Genomic analysis of 220 CTCLs identifies a novel recurrent gain-of-function alteration in RLTPR (p.Q575E)

Park, Joonhee; Yang, Jingyi; Wenzel, Alexander T.; Ramachandran, Akshaya; Lee, Wung J.; Daniels, Jay; Kim, Ju-Hyun; Martínez-Escala, Estela; Amankulor, Nduka; Pro, Barbara; Guitart, Joan; Mendillo, Marc L.; Savas, Jeffrey N.; Boggon, Titus J.; Choi, Jaehyuk

doi:10.1182/blood-2017-02-768234

Cited by 128 publications

(165 citation statements)

References 51 publications

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“…SNVs present in the dbSNP database were filtered out. We searched for pathogenic SNVs in 1461 genes involved in signaling pathways and cellular processes previously reported as affected in CTCL . Gene lists were retrieved from the PathCards database (http://pathcards.genecards.org/).…”

Section: Methodsmentioning

confidence: 99%

“…We searched for pathogenic SNVs in 1461 genes involved in signaling pathways and cellular processes previously reported as affected in CTCL. [7][8][9][16][17][18][19][20][21][22] Gene lists were retrieved from the PathCards database (http://pathcards.genecards.org/). Only SNVs predicted to produce highly deleterious amino acid substitutions by both SIFT and PolyPhen-2 were further investigated on ClinVar, COSMIC, and literature.…”

Section: Discovery Of Pathogenic Snvsmentioning

confidence: 99%

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Genomic analysis reveals recurrent deletion of JAK‐STAT signaling inhibitors HNRNPK and SOCS1 in mycosis fungoides

Torres

Cats

Mei

et al. 2018

Genes Chromosomes & Cancer

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Mycosis fungoides (MF) is the most common cutaneous T‐cell lymphoma (CTCL). Causative genetic alterations in MF are unknown. The low recurrence of pathogenic small‐scale mutations (ie, nucleotide substitutions, indels) in the disease, calls for the study of additional aspects of MF genetics. Here, we investigated structural genomic alterations in tumor‐stage MF by integrating whole‐genome sequencing and RNA‐sequencing. Multiple genes with roles in cell physiology (n = 113) and metabolism (n = 92) were found to be impacted by genomic rearrangements, including 47 genes currently implicated in cancer. Fusion transcripts involving genes of interest such as DOT1L, KDM6A, LIFR, TP53, and TP63 were also observed. Additionally, we identified recurrent deletions of genes involved in cell cycle control, chromatin regulation, the JAK‐STAT pathway, and the PI‐3‐K pathway. Remarkably, many of these deletions result from genomic rearrangements. Deletion of tumor suppressors HNRNPK and SOCS1 were the most frequent genetic alterations in MF after deletion of CDKN2A. Notably, SOCS1 deletion could be detected in early‐stage MF. In agreement with the observed genomic alterations, transcriptome analysis revealed up‐regulation of the cell cycle, JAK‐STAT, PI‐3‐K and developmental pathways. Our results position inactivation of HNRNPK and SOCS1 as potential driver events in MF development.

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Section: Methodsmentioning

confidence: 99%

Section: Discovery Of Pathogenic Snvsmentioning

confidence: 99%

Genomic analysis reveals recurrent deletion of JAK‐STAT signaling inhibitors HNRNPK and SOCS1 in mycosis fungoides

Torres

Cats

Mei

et al. 2018

Genes Chromosomes & Cancer

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“…These proteins increase binding to downstream complements of the NFκB signalling pathway, thereby selectively upregulating the NFκB pathway‐activated T cells and ultimately augmenting T‐cell‐receptor‐dependent production of IL‐2 by 34‐fold. In these extensive genomic analyses performed by Park et al, 55 genes in lymphoma genesis, including 17 genes not previously implicated in CTCL, were identified (Figure ) . These include 17 novel putative driver genes in CTCL.…”

Section: Aberrant Molecular Findings In Ctclmentioning

confidence: 98%

“…Affected pathways with driver genes in CTCL and 17 newly identified mutated genes by genomic analysis of 220 patients . The size of each pie represents the number of mutations found in the corresponding pathway.…”

Section: Aberrant Molecular Findings In Ctclmentioning

confidence: 99%

Molecular pathogenesis of cutaneous lymphomas

Stadler

Stranzenbach

2018

Experimental Dermatology

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Primary cutaneous T-cell lymphoma (CTCL) comprises the second most common group of extra-nodal non-Hodgkin's lymphoma. They represent incurable primary extra-nodal lymphomas of major T cells, uniformly present in the skin with 1%-2% risk of systemic dissemination in mycosis fungoides (MF), which represents the most common subtype of CTCL. In general, long-term antigen stimulation is thought, through key cytokine signalling pathways, to induce an inflammatory response with T-cell proliferation, leading to a clonal malignant T cell with continuous expansion.However, in recent years, using data harvested from high-throughput transcriptional profiling, substantial advances in the understanding of the molecular pathogenesis were made to understand the complex pathogenesis of CTCL. In this review, the actual data are summarised. K E Y W O R D Scutaneous, lymphoma, molecular, mutations, pathogenesis

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“…In this issue of Blood, Park et al expand the boundaries and improve the resolution of the known mutational map of CTCL. 1 T he term CTCL describes a heterogeneous family of incurable primary extranodal lymphomas of mature T cells that uniformly present in the skin, with a variable risk of systemic dissemination. The most common type of CTCL (;60%) is mycosis fungoides (MF), a low-grade lymphoma of skin-homing CD4 1 memory T cells.…”

mentioning

confidence: 99%