Post on 31-May-2022
CBCL An Overview and Newer Approaches
Steven M. Horwitz M.D.Lymphoma ServiceMemorial Sloan Kettering Cancer Center
Classification of Cutaneous Lymphomas
Blood 2005;105:3768-85
CUTANEOUS T/NK LYMPHOMAS
Mycosis fungoides
Sezary Syndrome
ATLL
Primary cutaneous CD 30+
Anaplastic large cell
Lymphomatoid papulosis
Subcutaneous panniculitis-like T-cell
Extranodal NK/T-cell
Primary cutaneous peripheral T-cell
Epidermotropic CD8+ T-cell
Cutaneous T-cell
CD4+ pleomorphic T-cell
CUTANEOUS B-CELL LYMPHOMAS
Primary cutaneous marginal zone
Primary cutaneous follicle center
Primary cutaneous diffuse large cell
Leg type
Intravascular
Primary Cutaneous B Cell Lymphoma
Background
Subtypes
Prognosis
NCCN
Clinical scenarios:
Do we need to stage low grade CBCL?
Use of low dose radiation
PCFCL in nodes
Unusual cases of PC-MZL
Primary Cutaneous B Cell Lymphoma
Definition:
– Lymphoma presenting in the skin
– No evidence of extracutaneous disease on complete staging at time of diagnosis
Approximately 20-25% of all cutaneous lymphomasPrimary cutaneous B-cell lymphomas have some unique clinical features
– Indolence-slow growth-majority- MZL/FC– Relapses are common, regardless of the treatment-not assoc with
worse prognosis– Relapses are largely confined to the skin
Primary Cutaneous Marginal Zone B-cell Lymphoma
Clinical Features: M>F (1.4 :1), median age=53
• Red papules, plaques, nodules, rare ulcerations
• Upper extremities > trunk > head
• Slow growth/ spontaneous regression
• Association with Borrelia burgdorferi ? (Europe)– Anecdotal responses to antibiotics
• Therapy-observation, local, topical
• Anecdotes/small series with rituximab, antibiotics, interferon
• Topical corticosteroids, nitrogen mustard
• 5-year survival > 95%
Primary Cutaneous Marginal Zone B-cell Lymphoma
Pathology
• Non-epidermotropic
• Nodular-diffuse infiltrates
• Some large cells
• Reactive T-cells
• CD20, CD79a,
• CD5, CD10, bcl-6-negative
• Light chain restriction, IGH rearranged
• Cases showing rearrangement 14:18 – IGH on 14 and MLT gene on 18
CD20 (B-cell)
CD3 (T-cell)
Primary Cutaneous Marginal Zone Lymphoma
Kappa LambdaLight chainrestriction
PC Follicle Center Lymphoma
• Solitary, grouped, or multifocal plaques or tumor nodules
• Scalp/forehead> trunk >extremities
• Less common disseminated lesions
• Slow growth/ Spontaneous regression
• Rare extracutaneous spread
• Most common; M>F (2.1:1)median age=58
• Excellent prognosis
• 5-yr DSS 95%
Senff NJ, Noordijk EM, Kim YH, et al. Blood 2008;112:1600
WHO monogram, 4th Edition, 2008
Primary Cutaneous Follicle Center Lymphoma
In contrast:PCLBCL-LT:Monotonous diffuse centroblasts & immunoblastsExtension to subcutaneous fat; MUM-1+, Bcl-2 + Frequent mitosis
Mix of centrocytes and centroblastsEpidermal sparingVarying amounts of large cellsFollicular or diffuseFrequent reactive T-cells
Immunohistochemistry/Genetics
• Tumor cells express CD20 and CD79
• Tumor cells will express HGAL, bcl-6, and LMO2 consistently
• PC FCL do not consistently express bcl-2 or CD10
• T(14;18) and bcl-2 gene rearrangement not present in most cases of PC FCL
Weinberg O et al. Am J Surg Pathol. 2009 Apr;33(4):591-8.
Xie X et al. Mod Pathol. 2008 Jun;21(6):653-9.
Morales A et al. Am J Dermatopathol. 2008 Oct;30(5):425-30.
