Journal Information
Vol. 96. Issue 4.
Pages 458-471 (1 July 2021)
Visits
7710
Vol. 96. Issue 4.
Pages 458-471 (1 July 2021)
Review
Open Access
Mycosis fungoides and Sézary syndrome: focus on the current treatment scenario
Visits
7710
José Antonio Sanchesa,
Corresponding author
jasanchesjr@gmail.com

Corresponding author.
, Jade Cury-Martinsa, Rodrigo Martins Abreub, Denis Miyashiroa, Juliana Pereirac
a Dermatology Clinic Division, Faculty of Medicine, Hospital das Clínicas, Universidade de São Paulo, São Paulo, SP, Brazil
b Medical Department, Private Institution, São Paulo, SP, Brazil
c Hematology Clinic Division, Faculty of Medicine, Hospital das Clínicas, Universidade de São Paulo, São Paulo, SP, Brazil
This item has received

Under a Creative Commons license
Article information
Abstract
Full Text
Bibliography
Download PDF
Statistics
Tables (8)
Table 1. Classification of T-cell lymphomas with primary cutaneous manifestations according to their clinical behavior, frequency and disease-specific 5-year survival. Based on the WHO-EORTC guidelines.1
Table 2. Revised TNMB classification for mycosis fungoides and Sézary syndrome.2,5
Table 3. Clinical staging system for mycosis fungoides and Sézary syndrome.2
Table 4. Response rates and duration of responses for skin treatments for MF/SS.
Table 5. Response rates and duration of responses for systemic treatments for MF/SS.
Table 6. Approval of topical treatments for cutaneous T-cell lymphoma in the United States, Europe and Brazil, according to the package insert registered in the local regulatory agencies (FDA, EMA and ANVISA), respectively.
Table 7. Approval of systemic treatments for cutaneous T-cell lymphomas in the United States, Europe and Brazil, according to the package insert registered at the local regulatory agencies (FDA, EMA and ANVISA), respectively.
Table 8. Recommendations of the Cutaneous Lymphomas Group of the Dermatology and Hematology Divisions of HC-FMUSP for the treatment of mycosis fungoides and Sézary syndrome.
Show moreShow less
Abstract

Cutaneous T-cell lymphomas are a heterogeneous group of lymphoproliferative disorders, characterized by infiltration of the skin by mature malignant T cells. Mycosis fungoides is the most common form of cutaneous T-cell lymphoma, accounting for more than 60% of cases. Mycosis fungoides in the early-stage is generally an indolent disease, progressing slowly from some patches or plaques to more widespread skin involvement. However, 20% to 25% of patients progress to advanced stages, with the development of skin tumors, extracutaneous spread and poor prognosis. Treatment modalities can be divided into two groups: skin-directed therapies and systemic therapies. Therapies targeting the skin include topical agents, phototherapy and radiotherapy. Systemic therapies include biological response modifiers, immunotherapies and chemotherapeutic agents. For early-stage mycosis fungoides, skin-directed therapies are preferred, to control the disease, improve symptoms and quality of life. When refractory or in advanced-stage disease, systemic treatment is necessary. In this article, the authors present a compilation of current treatment options for mycosis fungoides and Sézary syndrome.

Keywords:
Lymphoma, T-cell, cutaneous
Mycosis fungoides
Sezary syndrome
Therapeutics
Full Text
Introduction

Primary cutaneous lymphomas are a heterogeneous group of non-Hodgkin’s lymphomas that occur on the skin without evidence of extracutaneous disease at the time of diagnosis. They represent 19% of extranodal lymphomas, with an annual incidence in western countries of 1 case per 100,000 inhabitants/year. Primary cutaneous lymphomas are classified by the World Health Organization - European Organization for Cancer Research and Treatment (WHO-EORTC) into Cutaneous T-Cell Lymphomas (CTCL) and Cutaneous B-Cell Lymphomas (CBCL). In the West, CTCLs represent approximately 75% to 80% of all primary cutaneous lymphomas.1,2

CTCLs appear primarily on the skin and can progress to lymph nodes, blood and viscera. They are a heterogeneous group of tumors, with considerable variation regarding clinical presentation, as well as their histopathological, immunophenotypic and prognostic characteristics. The updated classification is shown in Table 1, as well as the division according to their agressiveness.1

Table 1.

Classification of T-cell lymphomas with primary cutaneous manifestations according to their clinical behavior, frequency and disease-specific 5-year survival. Based on the WHO-EORTC guidelines.1

  Clinical behavior  Frequency (%)  Disease-specific 5-year survival (%) 
Mycosis fungoides  Indolent  39  88 
Mycosis fungoides variants       
Folliculotropic mycosis fungoides  Indolent  75 
Pagetoid reticulosis  Indolent  <1  100 
Granulomatous slack skin  Indolent  <1  100 
Sézary syndrome  Aggressive  36 
Primary Cutaneous CD30+ Lymphoproliferative Disorders       
Primary cutaneous anaplastic large T-cell lymphoma  Indolent  95 
Lymphomatoid papulosis  Indolent  12  99 
Adult T-cell lymphoma/leukemia  Indolent / Aggressive  <1  NR 
Subcutaneous panniculitis-like T-cell lymphoma  Indolent  87 
Extranodal NK/T-cell lymphoma, nasal type  Aggressive  <1  16 
Chronic active EBV infection  Indolent  <1  NR 
Primary cutaneous T-cell lymphoma γ/δ  Aggressive  <1  11 
Primary cutaneous aggressive epidermotropic CD8+ T-cell lymphoma  Aggressive  <1  31 
Primary cutaneous acral CD8+ T-cell lymphoma  Indolent  <1  100 
Primary cutaneous CD4+ small/medium T-cell lymphoproliferative disorder  Indolent  100 
Primary Cutaneous Peripheral T-Cell Lymphoma, NOS  Aggressive  15 

NR, not reported; NOS, not otherwise specified.

Indolent lymphomas usually have a chronic course with frequent recurrences. The disease is generally considered incurable despite treatment, with a mean survival of 5 to 10 years. However, some patients can survive more than 20 years. Aggressive lymphomas progress faster when compared to indolent forms and can lead to death in a few months.1

Mycosis fungoides (MF) is the most common type and accounts for 60% of CTCLs and almost 50% of all primary cutaneous lymphomas. Most patients are adults or elderly, with a male to female ratio of 2:1, and a worldwide incidence of approximately 5–6 cases per million inhabitants/year. Sézary Syndrome (SS) is a rare leukemic variant of CTCL. This article will address the therapeutic possibilities for those two entities.1,2

Mycosis fungoides and Sézary syndrome

MF is a non-Hodgkin’s mature T-cell lymphoma with a primary presentation on the skin, but with potential secondary involvement of lymph nodes, blood and viscera. Skin lesions include patches or plaques that may be localized or disseminated, tumors and erythroderma. The course of MF is variable. In some patients the disease remains limited to the skin for many years, while in others, it may progress more quickly to extracutaneous involvement, with a worse prognosis. SS is an erythrodermic and pruritic form of CTCL, characterized by peripheral lymphadenopathy and the presence of neoplastic T-cells with cerebriform nuclei (Sézary cells), which are clonally related, in the skin, lymph nodes and peripheral blood.2

The histopathological analysis typically shows an epidermotropic lymphoma of small to medium-sized lymphocytes with cerebriform nuclei. The neoplastic cells have a mature T-cell phenotype, CD3+, CD4+, CD45RO+, CD8-, with variable loss of CD7 expression.1 The CD30 molecule may eventually be expressed in neoplastic cells, but this expression seems to be more frequent and more intense in cases that show transformation to large cell lymphoma. The transformed MF is defined by the presence of large cells (≥ 4-fold the size of a small lymphocyte) surpassing > 25% of the dermal infiltrate or presenting microscopic nodules and is generally associated with a worse prognosis.3

The clinical staging of MF and SS is based on the classification of cutaneous (T), lymph node (N), visceral (M) and hematological (B) involvement (Tables 2 and 3). The TNMB classification should include careful examination of the skin (paying attention to the scalp, palms, soles, and perineum), biopsy(ies) of skin lesion(s), complete blood count with screening for Sézary cells, peripheral blood flow cytometry, biochemical tests and imaging studies.2 As HTLV-1 is endemic in Brazil, screening for this retrovirus is mandatory for all patients with suspected or proven CTCL, to differentiate MF/SS from adult T-cell lymphoma/leukemia.4

Table 2.

