Primary cutaneous diffuse large B-cell lymphoma, leg type explained

Primary cutaneous diffuse large B-cell lymphoma, leg type
Synonyms:PCDLBCL-LT; PCDLBCL, leg type; primary cutaneous DLBCL, leg type
Field:Dermatology, hematology, oncology
Symptoms:One or more red/violaceous skin nodules/tumors on the legs and/or uncommonly elsewhere
Complications:Spread to other tissues
Diagnosis:Skin biopsy
Prognosis:guarded

Primary cutaneous diffuse large B-cell lymphoma, leg type (PCDLBCL-LT) (also termed PCDLBCL, leg type or primary cutaneous DLBCL, leg type) is a cutaneous lymphoma skin disease that occurs mostly in elderly females. In this disease, B cells (a type of lymphocyte) become malignant, accumulate in the dermis (i.e. the layer under the epidermis) and subcutaneous tissue below the dermis to form red and violaceous skin nodules and tumors. These lesions typically occur on the lower extremities but in uncommon cases may develop on the skin at virtually any other site.[1] In ~10% of cases, the disease presents with one or more skin lesions none of which are on the lower extremities; the disease in these cases is sometimes regarded as a variant of PCDLBL, LT termed primary cutaneous diffuse large B-cell lymphoma, other (PCDLBC-O).[2] PCDLBCL, LT is a subtype of the diffuse large B-cell lymphomas (DLBCL)[3] and has been thought of as a cutaneous counterpart to them.[4] Like most variants and subtypes of the DLBCL, PCDLBCL, LT is an aggressive malignancy. It has a 5-year overall survival rate of 40–55%, although the PCDLBCL-O variant has a better prognosis than cases in which the legs are involved.[5]

Most lymphomas begin in a lymph node, mucosa-associated lymphoid tissue, the spleen, or another lymphoid tissue within the lymphatic system and then may spread to the skin. In these cases the skin is a secondarily site of involvement. PCDLBC, LT is a primary cutaneous lymphoma, i.e. it begins in the skin and then may spread to lymphoid and/or non-lymphoid tissues in virtually any other site.[6] A suspect PCDLBCL, LT that is not limited to the skin at the time of diagnosis should be regarded as some other variant or subtype of the diffuse large B-cell lymphomas.[7]

PCDLBC, LT represents 5–10% of all primary cutaneous lymphomas.[8] It is to be distinguished from two other primary cutaneous lymphomas that involve B-cells, primary cutaneous follicle center lymphoma (PCFCL) and primary cutaneous marginal zone lymphoma (PCMZL),[8] as well as from a B-cell lymphoma that at diagnosis may appear to be limited to the skin but often is a systemic disease affecting numerous organs and tissues viz., intravascular large B-cell lymphoma (IVLBCL).[7] These three B-cell lymphomas differ from PCDLBCL, LT in numerous ways but most importantly in their aggressiveness.[7] IVLEBC is, like PCDLBCL, LT, an aggressive disease with a guarded prognosis, but unlike the former disease, is often widely disseminated at presentation.[7] PCFCL and PCMZL, in contrast, are indolent lymphomas with a relatively good prognosis.[1] Distinguishing between these four cutaneous B-cell lymphomas at the time of diagnosis is critical for their appropriate treatment.[7]

Presentation

Afflicted individuals (median age 76 years; range 49–92 years; more common in females[3]) typically present with one or more rapidly growing red to bluish-red, firm tumors located on the leg(s) at some site(s) below the knees.[5] Occasionally the lesions are ulcerated.[3] About 10% of cases do not have lesions on the legs but rather present with one or more skin lesions outside of the legs; ~20% of individuals present with cutaneous lesion(s) but on further or later investigation are found to have disease in non-cutaneous sites such as the lymph nodes, visceral organs,[1] bone marrow, and/or, rarely, central nervous system.[5] Some individuals, particularly those with widespread disease, complain of having the B symptoms of fever, night sweats, and/or weight loss.[1] DLBCL cases that have cutaneous lesions in association with widespread disease may be advanced PCDLBCL, LT but without evidence that the disease began in the skin are diagnosed as having and treated for some other variant or subtype of the diffuse large B-cell lymphomas that has spread to the skin.[7]

