Next-generation sequencing reveals germline mutations in an infant with synchronous occurrence of nephro- and neuroblastoma

Theruvath, Johanna; Russo, Alexandra; Kron, Bettina; Paret, Claudia; Wingerter, Arthur; Malki, Khalifa El; Neu, Marie A.; Alt, Francesca; Staatz, Gundula; Stein, R.; Seidmann, Larissa; Prawitt, Dirk; Faber, Jörg

doi:10.1080/08880018.2016.1184362

Cited by 7 publications

(7 citation statements)

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“…In NB, high expression levels of ALK closely correlates with poor outcomes, especially in high-risk NB [22, 42, 49]. It is reported that ALK with activating mutations in its tyrosine kinase domain occur in most cases of hereditary NB [17, 33].…”

Section: Introductionmentioning

confidence: 99%

The second-generation ALK inhibitor alectinib effectively induces apoptosis in human neuroblastoma cells and inhibits tumor growth in a TH-MYCN transgenic neuroblastoma mouse model

Guan

Zhao

et al. 2017

Cancer Letters

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Activating germline mutations of anaplastic lymphoma kinase (ALK) occur in most cases of hereditary neuroblastoma (NB) and the constitutively active kinase activity of ALK promotes cell proliferation and survival in NB. Therefore, ALK kinase is a potential therapeutic target for NB. In this study, we show that the novel ALK inhibitor alectinib effectively suppressed cell proliferation and induces apoptosis in NB cell lines with either wild-type ALK or mutated ALK (F1174L and D1091N) by blocking ALK-mediated PI3K/Akt/mTOR signaling. In addition, alectinib enhanced doxorubicin-induced cytotoxicity and apoptosis in NB cells. Furthermore, alectinib induced apoptosis in an orthotopic xenograft NB mouse model. Also, in the TH-MYCN transgenic mouse model, alectinib resulted in decreased tumor growth and prolonged survival time. These results indicate that alectinib may be a promising therapeutic agent for the treatment of NB.

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Section: Introductionmentioning

confidence: 99%

The second-generation ALK inhibitor alectinib effectively induces apoptosis in human neuroblastoma cells and inhibits tumor growth in a TH-MYCN transgenic neuroblastoma mouse model

Guan

Zhao

et al. 2017

Cancer Letters

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“…Most children with NBL do not have an established and clinically obvious CPS. Rare germline mutations of ALK (gene product is a receptor tyrosine kinase, MIM 105590) (Mosse et al, ; Theruvath, Russo, Kron, Paret, & Wingerter, ), GALNT14 (encoding a Golgi protein involved in a complex transferring N‐acetyl‐D‐galactosamine, MIM 608225) (De Mariano et al, ), and PHOX2B (encoding a transcription factor, which is mutated in central hypoventilation syndrome with or without Hirschsprung disease, MIM 209880) (Mosse et al, ; Trochet et al, ) are associated with an increased NBL risk and should be considered in children with familial disease. Patients with Beckwith–Wiedemann syndrome (Mussa et al, ) (MIM 130650; complex pathogenesis: (i) hypomethylation of imprinting control region 2; (ii) hypermethylation of imprinting control region 1; (iii) paternal uniparental disomy 11p15; (iv) microdeletion/‐duplication in 11p15.5; or (v) CDKN1C mutation; The CDKN1C ‐mutated group is especially associated with NBL), Weaver (Tatton‐Brown & Rahman, ), Sotos (Kulkarni, Stobart, & Noga, ), Simpson–Golabi–Behmel ( GPC3 , GPC4 coding for heparan sulfate proteoglycans involved in regulating cell division and growth; MIM 312870) (Hughes‐Benzie, Hunter, Allanson, & Mackenzie, ), Rubinstein–Taybi (Stevens, ), and Costello ( HRAS ; MIM 218040) (Gripp, ) syndromes have an elevated NBL risk.…”

