MDACC has, for the first time, given their experience of TKI
) M# N0 }9 _4 T; }discontinuation. The doctors at MDACC look at 26 patients who T2 r \4 N0 L0 R0 e
discontinued therapy from 2003-2012 for various reasons. These reasons
* e% A5 q# s% k, ]$ B! Zinclude long time in CMR, adverse side-effects, pregnancy and financial
/ \, R; R3 ^0 n+ uconstraints. Please note that 17 patients discontinued therapy in CMR w3 H t D. o t6 `+ t$ `9 {" W
and the rest in MMR. Of the patients in CMR who discontinued therapy,/ Q1 Y" s! O3 z& x7 y _2 E& j) k
47% had molecular relapse. Those in CMR who discontinued and had taken
+ E# J- s& y4 k1 {* ]7 Pprior Interferon to a TKI, 50% relapsed. Also note that of these 26 n+ C: ?# h4 D+ B O: i g
patients, most had been treated with high dose Gleevec. j; f$ G6 ]4 | M e8 Z! E+ S
; `, ]7 ^+ n. o6 M5 h/ c( ["All patients discontinued therapy in CML-CP, all in CCyR, of them, 17, C1 v) u H/ I0 E
(65%) had undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR.- L8 C6 z+ A2 c: R( s3 M$ Q" @
The median duration of CMR before TKI cessation was 62 mos, (0- 118).
; x9 y( N) P& |4 w" n4 Q& iThe median duration of total TKI therapy was 101 mos (3- 135)."' _. ~# |2 M8 h) \/ K1 V8 Q
4 C. c v/ e) v5 z5 p) z! _Therefore, the median time in CMR before discontinuation was about 59 I P! {! X% R8 J& ^
years. The median follow-up is only 11 months. The median time for
/ b2 j7 p9 |3 D+ ^$ V+ u8 Qmolecular relapse of 8 patients who had been in CMR was 4 months and
7 i. p. |, u) s5 R; Qthey relapsed with median PCR value of 0.01 on the International Scale.
, \0 u# ] w& d' P* y$ L+ q
: p- K$ n5 K; h# E: GOf the 7 patients who discontinued when in MMR, 4 remained in MMR at a
5 j7 [8 k N8 P6 L/ g( Z" ymedian follow-up of 21 months, 1 remained in CCR, 1 in active disease
7 ?3 p( P8 @' vand 1 transformed to accelerated phase off drugs. Therefore, from this1 ?0 \2 C9 W. T$ g9 ^, s2 _
data, scarce as it is, there is a risk of transformation to advanced% E( [: q5 k% r' n
disease if one discontinues drugs in MMR.0 E' Q' }8 ^5 h
- g( F I8 ~/ Y
2 patients were PCRU (4.5 log machine) and these patients relapsed1 P/ T) }1 n2 I$ x. c
into MMR when drugs were discontinued.0 y: ~3 s) ^' w
& B$ K; E$ \* }4 w: d; X( M0 A# zSeven pts with relapse were treated again with TKI, 3 with nilotinib,
5 l4 B' Y+ q+ o. W+ E% A2 with dasatinib, and one each with imatinib and bosutinib (the latter* U( y5 C3 z1 c: u: `1 z
in AP). After a median of 13 months on therapy (range 4-52) all patients9 Q4 I/ B+ K: |" [# }
improved their response, 5 with CMR and 2 MMR (including the pt that had+ c V/ W$ V8 J a* J, s
transformed to AP). They do not say why all patients were not retreated/ J/ g7 ~# E) W
with imatinib and had to take Nilotinib and Dasatinib. Also, note that
: J4 f/ P8 N' Z# lone did not regain CMR at the 13th month mark though it is good news. Z5 |& S' g9 M. l/ _
that 5 did. It may take some time to regain CMR for some who have gone) {) H1 L# U% x: o4 |; b/ W" y" X
off drugs and relapsed. However, from our own list experiences, some$ R- ]" Z' j0 ]: v% X
had regained CMR fast when they retook the TKI.
