MDACC has, for the first time, given their experience of TKI* D' {) U3 M. i9 H5 b
discontinuation. The doctors at MDACC look at 26 patients who
- H8 h& ^# A5 j2 Q/ W: L3 idiscontinued therapy from 2003-2012 for various reasons. These reasons
" N X, A" P! Binclude long time in CMR, adverse side-effects, pregnancy and financial
8 [8 c/ p3 F' m) T3 lconstraints. Please note that 17 patients discontinued therapy in CMR$ r6 w, a3 N$ W$ H' Y Z" r
and the rest in MMR. Of the patients in CMR who discontinued therapy,- P' w( r2 a: F+ M. k* z# s w
47% had molecular relapse. Those in CMR who discontinued and had taken* k8 G7 }0 F+ h
prior Interferon to a TKI, 50% relapsed. Also note that of these 26
0 G8 }& S/ X, P k$ P: Y( dpatients, most had been treated with high dose Gleevec.
5 s2 i7 [4 Y' g4 M( x) j- X& L9 c( [
"All patients discontinued therapy in CML-CP, all in CCyR, of them, 178 p- s" ~) W6 H
(65%) had undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR.0 H: U f7 D! N
The median duration of CMR before TKI cessation was 62 mos, (0- 118).
' G4 s2 s, ~" x; e& fThe median duration of total TKI therapy was 101 mos (3- 135)."9 u, z0 Z ~5 B; ]; i1 x
3 {7 y. f0 @9 }
Therefore, the median time in CMR before discontinuation was about 5
! k; s% b+ b! L/ Wyears. The median follow-up is only 11 months. The median time for, ^/ r) h+ V& ?0 l [
molecular relapse of 8 patients who had been in CMR was 4 months and. v: a& Z# P8 i' i
they relapsed with median PCR value of 0.01 on the International Scale.
' W: ^9 Y* C/ b9 i; Q
3 a5 M3 K" ?' I: p2 ^* T8 r% ^Of the 7 patients who discontinued when in MMR, 4 remained in MMR at a
) Q5 x' L8 i) jmedian follow-up of 21 months, 1 remained in CCR, 1 in active disease" T p1 y1 @) ?' i: s
and 1 transformed to accelerated phase off drugs. Therefore, from this9 G' G9 e; Q" w, m' [
data, scarce as it is, there is a risk of transformation to advanced
n. u4 m% m2 z. o4 T8 [4 p5 ]- Y9 cdisease if one discontinues drugs in MMR.& i5 p: T1 ?1 v! \$ g# f3 n# }& x1 N
. ]* p% ~' X6 M3 l2 E0 u- C! w
2 patients were PCRU (4.5 log machine) and these patients relapsed
0 O% d) ~0 [( N" q; d/ Ginto MMR when drugs were discontinued., t; N7 X- L- Q0 D1 J7 E
, Y# m) b4 I k5 I$ Z
Seven pts with relapse were treated again with TKI, 3 with nilotinib,
; A1 w3 k9 w' v2 with dasatinib, and one each with imatinib and bosutinib (the latter
" P: i9 J. M3 e' a" kin AP). After a median of 13 months on therapy (range 4-52) all patients& Z8 W1 m3 [; w
improved their response, 5 with CMR and 2 MMR (including the pt that had
* h+ R' Y: F8 n( f! Ytransformed to AP). They do not say why all patients were not retreated
$ ?) k$ _2 T( O# J( Ywith imatinib and had to take Nilotinib and Dasatinib. Also, note that9 I% L5 V/ R7 F' E- J1 I: R5 L. D
one did not regain CMR at the 13th month mark though it is good news
$ E1 U4 b; B" ^* s+ L6 P' a0 Bthat 5 did. It may take some time to regain CMR for some who have gone
) X9 h$ a6 v5 B0 [( x) o8 P& i; koff drugs and relapsed. However, from our own list experiences, some3 Z: r! Q/ q7 ]6 n a1 } P
had regained CMR fast when they retook the TKI.
