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Indolent CD56-Positive Clonal T-Cell Lymphoproliferative Disease of the Stomach Mimicking Lymphomatoid Gastropathy
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Brief Case Report
Indolent CD56-Positive Clonal T-Cell Lymphoproliferative Disease of the Stomach Mimicking Lymphomatoid Gastropathy
Mineui Hong, Won Seog Kim1, Young Hyeh Ko,
Korean Journal of Pathology 2014;48(6):430-433.
DOI: https://doi.org/10.4132/KoreanJPathol.2014.48.6.430
Published online: December 31, 2014

Department of Pathology, Hematology-Oncology Section, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea

1Department of Medicine, Hematology-Oncology Section, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea

Corresponding Author: Young Hyeh Ko, M.D. Department of Pathology, Samsung Medical Center, Sungkyunkwan University School of Medicine, 81 Irwon-ro, Gangnam-gu, Seoul 135-710, Korea Tel: +82-2-3410-2762, Fax: +82-2-3410-0025, E-mail: yhko310@skku.edu
• Received: July 8, 2014   • Revised: September 4, 2014   • Accepted: September 12, 2014

© 2014 The Korean Society of Pathologists/The Korean Society for Cytopathology

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

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Natural killer (NK)- or T-cell lymphomas of the gastrointestinal (GI) tract are uncommon, accounting for less than 10% of all malignant lymphomas arising in the GI tract [1]. According to the third national survey by the Hematopathology Study Group of the Korean Society of Pathologists, peripheral T-cell lymphoma, not otherwise specified (PTCL-NOS), is the most common type, followed by extranodal NK/T-cell lymphoma, nasaltype (ENKL). Enteropathy-associated T-cell lymphoma (EATL) is rare [1]. Malignant lymphoma of T and NK lineage is an aggressive disease with poor prognosis [2]. Recently, two indolent forms of mature T- or NK-cell lymphoproliferative diseases (LPD) of the GI tract have drawn the attention of pathologists. One is indolent NK cell proliferative lesion of the stomach and intestine reported under the name of lymphomatoid gastropathy [3] or NK-cell enteropathy [4]. The lesion is often self-limited, even when left untreated. Histological findings have been described as dense infiltration of lymphoid cells with mild to moderate atypia and peculiar eosinophilic cytoplasmic granules [3]. Frequently, there are lymphoepithelial lesion-like changes with or without necrosis. All cases published previously have been positive for both cytoplasmic CD3 and CD56 and negative for CD4 and CD8. T-cell receptor (TCR) gene rearrangement is polyclonal [3-5], and unlike ENKL, infiltrating cells were negative for Epstein-Barr virus (EBV). The other form of indolent T- or NK-cell LPD of the GI tract is a clonal T-cell proliferative disease involving the oral cavity, esophagus, stomach, small intestine, and colon [6]. The lesion shows a superficial and nondestructive lymphoid infiltrate that occasionally extends into the muscularis mucosae and submucosa. Infiltrating cells are small T-cells, which are CD4+ or CD8+ or uncommonly CD4/CD8phenotype [6-9]. CD56 and EBV-encoded RNA (EBER) are negative, and TCR gene rearrangement has been monoclonal in all cases reported so far. Unlike indolent NK-cell proliferative lesions, indolent T-cell LPD does not spontaneously regress, but is persistent without progression [6,9]. These two indolent entities can be easily mistaken as aggressive T- or NK-cell lymphoma; therefore, recognition of these entities is important to avoid unnecessary aggressive chemotherapy. Herein we report, to our knowledge, the first Korean case of indolent T-cell LPD of the stomach with expression of CD56.
