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Regular Article CLINICAL TRIALS AND OBSERVATIONS
Outcomes of patients with chronic lymphocytic leukemia after discontinuing ibrutinib Preetesh Jain,1,2 Michael Keating,1 William Wierda,1 Zeev Estrov,1 Alessandra Ferrajoli,1 Nitin Jain,1 Binsah George,1 Danelle James,3 Hagop Kantarjian,1 Jan Burger,1 and Susan O’Brien1 1
Department of Leukemia, The University of Texas MD Anderson Cancer Center, Houston, TX; 2Department of Internal Medicine, University of Texas Medical School at Houston, Houston, TX; and 3Pharmacyclics, Inc, Sunnyvale, CA
Ibrutinib is a Bruton tyrosine kinase inhibitor approved for the treatment of patients with relapsed refractory chronic lymphocytic leukemia (RR-CLL). We describe the characteristics, causes of discontinuation, and outcomes in patients who discon• Clinical characteristics, tinued treatment with ibrutinib. One hundred twenty-seven patients were enrolled in causes of discontinuation, and outcome of patients who various clinical trials of ibrutinib, with or without rituximab, at our center. Thirty-three (26%) patients have discontinued ibrutinib to date. The majority of those patients had progress or fail ibrutinib are high-risk features: 94% with unmutated immunoglobulin heavy chain variable gene described. rearrangement, 58% with del(17p) by fluorescence in situ hybridization, and 54% • Patients with CLL who with a complex karyotype. Causes of discontinuation were disease transformation progress early on ibrutinib (7), progressive CLL (7), stem cell transplantation (3), adverse events (11), serious therapy have poor outcomes. adverse events/deaths (3), and miscellaneous reasons (2). Twenty five patients (76%) died after discontinuing ibrutinib; the median overall survival was 3.1 months after discontinuation. Most patients with RR-CLL who discontinued ibrutinib early were difficult to treat and had poor outcomes. (Blood. 2015;125(13):2062-2067)
Key Points
Introduction Bruton tyrosine kinase (BTK) is a critical enzyme in the B-cell receptor signaling pathway1 and is a novel therapeutic target in CLL.2,3 Ibrutinib (previously known as PCI-32765) is an irreversible BTK inhibitor that binds to cysteine 481 within the adenosine triphosphate binding site of the kinase domain. Ibrutinib given at a daily dose of 420 mg received an accelerated approval by the US Food and Drug Administration in February 2014 for patients with relapsed refractory chronic lymphocytic leukemia (RR-CLL) who had received 1 or more prior treatment and was recently approved as initial therapy in patients with deletion 17p. Ibrutinib alone3,4 or in combination with rituximab has demonstrated favorable results in patients with relapsed CLL and highrisk disease [eg, del(17p)].5 In a phase 3 trial,6 patients with RR-CLL were randomly assigned to either treatment with ibrutinib 420 mg orally daily (n 5 195) or ofatumumab monotherapy (n 5 196). As per the investigator’s assessment, the overall response rate (ORR) (complete response 1 partial response (PR) 1 PR with lymphocytosis) was 85% in the ibrutinib group vs 24% in the ofatumumab group. Ibrutinib was well tolerated. The most common adverse effects were diarrhea, fatigue, pyrexia, nausea, anemia, and neutropenia, seen in more than 20% of patients. Grade 3 to 4 hematological toxicity was comparable in the ibrutinib group vs the ofatumumab group (neutropenia, 16% vs 14%; anemia, 5% vs 8%; thrombocytopenia,
6% vs 4%). Bleeding such as petechiae or ecchymosis was more frequent in patients treated with ibrutinib (44% vs 12% in those treated with ofatumumab); however, major bleeding requiring red blood cell transfusion or hospitalization was 1% vs 2% with ibrutinib vs ofatumumab, respectively. Grade 3 nonhematologic adverse effects were diarrhea and atrial fibrillation (4% and 3% in the ibrutinib group). Of note, atrial fibrillation (any grade) occurred in 5% vs 1% of patients treated with ibrutinib vs ofatumumab. Fourteen percent (n 5 28) of patients discontinued therapy after a median follow-up of 9.5 months. The most common causes of discontinuation of ibrutinib were disease progression, adverse events, deaths, patient decision, and stem cell transplant (SCT). Ibrutinib improved response rates, progression-free survival, and overall survival compared with ofatumumab in patients with RR-CLL. In a phase 2 trial3,4 of 85 (117 in the 2013 update) patients with RR-CLL treated with single-agent ibrutinib, 36% (n 5 31) of patients discontinued therapy after a median follow-up of 21 months. The most common causes of discontinuation of ibrutinib were disease progression, adverse events, patient decision, and SCT. Ibrutinib was also reported to be safe and efficacious in previously untreated patients with CLL aged 65 years or older with an ORR of 95% (8% complete response, 87% PR). 7 In addition, the combination of ibrutinib with rituximab has produced
Submitted September 28, 2014; accepted December 29, 2014. Prepublished online as Blood First Edition paper, January 8, 2015; DOI 10.1182/blood-201409-603670.
