Increased Incidence of Therapy Related Myeloid Neoplasia (t-MN) After Initial Therapy for CLL with Fludarabine-Cyclophosphamide (FC) Vs Fludarabine (F): Long-Term Follow-up of US Intergroup Study E2997

Blood ◽  
2010 ◽  
Vol 116 (21) ◽  
pp. 924-924
Author(s):  
Mitchell R Smith ◽  
Donna Neuberg ◽  
Ian W. Flinn ◽  
Michael R. Grever ◽  
John M. Bennett ◽  
...  
Keyword(s):  
Conflicts Of Interest ◽  
Initial Therapy ◽  
Lymphocytic Leukemia ◽  
Long Term Effects ◽  
Risk Of Death ◽  
Molecular Features ◽  
Myeloid Neoplasia ◽  
Additional Therapy

Abstract Abstract 924 Background: Therapy-related myeloid neoplasia (t-MN), including myelodysplastic syndrome and acute myeloid leukemia, has been reported at a higher frequency with chlorambucil + fludarabine as compared to fludarabine alone, but has not been rigorously studied in the context of cyclophosphamide as an alkylator agent. The intergroup prospective randomized Phase 3 trial, E2997, compared FC with F alone as initial therapy for patients (pt) with chronic lymphocytic leukemia (CLL). FC therapy led to higher complete and overall response rates and longer progression-free survival at the initial analysis (Flinn et al JCO 2007). One rationale for combining F with C is that F can inhibit repair of DNA damage induced by C. FC did cause more myelosuppression that could lead to more long-term effects on myeloid hematopoietic function, including t-MN. Methods: E2997 enrolled 278 pts, 141 on FC and 137 on F. These cases were assessed for t-MN by required reporting of these events. Baseline genetic and molecular features of CLL were available through a companion lab correlative trial for 235 pts, 122 on FC and 113 on F. Results: With median follow-up of 6.4 yrs, there have been 13 (4.7%) reported cases of t-MN, 9 after FC and 4 after F. By cumulative incidence methodology, adjusting for the competing risk of death, the rates of t-MN at 7 yr are 8.2% after FC and 4.6% after F (p=0.18 by the Gray test). Median age at study entry of the t-MN pts was 60 (range 45–80) yrs vs 61 (range 33–86) yrs among those not reported to have t-MN. Median time from initial therapy to diagnosis of t-MN was 5 (range 0.7–8) yrs and did not differ between FC and F. Ten of 13 affected pts received 6 chemotherapy cycles. Additional therapy prior to occurrence of t-MN was given to only 2 of 9 FC pts, in contrast to 3 of 4 F pts. Thus, t-MN occurred in only 1 pt treated with F and no further therapy vs 7 who received FC and no further therapy. Ten of 12 pts with available cytogenetics at diagnosis of t-MN had an abnormality of chromosome 5 and/or 7, common to alkylating agent-induced t-MN, usually (n=8) with complex karyotype. Of the 9 pts with t-MN after FC, all 7 with available CLL data had lower risk IgVH mutated disease, in contrast to 1 of 4 with t-MN after F and 44% in the entire cohort. Conclusion: Our analysis suggests that a higher incidence of t-MN has occurred after FC than after F. t-MN after FC occurred most often without additional therapy and in IgVH mutated CLL which is associated with more favorable outcome. The increased incidence of t-MN after FC in this study, usually in the absence of additional treatment, suggests that FC is more leukemogenic than F. This finding emphasizes a need for longer follow-up of toxicity and survival before concluding that FC is preferable to F as the chemotherapy backbone for initial therapy of both low and high risk CLL. Disclosures: No relevant conflicts of interest to declare.

scholarly journals Incidence of therapy-related myeloid neoplasia after initial therapy for chronic lymphocytic leukemia with fludarabine-cyclophosphamide versus fludarabine: long-term follow-up of US Intergroup Study E2997

