2007
DOI: 10.1182/blood-2006-12-061507
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Lesional gene expression profiling in cutaneous T-cell lymphoma reveals natural clusters associated with disease outcome

Abstract: Cutaneous T-cell lymphoma (CTCL) is defined by infiltration of activated and malignant T cells in the skin. The clinical manifestations and prognosis in CTCL are highly variable. In this study, we hypothesized that gene expression analysis in lesional skin biopsies can improve understanding of the disease and its management. Based on 63 skin samples, we performed consensus clustering, revealing 3 patient clusters. Of these, 2 clusters tended to differentiate limited CTCL (stages IA and IB) from more extensive … Show more

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Cited by 126 publications
(169 citation statements)
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“…Although the molecular pathogenesis of aggressive T-cell and NK cell malignancies remains unclear, ITK and RLK have been shown to be critical mediators of intracellular signaling that support the survival and growth of these malignancies (65)(66)(67). Our studies reveal that ITK-and RLK-based signaling in T-PLL can be blocked by PRN694, thereby starving these cells of an essential activation pathway.…”
Section: Discussionmentioning
confidence: 72%
“…Although the molecular pathogenesis of aggressive T-cell and NK cell malignancies remains unclear, ITK and RLK have been shown to be critical mediators of intracellular signaling that support the survival and growth of these malignancies (65)(66)(67). Our studies reveal that ITK-and RLK-based signaling in T-PLL can be blocked by PRN694, thereby starving these cells of an essential activation pathway.…”
Section: Discussionmentioning
confidence: 72%
“…More recently, peripheral blood monocytes (and their progeny) were shown to support the growth of malignant T cells in vitro, confer resistant to chemotherapy, and promote tumor engraftment in immunodeficient mice [45]. Lymphoma-derived IL-10, upregulated in patients with advanced-stage disease poorly responsive to therapy [47], impairs the maturation of lymphoma-associated dendritic cells, rendering them immunologically incompetent, thus promoting escape from host antitumor immune surveillance. In addition, lymphoma-associated dendritic cells were observed to express the T-cell coinhibitory ligand B7-H1 (PD-L1, CD274), which directly inhibits the proliferation of tumor-specific T cells, but also indirectly impairs antitumor immunity by promoting the induction of suppressive regulatory T cells [48].…”
Section: Immunopathogenesismentioning
confidence: 99%
“…In patients with advanced-stage disease, and half of patients with limited-stage disease, a dramatic loss of TCR diversity was observed. Whether this observation may be explained by tumor-mediated suppression of nonmalignant T cells, diminished thymic output of naïve T cells and compensatory homeostatic expansion of oligoclonal peripheral T cells, or some other mechanism, is unknown [47]. As lymphopenia is an adverse prognostic factor in many hematologic malignancies [59][60][61][62][63][64], and undoubtedly contributes to the infectious complications observed in CTCL, improved understanding of the causative mechanism(s) leading to this dramatic loss of T-cell diversity may have significant therapeutic implications.…”
Section: Immunopathogenesismentioning
confidence: 99%
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“…Indeed, several reports documented their positive activity in AITL cases (79)(80)(81)(82)(83)(84). More recently, a possible pathogenetic role of VEGF has been proposed for MF as well (85,86). Indeed, VEGF deregulation may be an early event in this disease.…”
Section: Figurementioning
confidence: 99%