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© 2015 by The American Society of Hematology
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BLOOD, 26 MARCH 2015 x VOLUME 125, NUMBER 13
From www.bloodjournal.org by guest on September 10, 2016. For personal use only. BLOOD, 26 MARCH 2015 x VOLUME 125, NUMBER 13
IBRUTINIB DISCONTINUATION IN CLL
Table 1. Summary of clinical trials of ibrutinib in this analysis
Protocol
Trial identification number
2010-0314
NCT01105247
Regimen Ibrutinib
Total number of patients enrolled
Number of patients who discontinued ibrutinib
41
15
40
15
17
2
29
1
127
33
(RR-CLL) 2011-0785
NCT01520519
Ibrutinib 1 rituximab (high-risk CLL)
2012-0707
NCT01578707
Ibrutinib vs ofatumumab (RR-CLL)
2012-0086
NCT01752426
Ibrutinib/heavy water
Total
positive early results with more rapid achievement of partial response compared with that seen with single-agent ibrutinib.5 In this report, we present the characteristics, causes of discontinuation, and outcome of those patients who discontinued ibrutinib.
Patients and methods Patients with CLL (n 5 127) enrolled in 4 different clinical trials of ibrutinib were included (Table 1). Patient characteristics at the time of starting ibrutinib are summarized in Table 2. Of note, 49 patients had missing karyotype data, 5 in those who discontinued (15%) and 44 in those who continued (47%); these patients were excluded from the comparison based on karyotype. Patients were treated at MD Anderson Cancer Center, Houston, Texas, from July 2010 until May 2014. Treatment protocols were approved by the institutional review board, and informed consent was obtained in accordance with the Declaration of Helsinki. These trials are registered at ClinicalTrials.gov. Patient charts were reviewed for the characteristics, causes of discontinuation, outcomes, and subsequent therapies. Kaplan-Meier survival postibrutinib was calculated from the date of discontinuing ibrutinib to the date of last follow-up. Duration of ibrutinib therapy was calculated from the date of starting ibrutinib to the date of discontinuing ibrutinib. Log-rank test was used to estimate the time to event outcomes.