A 41-year-old Korean woman without any symptoms was admitted to the hospital for her annual health checkup. Gastric endoscopy revealed diffuse mucosal atrophy, multiple ulcers, and ulcer scars up to 1.2 cm with surrounding mucosal nodularity on the body and proximal antrum. On sigmoidoscopy, no abnormal findings were observed. The chest and abdominal computed tomography (CT) showed mild and diffuse wall thickening of the stomach. On positron-emission tomography (PET), a focal increased 18F-2-fluoro-2-deoxy-D-glucose uptake in the lower body of the stomach was present. There was no organomegaly or significant lymphadenopathy.
Biopsies from the stomach revealed erosion of the mucosa with diffuse infiltration of small to medium atypical lymphoid cells in expanded lamina propria. Atypical lymphocytes had clear and abundant cytoplasm. The nuclei were round or indented with dispersed chromatin and inconspicuous nucleoli. Some of the atypical lymphocytes had eosinophilic cytoplasmic granules. The granules were less eosinophilic and finer than those of eosinophils. The gastric glands had been invaded by atypical cells leading to lymphoepithelial lesion-like appearance. Many plasma cells, eosinophils, and neutrophils were mixed with atypical lymphocytes. There was also focal necrosis. Angiocentric infiltration of atypical cells was not observed. Helicobacter pylori was seen on the surface of the mucosa. The atypical cells expressed cytoplasmic CD3, CD56, TIA-1, and granzyme B, but were negative for CD4, CD8, CD30, βF1, and TCRγ. The Ki-67 labeling index was low. EBER was not detected in any biopsies using in situ hybridization. Polymerase chain reaction analysis for TCRγ gene rearrangement revealed monoclonality (Fig. 1). Because the initial diagnosis was PTCL-NOS, Ann Arbor stage IE, the patient was treated with chemotherapy including cyclophosphamide, doxorubicin, vincristine, and prednisone for six cycles during 4 months. The patients achieved complete remission (CR) through three cycles of primary chemotherapy. Nine months after initial CR, the patient had no symptoms, but gastric biopsy revealed similar lesions in the lower body, antrum, and fundus. The patient postponed further therapy for 30 months and underwent regular follow-up with endoscopy and CT. During the 30 months, eight gastric biopsies revealed a persistent lesion, but there was no progression of the lesion in the stomach or to other sites. After 30 months, radiotherapy was given with disappearance of the infiltrate. However, 10 months later, a biopsy revealed reappearance of the infiltrate at the same site of the stomach. Subsequently, the patient was not been treated, but was checked by endoscopy and CT or PET. At 72 months after the first diagnosis, the patient still had localized gastric lesion, but no symptoms.
Indolent T-cell LPD of the GI tract is a nonprogressive clonal T-cell LPD. Chemotherapy is not effective, with little or no response, and most patients have persistent disease localized to the GI tract. Among 22 cases reported so far, all patients were alive during follow-up except for two patients who died of disease at 176 months [7] and 132 months [8] after diagnosis because of progression to other organs, and large cell transformation, respectively. The clinical course of the present case was indolent. The lesion responded transiently to chemotherapy or radiotherapy, but relapsed shortly after. Multiple biopsies showed a persistent lesion for 6 years without progression.
Abnormal infiltration of CD3+ CD56+ EBV-monoclonal T-lymphoid cells, which replaced the lamina propria of the gastric mucosa, led to the misdiagnosis of PTCL-NOS. CD56 is a marker of NK cells, but is expressed in various types of aggressive NK- or T-cell lymphomas of the GI tract including ENKL, EATL type II, and a subset of PTCL-NOS [2]. ENKL can be easily excluded because of EBV negativity in indolent T-cell LPD. In EATL type II, tumor cells are monomorphic and medium sized, and do not show eosinophilic granules of the cytoplasm as seen in the present case. In immunohistochemistry, tumor cells are usually CD4CD8+CD56+, and less frequently CD4CD8CD56+. Because indolent T-cell LPD shows superficial infiltration of small, mature appearing lymphoid cells with a low Ki-67 labeling index of less than 10%, Ki-67 staining is important for excluding aggressive T-cell lymphoma such as PTCL-NOS or EATL [6].