$ q- G, I+ M* z6 y. S8 m3 z3 Q1 G; _7 T! ~
The doctors conclude that treatment discontinuation is experimental9 n3 Y& T7 Y8 T" s& ?
and cannot be recommended at this stage as a standard procedure.8 [+ Y7 a# G: E7 x) E2 b% q
- {" B" ]' }3 B6 h. Y- H
Best Wishes,
# i s& I- ^% q" u7 w! o* R L- |) E; e+ C* R* M
Anjana5 L4 g* G5 ^8 M4 n2 ]
( c, K1 i. X4 C9 L, g6 Q4 P, z# z1 @, e& O; Z; g
) n% X( M# v H5 W( I2 L( y- s
/ `) y2 K" @! c" A* t+ t8 w7 _
1 |# l- C1 r. J3 R* C0 v; |8 F+ q7 e% o; C
4 m; r) O' s1 n# `9 r% v1 H
) D9 r3 @7 _% }5 [8 ?( F5 w6 z
5 B7 U( X6 O2 D
! I1 _2 K$ h8 L [2 A- U3783 Patient (Pt)-Driven Discontinuation of Tyrosine Kinase Inhibitor
4 _8 N3 o& x/ L! a/ J! b+ ZTheray in Chronic Phase Chronic Myeloid Leukemia (CML) - Single
; I8 X; E2 Z. \, E: CInstitution Experience
0 i1 l3 ?9 T" j7 f% M. \+ R: CProgram: Oral and Poster Abstracts
& L) m& N# ?, |Session: 632. Chronic Myeloid Leukemia - Therapy: Poster III! l* O1 X2 _. |% J
+ P: }- N) f5 t
Monday, December 10, 2012, 6:00 PM-8:00 PM
) ^; R2 H, W f3 t0 e1 Y; X8 `
Hall B1-B2, Level 1, Building B (Georgia World Congress Center): U9 U1 C4 R% d) y5 @
1 h6 B U3 p' ]9 i0 {# T6 C
Ohad Benjamini, MD1*, Hagop M. Kantarjian, MD1*, Mary Beth Rios, RN1,
/ t) @3 ]/ U( A* [% M6 |Elias Jabbour, MD2*, Susan O'Brien, M.D.1, Preetesh Jain, MD, DM, PhD1*,
( ?5 D2 s+ _; f, G. XStefan Faderl, MD1, Guillermo Garcia-Manero, MD1*, Farhad Ravandi, MD1,( u, K( ~% T L9 ^
Gautam Borthakur, M.D.1, Alfonso Quint醩-Cardama, MD1* and Jorge E.
$ u; W( a9 Q# T6 i1 G( _Cortes, MD1: Y5 t) w1 `7 B/ b* D% |9 }0 Y" s
3 ~+ m9 L- m8 z8 c+ m, x- N. j
1Department of Leukemia, The University of Texas MD Anderson Cancer+ M! F$ k7 E* n2 ~8 R
Center, Houston, TX/ q. n$ B2 [0 [) m# ^8 M K- g/ A
2Department of Leukemia, The University of Texas M.D. Anderson Cancer' s. d8 | y2 {6 N7 ~
Center, Houston, TX- o+ z5 K: |: x5 Z# M, \3 m! S
- ]% {8 i3 Q2 b1 I2 ~Introduction: Some recent studies have reported on the outcome of CML
; l/ n! p. W/ x. z2 M. _pts who discontinued thyrosin kinase inhibitors (TKI) after achieving, ]2 m; N- D0 F, r+ O+ B: q! f
sustained undetectable bcr-abl transcript level. Most patients who stop
" W8 W: C6 E( g$ n2 ~; _/ M, }. NTKI have experienced molecular relapse. Most patients respond after# F" d. `% u$ d r- }0 i
resuming TKIs regaining undetectable bcr-abl transcript levels. These* s, B0 N8 X0 H0 e
series have prospectively planned treatment discontinuation and included- { T! ~5 r: q7 E: R
only pts that have sustained complete molecular response (CMR) for at1 p8 ]3 W) y# s/ N" Z; f
least 2 yrs. However, in many instances pts may want to discontinue TKIs; q; H$ B. p: w( P* i8 o
not in CMR. Various reasons may lead patients to discontinue TKI
4 U3 l3 w. \% ?" Ctreatment unexpectedly, among them severe adverse effects, pregnancy or
/ y; h8 J6 W9 u, K; J1 y4 Z. ceconomic constraints. This single institution experience reflects the# F; d, O0 Y; }- c* x
heterogeneous nature of pt-driven TKI discontinuation.; n+ u3 d- Z: g' D
2 O; C! R! H8 A; _& d. {' m
Aim: To characterize the outcome and profile of CML pts who chose to
- f% Y S# \9 [4 ~$ u) i+ `discontinue TKI therapy in a single center regardless of their initial
5 j+ e2 R- Q8 p/ _4 K4 Fresponse to TKI therapy.
