2019
DOI: 10.1182/blood-2018-10-880831
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High subclonal fraction of 17p deletion is associated with poor prognosis in multiple myeloma

Abstract: K E Y P O I N T S l Association of del17p CCF threshold and poor prognosis in NDMM is established via fluorescence in situ hybridization and sequencing methods. l TP53 mutations are enriched in a high-risk patient segment characterized by high del17p CCF.Deletions of chromosome 17p (del17p) that span the TP53 gene are associated with poor outcome in multiple myeloma (MM), but the prognostic value of del17p cancer clonal fraction (CCF) remains unclear. We applied uniform cytogenetic assessments in a large cohor… Show more

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Cited by 91 publications
(75 citation statements)
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“…TP53 mutations are mostly detected in subclones, consistent with the idea that the abnormalities appear relatively late during the clonal evolution of MM [51]. Mutant p53 usually possesses oncogenic functions, including the ability to up-regulate c-Myc and genes encoding proteasome subunits [53], which induce further anti-cancer drug resistance [54][55][56].…”
Section: Genomic Changes During the Terminal Phase Of MMsupporting
confidence: 68%
“…TP53 mutations are mostly detected in subclones, consistent with the idea that the abnormalities appear relatively late during the clonal evolution of MM [51]. Mutant p53 usually possesses oncogenic functions, including the ability to up-regulate c-Myc and genes encoding proteasome subunits [53], which induce further anti-cancer drug resistance [54][55][56].…”
Section: Genomic Changes During the Terminal Phase Of MMsupporting
confidence: 68%
“…The MGP data also showed a significant association between the presence of CCF >0.55 and of mutation on the second allele of TP53, where 27 of 28 patients with a TP53 mutation had CCF >0.55 [6]. Patients with biallelic inactivation had significantly shorter PFS than patients with one wild-type copy of TP53 [6]. In an updated analysis of this dataset with longer clinical follow-up, patients with HR del17p + TP53 mutation have the shortest OS ( Figure 2, orange line, median 28.8 mo, p = 0.008).…”
Section: Biallelic Inactivation Of Tp53 In MMmentioning
confidence: 82%
“…Using the >0.55 CCF cutoff defined by genomics-based methods, analysis from MGP identified high-risk del17p patients as discussed in Section 3.1. The MGP data also showed a significant association between the presence of CCF >0.55 and of mutation on the second allele of TP53, where 27 of 28 patients with a TP53 mutation had CCF >0.55 [6]. Patients with biallelic inactivation had significantly shorter PFS than patients with one wild-type copy of TP53 [6].…”
Section: Biallelic Inactivation Of Tp53 In MMmentioning
confidence: 86%
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