Lenalidomide (LEN) is an immunomodulatory compound with significant activity versus relapsed/refractory multiple myeloma (RRMM).1  In Blood, Rajkumar et al2  reported striking efficacy of LEN plus dexamethasone (DEX) versus newly diagnosed multiple myeloma (NDMM). While structurally similar to thalidomide (THAL), also used to treat MM,3  LEN has a unique activity profile. Both agents appear to increase the risk of thromboembolic events (TEEs), although the actual baseline incidence is unclear. The TEE incidence in NDMM patients receiving THAL+DEX without thrombosis prophylaxis is approximately 15%.4,5  An 8.5% incidence of TEE in RRMM patients getting DEX+LEN without routine prophylaxis has been reported.1  Rajkumar et al2  described a 3% incidence in NDMM with DEX+LEN and daily aspirin (ASA; 80 mg or 325 mg).

The Southwest Oncology Group is conducting a double-blind randomized trial comparing DEX (40 mg/day on days 1-4, 9-11, and 17-20 every 35 days for 3 induction cycles, then 40 mg/day on days 1-4 and 15-18 every 28 days as maintenance thereafter) plus placebo versus DEX (same schedule) plus LEN (25 mg/day on days 1-28 every 35 days during induction, then 25 mg/day on days 1-21 every 28 days during maintenance). Crossover from DEX to DEX+LEN is permitted for progressive MM. Initially, no thrombosis prophylaxis was mandated. After 21 patients were enrolled, an increased incidence of TEEs in 1 arm became apparent: 9 (75%) of 12 patients receiving DEX+LEN developed TEEs (8 lower-extremity deep-vein thromboses with 2 pulmonary embolic events, 1 ischemic stroke) after a median of 50 days, versus 0 (0%) of 9 patients on DEX alone (P < .001). The study was modified to require 325 mg ASA daily, based on the low TEE incidence observed by Rajkumar et al,2  as well as a report showing low-dose ASA reduced TEE risk in MM patients receiving chemotherapythalidomide combinations.6 

As of October 31, 2005, 76 patients have been enrolled. Since mandating ASA prophylaxis, 6 TEEs have occurred among 55 additional patients: 4 (15%) of 26 randomized to DEX+LEN (P < .001 for comparison of TEE incidence on DEX+LEN before and after aspirin) and 2 (7%) of 29 on DEX alone (P = .41 for DEX vs DEX+LEN after ASA). Of interest, both of the patients randomized to DEX who developed clots had already crossed over from DEX to DEX+LEN due to progressive disease. One of these patients was noncompliant with ASA prophylaxis. Overall, 6 (19%) of 32 patients receiving DEX+LEN have developed TEEs since modification of the protocol to include ASA prophylaxis (P < .001 before vs after ASA).

In summary, although adding ASA markedly reduced the risk of TEEs in NDMM patients receiving DEX+LEN, we observed a much higher incidence of TEE than reported by Rajkumar et al.4  Potential reasons include higher DEX dose, longer LEN exposure during induction in our trial, or other factors such as possible differences in the use of recombinant erythropoietin. The 19% TEE incidence we observed is similar to that reported for NDMM patients treated with anthracycline-THAL combinations plus either 81 mg ASA6  or low-dose enoxaparin.7  At present, using one of these prophylaxis strategies during DEX+LEN treatment for NDMM is highly recommended. Further research is needed to determine the optimal prophylaxis strategy.

S. Vincent Rajkumar
S. Vincent Rajkumar
Morie A. Gertz
Morie A. Gertz

The importance of thromboprophylaxis with the use of lenalidomide and high-dose dexamethasone is well illustrated in this report by Zonder and colleagues. The incidence of deep-vein thrombosis (DVT) in their study decreased significantly when mandatory prophylaxis with aspirin was instituted but remains higher than the 3% risk of DVT observed with the same regimen in our trial, in which routine aspirin prophylaxis was used from the outset.

We believe that there are 2 factors that may affect the incidence of DVT in this setting, namely, the dose of dexamethasone and the use of concomitant erythropoietin. As we noted in our paper, a higher risk of DVT has also been observed in an Eastern Cooperative Oncology Group (ECOG) randomized trial testing lenalidomide plus either high- or low-dose dexamethasone as initial treatment for myeloma.1  In this trial, the increased DVT risk was seen in the high-dose dexamethasone arm, which uses doses of dexamethasone similar to those used in the Southwest Oncology Group and Mayo Clinic trials. In contrast, the risk of DVT did not appear to be much increased in patients treated on the lenalidomide plus low-dose dexamethasone arm. These findings, coupled with earlier observations that show no increased risk of DVT with single-agent lenalidomide,2  suggest that it may be possible to reduce DVT risk by optimizing the dose of dexamethasone that is used in combination with lenalidomide.

A higher risk of DVT has been observed with the concurrent use of erythropoietic agents in patients receiving either thalidomide or lenalidomide.3,4  Clinical trials sponsored by the National Cancer Institute Cancer Therapy Evaluation Program now recommend routine thromboprophylaxis when lenalidomide and erythropoietin are used concurrently.

We recommend that all patients receiving lenalidomide plus dexamethasone receive routine thromboprophylaxis. More data are needed on the best form of DVT prophylaxis. In the ECOG trial, we are requiring aspirin as the minimum mandatory prophylaxis, with a recommendation to consider either low-molecular-weight heparin or warfarin in the high-dose dexamethasone arm.

Correspondence: S. Vincent Rajkumar, Mayo Clinic, 200 First St SW, Rochester, MN 55905; e-mail: rajkumar.vincent@mayo.edu.

1
Rajkumar SV, Blood E. Lenalidomide and venous thrombosis in multiple myeloma [letter].
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List A, Kurtin S, Roe DJ, et al. Efficacy of lenalidomide in myelodysplastic syndromes.
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Steurer M, Sudmeier I, Stauder R, Gastl G. Thromboembolic events in patients with myelodysplastic syndrome receiving thalidomide in combination with darbepoietin-alpha.
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Knight R, DeLap RJ, Zeldis JB. Lenalidomide and venous thrombosis in multiple myeloma [letter].
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Supported in part by Celgene Corporation.

1
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Copyright © 2006 by The American Society of Hematology
2006
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