Blood ◽  
2011 ◽  
Vol 118 (13) ◽  
pp. 3525-3527 ◽  
Author(s):  
Mitchell R. Smith ◽  
Donna Neuberg ◽  
Ian W. Flinn ◽  
Michael R. Grever ◽  
Hillard M. Lazarus ◽  
...  
Keyword(s):  
Chronic Lymphocytic Leukemia ◽  
Late Toxicity ◽  
Initial Therapy ◽  
Lymphocytic Leukemia ◽  
Long Term Follow Up ◽  
After Cancer ◽  
Myeloid Neoplasia ◽  
Additional Therapy

Abstract Chemotherapy-related myeloid neoplasia (t-MN) is a significant late toxicity concern after cancer therapy. In the randomized intergroup phase 3 E2997 trial, initial therapy of chronic lymphocytic leukemia with fludarabine plus cyclophosphamide (FC) compared with fludarabine alone yielded higher complete and overall response rates and longer progression-free, but not overall, survival. Here, we report t-MN incidence in 278 patients enrolled in E2997 with a median 6.4-year follow-up. Thirteen cases (4.7%) of t-MN occurred at a median of 5 years from initial therapy for chronic lymphocytic leukemia, 9 after FC and 4 after fludarabine alone. By cumulative incidence methodology, rates of t-MN at 7 years were 8.2% after FC and 4.6% after fludarabine alone (P = .09). Seven of the 9 cases of t-MN after FC occurred without additional therapy. Abnormalities involving chromosomes 5 or 7 were found in 10 cases, which suggests alkylator involvement. These data suggest that FC may induce more t-MN than fludarabine alone.

scholarly journals Other Cancers in Long-Term Survivors of Chronic Lymphocytic Leukemia: Incidence and Prognostic Relevance

Blood ◽  
2014 ◽  
Vol 124 (21) ◽  
pp. 3323-3323 ◽  
Author(s):  
Lorenzo Falchi ◽  
Michael Keating ◽  
Susan Lerner ◽  
Xuemei Wang ◽  
Kplola Y Elhor Gbito ◽  
...  
Keyword(s):  
Bladder Cancer ◽  
Chronic Lymphocytic Leukemia ◽  
Conflicts Of Interest ◽  
Observation Time ◽  
Lymphocytic Leukemia ◽  
P Value ◽  
Prognostic Impact ◽  
Long Term Survivors

