MDACC has, for the first time, given their experience of TKI0 P7 N. z5 ]7 x$ l% m# [
discontinuation. The doctors at MDACC look at 26 patients who+ N" |4 d, v6 s; r
discontinued therapy from 2003-2012 for various reasons. These reasons" y( v! {$ O( a! j e9 o
include long time in CMR, adverse side-effects, pregnancy and financial0 z% a" p X7 M' t2 D& [
constraints. Please note that 17 patients discontinued therapy in CMR# I7 j2 M2 s& B$ P. q
and the rest in MMR. Of the patients in CMR who discontinued therapy,4 R8 i. _$ |$ c8 b& a
47% had molecular relapse. Those in CMR who discontinued and had taken
/ ^& V% L% j! E1 G/ I+ aprior Interferon to a TKI, 50% relapsed. Also note that of these 26
8 ~: x( k1 N* O7 vpatients, most had been treated with high dose Gleevec.( h r5 B) q2 G/ [2 N7 u
! n5 P; J6 Z6 f7 h/ j6 i+ b
"All patients discontinued therapy in CML-CP, all in CCyR, of them, 177 Z1 q: ?* T7 S, v4 ]
(65%) had undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR.
) U* f2 \$ d: m' F" r) T7 p3 vThe median duration of CMR before TKI cessation was 62 mos, (0- 118).
: g! u& ^- n& ?6 h; T6 H4 i( eThe median duration of total TKI therapy was 101 mos (3- 135)."
- f% a" d7 M. L' U$ S* s' V5 A p/ m5 f7 z
Therefore, the median time in CMR before discontinuation was about 5
b) R" r# }# h# ^- N* u! {years. The median follow-up is only 11 months. The median time for1 G/ d% f- g3 @/ S' l! p2 a6 q
molecular relapse of 8 patients who had been in CMR was 4 months and
! p3 s( B5 j! J$ l' o% x, hthey relapsed with median PCR value of 0.01 on the International Scale.; Q1 Y+ {* ~% u7 r, I
3 i s; \% ^' w3 a" P; }Of the 7 patients who discontinued when in MMR, 4 remained in MMR at a% F8 V3 G5 X5 }: c$ k" o! s- x# F
median follow-up of 21 months, 1 remained in CCR, 1 in active disease; z8 j" N' W' J. o3 P' s; Z! T3 h
and 1 transformed to accelerated phase off drugs. Therefore, from this
, s; C, o3 G, D# T/ I+ S* Xdata, scarce as it is, there is a risk of transformation to advanced/ f' _1 i& j& P/ \! T5 R! D2 \
disease if one discontinues drugs in MMR.5 G' \2 i3 G% J5 ]4 D% K3 L& A
( V5 F4 H3 T4 h7 V' X N* A# a
2 patients were PCRU (4.5 log machine) and these patients relapsed4 f+ N( n* A2 Q4 T$ Q* `* R
into MMR when drugs were discontinued.) i4 O! K( Z; f d5 s2 K! Q
* f! T* v5 r, L: w! sSeven pts with relapse were treated again with TKI, 3 with nilotinib,
# h8 d+ ?4 d! J( w. j2 with dasatinib, and one each with imatinib and bosutinib (the latter+ w; \4 O$ Y! `% x" p3 O+ R, |
in AP). After a median of 13 months on therapy (range 4-52) all patients0 G0 \0 i0 [2 j+ p$ d
improved their response, 5 with CMR and 2 MMR (including the pt that had
) h$ r7 {, M1 T/ dtransformed to AP). They do not say why all patients were not retreated
1 Y( \; t2 Z! J) g% uwith imatinib and had to take Nilotinib and Dasatinib. Also, note that. n0 m8 i5 B1 @; f. }8 c, i
one did not regain CMR at the 13th month mark though it is good news
5 g: K. V% L9 |that 5 did. It may take some time to regain CMR for some who have gone5 ?2 h# [* q/ R* H1 b8 P
off drugs and relapsed. However, from our own list experiences, some
% {" \! R+ Z6 F) ?6 L. z# Thad regained CMR fast when they retook the TKI.