Revised TNMB classification for mycosis fungoides and Sézary syndrome.2,5

Skin (T)   
T1  Limited patches/plaques (covering <10% of the total skin surface) 
T1a  Patches only 
T1b  Plaques ± patches 
T2  Generalized patches/plaques (covering ≥10% of the total skin surface) 
T2a  Patches only 
T2b  Plaques ± patches 
T3  Tumor(s) 
T4  Erythroderma 
Lymph node (N)   
N0  No clinically abnormal peripheral lymph nodes; 
N1  Clinically abnormal peripheral lymph nodes; dermatopathic lymphadenopathy or histopathological involvement by isolated atypical lymphocytes, without alteration of the lymph node architecture 
N1a  Negative clone 
N1b  Positive clone 
N2  Clinically abnormal peripheral lymph nodes; histopathological involvement by aggregates of atypical lymphocytes, without alteration of the lymph node architecture 
N2a  Negative clone 
N2b  Positive clone 
N3  Clinically abnormal peripheral lymph nodes; frank histopathological involvement and partial/complete effacement of the lymph node architecture 
NX  Clinically abnormal peripheral lymph nodes; without histopathological confirmation 
Viscera (M)   
M0  Without visceral involvement 
M1  With visceral involvement 
Blood (B)   
B0  There are no circulating atypical cells (Sézary cells; or <5% of atypical lymphocytes) 
B0a  Negative clone 
B0b  Positive clone 
B1  Low tumor load in the blood (≥5% of lymphocytes are Sézary cells, but not B2 cells) 
B1a  Negative clone 
B1b  Positive clone 
B2  Elevated tumor load in the blood and clonal rearrangement of the TCR (≥1000 Sézary cells/microL. and/or CD4:CD8 ≥ 10, and/or CD4 + CD7 - ≥40%, and/or CD4 + CD26 - ≥30%) 
Table 3.

Clinical staging system for mycosis fungoides and Sézary syndrome.2

Clinical staging  TNMB Classification
Ia  T1  N0  M0  B0 or B1 
Ib  T2  N0  M0  B0 or B1 
IIa  T1 or T2  N1 or N2  M0  B0 or B1 
IIb  T3  N0 to N2  M0  B0 or B1 
IIIa  T4  N0 to N2  M0  B0 
IIIb  T4  N0 to N2  M0  B1 
IVa1  T1 to T4  N0 to N2  M0  B2 
IVa2  T1 to T4  N3  M0  B0 to B2 
IVb  T1 to T4  N0 to N3  M1  B0 to B2 

T, Skin; N, Lymph node; M, Viscera; B, Peripheral blood.

Treatment options

Most treatments available for MF/SS rarely induce long-term remission. Treatment responses might include the overall response rate (complete remission rate + partial remission rate), complete remission, partial remission (remission of at least 50% of the disease burden), response duration, time until next treatment, progression-free survival, overall survival, disease-specific survival and symptoms and quality of life improvement (Tables 4 and 5). Both treatment and prognosis vary according to the stages of the disease.6

Table 4.

Response rates and duration of responses for skin treatments for MF/SS.

Treatment  Staging  Overall response (%)  Complete response (%)  Response duration  References 
Corticosteroid  T1–T2  82–94  25–63  RD: 9 months 
Nitrogen mustard  T1–T2  58.5–93  13.8–80  –  10, 11 
Carmustine  T1–T2  84–98  47–86  –  12 
Bexarotene  T1–T2  54–63  10–21  RD: 25 months  13 
Imiquimod  T1–T2  80  45  –  14 
Resiquimod  T1–T2  75  33  –  15 
NB-UVB  T1–T2  –  54–91  RD: 22 months  16 
PUVA  T1–T2  –  65–85  RD: 23 months  16 
Localized RTun. MF, 30Gy  100  –  DFS, 5 years: 86%  19 
Ia–III, 9–45Gy  94  88  PFS, 5 years: 85%  17 
Total skin irradiation with electronsT1–T2, 36Gy  95  85–88  PFS, 5 years: 50%  20 
Ia–III, 12Gy  88  27  RD: 70.7 weeks  21 

RD, Response Duration; PFS, Progression-Free Survival; DFS, Disease-Free Survival; NB-UVB, narrow-band UVB; RT, Radiotherapy; Gy, Gray; un. MF, unilesional mycosis fungoides.

Table 5.

Response rates and duration of responses for systemic treatments for MF/SS.

Treatment  Staging  Overall response (%)  Complete response (%)  Response Duration  References 
Isotretinoin  MF/ SS  43–80  8–33  RD: 3-15 months  22, 23 
Acitretin  Ia–IV  59–64  4–34.6  RD: 28 months  22–24 
BexaroteneI–IIa  54–67  7–27  RD: 9.9-17.2 months23, 25 
≥IIb  45–54  2–13  23, 25 
Alpha interferon  Ia–IVa  29–80  4–67  RD: 5-8 months  26, 29 
Pegylated alpha-interferon  Ib–III  50–83  33–67  –  28 
Pegylated liposomal doxorubicin  Ib–IV  41–88  RD: 6-13.3 months  32, 33 
Gemcitabine  T3–T4  47–70  11.5–22  RD: 10-15 months  34, 38 
ChlorambucilSS  85  35  RD: 16.5 months36 
III–IVb  100  53.8  35 
Methotrexate, low doseT2  33  33  RD: 15 months  39 
III  56  41  RD: 31 months  39 
Pralatrexate  IIa–IV  40.8  6.1  RD: 6 months  40 
Romidepsin  IIb  34–38  6–7  RD: 15 months  41 
Vorinostat  Ib–IVa  30  –  RD: 5 months  42 
Alemtuzumab  adv. MF–SS  38–84  0–47  RD: 4 months  44, 45 
Brentuximab vedotin  Ia–IVb  50  10  TNT: 13.4 months  46 
Mogamulizumab  Ia–IVb/SS  28 (MF: 21; SS: 37)  PFS: 7.7 months  47 
CHOP  IIb  66  –  TNT: 5.7 months  38 
EPOCH  IIb–IV  80  –  PFS: 8 months  38 
Fludarabine + CFM  IIb–III  55  –  RD: 10 months  38 
Fludarabine + IFN  IIa–IVb  40–58  –  PFS: 5.9 months  38 
IFN + PUVAIa–IVa80.6  75  RD: 32 months  30 
–  –  PFS, 5 years: 75%  30 
Ia–IIa  98  84  PFS, 5 years: 27%  31 
IFN peg + PUVA  Ia–IV  88  44  PFS: 30.9 months  27 
IFN + retinoid  Ia–IIb  38  –  29 
Bexaroteno + PUVA  Ib–IIa  77  31  RD: 5.8 months  52 
Isolated ECP  III–IVa1  24  TNT: 14 months  49–51 
ECP + IFN  III–IVa1  45.4  18.2  –  49, 50 
ECP + IFN + Bexarotene  III–IVa1  88.2  32.4  RD: 4 months  49, 50 

PFS, Progression-Free Survival; RD, Response Duration; TNT, Time to Next Treatment; adv. MF, Advanced Mycosis Fungoides; SS, Sézary syndrome;; CHOP, Cyclophosphamide, Doxorubicin, Vincristine, and Prednisolone; EPOCH, Etoposide, Vincristine, Doxorubicin, Cyclophosphamide, and Prednisolone; ECP, Extracorporeal Photopheresis; CFM, Cyclophosphamide; IFN, Interferon; peg. IFN, pegylated Interferon.

The treatment modalities can be divided into two groups: skin-directed therapies and systemic therapies. The treatments can be done as monotherapy or combined therapy. Skin-directed therapies include topical agents, phototherapy and radiotherapy.7 Systemic therapies include biological response modifiers, immunotherapies and chemotherapeutic agents.8 For early-stage MF (stage Ia – IIa), skin-directed therapies are the treatment of choice, aiming at controlling the disease, improving symptoms and quality of life. In refractory early-stage MF, late-stage MF (stage ≥ IIb) and SS, systemic treatment, combined or not with skin-directed therapy, is required. Treatment modalities are reviewed in this article.

The approval and availability of drugs in the United States, Europe and Brazil are described in Tables 6 and 7. Extracorporeal photopheresis, narrow-band UVB phototherapy, psoralen-UVA (PUVA) photochemotherapy, and radiotherapy are more widely available.