Abstract Introduction. The clinical course of chronic lymphocytic leukemia (CLL) is mostly indolent. About one third of the patients are managed with lifelong watch-and-wait (WW) and those who receive therapy often achieve a durable remission. As a result, the majority of patients with CLL will live with their disease for long periods of time, and be exposed to several complications, including the occurrence of other cancers (OC). Patients with CLL may have an increased incidence in OC. Published reports indicate an incidence of 3-27%, mostly in treated patients, however, very little is known on OC in patients with CLL not requiring therapy. Furthermore, observation time in published studies is limited to <5 years, and the incidence of OC in patients followed for longer than 10 years is unknown. We, therefore, studied the incidence and prognostic impact of OC in treatment-naïve patients with CLL followed for ≥10 years. Methods. We reviewed our database and identified all patients with CLL untreated at the time of referral. We selected long-term survivors (LTS), defined as patients with a follow-up ≥10 years, and analyzed the incidence and prognostic impact of OC in this population. Non-melanoma skin cancers were excluded since these were diagnosed and treated promptly in virtually all cases and felt not to have prognostic impact. Standardized incidence ratios (SIR) were calculated for OC occurring after the diagnosis of CLL that were reportable to the Surveillance, Epidemiology and End Results program.The estimated overall survival (OS) according to the presence of OC was plotted considering OC as a time-dependent covariate. Results. We identified 797 LTS of CLL seen at our institution between 1957 and 2003. Median age was 56 years (24-88). 57% of patients were males. Median follow-up for the entire population is 154 months (120-485). We recorded 383 OC in 286 (36%) patients. 76/286 (26%) patients had >1 OC (62 had 2 OC, 10 had 3, 2 had 4, 1 had 5 and 1 had 6).The firstOC preceded or was diagnosed concomitantly with CLL in 100 patients (35%), while in the remaining 186 (65%) it occurred later during the course of the disease. 570 patients (71%) required treatment for CLL. Median time to treatment was 18 months (0-454). In treated patients, the cumulative frequency of OC was 205/570 (36%) and in WW patients 81/227 (36%). The SIR for all OC was 1.2 (p = .034). Males and patients younger than 60 years had a significantly higher incidence of OC (SIR 1.31 and 1.27, respectively). Among OC types, secondary leukemia, melanoma and head and neck cancers had the highest observed-to-expected ratio. Surprisingly, lung, digestive tract, and bladder cancer had a lower-than-expected incidence (table). 474 patients (59%) are alive. 222/570 (39%) treated patients and 101/227 (44%) WW patients have died. The median OS was longer in patients without OC (279 months) vs. those with OC (189 months). Independent predictors of shorter survival in multivariate analysis included higher creatinine, the presence of OC, and older age. Discussion. This is the first study to address the incidence of OC in LTS of CLL, including WW patients. In our population, the frequency of OC is similar in treated and WW patients. Although the incidence of OC in LTS of CLL is higher compared to matched general population, the incidence of lung, digestive and bladder cancer is lower than expected. Reasons of this finding remain to be identified.The occurrence of OC is an independent predictor of shorter survival, thus constituting a relevant competing risk of mortality in LTS of CLL. Variable Observed Expected Person-years SIR (O/E) 95% CI for O/E P -value Overall 148 123.34 10956 1.20 1.01 – 1.40 0.034 Male 96 73.4 5885 1.31 1.06 – 1.58 0.013 Female 52 49.93 5071 1.04 0.78 – 1.36 0.67 Age ≥60 years 60 54.33 3416 1.10 0.84 – 1.42 0.44 Age <60 years 88 69.02 7540 1.27 1.02 – 1.57 0.027 OC type Prostate 28 25.92 11809 1.08 0.72 – 1.56 0.64 Lung 20 29.08 11942 0.69 0.42 – 1.06 0.04 Breast 19 18.60 11855 1.02 0.62 – 1.59 0.96 Melanoma 16 4.23 11926 3.78 2.16 – 6.14 0.00 Leukemia 15 4.27 12009 3.51 1.96 – 5.79 0.00 Non-Hodgkin lymphoma 6 6.38 11996 0.94 0.34 – 2.05 1.00 Digestive 16 40.4 11937 0.40 0.23 – 0.64 0.00 Colon 8 19.42 11972 0.41 0.18 – 0.81 0.006 Pancreas 2 4.83 12024 0.41 0.05 – 1.49 0.18 Rectal 3 8.69 12011 0.34 0.07 – 1.00 0.05 Bladder 3 11.18 11993 0.27 0.05 – 0.78 0.009 Multiple Myeloma 2 1.98 12012 1.01 0.12 – 3.64 1.00 Lip 3 0.02 12015 150 31.00 – 438.5 0.00 Salivary gland 2 0.03 12026 66.66 8.00 – 240.06 0.00 Disclosures No relevant conflicts of interest to declare.

Imatinib Long Term Effects (ILTE) Study: An International Study to Evaluate Long-Term Effects in CML Patients.

Blood ◽  
2009 ◽  
Vol 114 (22) ◽  
pp. 2199-2199
Author(s):  
Dong-Wook Kim ◽  
Laura Antolini ◽  
François-Xavier Mahon ◽  
Francois Guilhot ◽  
Michael Deininger ◽  
...  
Keyword(s):  
Adverse Events ◽  
Conflicts Of Interest ◽  
International Study ◽  
Imatinib Treatment ◽  
Long Term Effects ◽  
First Line ◽  
Serious Adverse Events ◽  
Second Cancers