1 A2 x6 t+ e! C. K% g% W: I* B% @+ T) Z- f
The doctors conclude that treatment discontinuation is experimental8 S( ^1 ~+ d; D4 v+ M* ~# q0 g
and cannot be recommended at this stage as a standard procedure.
# _# U$ ?. V" d z; B. }( }2 J v$ J% t2 G0 j
Best Wishes,7 a0 S: i# x" a) _7 _
' D( Q. }! q7 c3 w) r; B8 R4 V4 l
Anjana7 p+ {# o0 [. N) L0 U
9 {4 o6 S+ n& B V
# V! @* [6 b6 f1 a- J' @) ~2 ?/ \$ D1 F8 N2 K
" H0 X8 M- E2 Q6 |9 Q. D6 T2 ] d; e$ S2 _ j! g: f, o( P4 W
3 c" ^8 [8 z9 H8 w. N1 t
% A5 Z% ]; {+ { @+ `- c4 a5 I) G0 S- k) v9 H0 a0 o( D
" V& E( B+ S- G! g
3 s s7 h* P& K2 }
3783 Patient (Pt)-Driven Discontinuation of Tyrosine Kinase Inhibitor5 O- @7 t4 l0 E
Theray in Chronic Phase Chronic Myeloid Leukemia (CML) - Single
0 z4 O2 J4 @4 PInstitution Experience. B, e) X; U$ j+ f8 a$ c$ e
Program: Oral and Poster Abstracts
, x8 \- l( v; Z3 M JSession: 632. Chronic Myeloid Leukemia - Therapy: Poster III* ?/ G* |3 n) J/ O: { e
0 E# R f3 ?3 W) ^Monday, December 10, 2012, 6:00 PM-8:00 PM
; t) n9 K# } [, K' i
1 ? q% ]$ n$ yHall B1-B2, Level 1, Building B (Georgia World Congress Center)/ ]3 O4 K3 ~- _' \$ B
* @8 u4 Y' `' {' s3 @: ]+ OOhad Benjamini, MD1*, Hagop M. Kantarjian, MD1*, Mary Beth Rios, RN1,3 Y# `' R+ K: }# w" P6 E$ l1 b
Elias Jabbour, MD2*, Susan O'Brien, M.D.1, Preetesh Jain, MD, DM, PhD1*,( T7 Q4 K, K3 L9 Y4 F7 B4 ~
Stefan Faderl, MD1, Guillermo Garcia-Manero, MD1*, Farhad Ravandi, MD1,4 E0 M% V$ N+ Z9 u+ U+ |7 B
Gautam Borthakur, M.D.1, Alfonso Quint醩-Cardama, MD1* and Jorge E., I3 _& {" d, x6 ?( e: |3 m
Cortes, MD18 Z2 N; |0 g. M. X
0 U' D5 F' }$ S2 e/ B6 T1Department of Leukemia, The University of Texas MD Anderson Cancer9 D, ~0 @& {4 T7 Z
Center, Houston, TX
9 [1 e6 T8 M- K$ M: o! ~+ V* t- D2Department of Leukemia, The University of Texas M.D. Anderson Cancer8 p/ C, M8 ^! F, O
Center, Houston, TX7 D) `4 }. Q [9 B% ?5 C7 j' W
2 D+ Q* c: Z) S3 j2 G7 TIntroduction: Some recent studies have reported on the outcome of CML$ s9 ]' B% s! a
pts who discontinued thyrosin kinase inhibitors (TKI) after achieving$ K. i) j7 R* S2 i; X
sustained undetectable bcr-abl transcript level. Most patients who stop) c% o2 D) b7 P% _8 i
TKI have experienced molecular relapse. Most patients respond after5 P0 r G+ c) a) y5 k9 j
resuming TKIs regaining undetectable bcr-abl transcript levels. These
$ F j4 u8 C$ E, tseries have prospectively planned treatment discontinuation and included3 \0 I' z5 g: B0 Y. A! b
only pts that have sustained complete molecular response (CMR) for at2 I7 d) e: G3 ]" j* l( h# f
least 2 yrs. However, in many instances pts may want to discontinue TKIs
/ o0 I; g' ^1 r Hnot in CMR. Various reasons may lead patients to discontinue TKI
: P6 e3 w. h5 {treatment unexpectedly, among them severe adverse effects, pregnancy or
7 z7 h; |2 V8 Q& k+ I/ reconomic constraints. This single institution experience reflects the' o# G1 |" Q0 [0 a
heterogeneous nature of pt-driven TKI discontinuation.
