recent
trend
for
delayed
paternity
,
the
genomic
integrity
of
spermatozoa
of
older
men
has
become
a
focus
of
increased
interest
.
Older
fathers
are
at
higher
risk
for
their
children
to
be
born
with
several
monogenic
conditions
collectively
termed
paternal
age
effect
(
PAE
)
disorders
,
which
include
achondroplasia
,
Apert
syndrome
and
Costello
syndrome
.
These
disorders
are
caused
by
specific
mutations
originating
almost
exclusively
from
the
male
germline
,
in
genes
encoding
components
of
the
tyrosine
kinase
receptor
/
RAS
/
MAPK
signalling
pathway
.
These
particular
mutations
,
occurring
randomly
during
mitotic
divisions
of
spermatogonial
stem
cells
(
SSCs
)
,
are
predicted
to
confer
a
selective
/
growth
advantage
on
the
mutant
SSC
.
This
selective
advantage
leads
to
a
clonal
expansion
of
the
mutant
cells
over
time
,
which
generates
mutant
spermatozoa
at
levels
significantly
above
the
background
mutation
rate
.
This
phenomenon
,
termed
selfish
spermatogonial
selection
,
is
likely
to
occur
in
all
men
.
In
rare
cases
,
probably
because
of
additional
mutational
events
,
selfish
spermatogonial
selection
may
lead
to
spermatocytic
seminoma
.
The
studies
that
initially
predicted
the
clonal
nature
of
selfish
spermatogonial
selection
were
based
on
DNA
analysis
,
rather
than
the
visualization
of
mutant
clones
in
intact
testes
.
In
a
recent
study
that
aimed
to
identify
these
clones
directly
,
we
stained
serial
sections
of
fixed
testes
for
expression
of
melanoma
antigen
family
A
4
(
MAGEA
4
)
,
a
marker
of
spermatogonia
.
A
subset
of
seminiferous
tubules
with
an
appearance
and
distribution
compatible
with
the
predicted
mutant
clones
were
identified
.
In
these
tubules
,
termed
'
immunopositive
tubules
'
,
there
is
an
increased
density
of
spermatogonia
positive
for
markers
related
to
selfish
selection
(
FGFR
3
)
and
SSC
self-renewal
(
phosphorylated
AKT
)
.
Here
we
detail
the
properties
of
the
immunopositive
tubules
and
how
they
relate
to
the
predicted
mutant
clones
,
as
well
as
discussing
the
utility
of
identifying
the
potential
cellular
source
of
PAE
mutations
.
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Diseases presenting
"predicted mutant clones"
symptom
achondroplasia
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