Table 6.

Approval of topical treatments for cutaneous T-cell lymphoma in the United States, Europe and Brazil, according to the package insert registered in the local regulatory agencies (FDA, EMA and ANVISA), respectively.

Treatment  Class of Medication  United States of America (FDA)  Europe (EMA)  Brazil (ANVISA) 
CorticosteroidCorticosteroidAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
MechlorethamineAlkylating agentAvailable.  Available.  Not available. 
Approved for topical treatment of MF Ia and Ib in patients who previously received some type of skin therapy.  Approved for topical treatment of CTCL.  Not approved. 
CarmustineAlkylating agentAvailable for intravenous therapy.  Available for intravenous therapy.  Available for intravenous therapy. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
BexaroteneRetinoidAvailable.  Not available.  Not available. 
Approved for skin lesions in patients with CTCL Ia and Ib with refractory or persistent disease after other therapies or those who do not tolerate other therapies.  Not approved.  Not approved. 
ImiquimodImmune response modifierAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
ResiquimodImmune response modifierNot available.  Available.  Not available. 
Not approved.  Sole designation for the treatment of CTCL.  Not approved. 

FDA, Food and Drug Administration (https://www.fda.gov/drugs); EMA, European Medical Agency (https://www.ema.europa.eu/en); ANVISA, National Health Surveillance Agency (Agência Nacional de Vigilância Sanitária; http://portal.anvisa.gov.br/); CTCL, Cutaneous T-Cell Lymphoma; MF, Mycosis Fungoides.

Table 7.

Approval of systemic treatments for cutaneous T-cell lymphomas in the United States, Europe and Brazil, according to the package insert registered at the local regulatory agencies (FDA, EMA and ANVISA), respectively.

Treatment  Class of medication  United States of America (FDA)  Europe (EMA)  Brazil (ANVISA) 
IsotretinoinRetinoidAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
AcitretinRetinoidAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
BexaroteneRetinoidAvailable.  Available.  Not available. 
Approved for cutaneous manifestations of CTCL in patients refractory to at least one previous systemic therapy.  Approved for cutaneous manifestations of CTCL in patients refractory to at least one previous systemic therapy.  Not approved. 
Alpha-interferonImmunomodulatorAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
Pegylated liposomal doxorubicinAnthracycline chemotherapeutic drugAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
GemcitabinePyrimidine antagonist chemotherapeutic drugAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
ChlorambucilAlkylating chemotherapeutic drugAvailable.  Not available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Not approved.  Approved for non-Hodgkin's lymphomas. 
MethotrexateAntimetaboliteAvailable.  Available.  Available. 
Approved for advanced MF.  Approved, but does not have a package insert indication for CTCL.  Approved for non-Hodgkin's lymphomas. 
PralatrexateAntimetaboliteAvailable.  Not available.  Not available. 
Approved for recurrent or refractory peripheral T-cell lymphomas.  Not approved.  Not approved. 
RomidepsinHDAC inhibitorAvailable.  Not available.  Not available. 
Approved for patients with CTCL who received at least one previous systemic therapy.  Not approved.  Not approved. 
VorinostatHDAC inhibitorAvailable.  Not available.  Not available. 
Approved for patients with CTCL with progressive, persistent, or recurrent disease after two systemic therapies.  Not approved.  Not approved. 
Brentuximab vedotinAntibody-drug conjugateAvailable.  Available.  Available. 
Approved for patients with MF or PCALCL expressing CD30 who received previous systemic treatment.  Approved for patients with CD30-positive CTCL who received at least one previous treatment.  Approved for PCALCL or patients expressing CD30 who received previous systemic treatment 
AlemtuzumabMonoclonal antibodyAvailable.  Available.  Available. 
Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL.  Approved, but does not have a package insert indication for CTCL. 
MogamulizumabMonoclonal antibodyAvailable.  Available.  Not available. 
Approved for patients with relapsing or refractory MF or SS after at least one previous systemic therapy.  Approved for patients with MF or SS after at least one previous systemic therapy.  Not approved. 

FDA, Food and Drug Administration (https://www.fda.gov/drugs); EMA, European Medical Agency (https://www.ema.europa.eu/en); ANVISA, National Health Surveillance Agency (Agência Nacional de Vigilância Sanitária; http://portal.anvisa.gov.br/); CTCL, Cutaneous T-Cell Lymphomas; MF, Mycosis Fungoides; HDAC, histone deacetylase; PCALCL, Primary Cutaneous Anaplastic Large Cell Lymphoma; SS, Sézary Syndrome.

Skin-directed therapiesTopical drug therapiesCorticosteroids

Topical corticosteroids are the most widely used anti-inflammatory agents in dermatology. They inhibit the binding of lymphocytes to the endothelium, inhibit intercellular adhesion and induce apoptosis of neoplastic lymphoid cells. They are often formulated as cream, ointment, lotion or gel. According to the topical corticosteroid and the formulation, the drug potency can be stratified into seven classes: class I (super-high potency, e.g., 0.05% clobetasol propionate cream); class II (high potency, e.g., 0.05% betamethasone dipropionate ointment; class III (medium-high potency, e.g., 0.05% betamethasone dipropionate cream); class IV (medium potency, e.g., 0.1% triamcinolone acetonide cream); class V (lower-medium potency, e.g., 0.1% betamethasone valerate cream), class VI (low potency, e.g., 0.05% desonide cream) and class VII (lowest potency, e.g., 1% hydrocortisone acetate cream). Topical steroids are applied once or twice a day, for weeks to months, until complete regression or considerable improvement of the lesions is achieved. Prolonged use of topical corticosteroids can result in skin atrophy, striae and mild skin irritation. Systemic absorption with the use of high-potency corticosteroids applied to large surfaces of the skin, causing clinically evident adrenal insufficiency and Cushing's syndrome, are rarely observed.7,9

Mechlorethamine

Mechlorethamine, chlormethine or nitrogen mustard, is an alkylating chemotherapeutic agent that affects rapidly-dividing cells, acting as a cytotoxic agent in DNA. Nitrogenous mustard was originally available as a lyophilized powder. The powder could then be used in a cream or aqueous solution. The cream was prepared at the initial concentration of 10 to 20 mg of nitrogen mustard per 100 g of petrolatum or similar. Regarding the aqueous preparation, the patients prepared the solution at a concentration of 10 to 20 mg per 100 mL of water. The preparations were applied once a day on specific lesions or the total skin surface (depending on the T-classification), except in the genital area, for weeks to months. It is currently available in the United States and Europe as a 0.02% gel formulation for more localized use. Short-term adverse events include pruritus, burning sensation and irritant or allergic contact dermatitis. In the long term, skin hyper- or hypopigmentation and a slight increase in the risk of non-melanoma skin cancer can be observed, especially when combined with other therapies, such as phototherapy. The topical use of this substance does not cause myelosuppression.7,10,11

Carmustine

Carmustine, also known as bischlorethyl nitrosourea (BCNU), is an alkylating agent that forms cross-links in DNA, preventing DNA replication and transcription. To prepare the alcoholic solution, 100 mg of powdered carmustine is dissolved in 5 mL of 95% ethanol. This 5 mL solution is then placed in a glass container and diluted with an additional 50 mL of 95% ethanol. This results in a concentration of 2 mg / mL (0.2%), called stock solution. For total body use, 5 mL (10 mg of BCNU) of the stock solution is diluted in 60 mL of water. It is applied once a day. For localized lesions, the solution volume is adjusted to the affected skin area. For extremely limited disease (< 3% of skin affected), applications can be done with the undiluted stock solution. Topical carmustine can also be incorporated into a petrolatum ointment at a concentration of 10 mg/100 g of petrolatum. Usually, the maximum daily dose is 10 mg/day, with a treatment duration of six to twelve weeks. This treatment is usually not recommended for patients with skin involvement >3%, as systemic absorption can lead to hematological toxicity including leukopenia, thrombocytopenia and anemia. Local reactions are commonly observed, and most patients develop erythema and a burning sensation, especially in the skin folds.7,12

Bexarotene

Bexarotene is a retinoid (derived from vitamin A) that selectively activates retinoid X receptors, inducing cell differentiation and apoptosis. Topical bexarotene is available in a 1% formulation. Bexarotene is applied to the lesions every night during the first week of treatment and then twice a day. The use of this medication is generally limited to patients with less than 15% of the body surface affected. The most common adverse effects are mild to moderate irritant dermatitis, pruritus and burning sensation at the application site.7,13

