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BRIEF ARTICLE 
 

 

Clinical and Histological Spectrum of Primary Cutaneous B-Cell 
Lymphoma in an Ethnically-Diverse Group of Patients: A Case 
Series  
 

Sahira Farooq, BS1,, Madeline Frizzell, BS, MS2, Emily Limmer3, Ritu Swali, MD4, Stephen 
Tyring, MD, PhD, MBA4,5 

 
1McGovern Medical School, Houston, TX 
2 Texas A&M University College of Medicine, Houston, TX 
3University of Texas Southwestern Medical School, Dallas, TX 
4Department of Dermatology, University of Nebraska Medical Center, Omaha, NE 
5Department of Dermatology, McGovern Medical School at UT Houston Health Science Center, Houston, TX 
 

 

 
 

 
 
While dermatologic findings may not be 
what initially come to mind when identifying 
lymphomas, these neoplasms can and do 
present cutaneously. Primary cutaneous 
lymphomas, which are diagnosed with only 
skin involvement, can be of B or T cell 
origin, with B cells making up merely 25-
30% of cases. They commonly present with 
nodules or with plaques or papules.1 
Previously lymphomas were classified as 
simply Hodgkin or non-Hodgkin.2 However, 
due to their varied origin as well as their 
diverse presentations, these groups have 
been divided further into more descriptive 
and representative groups. Broadly, non-
Hodgkin lymphoma derived from B cells 
include diffuse large B cell lymphoma 

(DLBCL), Burkitt lymphoma, follicular 
lymphoma, and marginal zone lymphoma, 
among others.3 Here, we present the cases 
of three ethnically diverse patients with 
distinct clinical and histological forms of 
cutaneous B cell lymphoma. 
 

 
 
Patient A 
A 67-year-old Hispanic male, with a past 
medical history of coronary artery disease, 
hypertension, hyperlipidemia, and type 2 
diabetes, presented to the dermatology 
clinic with a two-month history of a red 
nodule on his left ear. He denied pain, 
pruritus, and/or bleeding. He had been using 
triamcinolone 1% ointment on the lesion with 
minor improvement. On clinical examination, 

ABSTRACT 

Primary cutaneous lymphomas, which are diagnosed with only skin involvement, can be of B or T cell 
origin. Due to their varied origin as well as their diverse presentations, these groups have been 
divided further into more descriptive and representative groups. The subtypes are primary cutaneous 
marginal zone lymphoma (PCMZL), primary cutaneous follicle center lymphoma (PCFCL), primary 
cutaneous diffuse large B cell lymphoma, leg type (PCDLBCL-LT) and intravascular large B-cell 
lymphoma. Here, we present the cases of three ethnically diverse patients with distinct clinical and 
histological forms of cutaneous B cell lymphoma. 
 

INTRODUCTION 

CASE PRESENTATION 



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there was a pearly nodule on the left anti-
tragus (Figure 1). A shave biopsy was 
performed to rule out basal cell carcinoma. 
Histopathological examination revealed an 
atypical dense infiltrate of lymphocytes with 
a Grenz zone. Immunohistochemistry 
demonstrated CD20+, CD3+, BCL-2+, 
CD10+, BCL-6+, and Ki67+, while MUM1-, 
CD30-, and CD21-. Results were consistent 
with germinal center type diffuse large B-cell 
lymphoma.  
 
Patient B 
A 79-year-old African American male, with a 
history of diabetes and hypertension, 
presented to the dermatology clinic with a 
scalp lesion present for the past two years. 
He noted that the lesion stung upon 
manipulation. No treatment had been 
pursued up to this point. On physical exam, 
there was a notable skin-colored nodule 
(33mm x 22mm) on the left crown of the 
scalp (Figure 2). A punch biopsy was 
performed. Histopathology revealed sheets 
of markedly atypical lymphoid cells. 
Immunohistochemical stains were CD20+, 
Ki-67+, CD3+, CD4+, CD8+, CD30+, CD10-, 
CD23-, S100-, AE1/3-. Lesional cells were 
MUM+, consistent with diffuse large B-cell 
lymphoma, leg type.  
 
Patient C 
A 73-year-old Caucasian male with a past 
medical history of hypertension, diabetes, 
and anemia, presented to the dermatology 
clinic with a bleeding growth on his right 
upper extremity for the past month. Clinical 
examination revealed a cluster of 2-4mm 
pink-red papules and vesicles on his right 
wrist (Figure 3). A shave biopsy was 
performed. Immunohistochemistry 
demonstrated CD20+, CD3+, CD4+, CD5+, 
CD8+, BCL-2+, CD10-, CD30-, S100-, 
CD21-, EBER-. The lambda/kappa ratio was 
elevated by in-situ hybridization. The 

diagnosis of marginal zone B-cell lymphoma 
was favored. 
 