$ Q% `) @; F3 s$ l
: D8 r* u1 F6 o) N7 Z9 x8 ~$ ]Methods:We retrospectively analyzed MDACC data on all patients with CML
8 U* ^+ J& K a4 Zthat were treated with TKIs in our institution and discontinued therapy.
( M) n/ P6 Q. b2 _/ N3 w) m
3 e+ t; O. J7 {9 g) SResults: A total of 26 patients with CML-CP managed at MDACC7 v( o6 f1 Z& I# z
discontinued TKI between 2003 and 2012. The total median follow up time0 e- J6 Z: l; S W* X$ N1 c/ `; H
since diagnosis was more than 120 months (mos) (range, 45 mos to 304
" w, \+ V* p# c4 h) gmos). The median age at diagnosis was 48 yrs (range, 28-73); 15 pts were9 `2 s0 V( ]. } `: @
female. All pts had been diagnosed and treated in chronic phase.! j; ?% [ e! K- b
Interferon was initial therapy in 11 pts (42%) and 15 pts received TKI5 [1 G4 q' i; T5 o4 D
as initial therapy (4 received imatinib 400mg/day, 10 imatinib
+ g/ i& u$ O" ]5 J600-800mg/day, and 1 bosutinib.) Of the 11 pts initially treated with
" }$ y8 Z9 ^5 x- \7 y: `: G( iIFN, 7 then received imatinib 400mg and 4 imatinib 800mg upon IFN
' x$ A) Y) o) Afailure. Pts treated frontline with TKI started therapy within a median
, P" D0 x& h: A& W6 E ~6 ?$ hof 0.8 mos from diagnosis (range 0 to 4) and those with previous2 F+ i2 h( E" U9 Q
interferon (n=11) after a median of 60 mos from diagnosis (31 to 164+ Z$ k0 ~% t {9 D5 m# v' q1 Y5 ?% Y
mos). Before TKI discontinuation 21pts (81%) were receiving their first8 o7 @8 ?5 Z* \+ K- n) c
TKI and 5 (19%) were receiving 2nd (4) or 3rd line (1) TKI. Complete
! Q3 c0 B, S. Q# V1 Zcytogenetic response (CCyR) had been achieved in all 26 pts at a median4 f5 m$ \' D3 z5 @" _
of 3.5 mos (3-93); Major molecular response (MMR) in all at a median of" S, r) ]( l* R" b9 K' x
9 mos (3-73) and CMR in 17 (65%) at a median of 22 mos (9-120). All5 b" j: I+ J; s9 S0 s; }
patients discontinued therapy in CML-CP, all in CCyR, of them, 17 (65%)8 O7 S' E( b; f8 D
had undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR. The
9 ^3 e! n" Z( Y% D# c" D5 p. Xmedian duration of CMR before TKI cessation was 62 mos, (0- 118). The
$ P* R- x7 \4 j( N& emedian duration of total TKI therapy was 101 mos (3- 135).5 V( N( c( E3 J( a1 K# Y7 Z) H
/ r; r% g" o& M( m4 J1 m
Fourteen pts (54%) discontinued TKI due to adverse events, 2 pts
5 o1 {9 [! i8 E5 qdiscontinued to become pregnant, 5 decided to stop after long CMR, and 54 h' t4 e4 @3 Y8 c* j7 u) O
pts discontinued for financial reasons. After TKI discontinuation# c# P0 n9 ~ s, V5 B5 o: i; g5 R