Imiquimod and resiquimod

Imiquimod is a toll-like receptor 7 agonist that increases interferon production. Interferon leads to antiviral, antiproliferative and antiangiogenic effects. It also stimulates Langerhans cells to migrate to the lymph nodes, activating T lymphocytes. Topical imiquimod is available as a 5% cream and is applied to the lesions, three to five times a week, until their resolution. The most often reported toxicity is a local inflammatory reaction, with erythema, edema, vesicles, and ulceration/erosion. These signs reflect the immune system activation and, if no inflammatory response is observed, an adequate response to therapy is less likely to occur. Some patients may experience systemic symptoms (e.g., flu-like symptoms).7,14 Resiquimod is an agonist of toll-like receptors 7 and 8. Toll-like receptor 8 is expressed by dendritic cells derived from myeloid cells and these are strongly activated by the drug. Similar to imiquimod, as a toll-like receptor 7 agonist, interferon production is increased. The drug, in a 0.06% or 0.03% gel, is applied to the skin lesions, three times a week, for eight weeks. There is less skin irritation compared to imiquimod, with erythema and superficial erosions. Low fever may occur for a short period. No serious adverse events have been described.7,15

Radiation therapiesPhototherapy

This is a physical therapy based on ultraviolet (UV) light. The UV light acts by stopping the cell cycle or apoptosis of keratinocytes, Langerhans cells and lymphocytes and by selectively decreasing the production of pro-inflammatory cytokines by T-cells. There are different treatment modalities based on the wavelength and its association or not with a psoralen (photosensitizing agent). The most widely used are narrow-band UVB phototherapy (NB-UVB) and PUVA (psoralen + ultraviolet A), also known as photochemotherapy. It is an important treatment option for patients with early-stage MF or as adjunctive therapy for more advanced stages. The treatment dose and duration vary between institutions, as well as the use or not of maintenance therapy after the lesions improve (being less frequently used to reduce the total accumulated dose of UV).7,16

Narrow-band UVB

Phototherapy with NB-UVB comprises a wavelength from 311 to 313 nm. Due to its shorter wavelength, it is absorbed mainly in the epidermis with less capacity to penetrate more deeply into the skin when compared to UVA. Therefore, its main direct effects are on epidermal keratinocytes, Langerhans cells, follicular infundibulum, and upper dermal cells, including lymphocytes. It is more frequently used when the disease is in the stage of non-infiltrated lesions (patches) (T1a and T2a). It has advantages over PUVA because it does not require the use of a photosensitizing agent (psoralen), with a lower risk of skin cancer (with cumulative doses) and can be used during pregnancy. The treatment is administered on an outpatient basis, three to five times a week, with a gradual increase in the dose. The most common acute adverse events (within 24 hours) are erythema, pruritus, burning sensation, blistering, tanning, and xerosis. Regarding skin neoplasms, a literature review published in 2005 that included more than 3,400 patients (mainly patients with psoriasis) treated with broadband UVB (BB-UVB) or NB-UVB, did not show an increase in the risk of skin cancer, except for those treated with UVB and PUVA. Chronic exposure to UV light is associated with the formation of cataracts and ocular pterygium. The use of eye protection during phototherapy with UVB is indicated to prevent this risk. However, for those who need periocular treatment, it is safe to undergo the sessions with their eyes closed, since there is only a negligible transmission of UV light through the eyelids.7,16

PUVA photochemotherapy

In this treatment modality, photosensitizing agents (psoralens) are used orally or topically before exposure to UVA (wavelength from 320 to 400 nm). UVA (especially UVA1 - 340 at 400 nm) can penetrate the entire dermis, affecting lymphocytes in the deep dermis, fibroblasts, dermal dendritic cells, mast cells, endothelial cells, macrophages, and deeper parts of the hair follicle. It is a better option for the treatment of more infiltrated lesions in plaques and folliculotropic MF. PUVA treatment is administered three times a week until lesion regression is achieved. Eye protection should be worn not only during sessions, but for 24 hours after ingesting the psoralen. It should be noted that cumulative UV doses are associated with an increased risk of associated skin malignancies, mainly squamous cell carcinoma, but also basal cell carcinoma. There are still controversies regarding the increased risk for melanoma. Oral psoralen can cause nausea and, rarely, hepatotoxicity. Psoralens are absorbed by the lens, although they disperse within 24 hours without exposure to UVA. In the presence of UVA, 8-MOP binds to nucleic acids and proteins in the lens and remains for long periods, theoretically increasing the risk of cataracts. Therefore, it is recommended to use UVA eye protection during exposure to sunlight, for 24 hours after ingesting the psoralen.7,16

Radiotherapy

Radiotherapy (RT) involves the use of ionizing radiation through photons or electrons to destroy neoplastic cells. Ionizing radiation acts by causing damage to the neoplastic tissue DNA, leading to cell death. Mycosis fungoides is a very radiosensitive tumor and radiotherapy is a very effective treatment modality.7

Local radiotherapy

For individual or localized lesions, conventional photon radiotherapy or electron beam radiotherapy is used.6,7 Low-dose regimens with 8 Gy in two fractions are effective for plaques or small tumors. For the treatment of large areas, smaller doses per fraction (20–30 Gy in 10 to 15 fractions) should be considered. The clinical target volume of radiotherapy is defined with a margin of at least 1 cm around the lesion. Peripheral nodal disease and visceral disease can also be treated with localized RT. MF is a multifocal disease, and local control with radiotherapy is frequently used as a palliative approach. Therefore, it is recommended to use the minimum dose of radiotherapy to attain local control, which allows retreatments or treatments in adjacent areas. The adverse event observed in localized radiotherapy is radiodermatitis, and the radiodermatitis recall phenomenon may occur in patients treated with chemotherapy.17–19

Total skin electron beam therapy

Total skin electron beam therapy (TSEBT) is a special technique that allows homogeneous irradiation of the entire skin surface. The usual total dose for treatment is 36 Gy, administered as one to two Gy per session for five to nine weeks.20 Complete remission rates are high; however, recurrences are frequent. Low-dose TSEBT is performed with 12 Gy, one Gy per fraction for three weeks.21 Consensus guidelines on the use of TSEBT in MF have been published.18 Treatment-related toxicity depends on the radiation dose used and the tumor location. Adverse events include erythema, hair loss, temporary nail growth arrest, hand and foot edema, minor nasal bleeding, blisters on the fingers and toes, anhidrosis, mild parotitis, gynecomastia in men, keratitis due to the use of internal eye shields, permanent nail dystrophy, xerosis, permanent alopecia, dysesthesia in the fingers.7 Low-dose TSEBT is better tolerated and adverse events are transient and milder when compared to the standard dose. However, the response rates are lower.21

Systemic therapyRetinoids: isotretinoin, acitretin and bexarotene

Retinoids are natural and synthetic analogs of vitamin A that bind to several classes of proteins, including retinoid-binding proteins and nuclear retinoid receptors. They lead to the activation of DNA regulatory regions involved in the regulation of cell growth, differentiation and apoptosis. The nuclear retinoid receptors belong to two families: Retinoic acid receptors (RARs) and retinoid X receptors (RXRs). Isotretinoin is a first-generation non-aromatic retinoid. It was the first retinoid used for the off-label treatment of CTCL. It is used in daily oral doses of 0.2 to 1.0 mg/kg. Adverse events include dry skin and mucous membranes, the elevation of blood lipids and teratogenicity (pregnancy should be avoided for one month after treatment discontinuation).22 Acitretin is a second-generation monoaromatic retinoid. Their structure makes them more lipophilic with greater bioavailability than the first-generation retinoids. It is used in daily oral doses of 0.3–0.5 mg/kg. The safety profile is similar to that of isotretinoin, but pregnancy should be avoided for two to three years after treatment discontinuation.22 Bexarotene is a third-generation polyaromatic retinoid that is highly selective for the RXR receptor. It is administered at a daily oral dose of 300 mg/m2. The safety profile is similar to that of isotretinoin and acitretin, but it has additional adverse events, such as central hypothyroidism and hypertriglyceridemia in most patients. Pregnancy should be avoided for one month after treatment discontinuation.8,23–25

