Genetics Abnormalities with Clinical Impact in Primary Cutaneous Lymphomas

Genetics Abnormalities with Clinical Impact in Primary Cutaneous Lymphomas

Primary cutaneous lymphomas comprise a heterogeneous group of extranodal non-Hodgkin lymphomas (NHL) that arise from skin resident lymphoid cells and are manifested by specific lymphomatous cutaneous lesions with no evidence of extracutaneous disease at the time of diagnosis. They may originate from...

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Veröffentlicht in:Cancers 2022-10, Vol.14 (20), p.4972
Hauptverfasser: Gallardo, Fernando, Pujol, Ramon M
Format: Artikel
Sprache:eng
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Anaplastic large-cell lymphoma
Apoptosis
B-cell lymphoma
Bcl-6 protein
Copy number
Cytotoxicity
Disease
DNA damage
DNA repair
Epigenetic inheritance
Epigenetics
Fas antigen
Fungal infections
Genes
Genetic aspects
Genomics
Genotype & phenotype
Health aspects
Hematology
Janus kinase 2
Kinases
Leukemia
Lymphocytes
Lymphocytes B
Lymphocytes T
Lymphoid cells
Lymphoma
Lymphomas
Medical prognosis
Mutation
Mutation (Biology)
Myc protein
Mycosis
Mycosis fungoides
MyD88 protein
NF-κB protein
Patients
Review
Signal transduction
T cell receptors
Tumors
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description Primary cutaneous lymphomas comprise a heterogeneous group of extranodal non-Hodgkin lymphomas (NHL) that arise from skin resident lymphoid cells and are manifested by specific lymphomatous cutaneous lesions with no evidence of extracutaneous disease at the time of diagnosis. They may originate from mature T-lymphocytes (70% of all cases), mature B-lymphocytes (25–30%) or, rarely, NK cells. Cutaneous T-cell lymphomas (CTCL) comprise a heterogeneous group of T-cell malignancies including Mycosis Fungoides (MF) the most frequent subtype, accounting for approximately half of CTCL, and Sézary syndrome (SS), which is an erythrodermic and leukemic subtype characterized by significant blood involvement. The mutational landscape of MF and SS by NGS include recurrent genomic alterations in the TCR signaling effectors (i.e., PLCG1), the NF-κB elements (i.e., CARD11), DNA damage/repair elements (TP53 or ATM), JAK/STAT pathway elements or epigenetic modifiers (DNMT3). Genomic copy number variations appeared to be more prevalent than somatic mutations. Other CTCL subtypes such as primary cutaneous anaplastic large cell lymphoma also harbor genetic alterations of the JAK/STAT pathway in up to 50% of cases. Recently, primary cutaneous aggressive epidermotropic T-cell lymphoma, a rare fatal subtype, was found to contain a specific profile of JAK2 rearrangements. Other aggressive cytotoxic CTCL (primary cutaneous γδ T-cell lymphomas) also show genetic alterations in the JAK/STAT pathway in a large proportion of patients. Thus, CTCL patients have a heterogeneous genetic/transcriptional and epigenetic background, and there is no uniform treatment for these patients. In this scenario, a pathway-based personalized management is required. Cutaneous B-cell lymphoma (CBCL) subtypes present a variable genetic profile. The genetic heterogeneity parallels the multiple types of specialized B-cells and their specific tissue distribution. Particularly, many recurrent hotspot and damaging mutations in primary cutaneous diffuse large B-cell lymphoma of the leg type, involving MYD88 gene, or BCL6 and MYC translocations and BLIMP1 or CDKN2A deletions are useful for diagnostic and prognostic purposes for this aggressive subtype from other indolent CBCL forms.
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They may originate from mature T-lymphocytes (70% of all cases), mature B-lymphocytes (25–30%) or, rarely, NK cells. Cutaneous T-cell lymphomas (CTCL) comprise a heterogeneous group of T-cell malignancies including Mycosis Fungoides (MF) the most frequent subtype, accounting for approximately half of CTCL, and Sézary syndrome (SS), which is an erythrodermic and leukemic subtype characterized by significant blood involvement. The mutational landscape of MF and SS by NGS include recurrent genomic alterations in the TCR signaling effectors (i.e., PLCG1), the NF-κB elements (i.e., CARD11), DNA damage/repair elements (TP53 or ATM), JAK/STAT pathway elements or epigenetic modifiers (DNMT3). Genomic copy number variations appeared to be more prevalent than somatic mutations. Other CTCL subtypes such as primary cutaneous anaplastic large cell lymphoma also harbor genetic alterations of the JAK/STAT pathway in up to 50% of cases. Recently, primary cutaneous aggressive epidermotropic T-cell lymphoma, a rare fatal subtype, was found to contain a specific profile of JAK2 rearrangements. Other aggressive cytotoxic CTCL (primary cutaneous γδ T-cell lymphomas) also show genetic alterations in the JAK/STAT pathway in a large proportion of patients. Thus, CTCL patients have a heterogeneous genetic/transcriptional and epigenetic background, and there is no uniform treatment for these patients. In this scenario, a pathway-based personalized management is required. Cutaneous B-cell lymphoma (CBCL) subtypes present a variable genetic profile. The genetic heterogeneity parallels the multiple types of specialized B-cells and their specific tissue distribution. Particularly, many recurrent hotspot and damaging mutations in primary cutaneous diffuse large B-cell lymphoma of the leg type, involving MYD88 gene, or BCL6 and MYC translocations and BLIMP1 or CDKN2A deletions are useful for diagnostic and prognostic purposes for this aggressive subtype from other indolent CBCL forms.</abstract><cop>Basel</cop><pub>MDPI AG</pub><doi>10.3390/cancers14204972</doi><oa>free_for_read</oa></addata></record>
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subjects Anaplastic large-cell lymphoma
Apoptosis
B-cell lymphoma
Bcl-6 protein
Copy number
Cytotoxicity
Disease
DNA damage
DNA repair
Epigenetic inheritance
Epigenetics
Fas antigen
Fungal infections
Genes
Genetic aspects
Genomics
Genotype & phenotype
Health aspects
Hematology
Janus kinase 2
Kinases
Leukemia
Lymphocytes
Lymphocytes B
Lymphocytes T
Lymphoid cells
Lymphoma
Lymphomas
Medical prognosis
Mutation
Mutation (Biology)
Myc protein
Mycosis
Mycosis fungoides
MyD88 protein
NF-κB protein
Patients
Review
Signal transduction
T cell receptors
Tumors
title Genetics Abnormalities with Clinical Impact in Primary Cutaneous Lymphomas
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