Section: Typical Childhood Cancer Types and Relevant Cpsmentioning

confidence: 99%

Childhood cancer predisposition syndromes—A concise review and recommendations by the Cancer Predisposition Working Group of the Society for Pediatric Oncology and Hematology

Ripperger

Bielack

Borkhardt

et al. 2017

American J of Med Genetics Pt A

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224

184

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Heritable predisposition is an important cause of cancer in children and adolescents. Although a large number of cancer predisposition genes and their associated syndromes and malignancies have already been described, it appears likely that there are more pediatric cancer patients in whom heritable cancer predisposition syndromes have yet to be recognized. In a consensus meeting in the beginning of 2016, we convened experts in Human Genetics and Pediatric Hematology/Oncology to review the available data, to categorize the large amount of information, and to develop recommendations regarding when a cancer predisposition syndrome should be suspected in a young oncology patient. This review summarizes the current knowledge of cancer predisposition syndromes in pediatric oncology and provides essential information on clinical situations in which a childhood cancer predisposition syndrome should be suspected.

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“…DNA repair genes have been reported in oncogenesis of multiple cancers including neuroblastoma, such as BRCA1/2, PALB2, FANCD2 and CHEK2 et al [50–55]. Pugh et al performed whole genome sequencing of peripheral blood DNA samples on 240 cases of NB patients, and found a few germline mutations including CHEK2 (c.433C > T, c.542G > A and c.539G > A), PINK1 (c.1040T > C and c.836G > A), BARD1(c.334C > T and c.1921C > T) and PALB2 (c.1684+1C > A) [12].…”

Section: Germline Mutations Of Nbmentioning

confidence: 99%

“…Brooks et al reported 20 cases of pediatric cancer including neuroblastoma among 379 families, uncovering mutations in either BRCA1 or BRCA2 [54]. Other studies also identified a deletion/insertion in the FANCD2 gene in nephro- and neuroblastomas [55]. Particularly, germline mutations in BRCA2 and PALB2, that PALB2 binds to the N terminus of BRCA2 and has a key role in localization and stabilization of BRCA2, have been detected that they were associated with the development of neuroblastoma [51, 52].…”

Section: Germline Mutations Of Nbmentioning

confidence: 99%

Research progress of neuroblastoma related gene variations

Cao

Jin

et al. 2016

Oncotarget

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Neuroblastoma, the most common extracranial solid tumor among children, is an embryonal tumor originating from undifferentiated neural crest cell. Neuroblastomas are highly heterogeneous, represented by the wide range of clinical presentations and likelihood of cure, ranging from spontaneous regression to relentless progression despite rigorous multimodal treatments. Approximately, 50% of cases are high-risk with overall survival rates less than 40%. With the efforts to collect large numbers of clinically annotated specimens and the advancements in technologies, researchers have revealed numerous genetic alterations that may drive tumor growth. However, the most lack mutations in genes that are recurrently mutated, which inspires researchers to identify disrupted pathways instead of single mutated genes to unearth biological systems perturbed in neuroblastoma. Stratification of patients and target therapy based on their molecular signatures have been the center of focus. This review provides a comprehensive summary of the recent advances in identification of candidate genes variations, targeted approaches to high-risk neuroblastoma and evaluates the methods utilized for detection, which will provide new avenues to develop therapies and further genetic researches.

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Next-generation sequencing reveals germline mutations in an infant with synchronous occurrence of nephro- and neuroblastoma

Cited by 7 publications

References 50 publications

The second-generation ALK inhibitor alectinib effectively induces apoptosis in human neuroblastoma cells and inhibits tumor growth in a TH-MYCN transgenic neuroblastoma mouse model

The second-generation ALK inhibitor alectinib effectively induces apoptosis in human neuroblastoma cells and inhibits tumor growth in a TH-MYCN transgenic neuroblastoma mouse model

Childhood cancer predisposition syndromes—A concise review and recommendations by the Cancer Predisposition Working Group of the Society for Pediatric Oncology and Hematology

Research progress of neuroblastoma related gene variations

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