Abstract Abstract 2199 Poster Board II-176 Imatinib is an effective first line therapy for chronic myeloid leukemia (CML) and has substantially changed its biological and clinical behavior. Durable complete cytogenetic responses (CCyR) were reported in the majority of patients, with a rather benign side effect profile, despite the ‘off target’ inhibition of several other kinases, including Kit, PDGFR and Lck. Since available information is largely based on sponsored trials and long-term field studies are lacking, the ILTE study was conceived as an independent, academic, multicenter trial supported by the Italian Drug Safety Agency (AIFA) and Regione Lombardia. ILTE is an international study on a retrospective cohort and includes 31 centers in Europe, North/South America, Africa, Middle East and Asia; therefore it is uniquely positioned to present a global picture of imatinib long-term effects. Consecutive patients with Ph+ CML who started imatinib between 01 September 1999 and 31 December 2004 were eligible if they were in CCyR after two years of imatinib treatment. Study endpoints were (a) survival, (b), serious adverse events (SAE, including second cancers), (c) toxicities not qualifying as SAE (NSAE) but judged by the referring physician as substantially impacting quality of life, (d) loss of CCyR, and (e) development of PCR negativity. A total of 948 patients were enrolled, 88% of which met eligibility criteria after centers were visited and monitored. The median age of eligible patients was 51 (range 18-92) years; 59% of patients were males and the median follow-up was 4.0 years (excluding the first 2 years of treatment). As of Dec. 31 2008, 3255 person years were available for analysis. Twenty one deaths were observed (only 6 of them [28%] caused by relapsed CML), with a standardized rate of 0.6/100 person years and an observed/expected ratio of 0.7 (95% CI = 0.43-1.07, p=ns). A total of 138 SAE were recorded (rate 4.2/100 person years, most frequent type “heart failure”), with 19.5% being considered related to imatinib. Second cancers were documented in 29 patients (rate 0.9/100 person years), with an observed/expected ratio of 1.02. Among the 761 NSAE recorded (rate 23.4/100 person years) the most frequent types were cramps, asthenia,edema, skin fragility, diarrhea; 69% of them were considered related to imatinib. A total of 18 patients (2.2 %) discontinued imatinib because of toxicities during the period of observation. Forty patients lost CCyR, corresponding to a rate of 1.3/100 person years (1.0 in patients with imatinib as first-line treatment, 1.4 in patients who were treated with imatinib >6 months after diagnosis), with stable or increasing rates over time. Finally, 256 patients (36.0 %) developed durable (> 1 year) PCR negativity. In conclusion, this report from ILTE shows that CML patients on imatinib die unfrequently of CML related causes, do not appear to have substantially higher second cancer rates than the general population, have mortality rates similar to an age/sex matched population and do not show new types of imatinib-related adverse events. They also experience a low but steady rate of loss of CCyR and develop PCR negativity in approximately 1/3 of cases. Follow-up and further analysis are ongoing. (Presented on behalf ofthe ILTE Investigators group) Disclosures: No relevant conflicts of interest to declare.

Long-Term Cause-Specific Mortality of Patients Treated for Hodgkin’s Disease

2003 ◽  
Vol 21 (18) ◽  
pp. 3431-3439 ◽  
Author(s):  
Berthe M.P. Aleman ◽  
Alexandra W. van den Belt-Dusebout ◽  
Willem J. Klokman ◽  
Mars B. van’t Veer ◽  
Harry Bartelink ◽  
...  
Keyword(s):  
General Population ◽  
Hodgkin's Disease ◽  
Hodgkin’S Disease ◽  
Initial Therapy ◽  
Second Primary ◽  
Risk Of Death ◽  
Increased Risk ◽  
Specific Mortality

Purpose: To assess long-term cause-specific mortality of young Hodgkin’s disease (HD) patients. Patients and Methods: The study population consisted of 1,261 patients treated for HD before age 41 between 1965 and 1987. Follow-up was complete until October 2000. For 95% of deaths, the cause was known. Long-term cause-specific mortality was compared with general population rates to assess relative risk (RR) and absolute excess risk (AER) of death. Results: After a median follow-up of 17.8 years, 534 patients had died (55% of HD). The RR of death from all causes other than HD was 6.8 times that of the general population, and still amounted to 5.1 after more than 30 years. RRs of death resulting from solid tumors (STs) and cardiovascular disease (CVD) were increased overall (RR = 6.6 and 6.3, respectively), but especially in patients treated before age 21 (RR = 14.8 and 13.6, respectively). When these patients grew older, this elevated mortality decreased. The overall AER of death from causes other than HD increased throughout follow-up. Patients receiving salvage chemotherapy had a significantly increased RR of death from STs, compared to patients receiving initial therapy only. Conclusion: The main cause of death among HD patients was lymphoma, but after 20 years, HD mortality was negligible. The RRs and AERs of death from second primary cancers (SCs) and CVDs continued to increase after 10 years. Even more than 30 years after diagnosis, HD patients experienced elevated risk of death from all causes other than HD. Increased risk of death from SCs and CVDs was found especially in patients treated before age 21, but these risks seemed to abate with age.