Interferon

Interferon (IFN) is a Th1 cytokine. There are three types of recombinant interferons (alpha, beta, gamma) currently available for therapeutic use. IFN-α can be found in its pegylated form. All recombinant IFNs are active in the treatment of MF/SS, but IFN-α is the most frequently studied. IFN-α regulates the cell cycle, promotes the suppression of oncogenes and modulates cell adhesion.26 IFN-γ is more frequently studied and used in Japan. Treatment with IFN-α is usually started with a dose of 3 million units via subcutaneous route, three times a week. The dose can be increased up to 9 million units per application. Pegylated IFN-α, a formulation in which the drug is encapsulated in liposomes, resulting in increased half-life and better accumulation in tumor tissues, is administered via subcutaneous route, at a dose of 1.5 μg/kg, once a week.27,28 IFN-γ is administered subcutaneously at a dose of 50 μg/m2 for patients with a body surface area >0.5 m2 and 1.5 μg/kg/dose for patients with a body surface area ≤ 0.5 m2. It is used daily or three times a week.29 Adverse events from interferons are dose-dependent and include flu-like symptoms, thyroid dysfunction, increased transaminases, leukopenia, thrombocytopenia, depression, and arrhythmias.29–31

Pegylated liposomal doxorubicin

Doxorubicin is an anthracycline cytotoxic agent. It binds to nucleic acids, inhibiting the progression of topoisomerase II, interrupting the DNA replication process. Pegylated liposomal doxorubicin is encapsulated in liposomes, resulting in increased half-life and better accumulation in tumor tissues. Pegylated liposomal doxorubicin is administered intravenously, at a dose of 20 mg/m2 on days 1 and 15, every 28 days. The main adverse events are usually mild or moderate and include anemia, asthenia, nausea, vomiting, and palmoplantar erythrodysesthesia.8,32,33

Gemcitabine

Gemcitabine (2',2'-difluorodeoxycytidine) is a classic chemotherapeutic agent from the family of nucleoside analogs. It acts by blocking the formation of new DNA, resulting in cell death. It is administered intravenously, in doses of 1200 mg/m2 on days 1, 8, and 15 of a 28-day regimen. Treatment is well tolerated and the main adverse event is hematological toxicity, which is generally mild.8,34

Chlorambucil

Chlorambucil is an alkylating agent and forms cross-links in DNA, causing DNA damage and affecting replication and transcription. Chlorambucil can be used orally in a continuous regimen with 2–6 mg/day of chlorambucil plus 20 mg/d of prednisone, or in pulses of 10 to 12 mg/day of chlorambucil for 3 days and fluocortolone, with a dose of 75 mg on the first day, 50 mg on the second day and 25 mg on the third day, every two weeks.35,36 Doses and intervals can be reduced and prolonged as the disease improves. The continuous and prolonged use of chlorambucil increases the risk of myelosuppression and the development of leukemia, especially acute myeloid leukemia.

Combined chemotherapy

The most frequently used combinations are Cyclophosphamide, Doxorubicin, Vincristine, and Prednisone (CHOP); Cyclophosphamide, Vincristine, and Prednisone (CVP); Cyclophosphamide, Doxorubicin, Vincristine, and Etoposide (CHOEP); CVP plus Methotrexate (MTX). Combined chemotherapy regimens are associated with high response rates (70%–80%), but often of short duration (around 4 months). Multidrug chemotherapy is also associated with myelosuppression and infectious complications. Therefore, with rare exceptions, the sequential administration of a single chemotherapeutic drug is the strategy of choice.37,38

Antifolate drugs: methotrexate and pralatrexate

MTX is an antifolate-type antimetabolite. It competitively inhibits dihydrofolate reductase and, consequently, the folic acid metabolism, acting by inhibiting the synthesis of DNA, RNA, thymidylates and proteins. Low-dose MTX has been used to treat early-stage MF and SS for many years.39 MTX is used in a dose of 10 to 25 mg, once a week, orally or subcutaneously. The adverse effects include gastrointestinal symptoms (nausea, vomiting, stomatitis, diarrhea), anemia, leukopenia, thrombocytopenia, increased transaminases, liver fibrosis, and pneumonitis.8,40 Pralatrexate is also a folate analog with activity demonstrated in patients with MF/SS. It is administered intravenously in a dose of 15 mg / m2 per week for three weeks, in four-week cycles. Adverse events are similar to those seen with MTX, but they tend to be more common and severe. The most common side effects include mucositis, fatigue, nausea, vomiting, anorexia, skin toxicity, epistaxis, and anemia.8,40

Histone deacetylase inhibitors: romidepsin and vorinostat

Histone Deacetylase (HDAC) is a class of enzymes responsible for catalyzing the removal of acetyl groups from histones, being crucial modulators of transcriptional epigenetic regulation. Two drugs from this class have FDA approval for use in CTCL, mainly in refractory cases: romidepsin and vorinostat.41,42 Romidepsin is administered as a single agent in a dose of 14 mg/m2 intravenously on days 1, 8 and 15 of a 28-day cycle. The most common related adverse events are nausea and fatigue.43 Vorinostat is an oral HDAC inhibitor. It is administered at a daily dose of 400 mg per day. If not tolerated, it can be reduced to 300 mg/day or 300 mg, five days a week. The most common adverse events are diarrhea, fatigue, nausea, and anorexia.43

Alemtuzumab

Alemtuzumab is a humanized anti-CD52 monoclonal antibody. CD52 is a surface glycoprotein present in T and B lymphocytes, monocytes and macrophages. Alemtuzumab binds to CD52, causing destruction of neoplastic cells by antibody-dependent cell cytotoxicity and complement fixation. Response rates are higher in SS than in MF, because alemtuzumab leads to the depletion of central memory T-cells in the blood and skin of patients with SS. On the other hand, the drug does not affect memory/effector T-cells residing on the skin in MF. Recent evidence suggests that alemtuzumab is not effective in tumoral or transformed MF. The standard dose is 30 mg administered intravenously, three times a week, for up to 12 weeks.8,44 Subcutaneous alemtuzumab can also be used in a low-dose regimen of 10 to 15 mg every other day, 3 times a week.45 Infusion reactions (fever, nausea, hypotension, fatigue, rash, hives, bronchospasm) are seen in more than half of the patients. Cytopenias (lymphopenia, neutropenia, anemia, thrombocytopenia) are observed in almost all patients. Severe infections (cytomegalovirus, generalized herpes simplex, fatal aspergillosis, and mycobacterial pneumonia), can be observed, especially in patients heavily pretreated.8 The low-dose regimen can reduce infectious complications in patients with MF.45 The treatment with alemtuzumab requires antibiotic and antiviral prophylaxis, as well as careful observation for the development of cardiac infection and toxicity.8

Brentuximab vedotin

Brentuximab vedotin (BV) is an antibody-drug conjugate directed to the CD30 molecule. CD30 belongs to the tumor necrosis factor receptor superfamily. The drug in the antibody-drug conjugate is monomethyl auristatin E (MMAE), an anti-tubulin agent. In normal tissues, CD30 has an expression profile that is rather restricted to activated T, B and NK/T-cells, but is highly expressed in Reed Sternberg cells of Hodgkin's lymphoma, in anaplastic large-cell lymphoma and other non-Hodgkin lymphoma subtypes, for instance, in primary cutaneous anaplastic large-cell lymphoma (pcALCL) and certain cases of MF. This expression profile makes CD30 an ideal target for therapies based on monoclonal antibodies. After the binding of BV to CD30 on the surface of neoplastic cells and their internalization, MMAE release occurs. MMAE will then exert its potent cytostatic effect, inhibiting the assemblage of the microtubules, inducing the cell cycle to stop, and resulting in death due to apoptosis of tumor cells. The safety and efficacy of BV were evaluated in the first phase 3 study against a standard therapy (MTX or bexarotene) for CTCL, demonstrating high rates of durable and clinically significant responses. The typical starting dose is 1.8 mg/kg given intravenously every three weeks. The main toxicities are peripheral neuropathy, neutropenia, fatigue, nausea, and alopecia.46