patients were followed for a median of 11 mos (5-131). Among pts with( S: Y9 U z0 x
CMR at discontinuation, molecular relapse occurred in 8 (47%) pts at a8 I1 n+ @1 `7 Z+ Y% h5 D8 W
median of 4 mos (1-11) from discontinuation with median transcript level: O( I: h5 j$ \$ \, P3 ~
at relapse of 0.07 (IS) (range, 0.004-2.17). Six pts with initial INF
, f6 E) n5 ?; c4 l6 \( atherapy had CMR at time of TKI discontinuation, 50% of them relapsed.9 f& N9 r; J. [1 t& ]
Among 7 pts who discontinued therapy in MMR, after a median follow-up
+ g. a8 y* |6 R v. ?/ y) _, mfrom discontinuation of 21.6 months (range, 4.6-106), 4 remained at MMR,
: u" R m$ J* W1 U" F. }one has minor CyR and one CCyR without retreatment at last follow up( X# @7 R4 ?% w) ^# L
after 78 and 105 months from TKI discontinuation, and one transformed to7 N; T' k! |$ R* S5 J, P7 c8 ]4 b5 H
accelerated phase (AP). The 2 pts with MR4.5at discontinuation relapsed5 q* S3 s: o( N; ^
to MMR. Three pts had a transient molecular recurrence with spontaneous
$ S5 p0 i% B$ H. gre-gain of CMR. Seven pts with relapse were treated again with TKI, 34 b2 K$ K! n6 g- l2 _0 u
with nilotinib, 2 with dasatinib, and one each with imatinib and( A8 m ~0 q: h/ G" A+ g/ W
bosutinib (the later in AP). After a median of 13 months on therapy: z9 F* m. Z& O# n$ `! ?
(range 4-52) all patients improved their response, 5 with CMR and 2 MMR0 A5 ]/ }7 O; E4 Y
(including the pt that had transformed to AP). There were no deaths or
- X T* G2 \; C" ~/ E) e0 Atransformations to blastic phase of CML. At last follow up 14 (54%) pts
; F# g- V8 O7 M' Q- U! Swere in CMR, 5 (19%) in MMR,5 (19%) in CCyR and 1 each in minor CyR and f7 ?' ^; k4 y1 M5 z3 L$ ]
PCyR.# L' O0 x1 w2 t0 p% K2 X
& ]" U9 R K0 z9 j' V- C
Conclusion: Pt-driven TKI discontinuation in CML-CP leads to molecular
3 Y0 t0 a! z6 b! F" J5 ] hrelapse in nearly half of the pts who discontinue therapy in CMR. Some
' ]' i' ]+ c. Z lpts who discontinue in MMR may have sustained MMR. Treatment
& J2 i2 k/ r1 C( mdiscontinuation should be considered experimental and cannot be3 B" n% S/ D+ }
recommended to pts as a standard approach.5 o: t4 W8 C% ^7 S3 K9 t
( R6 ?, I; ^3 ~, r- x
Disclosures: Ravandi: BMS: Honoraria, Research Funding. |
这是耐药了吗?
2024年8月份确诊肺腺癌四期,开始卡铂+培美曲塞+特瑞普利治疗6次,期间每两次治疗后复
发现肿瘤源头突变IDH1,助力患者生存
胆管癌被称为“小癌王“ ,恶性程度极高,早期胆管癌以手术为主,但术后一年内复发率
胆管癌国内第一款靶向药佩米替尼已上
佩米替尼二线治疗胆管癌FGFR融合或重排患者中位生存期21.1个月应答患者31.1个月,国内
好好吃饭能延长56个月生存期?肿瘤患
作者:小莱
现代医学之父希波克拉底曾说:“食物是最好的药品”。对于癌症患者来说,
一线直接吃伏美替尼,如何延长耐药?
2024年9月确诊肺腺癌,4a期,基因检测结果如下图,确诊后听医生的直接吃三代药伏美了
提升卡
置顶卡
沉默卡
喧嚣卡
变色卡
千斤顶
显身卡