scholarly journals An observational study of outcomes after initial infused therapy in Medicare patients diagnosed with chronic lymphocytic leukemia

Blood ◽  
2011 ◽  
Vol 117 (13) ◽  
pp. 3505-3513 ◽  
Author(s):  
Mark D. Danese ◽  
Robert I. Griffiths ◽  
Michelle Gleeson ◽  
Sacha Satram-Hoang ◽  
Kevin Knopf ◽  
...  
Keyword(s):  
Chronic Lymphocytic Leukemia ◽  
Lower Risk ◽  
Initial Therapy ◽  
Treatment Patterns ◽  
Lymphocytic Leukemia ◽  
Long Term Follow Up ◽  
Medicare Patients ◽  
Overall Mortality

Abstract The study goal was to characterize older chronic lymphocytic leukemia (CLL) patients and to evaluate outcomes in those patients who initiated infused therapy. Patients 66 years of age and older in the Surveillance, Epidemiology, and End Results (SEER) program with a CLL diagnosis were matched to their Medicare Part A and Part B claims for long-term follow-up. Treatment patterns, survival after initiation of infused therapy, and both hematologic and hospitalization outcomes were assessed. There were 6433 CLL patients identified, and 2040 received infused therapy. Treated patients were categorized as receiving rituximab monotherapy (16%), rituximab plus chemotherapy (14%), and chemotherapy alone (70%) based on the initial 60 days after infusion. Rituximab plus chemotherapy compared with chemotherapy alone was associated with a 25% lower risk of overall mortality (95% confidence interval, 9%-38%). Restricting to patients age 70 years and older did not change the risk reduction for rituximab plus chemotherapy. Hematologic interventions were more common with rituximab plus chemotherapy compared with chemotherapy alone, but there was no difference in all-cause hospitalizations. These analyses, based on observational data, suggest that the benefits of initial therapy with rituximab in a heterogeneous group of older CLL patients are comparable with those demonstrated in younger patients.

Initial Therapy for Mantle Cell Lymphoma with Abbreviated R-CHOP Followed By Y90-Ibritumomab Tiuxetan: Ten Year Follow-up of the Phase 2 ECOG-ACRIN Study E1499

Blood ◽  
2015 ◽  
Vol 126 (23) ◽  
pp. 2702-2702
Author(s):  
Mitchell R. Smith ◽  
Hailun Li ◽  
Fangxin Hong ◽  
Leo I. Gordon ◽  
Randy D. Gascoyne ◽  
...  
Keyword(s):  
Mantle Cell Lymphoma ◽  
Cell Lymphoma ◽  
Standard Dose ◽  
Intensive Therapy ◽  
Initial Therapy ◽  
Ibritumomab Tiuxetan ◽  
Mantle Cell ◽  
Additional Therapy

