MDACC has, for the first time, given their experience of TKI
v `: j. z2 n7 \discontinuation. The doctors at MDACC look at 26 patients who
' o% q3 \$ q* H& {/ Rdiscontinued therapy from 2003-2012 for various reasons. These reasons
" H1 K3 Q. {( T* vinclude long time in CMR, adverse side-effects, pregnancy and financial
8 Q4 [( t, k5 N' Y# O Sconstraints. Please note that 17 patients discontinued therapy in CMR
* q$ \; o5 p( xand the rest in MMR. Of the patients in CMR who discontinued therapy,
( f& d7 s2 r) p5 q; N47% had molecular relapse. Those in CMR who discontinued and had taken
. G/ H6 R8 f! Rprior Interferon to a TKI, 50% relapsed. Also note that of these 26+ r6 k) |! e( b! q6 f& w( W6 Y
patients, most had been treated with high dose Gleevec.
* V9 M( B" S$ H! e3 D' t) `2 ]4 I4 d
"All patients discontinued therapy in CML-CP, all in CCyR, of them, 17
- i1 a5 a2 b7 c- @4 n7 T(65%) had undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR.' T; c$ n2 s5 ^" c" G1 i6 f
The median duration of CMR before TKI cessation was 62 mos, (0- 118)./ ]% b( \8 ~2 g2 B% B+ W1 h
The median duration of total TKI therapy was 101 mos (3- 135).", {, J9 V5 q; W0 x) }
5 @8 E$ Y- A9 A# h3 ]1 V3 P9 x# jTherefore, the median time in CMR before discontinuation was about 5
1 Q4 V. D! g3 g0 `- }* [years. The median follow-up is only 11 months. The median time for
$ M3 u1 j/ m+ f3 F" ]molecular relapse of 8 patients who had been in CMR was 4 months and
: R% f4 n" `1 P, sthey relapsed with median PCR value of 0.01 on the International Scale.$ q5 m" Q3 R6 K' d+ D9 a
7 N' Y8 i5 ^2 Y& ]% a" b, e
Of the 7 patients who discontinued when in MMR, 4 remained in MMR at a
, I+ H0 `2 _- a! Pmedian follow-up of 21 months, 1 remained in CCR, 1 in active disease
) K3 y8 G- Q7 Iand 1 transformed to accelerated phase off drugs. Therefore, from this5 w8 x7 T b9 }/ s" e
data, scarce as it is, there is a risk of transformation to advanced) b0 w( T- ]# @9 D4 I
disease if one discontinues drugs in MMR.
- x' J( b: G! G# `0 `: Q I! d& n
" X- j. Y1 K a: r+ |+ e% z2 patients were PCRU (4.5 log machine) and these patients relapsed
; d9 X' j, S/ v; kinto MMR when drugs were discontinued.
: d. X1 `+ s' W! v" J# K$ A
& ]( _: L! g* e; qSeven pts with relapse were treated again with TKI, 3 with nilotinib,
* j. I2 J+ C1 W7 S2 with dasatinib, and one each with imatinib and bosutinib (the latter
/ m" N% a. R; ? j: U& k* {; Sin AP). After a median of 13 months on therapy (range 4-52) all patients9 [! n. x" T$ \
improved their response, 5 with CMR and 2 MMR (including the pt that had
6 h2 ?4 D2 B4 Qtransformed to AP). They do not say why all patients were not retreated
$ N) G: W2 B. Twith imatinib and had to take Nilotinib and Dasatinib. Also, note that
1 o. N( E- v- `6 ?; x/ Vone did not regain CMR at the 13th month mark though it is good news* b! Y: H% R- L$ p9 W* z
that 5 did. It may take some time to regain CMR for some who have gone
' _" s9 C# v0 y% s3 r: J* w* \off drugs and relapsed. However, from our own list experiences, some& d) e* l7 u! ~- Y7 _: o6 ?
