Whole-genome Sequencing of Recurrent Neuroblastoma Reveals Somatic Mutations That Affect Key Players in Cancer Progression and Telomere Maintenance

Overview

Journal Sci Rep

Specialty Science

Date 2021 Jan 1

PMID 33384420

Citations 16

Authors

Susanne Fransson

Angela Martinez-Monleon

Mathias Johansson

Rose-Marie Sjoberg

Caroline Bjorklund

Gustaf Ljungman

Torben Ek

Per Kogner

Tommy Martinsson

Affiliations

Soon will be listed here.

Abstract

Neuroblastoma is the most common and deadly childhood tumor. Relapsed or refractory neuroblastoma has a very poor prognosis despite recent treatment advances. To investigate genomic alterations associated with relapse and therapy resistance, whole-genome sequencing was performed on diagnostic and relapsed lesions together with constitutional DNA from seven children. Sequencing of relapsed tumors indicates somatic alterations in diverse genes, including those involved in RAS-MAPK signaling, promoting cell cycle progression or function in telomere maintenance and immortalization. Among recurrent alterations, CCND1-gain, TERT-rearrangements, and point mutations in POLR2A, CDK5RAP, and MUC16 were shown in ≥ 2 individuals. Our cohort contained examples of converging genomic alterations in primary-relapse tumor pairs, indicating dependencies related to specific genetic lesions. We also detected rare genetic germline variants in DNA repair genes (e.g., BARD1, BRCA2, CHEK2, and WRN) that might cooperate with somatically acquired variants in these patients with highly aggressive recurrent neuroblastoma. Our data indicate the importance of monitoring recurrent neuroblastoma through sequential genomic characterization and that new therapeutic approaches combining the targeting of MAPK signaling, cell cycle progression, and telomere activity are required for this challenging patient group.

Citing Articles

Whole-Exome Sequencing Reveals Novel Candidate Driver Mutations and Potential Druggable Mutations in Patients with High-Risk Neuroblastoma.

Nokchan N, Suthapot P, Choochuen P, Khongcharoen N, Hongeng S, Anurathapan U J Pers Med. 2024; 14(9).

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Heterogeneous SSTR2 target expression and a novel :: fusion clone in a progressive metastatic lesion following Lutetium-DOTATATE molecular radiotherapy in neuroblastoma: a case report.

Park S, Fransson S, Sundquist F, Nilsson J, Gryback P, Wessman S Front Oncol. 2024; 14:1408729.

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Structural basis for antibody recognition of the proximal MUC16 ectodomain.

Lee K, Perry K, Xu M, Veillard I, Kumar R, Rao T J Ovarian Res. 2024; 17(1):41.

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Telomere Maintenance Mechanisms in a Cohort of High-Risk Neuroblastoma Tumors and Its Relation to Genomic Variants in the and Genes.

Djos A, Thombare K, Vaid R, Gaarder J, Umapathy G, Reinsbach S Cancers (Basel). 2023; 15(24).

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Dilemmas in the Management of an Infant with Neuroblastoma Metastasized to the Muscles.

Van Heerden J, van den Akker M, Verlooy J, Van Roy N, Laureys G, Norga K Case Rep Oncol. 2023; 16(1):558-567.

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