Pathophysiology

The neoplastic cells in DLBCL are derived primarily from either germinal center B cells (i.e. GBC) or activated B cells (i.e. ABC)[9] with ABC-based DLBCL usually being a more aggressive disease than GBC-based DLBCL.[4] The neoplastic cells in PCDLBCL, LT are ABC,[6] bear gene abnormalities similar to those found in ABC-based DLBCL,[4] and as a likely result of this produce an aggressive disease. The potentially pathogenic gene abnormalities in the neoplastic cells of PCDLBCL, LT include:

These findings suggest that the development and/or progression of PCDLBCL, LT involves the step-wise acquisition by B-cells and/or their ABC descendants of gene abnormalities which promote the activation of NF-kappa B, B-cell receptor, JAK/STAT, and perhaps other signaling pathways. In consequence, these cells progressively acquire increased rates of proliferation, prolonged survival, the ability to spread to other tissues, the ability to avoid attack by the immune system, and other malignant behaviors that characterize this disease.[7]

Diagnosis

The diagnosis of PCDLBCL, LT depends on analyzing skin biopsies of the involved sites microscopically. These sites show dense, diffuse sheets of infiltrating large-sized B-cells that resemble centroblasts and immunoblasts.[5] The infiltrates are located in the dermis and subcutaneous tissue but, unless there is ulceration, they are separated from the epidermis by the "grenz zone" i.e. a narrow area of the papillary dermis (i.e. the uppermost layer of the dermis that separates the dermis from the epidermis[13]) that is not infiltrated by the disease.[5] In addition to the neoplastic B-cells, these infiltrates contain two types of cells that suppress immune reactions viz., M2 macrophages that express CD163 and myeloid-derived suppressor cells that express PD-L1 and CD33.[7] The sites may also contain poorly differentiated cells;[5] but rarely have T-cells, eosinophils, or plasma cells.[3] The lesion's neoplastic B-cells usually have a high proliferative index.[5] Immunostaining these tissues indicates that the neoplastic cells express B-cell marker proteins such as FOXP1 (90% of cases), (Bcl-2, (90% of cases), IRF4 (85% of cases), Bcl-6 (~60% of cases),[3] CD20, CD79a, PAX5, and cytoplasmic IgM.[5] The cells usually do not express CD5, CD10, CD30, or CD138.[5] The neoplastic cells are also usually characterized as being of the ABC phenotype as described in the section on the variants of DLBCL, NOS[6] and express the gene abnormalities indicated in the above Pathophysiology section. Patients should be evaluated for the involvement of non-cutaneous sites by CT scans of the chest, abdomen, and pelvis, a PET scan, and a bone marrow biopsy.[1] Individuals who present with an extra-cutaneous DLBCL-like disease should be diagnosed as having a variant or subtype of DLBCL other than PCDLBCL, LT unless in can be established that the disease began in the skin.[7]

Differential diagnosis

Primary cutaneous follicular center lymphoma differs from PCDLBCL, LT in that its neoplastic B cells are germinal center B cells rather than activated B cells (see Pathophysiology section) that often infiltrate tissues in a follicular (i.e. small spherical groups of cells) rather than diffuse pattern. Primary cutaneous mantle cell lymphoma differs from PCDLBCL, LT in that is neoplastic B cells appear more like monocytes and/or plasma cells rather than centroblasts or immunoblasts. Intravascular large B-cell lymphoma differs from PCDLBCL, LT in that involved tissues contain large, neoplastic B-cells that are strictly confined within the lumen of small- to medium-sized dermal and subcutaneous blood vessels.[1]