: V0 U0 \3 C/ \6 w7 u/ T
$ w. D& W0 F7 n# e3 qThe doctors conclude that treatment discontinuation is experimental
/ A* a X& {5 y% m( b1 fand cannot be recommended at this stage as a standard procedure.& [ T" }8 ~3 X2 B, l# B! W3 F
+ k) A( i M% p7 n! M: s% ^. XBest Wishes,1 H! D* {9 w0 P( j1 @6 V. x
! e7 y) _* D3 I: F
Anjana
& }* M6 u& E. \* _8 L/ i% a/ O$ A2 c* j: }! f# o q
; ^) n* Z. u& V% ^. `$ \
' W& i' M( h* G4 |& M; Y
7 f' R5 `# B# p: c: a
$ x" I J M4 ^4 r. j
9 F r9 S$ H! r' w4 w
; g1 T/ O' K8 J: P) \# U" ^
% X9 W. W! M1 @- L; ]: X8 l
! k/ Y9 i% {0 K) } z! G6 i. m W' ~
3783 Patient (Pt)-Driven Discontinuation of Tyrosine Kinase Inhibitor6 ^0 g- }$ D' F0 P7 x1 ^
Theray in Chronic Phase Chronic Myeloid Leukemia (CML) - Single
8 W7 D8 H1 k2 p) ^! {1 s( |Institution Experience
+ t! z& A/ f+ ^, w' b; t8 C5 \Program: Oral and Poster Abstracts) v! o8 X* N, v: v" w: G6 A }
Session: 632. Chronic Myeloid Leukemia - Therapy: Poster III; I$ q& Z& k/ o: F
$ C. ?+ Z3 C; d; i. _& T% x3 iMonday, December 10, 2012, 6:00 PM-8:00 PM
4 _; E$ R, s8 k! y c8 a3 } y2 u6 ~% i) R; F
Hall B1-B2, Level 1, Building B (Georgia World Congress Center)
! W# r9 Q7 \. j/ C8 v# G- _( o; s4 E8 E" k
Ohad Benjamini, MD1*, Hagop M. Kantarjian, MD1*, Mary Beth Rios, RN1," W, `! j( H3 |* J% r) r8 S. W
Elias Jabbour, MD2*, Susan O'Brien, M.D.1, Preetesh Jain, MD, DM, PhD1*,: M4 Q! [0 Q" u2 T
Stefan Faderl, MD1, Guillermo Garcia-Manero, MD1*, Farhad Ravandi, MD1,
) y2 F: u0 a5 d7 |5 Y% r3 aGautam Borthakur, M.D.1, Alfonso Quint醩-Cardama, MD1* and Jorge E.
' S$ j( L2 ]1 ^. V1 A8 W0 bCortes, MD14 T+ X y6 I9 z4 f% p
$ N6 A- p# C# X1Department of Leukemia, The University of Texas MD Anderson Cancer
' u8 b# m8 ~2 K1 f% i- lCenter, Houston, TX% e) ^. I/ {; m8 X
2Department of Leukemia, The University of Texas M.D. Anderson Cancer
' W) x! d* W4 s: \# A# |/ ZCenter, Houston, TX
R! ^+ g' y& x0 x
3 F* P3 j W7 z: Q2 B- _Introduction: Some recent studies have reported on the outcome of CML
" l' C2 S9 i( X- O! ]pts who discontinued thyrosin kinase inhibitors (TKI) after achieving1 h7 p2 c( E- D" i9 l) h" W" e! S/ `
sustained undetectable bcr-abl transcript level. Most patients who stop
4 j6 q1 ^8 a+ X; m. O- @TKI have experienced molecular relapse. Most patients respond after
! ]9 n4 H; U; y7 Y& s5 L& X6 ?resuming TKIs regaining undetectable bcr-abl transcript levels. These
4 i1 D5 \. X) I! s0 b/ @2 l; fseries have prospectively planned treatment discontinuation and included
! b' O; I a) Z$ Z. M; yonly pts that have sustained complete molecular response (CMR) for at
- P3 g( E1 Q! O8 oleast 2 yrs. However, in many instances pts may want to discontinue TKIs
7 ~. `, Y; ^" \( c* |2 x3 d) | N) Tnot in CMR. Various reasons may lead patients to discontinue TKI