Cutaneous MZL/FC LymphomaIndolent histologies
Treatment N CR Relapse Relapse:EC OS
5/10y
ALL 416 90% 44% 6-11% 96/90%
XRT 217 98% 49%
Chemo +/- XRT
(Variety)
96 80% 52%
Excision 103 97% 35%
Zinzani et al. J Clin Oncol 24:1376-1382. March 2006
Cutaneous MZL/FC LymphomaLocal therapy: XRT/Excision
All DFS
Treatment N 5 year 10 year
Single 247 64% 51% p<.001
Regional 125 43% 27%
Disseminated 57 45% 36%
Zinzani et al. J Clin Oncol 24:1376-1382. March 2006Reddy et al, ASCO 2007, a8028
Indolent N Relapse
Localized 65 34 52%
Generalized 19 13 68%
Primary Cutaneous Diffuse Large B-cell Lymphoma, Leg Type
• Rare; rapid growth
Lower extremities> anywhere else
• Especially elderly women(F>M 2:1; age >70)
• Extracutaneous involvement more common
than other lymphomas
• 5 year over-all survival 67%
Pathology• Dense diffuse infiltrate of large B cells, with obliteration of existing
adnexal structures
• Extends significantly into subcutaneous tissue
• Monomorphous large B cells, with appearance of immunoblasts
• Express CD79, CD20, MUM-1, FOXP1, IgM and IgD
• In some series, strong uniform expression of bcl-2 with variable expression of bcl-6
• Does not usually express CD10
Sundram U et al. J Cutan Pathol. 2005 Mar;32(3):227-34.Kodama K et al. Blood. 2005 Oct 1;106(7):2491-7.
MUM-1
CD20
Bcl-2
Bcl-6
Hoefnagel et al Blood 2005;105:3671-3678
Willemze et al Blood, 2005;105:3768-3785
de Leval et al Am J surg Pathol. 2001;25:732-741
Hoefnagel et al Br J Dermatol. 2003:149:1183-1191
Child et al Br J Dermatol. 2001;144:735-744
Cerroni et al J Invest Dermatol. 1994; 102:231-235
FCL LBC-L
CD20/CD 79a + +
Bcl-2 -/+ ++
Bcl-6 + +
CD10 -/+ -
MUM-1 - +
t(14:18) - -
Trans myc (fish) - +/-
ABC GC
Follicle center -Diffuse large B-cell, leg typePathology
DLBC-Leg Type
Treatment N CR Relapse Relapse:EC OS
5/10y
ALL 51 82% 55% 17% 73/47%
XRT 28 23% 52%
Chemo +/- XRT
(CHOP)
20 80% 63%
Excision 3 100% 33%
Zinzani et al. J Clin Oncol 24:1376-1382. March 2006
Senff, N. J. et al. Arch Dermatol 2007;143:1520-1526.
disease-specific survivalrelapse-free survival
Results after Primary Radiation for Cutaneous B-cell Lymphoma
Koens et al. Journal of Investigative DermatologyVolume 134, Issue 1, January 2014, Pages 290-292
JAMA Dermatol. 2014;150(11):1173-1179. doi:10.1001/jamadermatol.2014.821
MYD88 mutation was not present in 24 patients and was present in 34 patients.(P = .002).
Overall Survival of 58 Patients With Primary Cutaneous Diffuse Large B-Cell Lymphoma, Leg-Type According to the MYD88 Mutation
MarieBeylot-Barry J. Invest Derm Volume 138, Issue 9, September 2018, Pages 1982-1989
Lenalidomide for Cutaneous Diffuse Large B-Cell Lymphoma, Leg-Type
Anecdote with BTK inhibitor
6 had CR and 5 had PR
What is the utility of initial staging for low grade CBCL?