Treatment

Previously, most patients with PCDLBCL, LT were treated with the CHOP chemotherapy regimen of cycloheximide, hydroxydaunorubicin, oncovin, and prednisone. The more recent addition of the immunotherapy drug, rituximab, to this regimen has given better results.[14] Rituximab is a monoclonal antibody that kills cells which express high levels of CD20 by binding to this cell-surface protein and thereby targeting them for attack by the hosts immune system.[15] Accordingly, the addition of rituximab to CHOP, i.e. the R-CHOP chemoimmunotherapy regimen. with or without radiotherapy (used to treat symptoms resulting from specific localized lesions) is now recommended by the European Organisation for Research and Treatment of Cancer and the International Society for Cutaneous Lymphomas[16] as first line therapy for single, localized, and widespread diseases. Cases in which hydroxydaunorubicin is contraindicated because of, e.g. preexisting heart disease, may treated with the R-COP regiment (i.e. R-CHOP minus hydroxydaunorubicin). Patients who might be intolerant to R-CHO because of general health issues have been treated with just rituximab and radiotherapy[5] although more recent reports indicate that these patients may be successfully treated with a regimen that replaces hydroxydaunorubicin with PEGylated, liposome-encased doxorubicin in the R-CHOP regimen.[7]

Experimental treatments

A phase II clinical trial is recruiting individuals to study the efficacy and safety of nivolumab, a (monoclonal antibody that binds to programmed death-ligand 1 thereby blocking its ability to suppress immune responses) with or without varlilumab (a monoclonal antibody that binds to the CD27 protein expressed by cells and thereby promotes the anti-tumor activity of T cells) in treating patients with aggressive B-cell lymphomas, including PCDLBCL, LT that have relapsed after or do not respond to treatment.[17] Other agents are being evaluated in refractory or relapsed B-cell lymphoid malignancies but not PCDLBCL, NOS and ultimately may prove useful in PCDLBCL, LT. These include: ofatumumab, a monoclonal antibody that is stronger than rituximab in binding to CD20; two radioimmunotherapy monoclonal antibodies, Ibritumomab tiuxetan and Tositumomab that bind CD20 to deliver radiation from their attached radioactive isotopes to and kill CD20-bearing cells; lumiliximab, a monoclonal antibody that binds to CD23; dacetuzumab, a monoclonal antibody that binds CD40; Siglec-3 a monoclonal antibody that binds CD33; blinatumomab, a monoclonal antibody that binds both CD3 and CD19; chimeric antigen receptor T cell therapy using CD19-directed CAR-T cells; and lenalidomide, a drug with multiple anti-tumor actions.[7]