had regained CMR fast when they retook the TKI.& U+ E' b! Q0 b8 C6 s% n7 ]% v- g
$ V; y, O$ M" G
The doctors conclude that treatment discontinuation is experimental
8 Z) \$ Q" ?5 \6 ?# g8 Aand cannot be recommended at this stage as a standard procedure.
1 W& i& j( N* N: {8 n% \/ T7 V$ V! J# z7 j& w
Best Wishes,
# F* V9 M, u) l; ^5 d& i; n+ ?1 ^/ h) @, |) W! b
Anjana
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3783 Patient (Pt)-Driven Discontinuation of Tyrosine Kinase Inhibitor
8 i. Z5 ^- n* W. m4 v" kTheray in Chronic Phase Chronic Myeloid Leukemia (CML) - Single
& x* w7 O0 d& I' e; A/ WInstitution Experience
; W2 ~1 d& x ]4 J; Z2 @Program: Oral and Poster Abstracts
' E/ Z5 v; g7 ~7 A( J" \Session: 632. Chronic Myeloid Leukemia - Therapy: Poster III& `6 ?# m$ L O% `0 X) Z5 X/ p
# v$ k# X5 w5 G+ ]0 W# }Monday, December 10, 2012, 6:00 PM-8:00 PM( ]7 T/ e3 p- v( Q8 P( [
& ]) i! U6 l7 g! E. ?+ H
Hall B1-B2, Level 1, Building B (Georgia World Congress Center)
8 H5 [! T5 ~8 I4 r4 l+ T7 ]7 d3 r
Ohad Benjamini, MD1*, Hagop M. Kantarjian, MD1*, Mary Beth Rios, RN1,
. A) F$ ^7 C. H/ s7 ~7 mElias Jabbour, MD2*, Susan O'Brien, M.D.1, Preetesh Jain, MD, DM, PhD1*,
) C ]' c( o* u% CStefan Faderl, MD1, Guillermo Garcia-Manero, MD1*, Farhad Ravandi, MD1,. y; c0 S; d* I/ M% r
Gautam Borthakur, M.D.1, Alfonso Quint醩-Cardama, MD1* and Jorge E.4 D7 L/ X! Q. c. ~; G
Cortes, MD1$ d6 v, [0 |8 t+ `! L
4 P2 @# u8 G0 l$ U9 G; {+ q7 W1Department of Leukemia, The University of Texas MD Anderson Cancer9 X3 H; K E5 [6 g; V
Center, Houston, TX( _" I1 Q( W3 x& E: f1 M
2Department of Leukemia, The University of Texas M.D. Anderson Cancer2 m4 |8 d+ D( m5 i) g; f0 ?
Center, Houston, TX' A9 c# L D& v8 u; Z g
; \9 F/ W# h L% T+ CIntroduction: Some recent studies have reported on the outcome of CML
. B& I8 B$ _4 {5 t/ y' ppts who discontinued thyrosin kinase inhibitors (TKI) after achieving7 ^" u, T( s0 r& }5 D# L
sustained undetectable bcr-abl transcript level. Most patients who stop
% M$ t% U) C! NTKI have experienced molecular relapse. Most patients respond after) L3 a7 G! g$ [
resuming TKIs regaining undetectable bcr-abl transcript levels. These
) L% a1 d/ B$ G* p* oseries have prospectively planned treatment discontinuation and included
6 R! H5 w$ c& f, Uonly pts that have sustained complete molecular response (CMR) for at4 n4 A3 D4 u, r; k& a( M. H
least 2 yrs. However, in many instances pts may want to discontinue TKIs
! N& D, }* D* [5 I' l+ Xnot in CMR. Various reasons may lead patients to discontinue TKI
/ G6 [* ]3 Z* T$ Gtreatment unexpectedly, among them severe adverse effects, pregnancy or: U6 j/ V5 d7 |- b
economic constraints. This single institution experience reflects the
$ F' r$ x4 [7 `heterogeneous nature of pt-driven TKI discontinuation.( X3 K! @) {! i; r& ~7 `
: d9 _* _0 ^( Y3 B9 z0 ^Aim: To characterize the outcome and profile of CML pts who chose to
2 M" p$ x8 u, |, s- K# b. ddiscontinue TKI therapy in a single center regardless of their initial
+ W/ Q/ X7 G1 M$ \response to TKI therapy., z3 F g+ L. {& R& }' T
, i( J8 c1 `" ^( E8 Z ]Methods:We retrospectively analyzed MDACC data on all patients with CML v( F$ w$ k8 r5 e+ g: o
that were treated with TKIs in our institution and discontinued therapy.$ a% {9 h5 i9 e/ E3 |- u. B
! G+ t5 n4 j4 q/ q/ K- F, BResults: A total of 26 patients with CML-CP managed at MDACC* l4 V+ a4 c& s3 K6 l# D, }
discontinued TKI between 2003 and 2012. The total median follow up time
$ V& }8 X; ?6 v0 r' S rsince diagnosis was more than 120 months (mos) (range, 45 mos to 304. s) b6 Q5 J; Z0 b" s
mos). The median age at diagnosis was 48 yrs (range, 28-73); 15 pts were
* @3 a1 ~9 Z4 [0 L4 ]female. All pts had been diagnosed and treated in chronic phase.