2063
rates of unmutated IGHV, 17p deletion, and complex karyotype for the 94 patients who did not discontinue ibrutinib therapy were 74%, 25%, and 46%, respectively. The rates of 17p deletion and unmutated IGHV were significantly higher in patients who discontinued ibrutinib therapy (P 5 .0005 and .02, respectively). Seven patients transformed to an aggressive lymphoma: 6 had diffuse large B-cell lymphoma (Richter transformation) and 1 had a histiocytic sarcoma discovered only at autopsy. The cause of death in the patient with histiocytic sarcoma transformation was multiorgan dysfunction secondary to histiocytic sarcoma transformation. Four (58%) patients transformed within the first 12 months of starting ibrutinib. Among these 7 patients, 6 (86%) have died, and 1 patient died on study (transformation found at autopsy). One patient with Richter transformation is alive and being treated with a small molecule in a clinical trial. Among the 6 patients who died, 2 died within a month because of sepsis and disease progression without further therapy. Three died within 3 months after treatment with intensive chemoimmunotherapy (n 5 2) or an investigational agent (n 5 1). One patient failed chemoimmunotherapy and died in hospice after 15 months. Seven patients progressed without transformation. Four patients are alive, and 3 patients died. Among the 3 patients who died, 2 had pneumonia and progressive disease and 1 failed to respond to further therapy. Four patients are alive: 2 are receiving investigational agents, 1 responded to ofatumumab, and 1 is not receiving therapy. Three patients responding to ibrutinib proceeded to SCT; 2 patients have died and another is alive and in remission. Two patients died because of complications of SCT and severe graft vs host disease. Fourteen patients came off therapy because of adverse events (n 5 11) or death (n 5 3). Adverse events included extensive aspergillosis, diarrhea and subdural hematoma, recurrent ear bleeding, recurrent oral ulcers, subdural hematoma and atrial fibrillation, Pseudomonas sepsis, extensive fungal pneumonia, diarrhea and pneumonia, recurrent infections, gastrointestinal bleeding, and colitis (summarized in Table 3). Two patients discontinued ibrutinib for other reasons, including therapy-related myelodysplasia (prior therapy with fludarabine and bendamustine) and financial issues. Overall, 6 patients died on study. They received ibrutinib for a median of 12 months (range, 6-20 months). In addition to the patient dying of transformation to histiocytic sarcoma, there were 5 other deaths on study. Two patients died suddenly at home
Results Twenty-six percent (33/127) of patients have discontinued ibrutinib. The median age of the patients was 61 years. The majority of patients exhibited high-risk features at the time of starting ibrutinib: 25 (76%) patients had advanced Rai stage, 17 (52%) patients had overexpression of CD38, 21/30 (70%) overexpressed Zap-70, 20/33 (61%) had a Beta2 microglobin higher than 4 mg/L, 29/31 (94%) had unmutated immunoglobulin heavy chain variable gene rearrangement (IGHV), 19 patients (58%) had del(17p) by fluorescence in situ hybridization, and 15/28 (54%) had complex karyotype. The median number of prior therapies was 2 (range, 0-7), and 45% patients received 3 or more therapies before ibrutinib. The median time from diagnosis to the start of ibrutinib was 59 months (range, 8-150 months), and the median duration of ibrutinib treatment was 13 months (range, 2-39 months). Twenty-five patients died, and 8 are alive. Six were on-study deaths (Table 3). Of note, the
Table 2. Characteristics of patients who discontinued ibrutinib Characteristic
Category
Overall, N 5 33
Age, years
Median (range)
61 (36-83)
White blood cell, K/mL
Median (range)
24 (2-323)
Rai stage, 3-4
Advanced