Notes and References

  1. Chen ST, Barnes J, Duncan L . Primary cutaneous B-cell lymphomas- clinical and histopathologic features, differential diagnosis, and treatment . Seminars in Cutaneous Medicine and Surgery . 37 . 1 . 49–55 . March 2018 . 29719020 . 10.12788/j.sder.2018.014 . 22888927 .
  2. Jia J, Li W, Zheng Y . Primary cutaneous diffuse large B cell lymphoma-other successfully treated by the combination of R-CHOP chemotherapy and surgery: A case report and review of literature . Medicine . 96 . 8 . e6161 . February 2017 . 28225499 . 5569421 . 10.1097/MD.0000000000006161 .
  3. Sukswai N, Lyapichev K, Khoury JD, Medeiros LJ . Diffuse large B-cell lymphoma variants: an update . Pathology . 52. 1. 53–67. November 2019 . 31735345 . 10.1016/j.pathol.2019.08.013 .
  4. Grimm KE, O'Malley DP . Aggressive B cell lymphomas in the 2017 revised WHO classification of tumors of hematopoietic and lymphoid tissues . Annals of Diagnostic Pathology . 38 . 6–10 . February 2019 . 30380402 . 10.1016/j.anndiagpath.2018.09.014 . 53196244 .
  5. Selva R, Violetti SA, Delfino C, Grandi V, Cicchelli S, Tomasini C, Fierro MT, Berti E, Pimpinelli N, Quaglino P . A Literature Revision in Primary Cutaneous B-cell Lymphoma . Indian Journal of Dermatology . 62 . 2 . 146–157 . 2017 . 28400634 . 5363138 . 10.4103/ijd.IJD_74_17 . free .
  6. Jaffe ES . Navigating the cutaneous B-cell lymphomas: avoiding the rocky shoals . Modern Pathology . 33 . Suppl 1 . 96–106 . January 2020 . 31653979 . 10.1038/s41379-019-0385-7 . 204887118 . free .
  7. Tadiotto Cicogna G, Ferranti M, Lazzarotto A, Alaibac M . Biological Approaches to Aggressive Cutaneous B-Cell Lymphomas . Frontiers in Oncology . 9 . 1238 . 2019 . 31799195 . 6864397 . 10.3389/fonc.2019.01238 . free .
  8. Wilcox RA . Cutaneous B-cell lymphomas: 2019 update on diagnosis, risk stratification, and management . American Journal of Hematology . 93 . 11 . 1427–1430 . November 2018 . 30039522 . 10.1002/ajh.25224 . free . 2027.42/146398 . free .
  9. Cabanillas F, Shah B . Advances in Diagnosis and Management of Diffuse Large B-cell Lymphoma . Clinical Lymphoma, Myeloma & Leukemia . 17 . 12 . 783–796 . December 2017 . 29126866 . 10.1016/j.clml.2017.10.007 . 25304758 .
  10. Chavez JC, Locke FL . CAR T cell therapy for B-cell lymphomas . Best Practice & Research. Clinical Haematology . 31 . 2 . 135–146 . June 2018 . 29909914 . 6716161 . 10.1016/j.beha.2018.04.001 .
  11. Gravelle P, Burroni B, Péricart S, Rossi C, Bezombes C, Tosolini M, Damotte D, Brousset P, Fournié JJ, Laurent C . Mechanisms of PD-1/PD-L1 expression and prognostic relevance in non-Hodgkin lymphoma: a summary of immunohistochemical studies . Oncotarget . 8 . 27 . 44960–44975 . July 2017 . 28402953 . 5546533 . 10.18632/oncotarget.16680 .
  12. Heyman M, Einhorn S . Inactivation of the p15INK4B and p16INK4 genes in hematologic malignancies . Leukemia & Lymphoma . 23 . 3–4 . 235–45 . October 1996 . 9031104 . 10.3109/10428199609054826 .
  13. Abbas O, Mahalingam M . The grenz zone . The American Journal of Dermatopathology . 35 . 1 . 83–91 . February 2013 . 23348142 . 10.1097/DAD.0b013e31824feb4e . 24048289 .
  14. Ollila TA, Olszewski AJ . Extranodal Diffuse Large B Cell Lymphoma: Molecular Features, Prognosis, and Risk of Central Nervous System Recurrence . Current Treatment Options in Oncology . 19 . 8 . 38 . June 2018 . 29931605 . 6294323 . 10.1007/s11864-018-0555-8 .
  15. Li S, Young KH, Medeiros LJ . Diffuse large B-cell lymphoma . Pathology . 50 . 1 . 74–87 . January 2018 . 29167021 . 10.1016/j.pathol.2017.09.006 . 20839613 .
  16. Web site: International Society for Cutaneous Lymphomas (ISCL) > About the ISCL . www.cutaneouslymphoma.org . dead . https://web.archive.org/web/20150509070059/http://www.cutaneouslymphoma.org/Default.aspx?tabid=59 . 2015-05-09.
  17. Web site: A Randomized Phase 2 Study of CDX-1127 (Varlilumab) in Combination with Nivolumab in Patients with Relapsed or Refractory Aggressive B-cell Lymphomas. 23 October 2021.