/ I, E7 K$ v7 c2 l6 j9 d# Wtreatment unexpectedly, among them severe adverse effects, pregnancy or
: T3 Y5 o4 d! W- {$ }2 A" z Ieconomic constraints. This single institution experience reflects the
- n% c% B6 P3 O# A0 gheterogeneous nature of pt-driven TKI discontinuation.8 J! F) F4 o: ?' T
1 @0 V) n: }1 G$ G# z0 @% B
Aim: To characterize the outcome and profile of CML pts who chose to
7 v" `, R+ U- L8 n5 z! ydiscontinue TKI therapy in a single center regardless of their initial4 f9 ^# _0 f: Y* y" l0 d6 r
response to TKI therapy.$ V4 U! V. Z9 L7 D6 F l
n0 y' o8 I! Q1 w$ MMethods:We retrospectively analyzed MDACC data on all patients with CML1 c0 {& }9 y; Q) a& Y3 F
that were treated with TKIs in our institution and discontinued therapy.2 v3 ^9 E# H9 \* a
# M# ~7 d5 X/ `- u5 T, i% c CResults: A total of 26 patients with CML-CP managed at MDACC
, \ T6 Y8 ]% fdiscontinued TKI between 2003 and 2012. The total median follow up time% D! c+ ?) e5 a) L9 a
since diagnosis was more than 120 months (mos) (range, 45 mos to 304# g/ |/ y) M$ `5 @
mos). The median age at diagnosis was 48 yrs (range, 28-73); 15 pts were
$ z6 R# F7 H, I8 ~/ U" k" Tfemale. All pts had been diagnosed and treated in chronic phase.
2 \! U. Q% L$ q" w JInterferon was initial therapy in 11 pts (42%) and 15 pts received TKI5 u3 k" ~( o# ?$ }2 B& y* B
as initial therapy (4 received imatinib 400mg/day, 10 imatinib
# K8 r& Y# I& K: @: J6 f0 |600-800mg/day, and 1 bosutinib.) Of the 11 pts initially treated with
, C% W/ m& J) JIFN, 7 then received imatinib 400mg and 4 imatinib 800mg upon IFN
! N7 ~; p2 |& X& f$ ?failure. Pts treated frontline with TKI started therapy within a median. j L4 n- ^9 r: v
of 0.8 mos from diagnosis (range 0 to 4) and those with previous
) {. }( x6 t! ?0 I# B4 Pinterferon (n=11) after a median of 60 mos from diagnosis (31 to 164 H8 f" |3 c3 _9 g9 ]( r; A
mos). Before TKI discontinuation 21pts (81%) were receiving their first
' U$ A' S$ y, c3 GTKI and 5 (19%) were receiving 2nd (4) or 3rd line (1) TKI. Complete
: F3 y3 u3 H t7 y- [% T% Wcytogenetic response (CCyR) had been achieved in all 26 pts at a median7 b% t5 e0 g! c1 x" [
of 3.5 mos (3-93); Major molecular response (MMR) in all at a median of
( D/ R) o9 \; j8 f( G) e4 Z0 M, R9 mos (3-73) and CMR in 17 (65%) at a median of 22 mos (9-120). All. h2 c. B( u0 J' v
patients discontinued therapy in CML-CP, all in CCyR, of them, 17 (65%)
* U7 D$ S) w7 J' ] f! n) @4 thad undetectable transcripts, 2 (8%) had MR4.5, and 7 (27%) MMR. The# Q N+ W% M! Q r P
median duration of CMR before TKI cessation was 62 mos, (0- 118). The+ u h0 T: ~& V# H2 U
median duration of total TKI therapy was 101 mos (3- 135).