76%
CD38, .30%
High
52%
Zap-70 positive b2 M, mg/L IGHV mutation Fluorescence in situ
By immunohistochemistry
70%
$4 mg/L
61%
Unmutated
94%
del17p/del11q/others
58%/18%/24%
hybridization category Karyotype Number of prior therapies Median number of prior
Complex
54%
$3
45%
Median (range)
2 (0-7)
Median (range)
59 (8-150)
therapies Median time from diagnosis to ibrutinib, months
2
1
63
78
52
36
63
56
83
2‡
3‡
4‡
5
6
7
64
63
2‡
3‡
2.4 5.1
1
2.3
—
1
UM
UM
UM
UM
ND
UM
UM
UM
UM
UM
Del17p
Negative
1
3
3
4
del17p, 112, 13q
del17p 1 del 11q
2
5
2
2
2
1
4
0
2
1
3
4
5
del17p 1 13q
del11q 1 13q
del11q
del13q
del17p
del17p
del17p 1 11q 1 13q
del17p
del11q
del17p
del17p
del13q
del11q 1 del13q
Number of prior therapies
11.9
12.9
11.7
18.5
33.1
38.7
6.9
21.4
22.5
14.2
9.4
10
13.1
2
21.9
4.5
13.1
Duration of ibrutinib, months
Alive
Dead
Dead
Alive
Alive
Dead
Dead
Alive
Alive
Dead
Dead
Dead
Dead
Dead
Alive
Dead
Dead
Survival status
111
4.2
0.1
14.41
11.51
2.8
2.1
1.91
1.81
1.6
15.0
3.1
2.6
2.1
21
0.9
0.0
Survival postibrutinib, months
Stem cell transplantation
Stem cell transplantation
Stem cell transplantation
Progressive disease
Progressive disease
Progressive disease
Progressive disease
Progressive disease
Progressive disease
Progressive disease
Richter transformation
Richter transformation
Richter transformation
Richter transformation
Richter transformation
Richter transformation
transformation
Histiocytic sarcoma
Cause of discontinuation
Remission post-SCT
transplant
Complications of
disease
Died of graft vs host
Ofatumumab
clinical trial
on small molecule
R-MP (4 infusions, PR),
Pneumonia
of CLL
no further treatment
Infections, pneumonia,
clinical trial
On small molecule
Ofatumumab
treatment of CLL
infections, no further
pulmonary disease,
Chronic obstructive
Chemoimmunotherapy31*
Chemoimmunotherapy*
R-MP (1 course)
Chemoimmunotherapy 31*
clinical trial
On small molecule
Died
Died on study
Outcome of patients after ibrutinib
ara-C, rituximab; CVAD, cyclophosphamide, vincristine, adriamycin (doxorubicin) and dexamethasone; DIC, disseminated intravascular coagulation; M, mutated; MP, methylprednisolone; OFAR, oxaliplatin, fludarabine; R-MP, rituximab with methylprednisolone; UM, unmutated. *Chemoimmunotherapy - OFAR- Oxaliplatin, fludarabine, ara-C, Rituximab. 1Patients who are alive. †Cause of sudden death in these 2 patients was unknown (autopsies not performed), 1 patient had no prior cardiac history and another had prior hypertension but no arrhythmias. ‡Patients treated with ibrutinib and rituximab.
61
1
transplantation (n 5 3)
because of stem cell
4.1
1
10.8
5.1
1
—
5.9
3
1
—
5.2
4
—
1
UM
UM
UM
UM
UM
UM
UM
Fluorescence in situ hybridization
JAIN et al
Patients who discontinued
73
1‡
transformed (n 5 7)
Patients who progressed not
7
2.1
10
65
1
1
60
5
6
12
1
73
4
6 4
1
72
ND
52
3‡
6.8
b2 M (mg/L)
2
1
Zap-70 Status
57
Age, years
1‡
(n 5 7)
Patients who transformed
Patients
Patient characteristics
2064
IGHV mutation status
Table 3. Summary of patient characteristics, causes of discontinuation, and outcomes of patients after discontinuing ibrutinib (n 5 33)
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64
50
64
67
76
68
68
62
82
66
57
50
68
2
3
4
5‡
6‡
7‡
8
9‡
10‡
11
12‡
13
14
54
2
5.1 4.2
ND
1
3.4
1
UM
UM
UM
UM
M
UM
UM
UM
M
UM
UM
UM
UM
UM
ND
UM
Del17p
del13q
del17p 1 del11q 1
del13q
del13q
2
6
4
3
3
7
del17p 112 del13q
Del17p
1
Del17p
Del17p
0
5
del17p 1 del11q 1 del13q
2
2
1
0
1
3
1
Number of prior therapies
del11q
Del17p
Del11q
Trisomy 12
Negative
Del13q
Del17p
Fluorescence in situ hybridization
Patient characteristics
17
27.4
1.9
16.1
6
3.9
8.4
17
31.9
21.5
2.1
16.4
6.2
6
20
11
Duration of ibrutinib, months
Dead
Dead
Dead
Alive
Dead
Dead
Dead
Dead
Dead
Alive
Dead
Dead
Dead
Dead
Dead
Dead
Survival status
1.4
1.1
41.8
24.11
12.8
5
4
1.8
1
0.31
0.2
0
0
0
