Progression of mycosis fungoides occurs through divergence of tumor immunophenotype by differential expression of HLA-DR

Murray, Duncan; McMurray, Jack; Eldershaw, Suzy; Pearce, Hayden; Davies, Nick; Scarisbrick, Julia; Moss, Paul

doi:10.1182/bloodadvances.2018025114

Cited by 27 publications

(24 citation statements)

References 34 publications

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“…Ki-67 proliferation indices increase as the disease progresses, with tumor stage evolution or transformation to larger cells and may correlate with prognosis (Edinger, Clark, Pucevich, Geskin, & Swerdlow, 2009;Raghavan, Hong, Kim, & Kim, 2019). CD25 can also be identi- Although not routinely used at this time, FC of skin specimens may be able to distinguish between tumor cell and tumor infiltrating lymphocyte "immune escape" phenotypes using clonotypic TCR-Vβ staining and activation/exhaustion markers such as PD-1 and programmed death receptor ligand-1 (PD-L1), with the potential for eventual therapeutic stratification (Murray et al, 2019). FC has identified both small and large cell shared monoclonal populations in MF not seen by immunohistochemistry, with CD3+/CD26− T cells accounting for 70% of MF cases, and absent CD7 only in 57% of cases.…”

Section: Immunophenotyping Of Mf Cells In Skinmentioning

confidence: 99%

“…FC analysis of lymphocytes from mechanically extracted and digested skin biopsy specimens has shown diagnostic T‐cell aberrancies in patients with clinical and histologic findings consistent with MF, and not with indeterminate or negative findings (Jokinen et al, 2011; Oshtory, Apisarnthanarax, Gilliam, Cooper, & Meyerson, 2007). Although not routinely used at this time, FC of skin specimens may be able to distinguish between tumor cell and tumor infiltrating lymphocyte “immune escape” phenotypes using clonotypic TCR‐Vβ staining and activation/exhaustion markers such as PD‐1 and programmed death receptor ligand‐1 (PD‐L1), with the potential for eventual therapeutic stratification (Murray et al, 2019). FC has identified both small and large cell shared monoclonal populations in MF not seen by immunohistochemistry, with CD3+/CD26− T cells accounting for 70% of MF cases, and absent CD7 only in 57% of cases.…”

Section: Diagnosis Of Mf and Ss: Role Of Immunophenotypingmentioning

confidence: 99%

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Sézary syndrome and mycosis fungoides: An overview, including the role of immunophenotyping

Pulitzer

Horna

Almeida

2020

Cytometry Part B Clinical

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This review discusses the definition and major categories of cutaneous T-cell lymphoma, Sézary syndrome and mycosis fungoides, and the role of immunophenotyping in their diagnosis. The following key points are raised: (a) Sézary syndrome and mycosis fungoides cells most often have a characteristic CD3+ CD4+ CD7− and/or CD26− immunophenotype. (b) This immunophenotype is not specific, but can assist in the distinction from non-neoplastic T cells and other subtypes of mature T-cell neoplasm.

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Section: Immunophenotyping Of Mf Cells In Skinmentioning

confidence: 99%

Section: Diagnosis Of Mf and Ss: Role Of Immunophenotypingmentioning

confidence: 99%

Sézary syndrome and mycosis fungoides: An overview, including the role of immunophenotyping

Pulitzer

Horna

Almeida

2020

Cytometry Part B Clinical

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“…However, it has been shown that CD8+ T-cells are unable to exert an effective cytotoxic action, resulting in immune tolerance against the malignant CD4+ T-cells [15]. Specifically, TILs in MF patients exhibit an exhausted phenotype, which is characterized by the upregulation of various co-inhibitory receptors such as PD-1 (program death 1, encoded by PDCD1) and TIM-3 (T cell immunoglobulin and mucin domain-containing protein 3, encoded by HAVCR2/TIM-3) [99]. Transient upregulation of co-inhibitory receptors on T-cells can serve as a homeostatic mechanism to maintain self-tolerance and prevent excessive immune response [100].…”

Section: Immune Checkpointsmentioning

confidence: 99%

“…However, one study showed an upregulation of HAVCR2 and PDCD1 from isolated CD8+ T-cells of MF lesions, which suggests that these co-inhibitory genes are predominantly associated with the non-malignant T-cells [15]. However, it is also known that MF cells frequently express PD-1 [99]. Specifically, the interaction of PD-1 with its ligand, PD-L1/L2, transduces a negative signal that inhibits T-cell proliferation and cytotoxicity, impeding effective anti-tumor response [102].…”

Section: Immune Checkpointsmentioning

confidence: 99%

Patterns of Gene Expression in Cutaneous T-Cell Lymphoma: Systematic Review of Transcriptomic Studies in Mycosis Fungoides

Motamedi

Xiao

Iyer

et al. 2021

Cells

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Mycosis fungoides (MF) is the most prevalent type of skin lymphoma. In its early stages, it has a favorable prognosis. However, in its late stages, it is associated with an increased risk of mortality. This systematic review aimed to identify the transcriptomic changes involved in MF pathogenesis and progression. A literature search was conducted using the database PubMed, followed by the extraction of 2245 genes which were further filtered to 150 recurrent genes that appeared in two or more publications. Categorization of these genes identified activated pathways involved in pathways such as cell cycle and proliferation, chromosomal instability, and DNA repair. We identified 15 genes implicated in MF progression, which were involved in cell proliferation, immune checkpoints, resistance to apoptosis, and immune response. In highlighting the discrepancies in the way MF transcriptomic data is obtained, further research can focus on not only unifying their approach but also focus on the 150 pertinent genes identified in this review.

