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Vol. 113. Issue 5.
Pages T529-T531 (May 2022)
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Vol. 113. Issue 5.
Pages T529-T531 (May 2022)
Case and Research Letter
Open Access
Advanced-Stage CD30+ Mycosis Fungoides Treated With Brentuximab
Micosis fungoides en estadio avanzado CD30+ tratadas con brentuximab
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C. Vico-Alonsoa,
Corresponding author
c.vicoalonso@gmail.com

Corresponding author.
, J.J. Andrés-Lencinaa, J.L. Rodríguez-Peraltob, P.L. Ortiz Romeroa
a Servicio de Dermatología, Hospital Universitario 12 de Octubre, Universidad Complutense de Madrid, Madrid, Spain
b Servicio de Anatomía Patológica, Hospital Universitario 12 de Octubre, Universidad Complutense de Madrid, Madrid, Spain
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Actas Dermosifiliogr. 2022;113:529-3110.1016/j.ad.2020.05.021
C. Vico-Alonso, J.J. Andrés-Lencina, J.L. Rodríguez-Peralto, P.L. Ortiz Romero
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To the Editor,

Mycosis fungoides (MF) accounts for 60% of cutaneous lymphomas. Although it generally has an indolent course, 25% of cases progress to advanced stages, with a median survival of 68 months in stage IIB and 33 months in stage IVB.1 The therapeutic options for patients in these stages are limited. New molecules that have emerged in recent years include brentuximab vedotin (BV) for the treatment of CD30+ MF.2

We describe a series of 5 cases (2 women and 3 men) of advanced CD30+ MF treated with BV. The median age at diagnosis was 67 (range, 52–83) years. The cases corresponded to erythrodermic MF (1 patient), interstitial MF (1 patient), and MF with large cell transformation (3 patients).3 In all cases immunohistochemistry was positive for CD30, with expression exceeding 20% in some skin samples taken before starting treatment. The mean time since disease onset was 4.8 years. The mean number of previous treatments received by each patient was 6.6 (range, 4–9) and the median BV treatment duration was 3 cycles (range, 1–16) (Table 1).

Table 1.

Clinical Characteristics of Patients and Clinical Response to Treatment.

  Patient 1  Patient 2  Patient 3  Patient 4  Patient 5 
SexClinicopathological variant  FemaleMF with LCT  MaleMF with LCT  MaleMF with LCT  FemaleErythrodermic MF  MaleInterstitial MF 
Age  59  83  67  76  52 
Prior treatments  Phototherapy, INF, PEG-INF, bexarotene, methotrexate, mogamulizumab, liposomal doxorubicin, TSEB, photopheresis  Mtx-IL, alitretinoin, acitretin, liposomal doxorubicin, CHOP, bexarotene, vorinostat, mogamulizumab, INF  PUVA, gemcitabine, TSEB, alemtuzumab, liposomal doxorubicin  PUVA, mogamulizumab, bexarotene, liposomal doxorubicin, vorinostat  acitretin, bexarotene, RT, liposomal doxorubicin 
Clinical stage/TNMB  T4N0M0B0 IIIA  T3N0M1B2 IVB  T3N3M1B0 IVB  T4N0M0B2 IVA1  T3NxM0B0 IIB 
Cutaneous response7  PR  PR  PR  DP  PR 
Lymph node response  NA  NA  DP  NA  DP 
Response in viscera  NA  CR  DP  NA  NA 
Response in blood  NA  CR  NA  DP  NA 
Overall response  PR  CR  DP  DP  DP 
Number of BV cycles  16  16 
Adverse effects  Paresthesia Arthralgia Myalgia  Paresthesia Asthenia Arthralgia  –  –  – 

Abbreviations: BV, brentuximab vedotin; CHOP, cyclophosphamide, doxorubicin, vincristine, and prednisone; CR, complete response; DP, disease progression; INF, interferon; LCT, large cell transformation; MF, mycosis fungoides; Mtx-IL, intralesional methotrexate; NA, not applicable; PEG-INF, pegylated interferon; PUVA, psoralen-ultraviolet A; PR, partial response; RT, radiotherapy; TSEB, total skin electron beam therapy; TNMB, tumor-node-metastasis-blood.

Patient 1, a 59-year-old woman with stage T4N0M0B0 MF, exhibited a clinical cutaneous response 6 weeks after starting treatment, with a response duration of 12 months (Fig. 1A and B). Patient 2, an 83-year-old man with stage T3N0M1B2 MF, showed a partial cutaneous response at 12 weeks. This patient presented CD4+/CD30+ lymphocytic infiltration in both lungs, and showed a response in viscera 15 weeks after starting treatment (Fig. 1C and D). The duration of the response in viscera was 9 months. Patient 3, a 63-year-old man with stage T3N3M1B0 MF with tumor lesions, presented a rapid cutaneous response 2 weeks after starting treatment, with subsequent progression of both lymph node and visceral disease. Patient 4, a 76-year-old woman with erythrodermic stage T4N0M0B2 MF, experienced disease progression. Patient 5, a 52-year-old man with interstitial MF with tumor lesions (stage T3NxM0B0), showed a partial cutaneous response after 2 weeks, with subsequent progression of cutaneous and lymph node disease.