The patients were referred to oncology for 
further work up and therapy. 
 

 
Figure 1. Patient A. A pearly nodule, reminiscent of 
basal cell carcinoma, representing germinal center 
type diffuse large B-cell lymphoma on the ear of a 67-
year-old Hispanic male. 
 

 
Figure 2: Patient B. Symptomatic, skin-colored lesion 
representing diffuse large B-cell lymphoma, leg type, 
on the scalp of a 79-year-old African American male.  
 
 



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Figure 3: Patient C. Bleeding, erythematous papules 
and vesicles representing marginal zone B-cell 
lymphoma on the wrist of a 73-year-old Caucasian 
male.  

 

 
 
Primary cutaneous lymphomas, which are 
skin-limited lymphoproliferative neoplasms 
or B or T cell origin, are uncommon, 
occurring with an estimated incidence of 0.5 
to 1 case per 100,000 people annually.4 
Primary cutaneous B-cell lymphomas 
(PCBCLs) make up around one-quarter of 
the cutaneous lymphomas.4  
  
According to the World Health Organization 
- European Organization for Research and 
Treatment of Cancer (WHO-EORTC) 2018 
classifications for PCL, there are 4 subtypes 
of PCBCLs with one provisional subtype 
being EBV mucocutaneous ulcer. The 
subtypes are primary cutaneous marginal 
zone lymphoma (PCMZL), primary 
cutaneous follicle center lymphoma 
(PCFCL), primary cutaneous diffuse large B 
cell lymphoma, leg type (PCDLBCL-LT) and 
intravascular large B-cell lymphoma.5  

Primary cutaneous lymphomas (PCLs) are, 
by definition, a cutaneous manifestation that 
is not secondary to extracutaneous spread, 
so their diagnosis requires a thorough work-
up to exclude systemic disease. A biopsy is 
necessary to analyze morphology, 
immunohistochemistry (IHC), and staging to 
exclude systemic disease.6 
Immunophenotype workup is also necessary 
to differentiate between types of cutaneous 
lymphomas. Presence of the CD20 marker 
differentiates B-cell lymphomas from T-cell 
lymphomas.9 Additional markers are tested 
to determine the pattern and location of 
infiltrate to distinguish between the types of 
cutaneous B-cell lymphomas.9 Panel 
recommendations include CD3, CD5, CD10, 
BCL2, BCL6, and MUM1. Additional testing 
can include CD21, CD23, CD43, Cyclin D1, 
Ki-67, immunoglobulins IgM and IgD, as well 
as kappa/lambda light chain analysis.4  
 
WHO’s current classification system of 
PCBCLs considers primary cutaneous 
diffuse large B-cell lymphoma-leg type 
(PCDLBCL-LT) to be the only primary 
cutaneous diffuse large B-cell lymphoma. 
While patients A and B were both diagnosed 
with PCDLBCLs because there have been 
multiple reports of PCDLBCL that do not fit 
into the leg-type description, there is still 
debate as to whether they represent an 
atypical variant of the leg type or a separate 
entity.10 PCDLBCL-LT commonly presents 
in elderly females with rapidly progressive 
tumors on the legs. However, 15-20% of the 
lesions present at locations outside the legs, 
such as our patient B.5,6 On the other hand, 
PCDLBCL presents more commonly on the 
trunk of elderly men with frequent 
involvement of the limbs, head and neck 
regions.10 Histologically, the leg type is 
characterized by diffuse large cells 
infiltrating to subcutaneous tissue with rare 
intermingled reactive T lymphocytes; 
PCDLBCL has a histologic pattern that

DISCUSSION 



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Figure 4:  Primary Cutaneous Lymphoma: Stratification and Demographic Data. Stratification of primary cutaneous 
B-cell lymphoma into its subgroups is shown in the blue boxes. Demographic data overall and with respect to 
specific groups is detailed in the gray boxes.  

 

 
 
includes large centroblastic or 
immunoblastic cells.  
  
