MEZINÁRODNÍ CENTRUM KLINICKÉHO VÝZKUMU
„TVOŘÍME BUDOUCNOST MEDICÍNY“
Transformation of chronic atopic dermatitis to a cutaneous T- cell lymphoma: a case report
     M. Nečas,  V. Vašků
1st Dept. of Dermatovenereology, Masaryk University Faculty of Medicine, and St. Anne’s Faculty
Hospital in Brno

Patient T.B., born in 1983
Family history: father hay fever , cardiac arrhythmia
                   mother: healthy
                   siblings: brother - asthma, atopic dermatitis, allergy to pollen
                   children: 0

Personal history: common childhood diseases
                       asthma until 10 years
FA: Symbicort 200 inh. Pulv., Xyzal 1-0-0, 0-0-1 Dithiaden
AA: pollen, animal dander, dust mites
Abuse: smoker, little alcohol, coffee once daily
PP: height 181 cm, weight 58 kg,
PSA: Logistics at Pelikan Hard Copy comp., Kyjov,
              Lives with his wife in an apartment house. Animals: water turtle

Course of the disease
Atopic dermatitis since early childhood  / since 4 years of age/
Since 2009 erythroderma   IgE 2300 IU/ml (2010)
since the end of 2010 reccurent herpetication of AD,
thererefore topical KS discontinued. Treaterd repeatedly with  acyclovir
Severe  itching -  antihistamines, sedatives, with minimal effect
8/2010 LN biopsy /left axilla/ - benign lymphadenopathy within AD
Immunophenotyping  of periferal blood T cells (flow cytometry) - normal

Course of the disease
Treated with phototherapy: UVB 311 in spring 2010
for two months and in spring 2011
Inguinal lymphadenopathy appeared in  Aug 2011
Histology of the skin in the right  groin :  epidermotropic peripheral T-
cell lymphoma - mycosis fungoides, patch stage
Lymh node biopsy  /right groin/  histological picture compatible with dermatopatic lymphadenopathy
within MF / SS, LN involvement  is proportional to category I.

Aug 2011



Aug 2011



Aug 2011



Aug 2011



Sept-Oct /2011
Total IGE 11 942 IU/ml
Immunophenotyping  of periferal blood T cells /Flowcytometry/:
CD 3-+4+7 (MF)  cells  make 7,82 % of lymphocytes
Index CD4/CD8   2,157
Biopsy from right thigh: chronic dermatitis of AD type.  Signs
suggestive of mycosis fungoides are insufficient in this preparation.
Material submitted for a second reading and examination of clonality
Clonality test result was unassessable.

0ct-Dec/2011
PUVA : end of 10/2011 to half 12/2011 - terminated because of irritation
5/2012 erysipelas of  the right thigh, treated with procaine penicillin G
for 10 days, at the end benzathin PNC 1,5 MIU applicated.
Later 5 or 6 more erysipelas at the same site happened, probably
because of removed LN in the right groin, treatment with benzathin PNC
was introduced - pendeponization
Total IgE 8 030 IU/ml
flowcytometry - CD3 + 4 + 7 – MF cells make   6.35 % of lymphocytes
index CD4 / CD8   2,612.

July-Sept/2012
July/2012 PET/CT:  slightly increased metabolism in both axillary and inguinal lymphnodes
compatible with  suspected low grade lymphoma
Total IgE  5 837 IU/ ml
9/2012 biopsy from the left trunk : The finding corresponds with subacute
atopic eczema. For the diagnosis of mycosis fungoides there are not
enough signs. Yet sorting of the cells near basement membrane may
preceed the development of lymphoma. Clonality assessment
not possible
Sept/2012  biopsy from left axillary LN : negative for MF

Jan-May/2013
Phototherapy UVA- 1 from Jan 2013  to end of May 2013

Total IgE 6 564 IU/ ml
Immunophenotyping  of periferal blood T cells /flowcytometry/:
CD3+4+7- cells make 7,67% of lymphocytes
Index CD4/CD8   3,324
PET / CT shows stationary finding of a higher FDG activity
in LN of both axillary and groin LN, it might be an activity
accompanying a low grade lymphoma

Sept/2013
Biopsy from the skin lesions in the right forearm
Skin excision with psoriasiform hyperplasia of the epidermis covered by slightly
extended hyperkeratotic slats with small areas of parakeratosis. Papillary dermis
slightly expanded, with a vaguely nodular molded medium-dense infiltrates of
small and medium-sized lymphoid cells somewhere with irregular contours of
nuclei, inconspicuous focal pigment incontinence. Sporadically, the admixture of
eosinophilic granulocytes. In the epidermis rare isolated cells of lymphoid
appearance with cerebriform appearance of nuclei.
There is no sorting of lymphoid cells on the dermo-epidermal junction, no
intraepidermal aggregates of lymphoid cells. Reticular dermis without alteration.
Conclusion: rather chronic eczema/dermatitis. Not all features which
would allow an unambiguous diagnosis fulfilled.  Progression to MF should
be monitored.

Histology
Bohm 147 11.jpg
Photo:  ass. prof. Jedličková, Ph.D.

Nov/2013-Jun/2014
UVA -1 from Nov/2013 to June/2014
IgE   9 164,0 kU/l
9/2014  Flow cytometry  CD4+8+7- cells 8%  index. 2,594
9/2014 biopsy from the forehead skin
Epidermis with reduced straum corneum, distinct acanthosic pins.
Beneath the epidermis there are dense spherical lymphohistiocytic
infiltrates with deposits of pigment. Lymphocytes focally enter epidermis
RES: Density of the infiltrates and the character of the invasion of
lymphocytes into the epidermis is very suggestive of mycosis fungoides,
material sent for  immunostaining.
Clonality test: Isolated DNA of poor quality. Clonality can not be
assessed. Consider retesting for clonality and consultation in another
laboratory.

