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Carfilzomib, rituximab, and dexamethasone (CaRD) treatment offers a neuropathy-sparing approach for treating Waldenström's macroglobulinemia.
[waldenström macroglobulinemia]
Bortezomib
frequently
produces
severe
treatment-related
peripheral
neuropathy
(
PN
)
in
Waldenström
's
macroglobulinemia
(
WM
)
.
Carfilzomib
is
a
neuropathy
-sparing
proteasome
inhibitor
.
We
examined
carfilzomib
,
rituximab
,
and
dexamethasone
(
CaRD
)
in
symptomatic
WM
patients
naïve
to
bortezomib
and
rituximab
.
Protocol
therapy
consisted
of
intravenous
carfilzomib
,
20
mg
/
m
2
(
cycle
1
)
and
36
mg
/
m
(
2
)
(
cycles
2
-
6
)
,
with
intravenous
dexamethasone
,
20
mg
,
on
days
1
,
2
,
8
,
and
9
,
and
rituximab
,
375
mg
/
m
(
2
)
,
on
days
2
and
9
every
21
days
.
Maintenance
therapy
followed
8
weeks
later
with
intravenous
carfilzomib
,
36
mg
/
m
(
2
)
,
and
intravenous
dexamethasone
,
20
mg
,
on
days
1
and
2
,
and
rituximab
,
375
mg
/
m
(
2
)
,
on
day
2
every
8
weeks
for
8
cycles
.
Overall
response
rate
was
87
.
1
%
(
1
complete
response
,
10
very
good
partial
responses
,
10
partial
responses
,
and
6
minimal
responses
)
and
was
not
impacted
by
MYD
88
(
L
265
P
)
or
CXCR
4
(
WHIM
)
mutation
status
.
With
a
median
follow-up
of
15
.
4
months
,
20
patients
remain
progression
free
.
Grade
≥
2
toxicities
included
asymptomatic
hyperlipasemia
(
41
.
9
%
)
,
reversible
neutropenia
(
12
.
9
%
)
,
and
cardiomyopathy
in
1
patient
(
3
.
2
%
)
with
multiple
risk
factors
,
and
PN
in
1
patient
(
3
.
2
%
)
which
was
grade
2
.
Declines
in
serum
IgA
and
IgG
were
common
.
CaRD
offers
a
neuropathy
-sparing
approach
for
proteasome
inhibitor-based
therapy
in
WM
.
This
trial
is
registered
at
www
.
clinicaltrials
.
gov
as
#
NCT
01470196
.
Diseases
Validation
Diseases presenting
"severe treatment-related peripheral neuropathy"
symptom
waldenström macroglobulinemia
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