Mogamulizumab

Mogamulizumab is a humanized monoclonal antibody that targets the C-C chemokine receptor type 4 (CCR4) expressed on neoplastic cells. CCR4 is expressed on the surface of tumor cells of most patients with adult T-cell lymphoma/leukemia (ATLL) and is selectively expressed in other subtypes of peripheral T-cell lymphoma and cutaneous T-cell lymphoma. After binding to its target, mogamulizumab acts through antibody-dependent cell-mediated cytotoxicity to destroy tumor cells. Mogamulizumab is administered intravenously in a dose of 1.0 mg/kg weekly, for four weeks, followed by a dose every two weeks until disease progression. Infusion-related and drug-related rashes are common; other toxicities include diarrhea, nausea, thrombocytopenia, dysgeusia, and elevated serum creatinine levels.47

Extracorporeal photopheresis

Extracorporeal photopheresis (ECP) is an immunomodulatory therapy in which leukapheresis removes the patient's leukocytes, which are then treated with 8-methoxypsoralen and UVA and reinfused in the patient. It is the first-line treatment for SS and erythrodermic MF.6,48 Each cycle of ECP is generally administered on two consecutive days every two to four weeks for at least six months. With the development of 8-MOP in solution, ECP can be administered directly into the apheresis bag, and the patient is not exposed to the systemic drug absorption, minimizing adverse gastrointestinal effects and systemic photosensitivity. Sporadic side effects include headache, pyrexia, myalgia, mild anemia, thrombocytopenia, and photophobia. Hypotension, vasovagal syncope, infection at the injection site, worsening of skin lesions and sepsis, usually due to central venous access, are rare. There are no reports of opportunistic infections or malignancies, as ECP is not an immunosuppressive treatment.48–51

Combined therapies

The combination of treatments is a well-established strategy to increase therapeutic efficacy in treatments for MF. It includes combining skin-directed therapies with systemic ones, or two or more systemic therapies. The most widely used combinations are retinoids and PUVA (RE-PUVA), interferon, and PUVA or ECP with interferon and/or bexarotene.49,52

Hematopoietic stem cell transplantation (HSCT)

Allogeneic stem cell transplantation (allo-HSCT) can induce lasting remissions and is the only treatment with curative intent. Due to the high morbidity and mortality rates associated with allo-HSCT, good patient selection is essential for a successful treatment. Careful counseling is necessary and the indication should focus mainly on younger patients with good performance, with advanced stages of the disease and low tumor burden at the time of transplantation and who are aware of the high risk of progression and poor prognosis.53

Response rates and treatment recommendations

The response rates and duration with the different skin-directed treatments, systemic treatments and combinations of treatments reported in the literature are shown in Tables 4 and 5. It is important to note that the studies are methodologically heterogeneous and many are not controlled. The summary of the treatment recommendations of the Cutaneous Lymphoma Group of the Dermatology and Hematology Divisions of HC-FMUSP can be seen in Table 8. The recommendations take into account the clinical experience and the best scientific evidence for treatments at different stages of the disease. In refractory early disease and advanced disease, despite the use of systemic therapies (biological response modifiers and/or chemotherapy), the association of skin-directed therapies is frequent. The availability and/or approval in Brazil of the described treatments do not guarantee patient access to the medications, both in the public and private sectors. Several factors can influence access to treatments, such as institutional clinical protocols, state guidelines, supplementary health treatment protocols, particularities of health plans/health insurance, opinions of medication standardization commissions, or even individual requests for medications, made by the patients. There are drugs, both for skin-directed treatments and systemic treatments, which are of crucial importance in the treatment of MF and SS, not yet available in Brazil. Thus, it is suggested that the recommendations be evaluated and adapted to the reality of each service. The authors believe that the development of a National Clinical Protocol for the Approach of Cutaneous Lymphomas is fundamental to guarantee universal access, for all patients, to the different treatments available in the country. Unquestionably, the best care given to cancer patients translates into a reduction in the physical and emotional impacts related to the disease itself and the individual, as well as in a significant reduction in the associated economic costs, both direct and indirect ones.

Table 8.

Recommendations of the Cutaneous Lymphomas Group of the Dermatology and Hematology Divisions of HC-FMUSP for the treatment of mycosis fungoides and Sézary syndrome.

CS  First-line  Second line  Third line 
IaTopical corticosteroids  Localized topic PUVA  Localized radiotherapy (if regionalized disease)
Phototherapy with NB-UVB  PUVA
Topical mechlorethaminea 
Topical carmustine 
Bexarotene gela 
Imiquimod / Resiquimod 
Ib, IIaPhototherapy with NB-UVB  Systemic retinoidsb ± phototherapy with NB-UVB or PUVA  Total skin electron beam radiotherapy 
PUVA phototherapy  Alpha interferon ± phototherapy with NB-UVB or PUVA  Low-dose methotrexate 
IIbSystemic retinoids ± phototherapy with NB-UVB or PUVA ± localized RTTotal skin electron beam radiotherapy  Monochemotherapy (gemcitabine, pegylated liposomal doxorubicin)
Low-dose methotrexate 
Brentuximab vedotin (if CD30-positive)HDACia 
Alpha-interferon ± phototherapy with NB-UVB or PUVA ± localized RTMogamulizumab 
Polychemotherapy (CHOP type) 
Allogeneic hematopoietic stem cell transplantation 
IIIa, IIIbSystemic retinoidsb ± PUVA  Chlorambucil + prednisone  HDACia 
Alpha interferon ± PUVA  Low-dose methotrexate  Polychemotherapy (CHOP type) 
ECP ± systemic retinoidsb ± alpha-interferon  Monochemotherapy (gemcitabine, pegylated liposomal doxorubicin)  Allogeneic hematopoietic stem cell transplantation 
IVa1, SSECP ± alpha-interferon ± systemic retinoidsbChlorambucil + prednisone  Monochemotherapy 
Low-dose methotrexate  Polychemotherapy (CHOP type) 
Alpha interferon ± PUVAAlemtuzumab  Allogeneic hematopoietic stem cell transplantation
Mogamulizumaba 
IVa2Monochemotherapy (gemcitabine, pegylated liposomal doxorubicin)Brentuximab vedotin (if CD30-positive)HDACia 
Polychemotherapy (CHOP type) 
Radiotherapy if localized nodal disease  Allogeneic hematopoietic stem cell transplantation 
IVbMonochemotherapy (gemcitabine, pegylated liposomal doxorubicin)Brentuximab vedotin (if CD30-positive)Polychemotherapy (CHOP type) 
Allogeneic hematopoietic stem cell transplantation 

HC-FMUSP, Hospital de Clínicas, Faculdade de Medicina, Universidade de São Paulo; CS, clinical-stage; PUVA, psoralen + ultraviolet A; NB-UVB, narrow-band UVB; RT, radiotherapy; HDACi, histone deacetylase inhibitors; CHOP, cyclophosphamide, doxorubicin, vincristine, and prednisolone; SS, Sézary syndrome; ECP, extracorporeal photopheresis.

a

Agent not available in Brazil.

b

Bexarotene is not available in Brazil, being replaced by acitretin and, less commonly, by isotretinoin.

Conclusion

As most of the available treatments for MF and SS rarely induce long periods of remission or complete cure, the main treatment objectives are to control the disease symptoms, improve patient quality of life, prolong progression-free survival and overall survival. Also, as an indolent disease, with a 5-year disease-related survival of approximately 90% in most cases, and with the importance of the tumor microenvironment in controlling disease progression, one should initially choose therapies that can be used in the long term, postponing the use of aggressive systemic therapies, such as multidrug chemotherapy, reserved only for rare occasions. In the early stages of the disease, skin-directed therapies constitute the standard of care. In advanced or refractory disease, systemic therapies are used, alone or in combination with skin-directed therapies, despite the rarely observed complete remission rates and the few controlled studies that support them. The role of allo-HSCT is yet to be defined, but it can be useful in some highly selected patients. Treatment availability is also quite heterogeneous, both inside one country and among different countries.54 It is expected that the effort made by specialized centers worldwide, with the objective of conducting international multicentric and multidisciplinary studies, will provide a better understanding of the disease, the development of new treatments and a more efficient and uniform standard of care for patients with MF and SS.

Financial support

None declared.

Authors’ contributions

José Antonio Sanches: Conception and elaboration of the manuscript.

Jade Cury-Martins: Conception and elaboration of the manuscript.

Rodrigo Martins Abreu: Conception and elaboration of the manuscript.

Denis Miyashiro: Interpretation of data and critical review of the manuscript.

Juliana Pereira: Interpretation of data and critical review of the manuscript.

All authors have approved the final version of the manuscript and agree to be responsible for all aspects of the research, ensuring that issues related to the accuracy or integrity of any part of the study are adequately investigated and resolved.