Figure 1.

Clinical and radiological response of 2 patients treated with brentuximab. A, Skin lesions in Patient 1 before starting systemic treatment. B, Clinical cutaneous response 6 weeks after starting treatment, showing a decrease in erythema and infiltration, and in the extent of the lesions. C, Axial section of contrast computed tomography scan of the chest. Tumor masses in both lung fields correspond to a proliferation of CD4+/CD30+ lymphocytes. D, Complete disappearance of the tumor masses after eighth infusion of brentuximab.

(0.13MB).

In summary, a partial cutaneous response was observed in 4 patients, of whom 2 experienced disease progression, while 1 patient showed a complete response in viscera. The median time to clinical response was 6 (range, 2–12) weeks (skin) and 15 weeks (viscera). In the 2 patients who showed a response to treatment (partial cutaneous response, complete response in viscera), without progression, the overall response duration was 9 and 12 months, respectively.

The most frequent adverse events were peripheral sensory neuropathy (maximum, grade 3), which appeared after a mean number of 2 infusions, followed by asthenia and arthralgia. None of these events necessitated treatment discontinuation. In 1 patient sensory neuropathy had resolved upon completion of BV treatment, while in the other it persisted up to 16 weeks after completion.

BV is a monoclonal antibody for CD30, a transmembrane glycoprotein expressed on activated B and T lymphocytes. This antibody is bound to monomethyl auristatin E (MMAE), an agent that disrupts the microtubule network leading to cell cycle arrest and subsequent apostosis.4 The multicenter, randomized, phase 3 ALCANZA clinical trial concluded that BV treatment was superior to both bexarotene and methotrexate, regardless of age, sex, type of cutaneous lymphoma (CD30+ MF or cutaneous anaplastic large cell lymphoma), or involvement (cutaneous or cutaneous and visceral).5 However, up to a third of the patients had early-stage disease and a median of only 2 previous lines of treatment, thereby excluding, in our opinion, the majority of patients who receive this type of treatment in routine clinical practice. Papadavid et al. have shared their experience with BV treatment in 3 patients with folliculotropic MF and large cell transformation and 1 patient with Sézary syndrome (SS).6 The 3 MF patients showed complete or partial responses, while the SS patient presented stable disease.6,7

The most surprising finding in our case series was the rapid cutaneous response after the first infusion. This was particularly evident in the case of tumor lesions, which had been rapidly progressing to skin necrosis. Patient 5, who had a diagnosis of interstitial MF and tumor-like skin lesions, experienced this effect after a single dose of BV. Another interesting finding was the complete response in viscera, according to the relevant criterion, which was observed in a patient with specific pulmonary involvement and was maintained for 9 months.

In our experience BV offers a rapid tumor response, although maintenance of this response is highly variable. Knowledge of the type of patient and the disease stage is necessary to ensure optimal use. Furthermore, new studies are required to best position the drug in clinical practice, including its combination with other agents and maintenance therapy in cases in which a response is achieved.

Conflicts of Interest

The authors declare that they have no conflicts of interest.

References
[1]
J.J. Scarisbrick, et al.
Cutaneous lymphoma international consortium study of outcome in advanced stages of mycosis fungoides and sezary syndrome: effect of specific prognostic markers on survival and development of a prognostic model.
J Clin Oncol, 33 (2015), pp. 3766-3773
[2]
M. Duvic, et al.
Results of a phase ii trial of brentuximab vedotin for CD30+ cutaneous T-cell lymphoma and lymphomatoid papulosis.
J Clin Oncol, 33 (2015), pp. 3759-3765
[3]
H. Muñoz-González, A.-M. Molina-Ruiz, L. Requena.
Clinicopathologic variants of mycosis fungoides.
Actas Dermosifiliogr, 108 (2017), pp. 192-208
[4]
R. Stranzenbach, E. Dippel, M. Schlaak, R. Stadler.
Brentuximab vedotin in CD30+cutaneous lymphoma: how do we treat, how shall we treat? A review of the literature.
Br J Dermatol, 177 (2017), pp. 1503-1509
[5]
H.M. Prince, Y.H. Kim, S.M. Horwitz, R. Dummer, J. Scarisbrick, P. Quaglino, et al.
Brentuximab vedotin or physician's choice in CD30-positive cutaneous T-cell lymphoma (ALCANZA): an international, open-label, randomised, phase 3, multicentre trial.
[6]
E. Papadavid, E. Kapniari, L. Marinos, V. Nikolaou, A. Oikonomidi, J. Georgakopoulos, et al.
Efficacy and safety of brentuximab vedotin in advanced cutaneous T-cell lymphomas patients.
J Eur Acad Dermatol Venerol, 33 (2019), pp. e223-e232295
[7]
E.A. Olsen, S. Whittaker, Y.H. Kim, M. Duvic, H.M. Prince, S.R. Lessin, et al.
Clinical end points and response criteria in mycosis fungoides and Sézary syndrome: a consensus statement of the International Society for Cutaneous Lymphomas, the United States Cutaneous Lymphoma Consortium, and the Cutaneous Lymphoma Task Force of the European Organisation for Research and Treatment of Cancer.
J Clin Oncol, 29 (2011), pp. 2598-2607
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