( t) h$ M! s* h0 s
! ~8 _: c$ ?' l. W. P, s$ dFourteen pts (54%) discontinued TKI due to adverse events, 2 pts$ O7 H8 ]$ g7 W! g6 D* p; T9 F, D
discontinued to become pregnant, 5 decided to stop after long CMR, and 52 U/ G% T2 r& U2 ^: e/ `& s
pts discontinued for financial reasons. After TKI discontinuation
2 ?5 q8 d. J5 I: V/ G0 Rpatients were followed for a median of 11 mos (5-131). Among pts with; G' F* `8 s! l& Q% u" M2 L7 v
CMR at discontinuation, molecular relapse occurred in 8 (47%) pts at a* R; F7 E2 _+ a/ M' F. v& |, ~9 J
median of 4 mos (1-11) from discontinuation with median transcript level
' e5 q9 Q' V' ~! [at relapse of 0.07 (IS) (range, 0.004-2.17). Six pts with initial INF9 p% Z1 ^$ c, V6 p
therapy had CMR at time of TKI discontinuation, 50% of them relapsed.9 o7 I. I, z2 M5 \* i" G; C
Among 7 pts who discontinued therapy in MMR, after a median follow-up0 w: {( H1 n: \4 s2 O2 {
from discontinuation of 21.6 months (range, 4.6-106), 4 remained at MMR,( o; p5 X+ c2 h
one has minor CyR and one CCyR without retreatment at last follow up
/ E4 R8 D3 f7 k1 @" F: H, Bafter 78 and 105 months from TKI discontinuation, and one transformed to( S3 r7 X; H3 n8 i/ |- N2 B! b
accelerated phase (AP). The 2 pts with MR4.5at discontinuation relapsed2 N0 N. i5 @1 P, i: O# c4 V
to MMR. Three pts had a transient molecular recurrence with spontaneous
$ e' l% J! W6 s8 D9 X6 Y5 Y/ Kre-gain of CMR. Seven pts with relapse were treated again with TKI, 39 a; l# e& y2 s7 T; T) B) U
with nilotinib, 2 with dasatinib, and one each with imatinib and) L) b _' B+ t% `* I$ G. j3 @. h0 k
bosutinib (the later in AP). After a median of 13 months on therapy
?2 G: N& |& g% _- E(range 4-52) all patients improved their response, 5 with CMR and 2 MMR$ U" X" ]7 U) s4 C0 v4 {
(including the pt that had transformed to AP). There were no deaths or# I. ]: N+ D8 z
transformations to blastic phase of CML. At last follow up 14 (54%) pts
5 A8 C1 W' l7 jwere in CMR, 5 (19%) in MMR,5 (19%) in CCyR and 1 each in minor CyR and/ _5 e( Y1 E5 k9 v
PCyR.: v( i1 _! w- o( }
# s. L9 m: q, x* N$ uConclusion: Pt-driven TKI discontinuation in CML-CP leads to molecular( F; J( C( h! X0 o3 a$ Z
relapse in nearly half of the pts who discontinue therapy in CMR. Some% ]- n* w( `1 Z9 k9 r
pts who discontinue in MMR may have sustained MMR. Treatment0 I6 B* \& h1 @$ P! ~/ j q
discontinuation should be considered experimental and cannot be
" B S* N! ?& z$ G: irecommended to pts as a standard approach.2 x3 x" ]2 |8 Q8 S$ g
# O. n/ w. D2 J6 o
Disclosures: Ravandi: BMS: Honoraria, Research Funding. |
MET谷美替尼服用期间血酮血糖飙升居
去年11月底家人确诊肺腺癌IV期,右肺门及纵隔淋巴结转,心包,左侧肾上腺,脑转。经第
请教一下基测无靶、免疫高表达后面的
治疗历程
1.治疗历程中的病情描述的变化都是基于第一次,变化于前一次的。
2.检查报告
第七次白紫后 没有明显疗效 请教下一
之前治疗经过:
去年10月左侧股骨放疗后,一直培美+贝伐维持一共用了5次
2024年开始培
肺腺癌egfr21-l858r突变,egfr扩增、
老爸21年3月发现肺腺癌晚期,双肺转移,纵隔淋巴结增大,取组织基因检测结果为egfr21-
患癌一年内接受2次手术,我悟出5点抗
作者:尘埃落定
大家好,我是孙先生,今年52岁。一切都来得那么突然和猝不及防,怎样
提升卡
置顶卡
沉默卡
喧嚣卡
变色卡
千斤顶
显身卡