Utility of imaging in cutaneous marginal zone lymphoma and cutaneous follicle center lymphoma
Meenal Kheterpal, Shamir Geller, MD1, Julia Dai, Melissa Pulitzer , Patricia Myskowski, Alison Moskowitz, Ai Ni, Jinah Kim, MD Richard Hoppe, MD, Youn H. Kim, Steven M. Horwitz
1Memorial Sloan Kettering Cancer Center, Stanford University School of Medicine
Retrospective review:Patients with cutaneous presentation of FCL (CFCL) diagnosed between 1997-2016
evaluated at MSKCC or at Stanford UniversityPatients with cutaneous presentation of MZL (CMZL) diagnosed between 1998-2016,
evaluated at MSKCC or at Stanford University
Inclusion criteria:CMZL/CFCL confirmed by pathologists at MSKCC / StanfordSkin was the initial site of presentation of the cutaneous lymphomaImaging study (positron emission tomography scan and/or chest, abdomen and pelvic
computed tomography scan) within 12 months as part of the initial workup.
MZL
Marginal Zone LymphomaClinical characteristics of patients with systemic involvement at
presentation
45.4
63.6
36.4
0
36.4
9.1
45.536.4
18.227.3
9.10
27.3
54.5
0
10
20
30
40
50
60
70
% o
f p
atie
nts
Clinical Characteristics
FCCL
Follicular lymphoma presenting in the skinClinical characteristics of patients with systemic
involvement at presentation89.4
21.1
5.215.8
57.9
21.1 21.16.3
17.6 15.8 21.4
0
33 38.9
0102030405060708090
100%
of
pat
ien
ts
Clinical characteristics
Conclusions• 3.6% of patients with CMZL vs 8.8% of patients with CFCL histology presenting in the skin
have concurrent extracutaneous disease most consistent with systemic B-cell lymphoma
• Of the patients with systemic involvement at presentation, imaging alone detected 81.8% (9/11) of MZL cases and 89.4% (17/19) of FCL cases.
• Due to the rarity of extracutaneous disease, imaging had a low yield in CMZL in follow up
• Bcl2 positivity is suggestive of systemic nodal B-cell lymphoma in patients with CFCL Additionally, subcutaneous involvement, elevated LDH and lower extremity involvement may be associated with a higher likelihood of systemic disease.
• Large lesions with deep subcutaneous involvement in patients presenting with CMZL may be suggestive of systemic B-cell lymphoma although prospectively collected data is needed for validation
Use of low dose radiation for low grade CBCL
Boom Boom Radiation
Treatment
Karen Chau, Joanna Yang, Monica Chelius, Carla Hajj, and Joachim Yahalom
2Gy x 2 RT for Patients with Indolent Lymphomas
Background• Boom boom is 2Gy x 2 RT
– Option for patients with radiosensitive and indolent lymphomas
• Initially published in 1994 by Ganem, et al.1
– 89% of patients had a response
• Literature– Netherlands study (Haas, et al.2)
• 109 patients (304 sites)• Overall response rate was 92% (61% CR and 31% PR)• Median time to local progression: 42 months
– FORT trial (next slide)1 Ganem, GéRard, et al. "Potential role for low dose limited‐field radiation therapy (2× 2 grays) in advanced low‐grade
non‐Hodgkin's lymphomas." Hematological oncology 12.1 (1994): 1-8.2 Haas, R. L. M., et al. "High response rates and lasting remissions after low-dose involved field radiotherapy in indolent
lymphomas." Journal of clinical oncology 21.13 (2003): 2474-2480.
