Exome sequencing reveals germline NPAT mutation as a candidate risk factor for Hodgkin lymphoma

Saarinen, Silva; Aavikko, Mervi; Aittomäki, Kristiina; Launonen, Virpi; Lehtonen, Rainer; Franssila, Kaarle; Lehtonen, Heli; Kaasinen, Eevi; Broderick, Peter; Tarkkanen, Jussi; Bain, Barbara J.; Bauduer, Frédéric; Ünal, Ali; Swerdlow, Anthony; Cooke, Rosie; Mäkinen, Markus J.; Houlston, Richard S.; Vahteristo, Pia; Aaltonen, Lauri A.

doi:10.1182/blood-2011-03-341560

Cited by 69 publications

(42 citation statements)

References 37 publications

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“…37 Interestingly, we did not find shared variants in the three genes (KLHDC8B, NPAT, and ACAN) previously identified in high-risk HL families, [16][17][18] while we observed the POT1 rs202187871 variant also reported in a high-risk melanoma family. 20 Given the large total number of genes (2383) with family-shared variants that we identified, we also conducted pathway analyses using two independent tools, Ingenuity Variant Analysis (IVA) 38 Supplementary Table S6F).…”

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confidence: 47%

“…16 Recently, a mutation in the NPAT gene was identified in an extended pedigree segregating for the less common nodular lymphocytic predominant subtype of HL. 17 A homozygous deletion in the ACAN gene was identified in 3 siblings with classical HL. 18 We conducted a genome-wide linkage study in 44 HL families that revealed several regions of the genome possibly linked to HL, 19 but no susceptibility genes were subsequently identified.…”

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confidence: 99%

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Whole exome sequencing in families at high risk for Hodgkin lymphoma: identification of a predisposing mutation in the KDR gene

et al. 2016

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H odgkin lymphoma shows strong familial aggregation but no major susceptibility genes have been identified to date. The goal of this study was to identify high-penetrance variants using whole exome sequencing in 17 Hodgkin lymphoma prone families with three or more affected cases or obligate carriers (69 individuals), followed by targeted sequencing in an additional 48 smaller HL families (80 individuals). Alignment and variant calling were performed using standard methods. Dominantly segregating, rare, coding or potentially functional variants were further prioritized based on predicted deleteriousness, conservation, and potential importance in lymphoid malignancy pathways. We selected 23 genes for targeted sequencing. Only the p.A1065T variant in KDR (kinase insert domain receptor) also known as VEGFR2 (vascular endothelial growth factor receptor 2) was replicated in two independent Hodgkin lymphoma families. KDR is a type III receptor tyrosine kinase, the main mediator of vascular endothelial growth factor induced proliferation, survival, and migration. Its activity is associated with several diseases including lymphoma. Functional experiments have shown that p.A1065T, located in the activation loop, can promote constitutive autophosphorylation on tyrosine in the absence of vascular endothelial growth factor and that the kinase activity was abrogated after exposure to kinase inhibitors. A few other promising mutations were identified but appear to be "private". In conclusion, in the largest sequenced cohort of Hodgkin lymphoma families to date, we identified a causal mutation in the KDR gene. While independent validation is needed, this mutation may increase downstream tumor cell proliferation activity and might be a candidate for targeted therapy.

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Whole exome sequencing in families at high risk for Hodgkin lymphoma: identification of a predisposing mutation in the KDR gene

et al. 2016

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“…62,69 Lastly, certain germline polymorphisms of IL-10, IL-6, and NPAT may be associated with poorer prognosis (IL-10 and IL-6) or risk of development of nodular lymphocyte-predominant Hodgkin lymphoma (NPAT). 71 Several challenges arise, however, as we try to turn these interesting biological observations into clinically relevant biomarkers. Most problematic is the lack of wide validation of the significance of these biomarkers, which typically have been demonstrated in only small series of selected patients and have not been reproducibly shown to be significant in multiple independent series of patients.…”

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confidence: 99%

Risk assessment in the management of newly diagnosed classical Hodgkin lymphoma

Connors

2015

Blood

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Treatment of Hodgkin lymphoma is associated with 2 major types of risk: that the treatment may fail to cure the disease or that the treatment will prove unacceptably toxic. Careful assessment of the amount of the lymphoma (tumor burden), its behavior (extent of invasion or specific organ compromise), and host related factors (age; coincident systemic infection; and organ dysfunction, especially hematopoietic, cardiac, or pulmonary) is essential to optimize outcome. Elaborately assembled prognostic scoring systems, such as the International Prognostic Factors Project score, have lost their accuracy and value as increasingly effective chemotherapy and supportive care have been developed. Identification of specific biomarkers derived from sophisticated exploration of Hodgkin lymphoma biology is bringing promise of further improvement in targeted therapy in which effectiveness is increased at the same time off-target toxicity is diminished. Parallel developments in functional imaging are providing additional potential to evaluate the efficacy of treatment while it is being delivered, allowing dynamic assessment of risk during chemotherapy and adaptation of the therapy in real time. Risk assessment in Hodgkin lymphoma is continuously evolving, promising ever greater precision and clinical relevance. This article explores the past usefulness and the emerging potential of risk assessment for this imminently curable malignancy.

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“…Saarinen and colleagues combined 2 modern genetic methods, single nucleotide polymorphism chips and whole exome sequencing, and applied them to a unique Finnish family with 4 cousins all presenting from 22-26 years of age with NLPHL. 1 A germ line mutation in the NPAT (nuclear protein, ataxia-telangiectasia locus) gene was found in all 4 patients (see figure). The mutation was a 2 base pair deletion causing a frame shift and in consequnce a truncation of the protein.…”

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“…Cells from patients with NPAT mutations indeed showed reduced expression levels of the gene. 1 NPAT germ line mutations were found in NLPHL as well as in classic HL cases, suggesting that such mutations may contribute to the pathogenesis of both subtypes of Hodgkin lymphoma. This is a remarkable finding, because although classic and NLPHL are considered 2 forms of 1 disease, there is presently little indication for common genetic lesions or other shared transforming events in the tumor cells of these lymphomas.…”

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confidence: 99%

NPAT mutations in Hodgkin lymphoma

Küppers

2011

Blood

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Exome sequencing reveals germline NPAT mutation as a candidate risk factor for Hodgkin lymphoma

Cited by 69 publications

References 37 publications

Whole exome sequencing in families at high risk for Hodgkin lymphoma: identification of a predisposing mutation in the KDR gene

Whole exome sequencing in families at high risk for Hodgkin lymphoma: identification of a predisposing mutation in the KDR gene

Risk assessment in the management of newly diagnosed classical Hodgkin lymphoma

NPAT mutations in Hodgkin lymphoma

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