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Host natural killer immunity is a key indicator of permissiveness for donor cell engraftment in patients with severe combined immunodeficiency.
[severe combined immunodeficiency]
Severe
combined
immunodeficiency
(
SCID
)
can
be
Â
cured
by
using
allogeneic
hematopoietic
stem
cell
transplantation
,
and
the
absence
of
host
immunity
often
obviates
the
need
for
preconditioning
.
Depending
on
the
underlying
genetic
defect
and
when
blocks
in
differentiation
occur
during
lymphocyte
ontogeny
,
infants
with
SCID
have
absent
or
greatly
reduced
numbers
of
functional
T
cells
.
Natural
killer
(
NK
)
cell
populations
are
usually
absent
in
the
SCID
-X
1
and
Janus
kinase
3
forms
of
SCID
and
greatly
reduced
in
adenosine
deaminase
deficiency
SCID
but
often
present
in
other
forms
of
the
disorder
.
To
determine
if
SCID
phenotypes
indicate
host
permissiveness
to
donor
cell
engraftment
.
A
retrospective
data
analysis
considered
whether
host
NK
cells
influenced
donor
T
-
cell
engraftment
,
immune
reconstitution
,
and
long
-term
outcomes
in
children
who
had
undergone
nonconditioned
allogeneic
stem
cell
transplantation
between
1990
and
2011
in
the
United
Kingdom
.
Detailed
analysis
of
T
-
and
B-
cell
immune
reconstitution
and
donor
chimerism
was
compared
between
the
NK
(
+
)
(
n
Â
=
24
)
and
NK
(
-
)
(
n
Â
=
53
)
forms
of
SCID
.
Overall
,
77
children
underwent
transplantation
,
with
survival
of
90
%
in
matched
sibling
donor
/
matched
family
donor
transplants
compared
with
60
%
when
alternative
donors
were
used
.
Infants
with
NK
(
-
)
SCID
were
more
likely
to
survive
than
NK
(
+
)
recipients
(
87
%
vs
62
%
,
P
Â
<
.
01
)
and
had
high
-level
donor
T
-
cell
chimerism
with
superior
long
-term
recovery
of
CD
4
T
-
cell
immunity
.
Notably
,
33
%
of
children
with
NK
(
+
)
SCID
required
additional
transplantation
procedures
compared
with
only
8
%
of
children
with
NK
(
-
)
SCID
(
P
Â
<
.
005
)
.
NK
(
-
)
SCID
disorders
are
highly
permissive
for
donor
T
-
cell
engraftment
without
preconditioning
,
whereas
the
presence
of
NK
cells
is
a
strong
indicator
that
preparative
conditioning
is
required
for
engraftment
of
T
-
cell
precursors
capable
of
supporting
robust
T
-
cell
reconstitution
.