Abstract There is no single accepted treatment approach for mantle cell lymphoma (MCL), varying from intensive therapy in young, fit patients (pts) to less intensive for the more common older or less fit pts. R-CHOP remains a commonly used initial therapy for MCL, yielding high response rates but with limited durability, and still serves as a comparator in recently published studies. E1499 was designed to test the hypothesis that 1 dose of radioimmunotherapy (RIT) consolidation with 90Y-ibritumomab tiuxetan after only 4 cycles of R-CHOP-21 as initial therapy for MCL would be safe, well-tolerated and improve time-to-treatment failure (TTF) compared with historical R-CHOP data. E1499 met its primary endpoint with TTF at 1.5 years of 69% (95% CI 58-78%) (Smith et al JCO 2012) and treatment was well-tolerated. Here we report 10 year follow-up data on this uniformly-treated cohort of pts with MCL. 56 eligible pts with previously untreated MCL and adequate organ function were enrolled between 11/03-2/05. Median age at enrollment was 60 (range 33-83) yrs, 73% were male and MIPI was low in 50%, intermediate in 27% and high in 21%. All cases were centrally reviewed. Therapy was standard dose R-CHOP given every 3 weeks for only 4 cycles, followed in pts whose disease did not progress with a single standard administration of 90Y-ibritumomab tiuxetan. All planned therapy was administered to 91% (5 did not receive RIT: 3 PD, 1 death from MI, 1 pt preference). The overall response rate after all treatment was 82% (55% CR/CRu). Median follow-up is now 9.8 years (May 2015 data cut-off). Median TTF is 34 months (mos). By MIPI, TTF was 36 mos for low, 25 mos for intermediate and 10 mos for the 12 pts with high MIPI. Pts who achieved CR had median TTF of 38 mos vs 15 mos for PR (p = 0.01). Median overall survival (OS) for the 56 eligible pts is 7.9 yrs. For pts < 65 median OS has not been reached at 10 yrs, compared with 7 yrs for those ≥ 65 (p = 0.07). OS for low MIPI pts also has not been reached at 10 yr, is 8 yr for intermediate and 5.5 yrs for high MIPI. Although TTF was longer for pts with CR/CRu, OS did not differ. There has been no additional therapy-related myeloid neoplasia (t-MN) other than 1 previously reported t-MN which occurred after additional therapy. Other malignancies include 2 non-small cell lung cancers, 1 bladder cancer, 1 ampullary adenocarcinoma and 2 resected localized non-melanoma skin cancers. Long-term follow-up of this cohort of pts treated with a simple 4 month outpatient regimen continues to suggest a benefit for RIT consolidation in prolonging TTF, with median TTF of almost 3 yrs. Though in somewhat older populations, median PFS was 14 mos for 6xR-CHOP alone and 25 mos for 6xVR-CAP (Robak T NEJM 2015), and 22 mos for 6xR-CHOP in StiL trial (Rummel M Lancet 2013). Ongoing rituximab maintenance after 8xR-CHOP is also effective (Kluin-Nelemans NEJM 2015) with 57% of pts progression-free at 4 yrs. For OS, age is the single most important prognostic factor in this cohort. Pts with high MIPI had short TTF, but their OS suggests that additional therapies were effective. As novel agents rapidly move into first-line regimens, often based on early assessments of efficacy, these long-term data inform benchmark expectations of PFS and OS in MCL. OS in our cohort is comparable to contemporaneous studies using either intense or non-intense initial therapy, raising questions regarding the value of intensive treatment strategies in MCL. Figure 1. Figure 1. Disclosures Smith: celegene, spectrum, genentech: Honoraria. Off Label Use: Y90-ibritumomab tiuxetan is not approved for use in mantle cell lymphoma. Gordon:Dr Leo I. Gordon: Patents & Royalties: Patent for gold nanoparticles pending; Northwestern University: Employment. Horning:Genentech: Employment.

Long-term Effects of Two Different Treatments for Dental Fear and Avoidance

1986 ◽  
Vol 65 (6) ◽  
pp. 874-876 ◽  
Author(s):  
U. Berggren
Keyword(s):  
Avoidance Behavior ◽  
Dental Treatment ◽  
Behavioral Therapy ◽  
Dental Anxiety ◽  
Initial Therapy ◽  
Dental Fear ◽  
Long Term Effects ◽  
Community Based

Follow-up clinical studies of treatment for dental fear and avoidance behavior are infrequent in the literature. The present investigation reports follow-up results over more than two years from 84 out of 99 patients treated for dental fear in a Swedish community-based dental fear clinic. Broad-based behavioral therapy (BT) or general anesthesia (GA), both in combination with adjusted conventional dental treatment, were used. The frequency of patients' attendance for regular dental care after two years was unchanged or even somewhat increased and was significantly higher in those who had received the BT therapy. Most patients stated that they had no problems after leaving the dental fear clinic. Among patients reporting such problems, the change of dentist was most frequently reported. The level of dental anxiety as measured by Corah's DAS was still at a low level, in spite of a slight increase over the two years since initial therapy.

