Cutaneous T-cell lymphoma (CTCL): Current practices in blood assessment and the utility of T-cell receptor (TCR)-Vβ chain restriction

Gibson, Juliet Fraser; Huang, Jing; Liu, Kristina J.; Carlson, Kacie R.; Foss, Francine M.; Choi, Jaehyuk; Edelson, Richard L.; Hussong, Jerry W.; Mohl, Ramsey; Hill, Sally M.; Girardi, Michael

doi:10.1016/j.jaad.2015.12.018

Cited by 39 publications

(49 citation statements)

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“…Malignant T cells were identified by their expression of a dominant TCRVb clone (SS6, SS8, SS9, SS10, and SS11) and their characteristic low expression of CD7 and/or CD26. 12,13 In accordance with the Declaration of Helsinki, the samples were obtained with informed consent after approval by the Committee on Health Research Ethics (H-16025331).…”

Section: Malignant Cells From Patients With Ssmentioning

confidence: 99%

“…Dead cells were removed using 7-amino-actinomycin D, and after demultiplexing, malignant cells were gated based on low expression of CD7 and/or CD26. 12,13 The 240 screened surface markers were filtered as "expressed" by having at least 10% of cells from at least 1 patient expressing more than the median fluorescence intensity (MFI) of the isotype plus 10 standard deviations (SDs) of the isotype: MFI 90% quantile . (MFI Isotype 1 10 3 SD Isotype ).…”

Section: Surface Marker Screeningmentioning

confidence: 99%

“…[7][8][9][10][11] Malignant SS cells often exhibit abnormal expression of T-cell surface markers and can be isolated on the basis of their clonal T-cell receptor (TCR) or their characteristic low expression of CD7 and/or CD26. 12,13 On the basis of their presence in the blood and lymph nodes and their expression of distinct surface markers such as CD197 (CCR7), CD27, and CD62L (L-selectin), SS cells are suspected to derive from transformed central memory T (T CM ) cells. 14 However, studies have found that although the majority of malignant cells from most patients with SS do exhibit a T CM surface phenotype, some malignant cells express surface markers inconsistent with the T CM phenotype, such as high levels of CD45RA.…”

Section: Introductionmentioning

confidence: 99%

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Single-cell heterogeneity in Sézary syndrome

et al. 2018

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Sézary syndrome (SS) is an aggressive leukemic variant of cutaneous T-cell lymphoma (CTCL) with a median life expectancy of less than 4 years. Although initial treatment responses are often good, the vast majority of patients with SS fail to respond to ongoing therapy. We hypothesize that malignant T cells are highly heterogeneous and harbor subpopulations of SS cells that are both sensitive and resistant to treatment. Here, we investigate the presence of single-cell heterogeneity and resistance to histone deacetylase inhibitors (HDACi) within primary malignant T cells from patients with SS. Using single-cell RNA sequencing and flow cytometry, we find that malignant T cells from all investigated patients with SS display a high degree of single-cell heterogeneity at both the mRNA and protein levels. We show that this heterogeneity divides the malignant cells into distinct subpopulations that can be isolated by their expression of different surface antigens. Finally, we show that treatment with HDACi (suberanilohydroxamic acid and romidepsin) selectively eliminates some subpopulations while leaving other subpopulations largely unaffected. In conclusion, we show that patients with SS display a high degree of single-cell heterogeneity within the malignant T-cell population, and that distinct subpopulations of malignant T cells carry HDACi resistance. Our data point to the importance of understanding the heterogeneous nature of malignant SS cells in each individual patient to design combinational and new therapies to counter drug resistance and treatment failure.