Based on expression of BCL-6, CD10, and 
MUM-1, diffuse large b-cell lymphomas can 
be further divided into germinal center (GC) 
and non-germinal center subtypes.11  Given 
that BCL-6 and CD10 are markers for 
germinal center B-cells, patient A’s IHC 
results were consistent with a diagnosis of 
PCDLBCL, GC subtype.11  Patient’s B’s IHC 

results were consistent with a diagnosis of 
PCDLBCL-LT, as leg type is usually positive 
for BCL2, MUM1 and BCL6, but negative for 
CD10.4 
  
Primary cutaneous marginal zone 
lymphomas (PCMZL) is an indolent 
lymphoma, classically presenting as solitary 
or multifocal erythematous to brown-colored 
plaques, papules, or nodules. They typically 
appear in young adults distributed on the 



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trunk or upper extremities.4,5 Pruritus is 
commonly associated with PCMZL, but pain, 
night sweats, fever and weight loss are not 
expected.5 On histopathology, PCMZL 
reveals a nodular or diffuse mixed infiltrate 
of small, marginal zone B-cells, 
lymphoplasmacytic cells, plasma cells, and 
reactive T cells. These findings typically 
spare the epidermis and superficial papillary 
dermis. Marginal zone B cells are 
characteristically BCL‐2 and MUM-1 
positive, but lack BCL‐6 or CD10 
expression.4,6 The immunohistochemistry 
features of Patient C’s biopsy and the 
characteristics of the tumor on 
histopathology favored a diagnosis of 
PCMZL. 
 
Another PCBCL worth mentioning, although 
not found in our three patients, is primary 
cutaneous follicle center B cell (PCFCL). 
The median age of presentation is 60 and 
typically presents with localized skin lesions 
on the head, neck and trunk.4 PCFCL is 
characterized by a predominance of large 
centrocytes and centroblasts that stain 
positive for CD20, BCL-6, CD10 and 
negative for BCL-2 and MUM-1. This 
lymphoma has an excellent prognosis and 
can be easily managed with local 
radiotherapy.5 
 
There are limited trials and data regarding 
treatment for PCBCLs, and therapy is 
primarily guided by whether the nature of the 
lymphoma is indolent or aggressive.4 No 
standard of treatment exists for the indolent 
lymphomas, such as PCMZL and PCFCL, 
however, treatment options include local 
radiotherapy, excision, and intralesional 
steroids.4,7 Prognosis is excellent with 5-
year survival of > 95%.4,7 In contrast, 
PCDLBCL is aggressive in nature, and first 
line treatment is intravenous rituximab with a 
combination of chemotherapy 
agents.4,7  Prognosis is poorer with 5-year 

survival of 50-70%.4,7 Relapses and 
systemic spread are common for PCDLBCL 
despite therapy.7 
 

 
 
Overall, though PCBCLs are uncommon, it 
is important for clinicians to be aware of the 
diverse clinical and histological 
presentations of these indolent lymphomas, 
because they have a relatively good 
prognosis with appropriate therapy. The 
more aggressive, leg type lymphoma must 
be closely managed given its poorer 
prognosis. Optimal care of PCBCLs may 
involve a multidisciplinary approach, 
consisting of dermatology, medical 
oncology, and radiation oncology.6 
 
Conflict of Interest Disclosures: None 
 
Funding: None 
 
Corresponding Author: 
Ritu Swali, MD 
985645 Nebraska Medical Center 
Omaha, NE, 68198 
Phone: 402-552-5525 
Email: rituswali@gmail.com 

 
 
References: 
1. Kempf W, Kazakov DW, Mitteldorf C. Cutaneous 

lymphomas: an update. Part 2: B-cell lymphomas 
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2. Alizadeh AA, et al. Distinct types of diffuse large 
B-cell lymphoma identified by gene expression 
profiling. Nature. 2000. 403(6769): p. 503-11. 

3. Teras, LR, et al., 2016 US lymphoid malignancy 
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CA Cancer J Clin. 2016. 66(6): p. 443-459. 

4. Malachowski SJ, Sun J, Chen P-L, Seminario-
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5. Willemze R, Cerroni L, Kempf W, Berti E, 
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CONCLUSION 



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6. Campbell SM, Peters SB, Zirwas MJ, Wong HK, 
Campbell SM. Immunophenotypic diagnosis of 
primary cutaneous lymphomas: A review for the 
practicing dermatologist. J Clin Aesthet Dermatol. 
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7. Sica A, Vitiello P, Caccavale S, et al. Primary 
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8. Bradford PT, Devesa SS, Anderson WF, Toro 
JR. Cutaneous lymphoma incidence patterns in 
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9. Wilcox RA (2013), Cutaneous B‐cell lymphomas: 
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10. Hans CP, Weisenburger DD, Greiner TC, et al. 
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11. Goyal A, Leblanc RE, Carter JB. Cutaneous B-
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