FORT trial• 4Gy versus 24Gy radiotherapy for patients with indolent lymphoma
(FORT): a randomized phase 3 non-inferiority trial
– Eligibility
• 18+ years old with FL or MZL and no previous treatment for at least 1 month pre-RT
– Between April 7, 2006, and June 8, 2011
• 24Gy: 299 sites
• 4Gy: 315 sites
– Median f/u: 26 months (range: 0.39 – 75.4)
FORT trial– Outcomes
• Initial response measured at 12 weeks
– 24Gy: 236 (91%) had a CR/PR
– 4Gy: 227 (81%) had a CR/PR
24Gy 4Gy
Complete response 176 (68%) 137 (49%)
Partial response (>30%) 60 (23%) 90 (32%)
Stable disease (including <30% regression) 22 (8%) 44 (16%)
Progression 2 (<1%) 10 (4%)
Total 260 281
FORT trial– Outcomes
• 91 local progressions (24Gy group: 21; 4Gy group: 70)• Time to local POD with 4Gy was not non-inferior to 24Gy• 24Gy is more effective than 4Gy but 4Gy remains useful alternative
for palliative Tx
• Difference in local progression-free interval at 3 years: 20%
Boom Boom: Retrospective Review of Our Experience at MSKCC
Patient selection• Received 2Gy x 2 RT between 2006 – 2017 at MSKCC
• ≥18 years of age at Dx
• MSKCC confirmed pathology of indolent lymphoma prior to RT
–Follicular lymphoma
–Marginal zone lymphoma
Histology65%
Follicular Lymphoma33% Marginal Zone
Lymphoma
2% Other
Cohort characteristics
54%Early stage
46%Advanced stageInitial stage (early vs. advance)
40%Stage I
13%Stage II
18%Stage III
29%Stage IVInitial stage (breakdown)
First line treatment66%
Other34%
Boom boom RT
Lesion type (nodal vs. extranodal)60%
Extranodal35%
Nodal
5% Both
Timeline
2Gy x 2
(Radiation therapy)
Follow-up at 2 months
(Evaluation of initial response)
Further treatment or
f/u
(if needed)
Response at 2 month f/u (by histology)
CR
PR
NR
Follicular Lymphoma
Response rate: 85%
111 sites
60%(n = 67)
25%(n = 28)
15%(n = 16)
CR
PR
NR
Response rate: 90%
57 sites
72%(n = 41)
18%(n = 10)
10%(n = 6)
Marginal Zone Lymphoma
CR
PR
NR
Nodal
Response rate: 75%60 sites
58%(n = 35)17%
(n = 10)
25%(n = 15)
Response at 2 month f/u (by lesion type)
CR
PR
NR
Response rate: 94%103 sites
71%(n = 73)
23%(n = 24)
6%(n = 6)
Extranodal
In-field progression (pts with initial CR/PR)
n = 109
n = 38
p < 0.001
Conclusion• Patients with FL and MZL in this series appeared to have excellent initial
response
–ORR was 87%
• A complete response is durable
–2 year FFLF: 92%
–5 year FFLF: 85%
• A partial response remains stable/disease-free approximately 50% of the time
• Very low dose radiation appears to be a viable option for pts with PCBCL
How to approach PC-FCCL when it involves lymph nodes?
Cutaneous Large B-cell LymphomaOS by Site
Grange et al J Clin Oncol 19:3602-3610, 2001
2
5
5
0
7
5
10
0
%
0 1 2 3 4 5Years
Leg
Non-Leg
80 yo M with PCFCCL• Multiple lesions – chest and abdomen, 3 mo duration
• Bx outside (1/10): PCFCCL (Large Cells, CD20+ BCL-2+/- BCL-6+ focally, MUM-1 -, CD10+), confirmed also at MSK
• Workup: PET (2/25/2010) : No evidence of FDG-avid lymphoma. CBC, LDH – wnl
• F/U – PR with topical CS, RT was given to a tumor lesion on the back. Local recurrences treated with IL CS
PC-FCCL• Indolent course whether cells large or small
• Large cells in node (same cells) will be often called DLBCL
• Unclear best way to tell whether at that point its an aggressive or indolent lymphoma
• Clinically?
Unusual presentations of PC-MZL?
CD20
CD3
Bcl-2
PC-MZL
• Antigen stimulation
• Secondary to external trauma/stimulation?
• Bicycle helmet straps
• Right leg prosthesis
• Laser hair removal
• Chandelier
Primary Cutaneous B Cell Lymphoma
Overview
Do we need to stage low grade CBCL?
Use of low dose radiation-”Boom- Boom”
PCFCL in nodes
Unusual cases of PC-MZL
MSKCC Cutaneous LymphomaAlison MoskowitzPatricia MyskowskiSarah NoorShamir GellerMeenal KhetterpalJoachim Yahalom-XRT
Dermatopathology
Melissa Pulitzer
Klaus Busam
Travis Hollman
Acknowledgements
Thank you