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Section: Malignant Cells From Patients With Ssmentioning

confidence: 99%

Section: Surface Marker Screeningmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Single-cell heterogeneity in Sézary syndrome

et al. 2018

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“…FISH technology particularly suits CTCL, a cancer whose mutational landscape is characterized by a preponderance of gene copy number amplifications and deletions compared to single nucleotide variants relatively overrepresented in many other forms of cancer. In this study, we used the 11-probe panel to assess for genetic abnormalities in sorted or unsorted peripheral blood from 24 patients (patient characteristics in Supplementary Materials) with a range of disease presentations including SS, patch/plaque mycosis fungoides (MF), follicular mycosis fungoides (F-MF), tumor-stage mycosis fungoides, and follicular mucinosis –with evidence of blood involvement (Gibson et al , 2016). …”

Section: To the Editormentioning

confidence: 99%

FISH Panel for Leukemic CTCL

Weed

Gibson

Lewis

et al. 2017

Journal of Investigative Dermatology

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“…Впоследнеевремя,согласнорекомендациямНациональногоонкологическогообщества,дляпостанов-кидиагнозаТКЛКпроводитсябиопсияпатологических участковкожиспоследующимгистоморфологическим, иммуногистохимическимимолекулярно-генетическим анализом(трансформациягенаTCR).Осмотрипальпация кожи остаются основными при подозрении наТКЛК.ОбязательнойявляетсяпальпацияЛУ [24,81,84].Достаточночастодляпостановкиокончательного диагнозаТКЛКпоказанопроведениесериибиопсий, таккакморфологическиеифенотипическиепризнаки ТКЛКвариабельныиприоднократнойбиопсиисуществуетрискнеправильногодиагноза [32,33,81,84,85]. ИдентификациязлокачественныхклетоквПКпаци-ентовсТКЛКнеоценимадлядиагностикиипрогноза СС на ранних стадиях [86,87]. Однако анализ крови имеетограниченнуюценностьиз-заотсутствияточного высокочувствительного маркера для диагностики клетокСезари.Внастоящеевремяотсутствиемаркеров СD7и / илиCD26наСD4-клеткахявляетсясуррогатнымпоказателемзлокачественности.Лактатдегидрогеназаявляетсянеспецифическиммаркеромопухолевой нагрузки и указывает на неблагоприятный прогноз ТКЛК [24,29,88].…”

Section: диагностикаunclassified

Cutaneous T-cell lymphomas: modern data of pathogenesis, clinics and therapy

2018

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Контакты: Ольга Михайловна Демина demina.om@mail.ru Т-клеточные лимфомы кожи (ТКЛК) представляют собой гетерогенную группу экстранодальных неходжкинских лимфом, которые характеризуются инфильтрацией кожи злокачественными моноклональными Т-лимфоцитами. Чаще болеют взрослые в возрасте от 55 до 60 лет, годовая заболеваемость составляет около 0,5 на 100 тыс. человек. Грибовидный микоз, синдром Сезари и СD30 + лимфопролиферативные заболевания являются основными подтипами ТКЛК. На сегодняшний день ТКЛК имеют сложную концепцию этиопатогенеза, диагностики, терапии и прогноза. В статье представлены обобщенные данные по этой проблеме. Ключевые слова: Т-клеточные лимфомы кожи, экспрессия генов, противоопухолевое лечение Для цитирования: Демина О.М., Акилов О.Е., Румянцев А.Г. Т-клеточные лимфомы кожи: современные данные патогенеза, клиники и терапии. Онкогематология 2018;13(3):25-38Cutaneous T-cell lymphomas (CTCL) are a heterogeneous group of extranodal non-Hodgkin's lymphomas that are characterized by skin infiltration with malignant monoclonal T lymphocytes. More common in adults aged 55 to 60 years, the annual incidence is about 0.5 per 100 000 people. Mycosis fungoides, Sézary syndrome and CD30 + lymphoproliferative diseases are the main subtypes of CTCL. To date, CTCL have a complex concept of etiopathogenesis, diagnosis, therapy and prognosis. The article presented summary data on these issues.For citation: Demina O.M., Akilov O.E., Rumyantsev A.G. Cutaneous T-cell lymphomas: modern data of pathogenesis, clinics and therapy. Onkogematologiya = Oncohematology 2018;13(3):25-38

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Cutaneous T-cell lymphoma (CTCL): Current practices in blood assessment and the utility of T-cell receptor (TCR)-Vβ chain restriction

Cited by 39 publications

References 29 publications

Single-cell heterogeneity in Sézary syndrome

Single-cell heterogeneity in Sézary syndrome

FISH Panel for Leukemic CTCL

Cutaneous T-cell lymphomas: modern data of pathogenesis, clinics and therapy

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