Please use this identifier to cite or link to this item: https://doi.org/10.1186/s12885-022-09800-0
Title: Mutations of 1p genes do not consistently abrogate tumor suppressor functions in 1p-intact neuroblastoma
Authors: Kuick, Chik Hong
Tan, Jia Ying
Jasmine, Deborah
Sumanty, Tohari
Ng, Alvin YJ
Venkatesh, Byrrappa
Chen, Huiyi
Loh, Eva
Jain, Sudhanshi 
Seow, Wan Yi
Ng, Eileen HQ
Lian, Derrick WQ 
Soh, Shui Yen 
Chang, Kenneth TE 
Chen, Zhi Xiong 
Loh, Amos HP 
Keywords: Science & Technology
Life Sciences & Biomedicine
Oncology
Neuroblastoma
Chromosome 1
Tumor suppressor
Next-generation sequencing
Synchronous Mutations
CHD5
FAMILY
BARD1
IDENTIFICATION
ASSOCIATION
MECHANISMS
EXPRESSION
PHEOCHROMOCYTOMA
PREDISPOSITION
SUSCEPTIBILITY
Issue Date: 30-Jun-2022
Publisher: BMC
Citation: Kuick, Chik Hong, Tan, Jia Ying, Jasmine, Deborah, Sumanty, Tohari, Ng, Alvin YJ, Venkatesh, Byrrappa, Chen, Huiyi, Loh, Eva, Jain, Sudhanshi, Seow, Wan Yi, Ng, Eileen HQ, Lian, Derrick WQ, Soh, Shui Yen, Chang, Kenneth TE, Chen, Zhi Xiong, Loh, Amos HP (2022-06-30). Mutations of 1p genes do not consistently abrogate tumor suppressor functions in 1p-intact neuroblastoma. BMC CANCER 22 (1). ScholarBank@NUS Repository. https://doi.org/10.1186/s12885-022-09800-0
Abstract: Background: Deletion of 1p is associated with poor prognosis in neuroblastoma, however selected 1p-intact patients still experience poor outcomes. Since mutations of 1p genes may mimic the deleterious effects of chromosomal loss, we studied the incidence, spectrum and effects of mutational variants in 1p-intact neuroblastoma. Methods: We characterized the 1p status of 325 neuroblastoma patients, and correlated the mutational status of 1p tumor suppressors and neuroblastoma candidate genes with survival outcomes among 100 1p-intact cases, then performed functional validation of selected novel variants of 1p36 genes identified from our patient cohort. Results: Among patients with adverse disease characteristics, those who additionally had 1p deletion had significantly worse overall survival. Among 100 tumor-normal pairs sequenced, somatic mutations of 1p tumor suppressors KIF1Bβ and CHD5 were most frequent (2%) after ALK and ATRX (8%), and BARD1 (3%). Mutations of neuroblastoma candidate genes were associated with other synchronous mutations and concurrent 11q deletion (P = 0.045). In total, 24 of 38 variants identified were novel and predicted to be deleterious or pathogenic. Functional validation identified novel KIF1Bβ I1355M variant as a gain-of-function mutation with increased expression and tumor suppressive activity, correlating with indolent clinical behavior; another novel variant CHD5 E43Q was a loss-of-function mutation with decreased expression and increased long-term cell viability, corresponding with aggressive disease characteristics. Conclusions: Our study showed that chromosome 1 gene mutations occurred frequently in 1p-intact neuroblastoma, but may not consistently abrogate the function of bonafide 1p tumor suppressors. These findings may augment the evolving model of compounding contributions of 1p gene aberrations toward tumor suppressor inactivation in neuroblastoma.
Source Title: BMC CANCER
URI: https://scholarbank.nus.edu.sg/handle/10635/239176
ISSN: 1471-2407
DOI: 10.1186/s12885-022-09800-0
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