Association Of More Than One B Cell Clone Arises In Any Type Of Leukemic Chronic B Cell Disorder

Blood ◽  
2013 ◽  
Vol 122 (21) ◽  
pp. 4161-4161
Author(s):  
Gregory Lazarian ◽  
Herve Roudot ◽  
Riham Farrah ◽  
Chadi Al Nawakil ◽  
Remi Letestu ◽  
...  
Keyword(s):  
B Cell ◽  
Conflicts Of Interest ◽  
Cell Clone ◽  
Extensive Study ◽  
Lymphoproliferative Disorders ◽  
Lymphocytic Leukemia ◽  
Phase Discrimination ◽  
Molecular Features ◽  
Leukemic Phase

Abstract The identification of more than one clone in B cell chronic lymphoproliferative disorders (B-CLPD) is known to occur occasionally. Nonetheless, to our knowledge, there is no extensive study of their incidence, their clinical and biological features, and their prognosis at diagnosis. At our institution, between 01/2006 and 12/2012, 1152 cases of chronic lymphoproliferative disorders with leukemic phase were diagnosed. Among those cases we have identified 44 cases (3,8%) with at least two B cell clones at diagnosis through systematic immunophenotyping of blood lymphocytes. We only considered cases in which both clones were of B cell origin and present in blood. Association of two haematological disorders arising from cells of different origin (i.e. myeloid or T cells) were excluded. Size of smallest second clone identified was 1% of B cells, in 11/44 cases it was less than 10% whereas in the remaining cases, both clones had up to approximately the same size. We aimed at further characterize these biclonal B-CLPD with leukemic phase. Discrimination of the clones relied on a combination of at least 2 phenotypic markers (presence or absence and not on level of expression). Diagnosis of biclonality relied on different surface immunoglobulin light chains in 21 cases. In the remaining 23 cases, displaying the same light chain, genescan analysis showed the presence of two peaks. Further cloning allowed to identify the presence of two functional rearrangements in 12 cases. Among those, IGHV were unmutated in both clones in 4 cases, mutated in both clones in 6 cases, and mixed (mutated/unmutated) in 2 cases. Based on clinical presentation, cytology and immunophenotype analysis and molecular features, the various B CLPD clones were identified the following: monoclonal B lymphocytosis (MBL) in 27 cases, chronic lymphocytic leukemia (CLL) in 14 cases, CD5+ atypical chronic B-CLPD in 22 cases, marginal zone lymphoma (MZL) in 12 cases, CD5- atypical B-CLPD in 11 cases, Waldenström macroglobulinemia (WM) in 4 cases, mantle cell lymphoma (MCL) in 3 cases and hairy cell leukemia (HCL) in 1 case. All possible associations between the various B-CLPD were seen: CD5+ B-CLPD associated with either CD5+ or CD5- B CLPD. The predominant clone was CD5+ in 56,8% cases, whereas the second clone was CD5+ in the majority of cases (82% cases). Therefore, presence of two concomitant CD5 negative clones was rare. This is exemplified in the Circos representation below (figure 1) Four patients displayed an association of three clones and one patient had four. Analysis of IGHV gene sequence did not show a preferential use of any VH. Fifteen patients had unmutated IGHV genes, including CD5 negative cases. Of note, in CLL patients, 60% cases had unmutated IGHV genes, which is higher than what is normally observed in CLL at diagnosis. At presentation, most cases showed features of indolent disease; lymphnodes were present in 13/44 cases (29%), splenomegaly 10/44 cases (22%). Median Hb level was 13,2 g/dl (12,1 – 14,1 g/dl ) platelets level was 199 G/l (132 – 245 G/l). Mild cytopenias were observed in 5 patients, all with MZL, and likely related to splenomegaly. Follow up data were available for 35 cases. 23 /35 cases remained untreated with a median follow up of 16,2 months. Among those who required treatment, different chemotherapy regimen were used and 66 % patients are in remission after this first line of treatment. In conclusion, in this large prospective cohort, biclonal B CLPD were observed in less than 5% cases, and do not appear related to an adverse prognosis. The absence of predominant association, or of VH usage, and the presence of both IGHV mutated and unmutated clones do not favor a major role for the antigen to explain the presence of two clones at diagnosis in the same patient. This suggest that the mechanisms leading to the emergence of a second clone are not specific of one particular disease but may be common to all chronic lymphoproliferative disorders of B cell origin. Disclosures: No relevant conflicts of interest to declare.

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