' X; w: i! ]# v1 w
$ D9 K6 o2 j2 g4 N0 B& kAim: To characterize the outcome and profile of CML pts who chose to
8 d5 z: {8 S; i/ |5 Jdiscontinue TKI therapy in a single center regardless of their initial
8 F8 L C+ Z. {6 }* Z/ Eresponse to TKI therapy.& U1 t4 s: W6 d9 C
' K' _4 ~5 h' G" B! H' HMethods:We retrospectively analyzed MDACC data on all patients with CML
" @" @) Q2 W' r9 pthat were treated with TKIs in our institution and discontinued therapy. P6 B4 _) P; m+ M) I
; W S: c# F5 m' Z, R/ W; |" T4 m: r# d
Results: A total of 26 patients with CML-CP managed at MDACC
* w2 v$ @3 F* x. r0 |/ [discontinued TKI between 2003 and 2012. The total median follow up time
. i! D% D* M7 t0 r# b" ysince diagnosis was more than 120 months (mos) (range, 45 mos to 304
; x' s) f1 J9 H- a( W- `4 ^mos). The median age at diagnosis was 48 yrs (range, 28-73); 15 pts were
, b6 X: x; h7 j4 l, sfemale. All pts had been diagnosed and treated in chronic phase.% M* l% a! C& [; m$ r4 W. B6 N
Interferon was initial therapy in 11 pts (42%) and 15 pts received TKI
1 L, t& T% S' [$ {7 W- o( ]( Oas initial therapy (4 received imatinib 400mg/day, 10 imatinib
! ~- Z) j0 o* i2 m, Y600-800mg/day, and 1 bosutinib.) Of the 11 pts initially treated with) `! t! a8 P4 t6 e. h" }% Z& z
IFN, 7 then received imatinib 400mg and 4 imatinib 800mg upon IFN1 x+ m0 R8 g+ g! F2 k
failure. Pts treated frontline with TKI started therapy within a median
7 y& @! W& b7 D6 b E$ _6 I0 Pof 0.8 mos from diagnosis (range 0 to 4) and those with previous
) o& ~- ? f4 [$ }interferon (n=11) after a median of 60 mos from diagnosis (31 to 164
) y% L6 D' R2 {( |mos). Before TKI discontinuation 21pts (81%) were receiving their first
, Z6 t( }! u' f# [$ E3 j# ITKI and 5 (19%) were receiving 2nd (4) or 3rd line (1) TKI. Complete
8 B0 F- g+ X$ m0 |$ z \$ y( Ccytogenetic response (CCyR) had been achieved in all 26 pts at a median5 D+ B6 |- p9 P8 P+ z' v! P. i
of 3.5 mos (3-93); Major molecular response (MMR) in all at a median of
1 ^# S' ]2 C1 n, E& L! m0 D9 mos (3-73) and CMR in 17 (65%) at a median of 22 mos (9-120). All
8 v/ V, s/ }4 l$ ~5 `patients discontinued therapy in CML-CP, all in CCyR, of them, 17 (65%)9 L3 ?1 \; Z/ Z9 O) l
had undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR. The# H! {8 I8 \7 b8 m; |$ O
median duration of CMR before TKI cessation was 62 mos, (0- 118). The: R) K' h9 w- B8 @5 t5 t
median duration of total TKI therapy was 101 mos (3- 135).