0
0
Survival postibrutinib, months
Suicide
ofatumumab
acquired von Willebrand
restarted
Patient choice
myelodysplasia, cytopenias
Therapy-related
atrial fibrillation
Subdural hematoma,
No further treatment
related myelodysplasia
Died because of therapy-
Metastatic cancer of jejunum
C1 OFAR-2 again on ibrutinib
progressed with ascites and
Ofatumumab and MP,
intolerance Diarrhea, colitis
OFAR1 cycle, ibrutinib
Recurrent oral ulcers,
disease, accelerated CLL
Hyper-CVAD with
Gastrointestinal bleeding,
pulmonary disease
infections, chronic obstructive
No further treatment
ibrutinib Comorbidities and recurrent
Died on study, but off
Recurrent ear bleeding, past
No treatment
Plan to restart ibrutinib
further treatment of CLL
Multifocal aspergillosis, no
Died on study
Died on study
history of cancer oropharynx
DIC
Diarrhea and pneumonia with
hematoma,
Diarrhea, subdural
Extensive aspergillosis
Sudden death†
Died on study
died on study
Sudden death†
No further treatment,
altered mental status
No further treatment
Outcome of patients after ibrutinib
Recurrent fungal pneumonia,
bronchiectasis
Pseudomonas sepsis and
Cause of discontinuation
ara-C, rituximab; CVAD, cyclophosphamide, vincristine, adriamycin (doxorubicin) and dexamethasone; DIC, disseminated intravascular coagulation; M, mutated; MP, methylprednisolone; OFAR, oxaliplatin, fludarabine; R-MP, rituximab with methylprednisolone; UM, unmutated. *Chemoimmunotherapy - OFAR- Oxaliplatin, fludarabine, ara-C, Rituximab. 1Patients who are alive. †Cause of sudden death in these 2 patients was unknown (autopsies not performed), 1 patient had no prior cardiac history and another had prior hypertension but no arrhythmias. ‡Patients treated with ibrutinib and rituximab.
55
1
causes (n 5 2)
because of miscellaneous
2.2
ND
3.2
1
4.1
1
4.3
5.4
1
ND
6
—
3.9
6
1
—
2.6
3
1
—
3.7
10.8
1
ND
5.1
b2 M (mg/L)
1
Zap-70 Status
IGHV mutation status
BLOOD, 26 MARCH 2015 x VOLUME 125, NUMBER 13
Patients who discontinued
61
Age, years
1‡
or sudden death (n 5 14)
because of adverse events
Patients who discontinued
Patients
Table 3. (continued)
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BLOOD, 26 MARCH 2015 x VOLUME 125, NUMBER 13
JAIN et al
Figure 1. Survival of patients after discontinuation of ibrutinib. Patients survived for a median of 3.1 months after discontinuation of ibrutinib (n 5 33).
(cause of death is unknown in these 2 patients), and 1 patient committed suicide because of depression. Two patients developed severe infections. We assessed whether there was any difference in the causes of discontinuation between patients enrolled on studies with rituximab (n 5 15) vs without (n 5 18). Of 15 patients treated with rituximab and ibrutinib, 2 patients discontinued because of transformation, 4 because of disease progression, 2 because of SCT, and 7 secondary to adverse events (including 1 because of suicide). There does not appear to be any significant difference in reasons for discontinuation between patients enrolled on studies with rituximab vs those without. Of the 33 patients in this analysis, only 3 patients were previously untreated, and they discontinued ibrutinib secondary to Richter transformation, suicide, and recurrent ear bleeding. Figure 1 shows the survival of patients after discontinuing ibrutinib. The median survival for all the patients was 3.1 months and did not differ significantly between transformed and untransformed (those who progressed and those who discontinued for other reasons) patients with CLL. We also compared the postibrutinib survival of patients who transformed with those patients who progressed with CLL (Figure 2). Median survival in patients who progressed (untransformed) was not reached vs 2.6 months in those who transformed. There was no significant difference in survival (P 5 .44).