' @ E5 S# b% i; q/ `+ t7 T! zInterferon was initial therapy in 11 pts (42%) and 15 pts received TKI
. s, o" \/ K7 @% z% X- mas initial therapy (4 received imatinib 400mg/day, 10 imatinib2 }! h2 @( }+ O# S
600-800mg/day, and 1 bosutinib.) Of the 11 pts initially treated with
1 B0 C* k7 f2 Y" s+ E2 [IFN, 7 then received imatinib 400mg and 4 imatinib 800mg upon IFN
5 M0 w# k+ B. g2 ?; }5 dfailure. Pts treated frontline with TKI started therapy within a median
1 r# @' Z8 A9 }# U# Xof 0.8 mos from diagnosis (range 0 to 4) and those with previous9 m0 U# b) o, ]+ g- i" `9 n0 v
interferon (n=11) after a median of 60 mos from diagnosis (31 to 164
) t9 |1 }0 f- M# ]5 U6 }! C9 \mos). Before TKI discontinuation 21pts (81%) were receiving their first
) L6 Q' z+ q/ FTKI and 5 (19%) were receiving 2nd (4) or 3rd line (1) TKI. Complete
. Z4 T2 R" N+ Q ^cytogenetic response (CCyR) had been achieved in all 26 pts at a median a3 x, Y7 A x( E+ F% M
of 3.5 mos (3-93); Major molecular response (MMR) in all at a median of
% J# P( X3 b# S% A# B) h9 mos (3-73) and CMR in 17 (65%) at a median of 22 mos (9-120). All2 w! D# {- z3 D! |5 d
patients discontinued therapy in CML-CP, all in CCyR, of them, 17 (65%)
" V8 Q/ l& c! L: ^had undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR. The
( r5 b0 H W# B" [: V) @! _7 T! Amedian duration of CMR before TKI cessation was 62 mos, (0- 118). The
, G3 @% i! x$ S8 u& B' Kmedian duration of total TKI therapy was 101 mos (3- 135)./ n' Y* E# e, P: }& F9 ^9 Z/ k
+ L" D: i5 Q$ T$ O, uFourteen pts (54%) discontinued TKI due to adverse events, 2 pts! I7 A9 k) \. j+ u @& B
discontinued to become pregnant, 5 decided to stop after long CMR, and 5 r, V. ~- ?' s/ h* z/ I% \
pts discontinued for financial reasons. After TKI discontinuation( s& V& O; H$ L; ^: ^5 @8 B
patients were followed for a median of 11 mos (5-131). Among pts with) a2 ?8 I/ g* a0 \" b
CMR at discontinuation, molecular relapse occurred in 8 (47%) pts at a
, Q- q( a! m/ q8 B, T. o% amedian of 4 mos (1-11) from discontinuation with median transcript level4 B& x( T+ u# ?3 Z# z$ F
at relapse of 0.07 (IS) (range, 0.004-2.17). Six pts with initial INF
$ l% C# ]. W, f |therapy had CMR at time of TKI discontinuation, 50% of them relapsed.
# p# J& ]' L2 q9 b) b: o* z" h. ?6 jAmong 7 pts who discontinued therapy in MMR, after a median follow-up
7 b, H. K1 C8 j# O" _3 ~! Sfrom discontinuation of 21.6 months (range, 4.6-106), 4 remained at MMR,
* `- Q! W" L. h" ~7 v; S: gone has minor CyR and one CCyR without retreatment at last follow up
2 n9 R+ R' K9 |after 78 and 105 months from TKI discontinuation, and one transformed to
* F* g, |7 e. I ^2 H7 h( [$ A$ taccelerated phase (AP). The 2 pts with MR4.5at discontinuation relapsed
% S: [* T% _0 `( c5 R# z$ `to MMR. Three pts had a transient molecular recurrence with spontaneous
) a2 x2 b( ?# \8 qre-gain of CMR. Seven pts with relapse were treated again with TKI, 3
( Y2 \8 H( [% H: s7 o5 ]1 A1 U+ lwith nilotinib, 2 with dasatinib, and one each with imatinib and% }. O( ?3 g- P; L5 w$ O
bosutinib (the later in AP). After a median of 13 months on therapy
; \$ o1 ?9 p' H/ o! H3 i, y(range 4-52) all patients improved their response, 5 with CMR and 2 MMR
! j" F7 I7 A) R; D' `* \* A(including the pt that had transformed to AP). There were no deaths or4 N* o7 r4 v! ]! L
transformations to blastic phase of CML. At last follow up 14 (54%) pts
2 T/ e# [3 t( G* R: k7 _5 pwere in CMR, 5 (19%) in MMR,5 (19%) in CCyR and 1 each in minor CyR and. r& u8 Y$ k' w w# o, s
PCyR.$ x+ N3 Q# Q! \/ l# b
- V# v4 L" R( Q% @9 V0 u a
Conclusion: Pt-driven TKI discontinuation in CML-CP leads to molecular6 ~( N* r5 @. [* T
relapse in nearly half of the pts who discontinue therapy in CMR. Some2 V6 p; O$ M( }. W( _, w
pts who discontinue in MMR may have sustained MMR. Treatment# K& Z! e% J# U0 Z1 q
discontinuation should be considered experimental and cannot be+ ~6 F, U- g( z' l' C9 S+ T
recommended to pts as a standard approach.. c |$ }' l, ?
6 G# g* h/ i) l% O+ RDisclosures: Ravandi: BMS: Honoraria, Research Funding. |
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