1 S0 a( c" [' m- P" @( Z' ?
$ c3 v9 S# \- b! A. Q/ b/ ZFourteen pts (54%) discontinued TKI due to adverse events, 2 pts6 }; X- D$ N9 \+ d7 m- w+ I/ D& Q
discontinued to become pregnant, 5 decided to stop after long CMR, and 5
! G% T$ K- u: p4 G# Z; upts discontinued for financial reasons. After TKI discontinuation5 {* o8 x' [* H" r
patients were followed for a median of 11 mos (5-131). Among pts with
9 R0 N8 Y& [" W J. i$ WCMR at discontinuation, molecular relapse occurred in 8 (47%) pts at a' \! C4 P: |9 r) v+ |! O& S/ s3 E4 ?
median of 4 mos (1-11) from discontinuation with median transcript level
% z! b2 B: b9 ?6 rat relapse of 0.07 (IS) (range, 0.004-2.17). Six pts with initial INF
# r) u0 g! I! ] a( X3 W. V- @therapy had CMR at time of TKI discontinuation, 50% of them relapsed.4 {6 H9 u l1 |+ H
Among 7 pts who discontinued therapy in MMR, after a median follow-up
4 p4 x( f" H4 e: z# t6 a3 kfrom discontinuation of 21.6 months (range, 4.6-106), 4 remained at MMR,6 s! `. h2 `, r3 A T
one has minor CyR and one CCyR without retreatment at last follow up/ ]* w( D, v# o
after 78 and 105 months from TKI discontinuation, and one transformed to
1 i) U: I) c6 L7 C- D; j9 Taccelerated phase (AP). The 2 pts with MR4.5at discontinuation relapsed
u& u. X7 ^/ @( u2 vto MMR. Three pts had a transient molecular recurrence with spontaneous
. T/ g' I" S2 m) Hre-gain of CMR. Seven pts with relapse were treated again with TKI, 3
+ D3 }$ J. v4 j" p6 c9 zwith nilotinib, 2 with dasatinib, and one each with imatinib and
* ?) L; h5 m2 n* O0 ~8 Qbosutinib (the later in AP). After a median of 13 months on therapy
1 y5 h' J) v9 a. X(range 4-52) all patients improved their response, 5 with CMR and 2 MMR
4 q7 K7 ~8 y) \" J+ j(including the pt that had transformed to AP). There were no deaths or
/ R( o! e/ Z: u7 mtransformations to blastic phase of CML. At last follow up 14 (54%) pts
8 g- P3 H. w9 D1 z9 P Cwere in CMR, 5 (19%) in MMR,5 (19%) in CCyR and 1 each in minor CyR and
4 l' l+ q4 C4 X1 B& f- `PCyR.
7 l# d2 }, H( V( v, ]; w. e u0 A; R$ ]. v- O6 N
Conclusion: Pt-driven TKI discontinuation in CML-CP leads to molecular0 G8 v/ k4 t" C0 o/ Q+ B k
relapse in nearly half of the pts who discontinue therapy in CMR. Some- T, S6 S* ^. j
pts who discontinue in MMR may have sustained MMR. Treatment0 k! O% s; f% f; P0 d
discontinuation should be considered experimental and cannot be' @2 K! \7 m! X0 A
recommended to pts as a standard approach.
6 i: [! P' o0 a3 E: W9 U. u5 A0 u0 L- f7 L9 d7 x$ H" V! U
Disclosures: Ravandi: BMS: Honoraria, Research Funding. |
EGFR突变肺癌治疗策略及进展研究——
EGFR突变肺癌治疗策略及进展研究——周斐教授讲座学习笔记
直播链接:
https://live.
即将4年,EGFR19+TP53+CDK4扩增+EGFR
母亲20年9月底确诊肺腺癌IV期,EGFR19突变,阿美31个月耐药—>化疗—>SBRT—>化疗
目
大病恢复,野生灵芝确证有效
分享一个良方,希望能帮助到有需要的人。姑妈和大舅妈都生过重病(这里不说是啥病了哈
EGFR罕见突变种类多,哪种靶向药治疗
作者:seacat
针对EGFR罕见突变(排除外显子20插入 Exon 20ins),目前获批的靶向药是
ADC药物如何狙击肺癌——2024.8.27董
ADC药物如何狙击肺癌——2024.8.27董晓荣教授直播笔记
直播链接:
https://live.yuaig
提升卡
置顶卡
沉默卡
喧嚣卡
变色卡
千斤顶
显身卡