Conflicts of interest

Cury-Martins J and Pereira J were sub-investigators in a study funded by Takeda and received fees from Takeda for occasional lectures. Miyashiro D has nothing to declare. Abreu RM is Takeda's scientific medical manager in onco-hematology. Sanches JA was the main investigator of a study funded by Takeda.

References
[1]
R. Willemze, L. Cerroni, W. Kempf, E. Berti, F. Facchetti, S.H. Swerdlow, et al.
The 2018 update of the WHO-EORTC classification for primary cutaneous lymphomas.
Blood, 133 (2019), pp. 1703-1714
[2]
E.A. Olsen.
Evaluation, Diagnosis, and Staging of Cutaneous Lymphoma.
Dermatol Clin, 33 (2015), pp. 643-644
[3]
M.E. Kadin, L.C. Hughey, G.S. Wood.
Large-cell transformation of mycosis fungoides-differential diagnosis with implications for clinical management: a consensus statement of the US Cutaneous Lymphoma Consortium.
J Am Acad Dermatol, 70 (2014), pp. 374-376
[4]
D. Miyashiro, J.A. Sanches.
Cutaneous manifestations of adult T-cell leukemia/lymphoma.
Semin Diagn Pathol, 37 (2020), pp. 81-91
[5]
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 Sezary 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
[6]
F. Trautinger, J. Eder, C. Assaf, M. Bagot, A. Cozzio, R. Dummer, et al.
European Organisation for Research and Treatment of Cancer consensus recommendations for the treatment of mycosis fungoides/Sezary syndrome - Update 2017.
Eur J Cancer, 77 (2017), pp. 57-74
[7]
E.S. Tarabadkar, M.M. Shinohara.
Skin Directed Therapy in Cutaneous T-Cell Lymphoma.
Front Oncol, 9 (2019), pp. 260
[8]
O. Alpdogan, S. Kartan, W. Johnson, K. Sokol, P. Porcu.
Systemic therapy of cutaneous T-cell lymphoma (CTCL).
Chin Clin Oncol, 8 (2019), pp. 10
[9]
H.S. Zackheim.
Treatment of patch-stage mycosis fungoides with topical corticosteroids.
Dermatol Ther, 16 (2003), pp. 283-287
[10]
E.C. Vonderheid, E.T. Tan, A.F. Kantor, L. Shrager, B. Micaily, E.J. Van Scott.
Long-term efficacy, curative potential, and carcinogenicity of topical mechlorethamine chemotherapy in cutaneous T cell lymphoma.
J Am Acad Dermatol, 20 (1989), pp. 416-428
[11]
S.R. Lessin, M. Duvic, J. Guitart, A.G. Pandya, B.E. Strober, E.A. Olsen, et al.
Topical chemotherapy in cutaneous T-cell lymphoma: positive results of a randomized, controlled, multicenter trial testing the efficacy and safety of a novel mechlorethamine, 0.02%, gel in mycosis fungoides.
JAMA Dermatol, 149 (2013), pp. 25-32
[12]
H.S. Zackheim, E.H.J. Epstein, W.R. Crain.
Topical carmustine (BCNU) for cutaneous T cell lymphoma: a 15-year experience in 143 patients.
J Am Acad Dermatol, 22 (1990), pp. 802
[13]
P. Heald, M. Mehlmauer, A. Martin, C. Crowley, R. Yocum, S. Reich, et al.
Topical bexarotene therapy for patients with refractory or persistent early-stage cutaneous T-cell lymphoma: results of the phase III clinical trial.
J Am Acad Dermatol, 49 (2003), pp. 801
[14]
D.J. Lewis, Y.A. Byekova, D.A. Emge, M. Duvic.
Complete resolution of mycosis fungoides tumors with imiquimod 5% cream: a case series.
J Dermatolog Treat, 28 (2017), pp. 567-569
[15]
A.H. Rook, J.M. Gelfand, M. Wysocka, A.B. Troxel, B. Benoit, C. Surber, et al.
Topical resiquimod can induce disease regression and enhance T-cell effector functions in cutaneous T-cell lymphoma.
Blood, 126 (2015), pp. 1452-1461
[16]
E.A. Olsen, E. Hodak, T. Anderson, J.B. Carter, M. Henderson, K. Cooper, et al.
Guidelines for phototherapy of mycosis fungoides and Sezary syndrome: A consensus statement of the United States Cutaneous Lymphoma Consortium.
J Am Acad Dermatol, 74 (2016), pp. 27-58
[17]
R. Piccinno, M. Caccialanza, E. Cuka, S. Recalcati.
Localized conventional radiotherapy in the treatment of Mycosis Fungoides: our experience in 100 patients.
J Eur Acad Dermatol Venereol, 28 (2014), pp. 1040-1044
[18]
L. Specht, B. Dabaja, T. Illidge, L.D. Wilson, R.T. Hoppe.
International Lymphoma Radiation Oncology G. Modern radiation therapy for primary cutaneous lymphomas: field and dose guidelines from the International Lymphoma Radiation Oncology Group.
Int J Radiat Oncol Biol Phys, 92 (2015), pp. 32-39
[19]
B. Micaily, C. Miyamoto, G. Kantor, S. Lessin, A. Rook, L. Brady, et al.
Radiotherapy for unilesional mycosis fungoides.
Int J Radiat Oncol Biol Phys, 42 (1998), pp. 361-364
[20]
P.A. Quirós, G.W. Jones, B.M. Kacinski, I. Braverman, P. Heald, R. Edelson, et al.
Total skin electron beam therapy followed by adjuvant psoralen/ultraviolet-A light in the management of patients with T1 and T2 cutaneous T-cell lymphoma (mycosis fungoides).
Int J Radiat Oncol Biol Phys, 38 (1997), pp. 1027
[21]
R. Hoppe, C. Harrison, M. Tavallaee, S. Bashey, U. Sundram, S. Li, et al.
Low-dose total skin electron beam therapy as an effective modality to reduce disease burden in patients with mycosis fungoides: results of a pooled analysis from 3 phase-II clinical trials.
J Am Acad Dermatol, 72 (2015), pp. 286
[22]
I. Amitay-Laish, O. Reiter, H. Prag-Naveh, R. Kershenovich, E. Hodak.
Retinoic acid receptor agonist as monotherapy for early-stage mycosis fungoides: does it work?.
J Dermatolog Treat, 30 (2019), pp. 258-263
[23]
A.O. Huen, E.J. Kim.
The Role of Systemic Retinoids in the Treatment of Cutaneous T-Cell Lymphoma.
Dermatol Clin, 33 (2015), pp. 715-729
[24]
V. Nikolaou, A. Patsatsi, P. Sidiropoulou, G. Chlouverakis, E. Kavvalou, T. Koletsa, et al.
Monotherapy and combination therapy with acitretin for mycosis fungoides: results of a retrospective, multicenter study.
J Eur Acad Dermatol Venereol, 34 (2020), pp. 2534-2540
[25]
M. Duvic, K. Hymes, P. Heald, D. Breneman, A. Martin, P. Myskowski, et al.
Bexarotene is effective and safe for treatment of refractory advanced-stage cutaneous T-cell lymphoma: multinational phase II-III trial results.
J Clin Oncol, 19 (2001), pp. 2456-2471
[26]
O. Jumbou, J.M. N’Guyen, M.H. Tessier, B. Legoux, B. Dreno.
Long-term follow-up in 51 patients with mycosis fungoides and Sezary syndrome treated by interferon-alfa.
Br J Dermatol, 140 (1999), pp. 427-431
[27]
A.C. Husken, A. Tsianakas, P. Hensen, D. Nashan, C. Loquai, S. Beissert, et al.
Comparison of pegylated interferon alpha-2b plus psoralen PUVA versus standard interferon alpha-2a plus PUVA in patients with cutaneous T-cell lymphoma.
J Eur Acad Dermatol Venereol, 26 (2012), pp. 71-78
[28]
M. Schiller, A. Tsianakas, W. Sterry, R. Dummer, A. Hinke, D. Nashan, et al.
Dose-escalation study evaluating pegylated interferon alpha-2a in patients with cutaneous T-cell lymphoma.
J Eur Acad Dermatol Venereol, 31 (2017), pp. 1841-1847
[29]
N. Spaccarelli, A.H. Rook.
The Use of Interferons in the Treatment of Cutaneous T-Cell Lymphoma.
Dermatol Clin, 33 (2015), pp. 731-745
[30]
V. Chiarion-Sileni, A. Bononi, C.V. Fornasa, M. Soraru, M. Alaibac, E. Ferrazzi, et al.
