Acquired genetic alterations in tumor cells dictate the development of high-risk neuroblastoma and clinical outcomes

Faizan H Khan; Vijayabaskar Pandian; Satishkumar Ramraj; Mohan Natarajan; Sheeja Aravindan; Terence S Herman; Natarajan Aravindan

doi:10.1186/s12885-015-1463-y

Acquired genetic alterations in tumor cells dictate the development of high-risk neuroblastoma and clinical outcomes

BMC Cancer. 2015 Jul 10:15:514. doi: 10.1186/s12885-015-1463-y.

Authors

Faizan H Khan¹, Vijayabaskar Pandian², Satishkumar Ramraj³, Mohan Natarajan⁴, Sheeja Aravindan⁵, Terence S Herman^{6

7}, Natarajan Aravindan⁸

Affiliations

¹ Department of Radiation Oncology, University of Oklahoma Health Sciences Science Center, 940 Stanton L. Young Blvd., BMSB 737, Oklahoma City, OK, 73104, USA. Faizan-Khan@ouhsc.edu.
² Department of Radiation Oncology, University of Oklahoma Health Sciences Science Center, 940 Stanton L. Young Blvd., BMSB 737, Oklahoma City, OK, 73104, USA. Vijayabaskar-Pandian@ouhsc.edu.
³ Department of Radiation Oncology, University of Oklahoma Health Sciences Science Center, 940 Stanton L. Young Blvd., BMSB 737, Oklahoma City, OK, 73104, USA. Satish-Ramraj@ouhsc.edu.
⁴ Department of Pathology, University of Texas Health Sciences Center, San Antonio, TX, USA. natarajan@uthscsa.edu.
⁵ Stephenson Cancer Center, Oklahoma City, OK, USA. Sheeja-Aravindan@ouhsc.edu.
⁶ Department of Radiation Oncology, University of Oklahoma Health Sciences Science Center, 940 Stanton L. Young Blvd., BMSB 737, Oklahoma City, OK, 73104, USA. Terence-Herman@ouhsc.edu.
⁷ Stephenson Cancer Center, Oklahoma City, OK, USA. Terence-Herman@ouhsc.edu.
⁸ Department of Radiation Oncology, University of Oklahoma Health Sciences Science Center, 940 Stanton L. Young Blvd., BMSB 737, Oklahoma City, OK, 73104, USA. naravind@ouhsc.edu.

Abstract

Background: Determining the driving factors and molecular flow-through that define the switch from favorable to aggressive high-risk disease is critical to the betterment of neuroblastoma cure.

Methods: In this study, we examined the cytogenetic and tumorigenic physiognomies of distinct population of metastatic site- derived aggressive cells (MSDACs) from high-risk tumors, and showed the influence of acquired genetic rearrangements on poor patient outcomes.

Results: Karyotyping in SH-SY5Y and MSDACs revealed trisomy of 1q, with additional non-random chromosomal rearrangements on 1q32, 8p23, 9q34, 15q24, 22q13 (additions), and 7q32 (deletion). Array CGH analysis of individual clones of MSDACs revealed genetic alterations in chromosomes 1, 7, 8, and 22, corresponding to a gain in the copy numbers of LOC100288142, CD1C, CFHR3, FOXP2, MDFIC, RALYL, CSMD3, SAMD12-AS1, and MAL2, and a loss in ADAM5, LOC400927, APOBEC3B, RPL3, MGAT3, SLC25A17, EP300, L3MBTL2, SERHL, POLDIP3, A4GALT, and TTLL1. QPCR analysis and immunoblotting showed a definite association between DNA-copy number changes and matching transcriptional/translational expression in clones of MSDACs. Further, MSDACs exert a stem-like phenotype. Under serum-free conditions, MSDACs demonstrated profound tumorosphere formation ex vivo. Moreover, MSDACs exhibited high tumorigenic capacity in vivo and prompted aggressive metastatic disease. Tissue microarray analysis coupled with automated IHC revealed significant association of RALYL to the tumor grade in a cohort of 25 neuroblastoma patients. Clinical outcome association analysis showed a strong correlation between the expression of CFHR3, CSMD3, MDFIC, FOXP2, RALYL, POLDIP3, SLC25A17, SERHL, MGAT3, TTLL1, or LOC400927 and overall and relapse-free survival in patients with neuroblastoma.

Conclusion: Together, these data highlight the ongoing acquired genetic rearrangements in undifferentiated tumor-forming neural crest cells, and suggest that these alterations could switch favorable neuroblastoma to high-risk aggressive disease, promoting poor clinical outcomes.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cell Line, Tumor
Chromosome Aberrations
Chromosome Banding
Comparative Genomic Hybridization
DNA Copy Number Variations
Disease Models, Animal
Disease Progression
Genetic Association Studies*
Heterografts
Humans
Neoplasm Metastasis
Neoplasm Staging
Neoplastic Stem Cells / metabolism
Neoplastic Stem Cells / pathology
Neuroblastoma / genetics*
Neuroblastoma / mortality*
Neuroblastoma / pathology
Prognosis
Ribosomal Protein L3

Abstract

Publication types

MeSH terms

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