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“…Σε πρόσφατη μελέτη από τους Murray et al, βρέθηκε ότι η IL-17 παράγεται από τα κακοήθη λεμφοκύτταρα του δέρματος στη σπογγοειδή μυκητίαση, αλλά κι από ένα ποσοστό φυσιολογικών Τ-λεμφοκυττάρων που διηθούν τις δερματικές βλάβες και βοηθούν στην άμυνα του οργανισμού (TILs: Tumor infiltrating cells). Επίσης παρατηρήθηκε ότι η έκφραση της IL-17 ήταν αυξημένη ιδίως στα αρχικά στάδια της νόσου και μειωνόταν σε πιο προχωρημένα στάδιά της 74 .…”

Section: η ε π ι δ ρ α σ η τ ω ν I L -1 7 a I L -1 7 F κ α ι I L -2 2 σ τ O δ ε ρ μ αunclassified

Προσδιορισμός Των Κυτταροκινών IL-17A, IL-17F Και IL-22 Σε Ασθενείς Με Σπογγοειδή Μυκητίαση

Παπαθεμελή¹

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Εισαγωγή: Είναι γνωστή η συμμετοχή των IL-17A, IL-17F και IL-22 σε πολλές φλεγμονώδεις και αυτοάνοσες παθήσεις. Οι γνώσεις μας ωστόσο για το ρόλο αυτών των κυτταροκινών στη σπογγοειδή μυκητίαση είναι περιορισμένες. Σκοπός μελέτης: Ο σκοπός αυτής της μελέτης είναι να εξετάσει τα επίπεδα έκφρασης των IL-17A, IL-17F και IL-22 σε δείγματα αίματος και ιστού ασθενών με σπογγοειδή μυκητίαση. Μέθοδοι: Χρησιμοποιήθηκαν δείγματα αίματος από 50 ασθενείς με σπογγοειδή μυκητίαση και 50 υγιείς μάρτυρες και δείγματα ιστού από βιοψίες δέρματος από 26 ασθενείς με σπογγοειδή μυκητίαση και 5 υγιείς μάρτυρες. Τα επίπεδα πρωτεϊνών αυτών των κυτταροκινών μετρήθηκαν σε δείγματα ορού με Multiplex ELISA και τα επίπεδα έκφρασης mRNA αυτών των κυτταροκινών μετρήθηκαν σε δείγματα αίματος και δέρματος με RT-PCR. Αποτελέσματα: Τα επίπεδα έκφρασης mRNA των IL-17A και IL-17F στο αίμα ήταν σημαντικά χαμηλότερα σε ασθενείς με σπογγοειδή μυκητίαση σε σύγκριση με υγιείς μάρτυρες (παραμετρικός έλεγχος: p=0.0089 και p=0.0004 αντιστοίχως, μη παραμετρικός έλεγχος: p=0.0069 και p=0.0006). Τα επίπεδα της IL-22 στον ορό καθώς και τα επίπεδα έκφρασης mRNA της IL-22 στον ιστό του δέρματος ήταν αυξημένα σε ασθενείς με σπογγοειδή μυκητίαση σε σύγκριση με υγιείς μάρτυρες (παραμετρικός έλεγχος: p=0.0076 και p=0.0319 αντιστοίχως, μη παραμετρικός έλεγχος: p=0.0165 και p=0.1435 αντιστοίχως). Συμπεράσματα: Τα αποτελέσματά μας υποδηλώνουν ότι τα χαμηλά επίπεδα IL-17A και IL-17F στη σπογγοειδή μυκητίαση μπορεί να συνδέονται με απώλεια της ανοσολογικής απάντησης που οδηγεί σε ογκογένεση. Τα αυξημένα επίπεδα της IL-22 καταδεικνύουν την πιθανή συμμετοχή της IL-22 στo μικροπεριβάλλον της νεοπλασίας.

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Progression of mycosis fungoides occurs through divergence of tumor immunophenotype by differential expression of HLA-DR

Cited by 27 publications

References 34 publications

Sézary syndrome and mycosis fungoides: An overview, including the role of immunophenotyping

Sézary syndrome and mycosis fungoides: An overview, including the role of immunophenotyping

Patterns of Gene Expression in Cutaneous T-Cell Lymphoma: Systematic Review of Transcriptomic Studies in Mycosis Fungoides

Προσδιορισμός Των Κυτταροκινών IL-17A, IL-17F Και IL-22 Σε Ασθενείς Με Σπογγοειδή Μυκητίαση

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