Histological and immunohistochemical findings of present case are very similar to those of lymphomatoid gastropathy. Atypical cells of lymphomatoid gastropathy are NK-cells with a CD4CD5CD8CD56+TCRβF1TCRδγTIA-1+GranzymeB+ immunophenotype and no clonality detected by TCR gene rearrangement [3,4]. In the present case, infiltrated cells were CD4CD56+CD8TCRβF1TCRγTIA-1+, which might suggest NK cell origin, but gene rearrangement analysis demonstrated a T-cell lineage of atypical cells. Clinically, most patients with lymphomatoid gastropathy undergo spontaneous regression without treatment [3-5]. A few patients relapsed, but none of the patients died. Unlike lymphomatoid gastropathy, our patient had nonprogressive, but persistent disease. Treatment was not effective.
The CD4CD8CD56+TCR-silent phenotype is uncommon among the indolent T-cell LPD of the GI tract reported thus far. In a large series of indolent T-cell LPDs reported by Perry et al. [6], the infiltrates comprised mainly of CD4CD8+CD56TCRβF1+ T-cells. There was one case showing a CD4CD8CD56TCRβF1+ T-cell phenotype and one case showing a CD4+CD8CD56TCRβF1+ T-cell phenotype [6]. Other reports for indolent T-cell LPD have described cases with CD4+ T-cell phenotype [7,8]. Although atypical cells did not express TCR, one may raise the possibility of γδ T-cells or NKT-cells as the pathogenesis of our case. NKT-cells represent a minor subset of T-lymphocytes that share cell-surface proteins with conventional T-cells and NK-cells [9]. In the intestine, these cells are located among intraepithelial lymphocytes and within the lamina propria. The role of NKT-cells is related to mucosal immunity. A group of T-cells coexpress NK markers, so-called γδNKT-cells, constitute 1%–5% of the blood or peripheral organ lymphocytes. γδNKT-cells express a γδTCR instead of an αβTCR. These subsets can include CD4+, CD8+, CD4+/CD8+, and a minor subset (1%–2%) of double negative [10].
In summary, this is the first case of indolent T-cell proliferative disease of the GI tract with expression of CD56, which needs to be distinguished from aggressive T- and NK-cell lymphoma and indolent lymphomatoid gastropathy. While the origin and function of CD4CD8CD56+TCR-silent T-cells remain to be explored, our case expands the immunophenotypic spectrum of indolent T-cell LPD.
Fig. 1.
Indolent T-cell lymphoproliferative disease. (A) Gastroendoscopy reveals diffuse mucosal atrophy and nodular elevated lesions with ulcer. (B) The mucosa is infiltrated by small lymphoid cells that invaded the gastric glands. (C) Some of the atypical cells have eosinophilic cytoplasmic granules, which are described in lymphomatoid gastropathy. Immunohistochemically, lymphoid cells are CD3+ (D) and CD56+ (E). (F) BIOMED-II multiplex PCR for TCRγ gene rearrangement demonstrates clonal peaks.
kjpathol-48-6-430f1.jpg
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    Indolent CD56-Positive Clonal T-Cell Lymphoproliferative Disease of the Stomach Mimicking Lymphomatoid Gastropathy
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    Fig. 1. Indolent T-cell lymphoproliferative disease. (A) Gastroendoscopy reveals diffuse mucosal atrophy and nodular elevated lesions with ulcer. (B) The mucosa is infiltrated by small lymphoid cells that invaded the gastric glands. (C) Some of the atypical cells have eosinophilic cytoplasmic granules, which are described in lymphomatoid gastropathy. Immunohistochemically, lymphoid cells are CD3+ (D) and CD56+ (E). (F) BIOMED-II multiplex PCR for TCRγ gene rearrangement demonstrates clonal peaks.
    Indolent CD56-Positive Clonal T-Cell Lymphoproliferative Disease of the Stomach Mimicking Lymphomatoid Gastropathy

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