Figure 2. Postibrutinib survival of patients who progressed (without transformation; n 5 7) vs those who transformed (n 5 7). Median survival in patients who progressed (untransformed) was not reached vs 2.6 months in those who transformed (P 5 .44).
discontinuing ibrutinib could be the higher proportion of these patients having del(17p) (58% vs 25%) and unmutated IGHV (94% vs 74%) compared with the 94 patients who continued receiving ibrutinib therapy. Response rates with ibrutinib are high; however, some patients develop progressive CLL or transform when receiving ibrutinib. Many of the patients enrolled on clinical trials with ibrutinib had relapsed CLL with poor prognostic features [eg, unmutated IGHV, del(17p), multiple prior therapies, and complex karyotype]. The presence of del(17p)/TP53 mutation and complex karyotype may also contribute to the genomic instability in CLL cells, and prior therapies can promote subclonal mutations and refractory disease in patients with CLL. BTK mutations and clonal evolution may occur and produce ibrutinib resistance. Two groups have reported on acquired ibrutinib resistance and BTK mutation (C481S and phospholipase Cg2) in patients with CLL who progressed on ibrutinib therapy.9,10 It is unclear whether BTK mutations contribute to clonal evolution and promote transformations of CLL on ibrutinib therapy. Further studies are required to characterize the BTK mutations in our cohort. Patients with relapsed refractory CLL who progress early on ibrutinib are difficult to treat and have poor outcomes.
Authorship Discussion Our data suggest that survival of most previously treated patients who discontinued ibrutinib “early” is poor, and few salvage treatment options are available for these patients. The median duration of ibrutinib therapy before discontinuation in our study population was 13 months. In the most recent follow-up of the phase 2 study of ibrutinib, the median progression-free survival was not reached at 30 months. In our analysis, all but 3 patients relapsed before the median of 30 months, and therefore are considered “early” progressors, partly accounting for such poor outcomes.8 Another possible reason for poor salvageability of these patients after
Contribution: P.J. and S.O. designed the study and analyzed results; P.J., M.K., W.W., B.G., D.J., J.B., and S.O. wrote and reviewed the article; M.K., J.B., W.W., N.J., A.F., Z.E., H.K., and S.O. contributed patient samples; and all authors reviewed and gave the final approval for the article. Conflict-of-interest disclosure: S.O. and D.J. received research support from Pharmacyclics; D.J. is an employee of Pharmacyclics. The remaining authors declare no competing financial interests. Correspondence: Susan O’Brien, Department of Leukemia, Unit 428, 1515 Holcombe Blvd, Houston, TX; e-mail: sobrien@ mdanderson.org.
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4. Byrd JC, Furman RR, Coutre SE, et al. Targeting BTK with ibrutinib in relapsed chronic lymphocytic leukemia. N Engl J Med. 2013;369(1):32-42. 5. Burger JA, Keating MJ, Wierda WG, et al. Safety and activity of ibrutinib plus rituximab for patients with highrisk chronic lymphocytic leukaemia: a single-arm, phase 2 study. Lancet Oncol. 2014;15(10):1090-1099.
8. O’Brien S, Coutre S, Flinn I, et al. Independent evaluation of ibrutinib efficacy 3 years postinitiation of monotherapy in patients with chronic lymphocytic leukemia/small lymphocytic leukemia including deletion 17p disease. J Clin Oncol. 2014;32(5s). Abstract 7014.
6. Byrd JC, Brown JR, O’Brien S, et al; RESONATE Investigators. Ibrutinib versus ofatumumab in previously treated chronic lymphoid leukemia. N Engl J Med. 2014;371(3):213-223.
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7. O’Brien S, Furman RR, Coutre SE, et al. Ibrutinib as initial therapy for elderly patients with chronic lymphocytic leukaemia or small lymphocytic lymphoma: an open-label, multicentre, phase 1b/2 trial. Lancet Oncol. 2014;15(1):48-58.
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2015 125: 2062-2067 doi:10.1182/blood-2014-09-603670 originally published online January 8, 2015
Outcomes of patients with chronic lymphocytic leukemia after discontinuing ibrutinib Preetesh Jain, Michael Keating, William Wierda, Zeev Estrov, Alessandra Ferrajoli, Nitin Jain, Binsah George, Danelle James, Hagop Kantarjian, Jan Burger and Susan O'Brien
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