Histology
bohm 108 14 a.jpg
Photo:  ass. prof. Jedličková, Ph.D.

Sep/2014



Sep/2014



Sep/2014



Sep/2014



Nov/2014
Nov/2014 Treatment with acitretin 40 mg daily
                + interferon a gradually increased to 6 MIU 3 times a week s.c.
Jan/2015 skin finding except the face satisfactory, significant reduction of
lymphatic nodes
Tolerance of the treatment - very good
Laboratory findings satisfactory - slight elevation of LT and lipids
acitretin reduced to 30 mg daily, interferon a to 4.5 MIU 3 times a week

1/2015
Jan/2015 PET CT:
significant metabolic and size regression of axillary and inguinal LN
higher metabolism of bone marrow especially in the pelvic bone and of the spine of unclear
etiology. Several minor active areas in the       S8 / 9 segment of the lungs –probably a
postinflammatory       change
light progression of the spleen size
PET CT Bohm 1 2015.jpg

Feb/2015-May/2015
2/2015: bone marrow aspiration  was performed  from the left hip
result:  histologically in the bone marrow without an evidence of the
             infiltration of the bone marrow with a lymphoma
flowcytometry - normal
in myelogram rare atypical lymphocytes
res: no ivolvement of bone marrow by a lymphoma
5/2015 acitretin reduced to 20 mg daily, interferon a left  on dose of
4.5 MIU 3 times a week
Laboratory: LT and cholesterol normalized

Jun/2015-Sept/2016
6/2015  flowcytometry : CD4+8+7-  13% of lymphpocytes
index CD4/CD8 3,538
10/2015 total IgE 5 770 IU/ml
5/2016 total IgE 6 305 IU/ml
Lab: slight leucopenia (minim. 3,4 109/l) between 9/2015 and 11/2015
Interferon a reduced to 3 MIU and then to 1,5 MIU 3 times a week
7/2016 flowcytometry : CD4+8+7-       7,4 % of lymphocytes
index CD4/CD8     2,647

Sept/2016
DSC_5843.JPG


Sept/2016
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Sept/2016
DSC_5838.JPG


Sept/2016
DSC_5837.JPG


Classification of CTCL
Primary cutaneous T-cell and NK-cell lymphomas
Mycosis fungoides
Variants of mycosis fungoides: Folliculotropic mycosis fungoides
                                                  Pagetoid reticulosis
                                                  Granulomatous slack skin
Sezary syndrome
Leukemia/adult T-cell lymphoma
CD30+ T-cell lymphoproliferative hyperplasias: CD30+ anaplastic large T-cell lymphoma
                                                                            Lymphomatoid papulosis
Subcutaneous panniculitis-like T-cell lymphoma
Extranodal NK/T-cell lymphoma, nasal type
Primary cutaneous peripheral T-cell lymphomas, unclassified
Primary cutaneous aggressive epidermotropic CD8+ T-cell lymphoma
Cutaneous γ/δ T-cell lymphoma
Primary cutaneous small/medium CD4+ T-cell lymphoma

Discussion
AD associated CTCL – quite rare:
CD30+ lymphomas ( 8 cases)
Sezary syndrome ( 2 cases)
Mycosis fungoides ( 3 cases)
Probably underdiagnosed (or unpublished)

Discussion
•Mechanisms leading to the development of
    malignant T cell population:
•
•Chronic antigenic stimulation (of cutaneous
•lymphocytes) or chronic inflammation itself
•Immunosupressive nature of the disease,
•Treatment (cyclosporine, TIMs)
•Phototherapy??
•

Conclusion
In a long lasting severe AD dermatologist must be aware of
posssible transformation of the condition to a CTCL
especially if the diseases does not react properly to
usual treatment of AD
Repeated histology, immunophenotyping, flow cytometry,
TCR gene rearrangement (clonality)
Staging (X-ray, CT, PET/CT, US of LN or biopsy,
              bone marrow biopsy or trepanobiopsy)

Markers to differentiate AD/CTCL
sIL-2R, serum LDH, IgE  - elevated in both
Low specific IgE, high CD4/8 ratio  - usualy in CTCL
CCL 17 (TARC) – CCL 8 or CCR 4     elevated in both
CCR 11 and CCR 26 – CCR 3            elevated in both
CCL 27 (CTAC) – CCR 10                  elevated in CTCL
FoxP3+ regulatory T cells (T regs) elevated in AD not CTCL
Hanafusa T, Matsui S, Murota H, Tani M, Igawa K, and Katayama I. Increased frequency of
skin-infiltrating FOXP3+ regulatory
T cells as a diagnostic indicator of severe atopic dermatitis from cutaneous T cell lymphoma. Clin
Exp Immunol. 2013 Jun,
172(3): 507-512

MEZINÁRODNÍ CENTRUM KLINICKÉHO VÝZKUMU
„TVOŘÍME BUDOUCNOST MEDICÍNY“
Thank you for your attention
contact:
miroslav.necas@fnusa.cz
St. Ann´s Faculty Hospital Brno
Pekařská 53, Brno 656 91
Czech Republic
Phone:  + 420 543 181 111

 www.fnusa.cz
CZ1411270226/11/2014