Phase II trial of interferon-alpha-2a plus psolaren with ultraviolet light A in patients with cutaneous T-cell lymphoma.
Cancer, 95 (2002), pp. 569-575
[31]
S. Rupoli, G. Goteri, S. Pulini, A. Filosa, A. Tassetti, M. Offidani, et al.
Long-term experience with low-dose interferon-alpha and PUVA in the management of early mycosis fungoides.
Eur J Haematol, 75 (2005), pp. 136-145
[32]
U. Wollina, R. Dummer, N.H. Brockmeyer, H. Konrad, J.O. Busch, M. Kaatz, et al.
Multicenter study of pegylated liposomal doxorubicin in patients with cutaneous T-cell lymphoma.
Cancer, 98 (2003), pp. 993-1001
[33]
R. Dummer, P. Quaglino, J.C. Becker, B. Hasan, M. Karrasch, S. Whittaker, et al.
Prospective international multicenter phase II trial of intravenous pegylated liposomal doxorubicin monochemotherapy in patients with stage IIB, IVA, or IVB advanced mycosis fungoides: final results from EORTC 21012.
J Clin Oncol, 30 (2012), pp. 4091-4097
[34]
P.L. Zinzani, F. Venturini, V. Stefoni, M. Fina, C. Pellegrini, E. Derenzini, et al.
Gemcitabine as single agent in pretreated T-cell lymphoma patients: evaluation of the long-term outcome.
Ann Oncol, 21 (2010), pp. 860-863
[35]
E.A. Coors, P. von den Driesch.
Treatment of erythrodermic cutaneous T-cell lymphoma with intermittent chlorambucil and fluocortolone therapy.
Br J Dermatol, 143 (2000), pp. 127-131
[36]
R.K. Winkelmann, J.L. Diaz-Perez, S.A. Buechner.
The treatment of Sezary syndrome.
J Am Acad Dermatol, 10 (1984), pp. 1000-1004
[37]
D.C.J. Case.
Combination chemotherapy for mycosis fungoides with cyclophosphamide, vincristine, methotrexate, and prednisone.
Am J Clin Oncol, 7 (1984), pp. 453
[38]
C. Hughes, A. Khot, C. McCormack, S. Lade, D. Westerman, R. Twigger, et al.
Lack of durable disease control with chemotherapy for mycosis fungoides and Sézary syndrome: a comparative study of systemic therapy.
[39]
H.S. Zackheim, M. Kashani-Sabet, A. McMillan.
Low-dose methotrexate to treat mycosis fungoides: a retrospective study in 69 patients.
J Am Acad Dermatol, 49 (2003), pp. 873-878
[40]
G.S. Wood, J. Wu.
Methotrexate and Pralatrexate.
Dermatol Clin, 33 (2015), pp. 747-755
[41]
S.J. Whittaker, M.F. Demierre, E.J. Kim, A.H. Rook, A. Lerner, M. Duvic, et al.
Final results from a multicenter, international, pivotal study of romidepsin in refractory cutaneous T-cell lymphoma.
J Clin Oncol, 28 (2010), pp. 4485-4491
[42]
E.A. Olsen, Y.H. Kim, T.M. Kuzel, T.R. Pacheco, F.M. Foss, S. Parker, et al.
Phase IIb multicenter trial of vorinostat in patients with persistent, progressive, or treatment refractory cutaneous T-cell lymphoma.
J Clin Oncol, 25 (2007), pp. 3109-3115
[43]
E.J. Kim, Y.H. Kim, A.H. Rook, A. Lerner, M. Duvic, S. Reddy, et al.
Clinically significant responses achieved with romidepsin across disease compartments in patients with cutaneous T-cell lymphoma.
Leuk Lymphoma, 56 (2015), pp. 2847-2854
[44]
A. de Masson, P. Guitera, P. Brice, I. Moulonguet, F. Mouly, J.D. Bouaziz, et al.
Long-term efficacy and safety of alemtuzumab in advanced primary cutaneous T-cell lymphomas.
Br J Dermatol, 170 (2014), pp. 720-724
[45]
M.G. Bernengo, P. Quaglino, A. Comessatti, M. Ortoncelli, M. Novelli, F. Lisa, et al.
Low-dose intermittent alemtuzumab in the treatment of Sezary syndrome: clinical and immunologic findings in 14 patients.
Haematologica, 92 (2007), pp. 784-794
[46]
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.
[47]
Y.H. Kim, M. Bagot, L. Pinter-Brown, A.H. Rook, P. Porcu, S.M. Horwitz, et al.
Mogamulizumab versus vorinostat in previously treated cutaneous T-cell lymphoma (MAVORIC): an international, open-label, randomised, controlled phase 3 trial.
Lancet Oncol, 19 (2018), pp. 1192-1204
[48]
R. Knobler, G. Berlin, P. Calzavara-Pinton, H. Greinix, P. Jaksch, L. Laroche, et al.
Guidelines on the use of extracorporeal photopheresis.
J Eur Acad Dermatol Venereol, 28 (2014), pp. 1-37
[49]
E.A. Olsen, A.H. Rook, J. Zic, Y. Kim, P. Porcu, C. Querfeld, et al.
Sezary syndrome: immunopathogenesis, literature review of therapeutic options, and recommendations for therapy by the United States Cutaneous Lymphoma Consortium (USCLC).
J Am Acad Dermatol, 64 (2011), pp. 352-404
[50]
J.A. Zic.
Extracorporeal Photopheresis in the Treatment of Mycosis Fungoides and Sezary Syndrome.
Dermatol Clin, 33 (2015), pp. 765-776
[51]
C. Gao, C. McCormack, C. van der Weyden, M.S. Goh, B.A. Campbell, R. Twigger, et al.
Prolonged survival with the early use of a novel extracorporeal photopheresis regimen in patients with Sezary syndrome.
Blood, 134 (2019), pp. 1346-1350
[52]
S. Whittaker, P. Ortiz, R. Dummer, A. Ranki, B. Hasan, B. Meulemans, et al.
Efficacy and safety of bexarotene combined with psoralen-ultraviolet A (PUVA) compared with PUVA treatment alone in stage IB-IIA mycosis fungoides: final results from the EORTC Cutaneous Lymphoma Task Force phase III randomized clinical trial (NCT00056056).
Br J Dermatol, 167 (2012), pp. 678-687
[53]
R.F. Duarte, A. Boumendil, F. Onida, I. Gabriel, R. Arranz, W. Arcese, et al.
Long-term outcome of allogeneic hematopoietic cell transplantation for patients with mycosis fungoides and Sezary syndrome: a European society for blood and marrow transplantation lymphoma working party extended analysis.
J Clin Oncol, 32 (2014), pp. 3347-3348
[54]
P. Quaglino, M. Maule, H.M. Prince, P. Porcu, S. Horwitz, M. Duvic, et al.
Global patterns of care in advanced stage mycosis fungoides/Sezary syndrome: a multicenter retrospective follow-up study from the Cutaneous Lymphoma International Consortium.
Ann Oncol, 28 (2017), pp. 2517-2525

How to cite this article: Sanches JA, Cury-Martins J, Abreu RM, Miyashiro D, Pereira J. Mycosis fungoides and Sézary syndrome: focus on the current treatment scenario. An Bras Dermatol. 2021;96:458–71.

Study conducted at the Dermatology Clinic Division, Hospital das Clínicas, Faculdade de Medicina, Universidade de São Paulo, São Paulo, SP, Brazil.

Copyright © 2021. Sociedade Brasileira de Dermatologia
Download PDF
Idiomas
Anais Brasileiros de Dermatologia
Article options
Tools
en pt
Cookies policy Política de cookies
To improve our services and products, we use "cookies" (own or third parties authorized) to show advertising related to client preferences through the analyses of navigation customer behavior. Continuing navigation will be considered as acceptance of this use. You can change the settings or obtain more information by clicking here. Utilizamos cookies próprios e de terceiros para melhorar nossos serviços e mostrar publicidade relacionada às suas preferências, analisando seus hábitos de navegação. Se continuar a navegar, consideramos que aceita o seu uso. Você pode alterar a configuração ou obter mais informações aqui.