An approach to diagnosis of T‐cell lymphoproliferative disorders by flow cytometry

Gorczyca, Wojciech; Weisberger, James; Liu, Z.; Tsang, Patricia; Hossein, Monowar; Wu, Chaowei; Dong, Henry Y.; Wong, John Y. L.; Tugulea, Sorina; Dee, Simpson L.; Melamed, Myron R.; Darzynkiewicz, Zbigniew

doi:10.1002/cyto.10003

Cited by 121 publications

(80 citation statements)

References 33 publications

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“…Expression of one or more pan-T-cell antigens (CD45RO, CD2, CD3, CD5, and CD7), absence of pan-B-cell antigens, and histopathologic findings combine to make the diagnosis (8). In the West, nodal PTCL-NOS predominates, whereas in the East extranodal PTCL is more common, particularly the nasal type.…”

Section: Introductionmentioning

confidence: 99%

Transcript profiling in peripheral T-cell lymphoma, not otherwise specified, and diffuse large B-cell lymphoma identifies distinct tumor profile signatures

Mahadevan

Spier²,

Croce

et al. 2005

Molecular Cancer Therapeutics

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To glean biological differences and similarities of peripheral T-cell lymphoma-not otherwise specified [PTCL-NOS] to diffuse large B-cell lymphoma (DLBCL), a transcriptosome analysis was done on five PTCL-NOS and four DLBCL patients and validated by quantitative real-time reverse transcription-PCR on 10 selected genes. Normal peripheral blood T cells, peripheral blood B cells, and lymph node were used as controls. The resultant gene expression profile delineated distinct ''tumor profile signatures'' for PTCL-NOS and DLBCL. Several highly overexpressed genes in both PTCL-NOS and DLBCL involve the immune network, stroma, angiogenesis, and cell survival cascades that make important contributions to lymphomagenesis. Inflammatory chemokines and their receptors likely play a central role in these complex interrelated pathways: CCL2 and CXCR4 in PTCL-NOS and CCL5 and CCR1 in DLBCL. Highly overexpressed oncogenes unique to PTCL-NOS are SPI1, STK6, a-PDGFR, and SH2D1A, whereas in DLBCL they are PIM1, PIM2, LYN, BCL2A1, and RAB13. Oncogenes common to both lymphomas are MAFB, MET, NF-kB2, LCK, and LYN. Several tumor suppressors are also down-regulated (TPTE, MGC154, PTCH, ST5, and SUI1). This study illustrates the relevance of tumor-stroma immune trafficking and identified potential novel prognostic markers and targets for therapeutic intervention.

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Section: Introductionmentioning

confidence: 99%

Transcript profiling in peripheral T-cell lymphoma, not otherwise specified, and diffuse large B-cell lymphoma identifies distinct tumor profile signatures

Mahadevan

Spier²,

Croce

et al. 2005

Molecular Cancer Therapeutics

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“…Abnormal T-cell populations are detected by identifying diminished or absent expression of T-cell surface-antigen expression. 20 The most commonly described aberrant immunophenotype in MF/SS is the loss of surface CD7 expression, [20][21][22] but diminished CD7 expression has also been noted in reactive T-cell populations. 22,23 Other possible aberrant T-cell antigen expression profiles in MF/ SS include diminished CD2, CD3, and/or CD26 expression.…”

Section: Discussionmentioning

confidence: 99%

Cytologic evaluation of lymphadenopathy associated with mycosis fungoides and Sezary syndrome

Pai

Mullins

Kim

et al. 2008

Cancer

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“…Prawidłowe komórki T-LGL charakteryzują się fenotypem CD2+CD3+CD4-CD5+CD7+CD8+CD16--C D 5 6 -T C R a b + i T C R g d -. Ko m ó r k i nowotworowe T-LGL mają również fenotyp dojrzałych komórek T lub NK, ale w 80% wykazują nieprawidłową ekspresję antygenów pan-T-komórkowych, na przykład CD5 czy CD7, oraz obecność antygenów komórek NK, takich jak CD16+ (w 80%) i CD57+ (100%) [19,59,60]. Antygen CD57 jest charakterystycznym markerem białacz-ki T-LGL, co sugeruje, że białaczkowe limfocyty T-LGL pochodzą z CD57(-) komórek T pamięci, które nabywają antygen CD57 jako komórki efektorowe [61].…”

Section: Badania Diagnostyczneunclassified

“…Komórki przewlekłej białaczki/przetrwałej limfocytozy reaktywnej NK-LGL wykazują ekspresję antygenów CD2+CD16+CD56+, brakuje ekspresji CD3, a antygen CD57 występuje ze zmienną częstością [17,87]. U pacjentów z przewlekłą białaczką NK-LGL opisano ponadto zmienioną ekspresję trzech rodzin receptorów związanych z komórkami NK, receptorów KIR, typu C i receptorów NK [60,88,89]. Panel przeciwciał przeciw tym receptorom mógłby być bardzo użyteczny w diagnostyce różnicowej przewlekłej białaczki NK i reaktywnej limfocytozy NK.…”

Section: Przewlekłe Choroby Limfoproliferacyjne Z Komórek Nkunclassified

Białaczki z dużych ziarnistych limfocytów T i komórek naturalnej cytotoksyczności

Budziszewska¹

2015

Hematologia

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Streszczenie Białaczki z dużych ziarnistych limfocytów (LGL) obejmują biologicznie heterogenną grupę rzadkich nowotworów układu chłonnego wywodzących się z limfocytów T (T-LGL) lub z komórek naturalnej cytotoksyczności (NK-LGL Abstract Leukemias of large granular lymphocytes (LGL) include a heterogeneous group of rare lymphoid malignancies derived from T cells (T-LGL) and natural killers (NK-LGL) T-LGL leukemia arises from long-term antigen stimulation and the survival of LGL cells is associated with constitutive activation of anti-apoptotic intracellular pathways JAK/STAT, RAS/RAF/MEK/ERK

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An approach to diagnosis of T‐cell lymphoproliferative disorders by flow cytometry

Cited by 121 publications

References 33 publications

Transcript profiling in peripheral T-cell lymphoma, not otherwise specified, and diffuse large B-cell lymphoma identifies distinct tumor profile signatures

Transcript profiling in peripheral T-cell lymphoma, not otherwise specified, and diffuse large B-cell lymphoma identifies distinct tumor profile signatures

Cytologic evaluation of lymphadenopathy associated with mycosis fungoides and Sezary syndrome

Białaczki z dużych ziarnistych limfocytów T i komórek naturalnej cytotoksyczności

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