t(11;14) status is stable between diagnosis and relapse, and concordant between detection methodologies based on fluorescence &lt;i&gt;in situ&lt;/i&gt; hybridization and next-generation sequencing in patients with multiple myeloma

Avet-Loiseau, Hervé; Thiébaut-Millot, Raphaële; Li, Xiaotong; Ross, Jeremy A.; Hader, Carlos

doi:10.3324/haematol.2023.284072

Cited by 2 publications

(1 citation statement)

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“… 17 Avet-Loiseau confirmed the presence of a markedly increased frequency of DIS3 mutations and a decreased frequency of BRAF mutations in t(11;14) MM. 18 …”

Section: Primary Genetic Abnormalities In MMmentioning

confidence: 99%

Recent Advances in the Definition of the Molecular Alterations Occurring in Multiple Myeloma

Testa,

Pelosi,

Castelli

et al. 2024

Mediterr J Hematol Infect Dis

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Multiple myeloma (MM) is a disorder of the monoclonal plasma cells and is the second most common hematologic malignancy. MM initiation and progression are dependent upon complex genomic abnormalities. The current pathogenic model of MM includes two types of primary events, represented by chromosome translocations or chromosome number alterations resulting in hyperdiploidy. These primary molecular events are observed both in MM and in monoclonal gammopathy, its premalignant precursor. Subsequent genetic events allow the progression of monoclonal gammopathy to MM and, together with primary events, contribute to the genetic complexity and heterogeneity of MM. Newer therapies have considerably improved patient outcomes; however, MM remains an incurable disease and most patients experience multiple relapses. The dramatic progresses achieved in the analysis of the heterogeneous molecular features of different MM patients allowed a comprehensive molecular classification of MM and the definition of an individualized prognostic model to predict an individual MM patient’s response to different therapeutic options. Despite these progresses, prognostic models fail to identify a significant proportion of patients destined to early relapse. Treatment strategies are increasingly. Based on disease biology, trials are enriched for high-risk MMs, whose careful definition and categorization requires DNA sequencing studies. Keywords: Multiple Myeloma; Chromosome Abnormalities; Molecular Events; Mutations.

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“… 17 Avet-Loiseau confirmed the presence of a markedly increased frequency of DIS3 mutations and a decreased frequency of BRAF mutations in t(11;14) MM. 18 …”

Section: Primary Genetic Abnormalities In MMmentioning

confidence: 99%