Molecular-clinical correlation in pediatric medulloblastoma: A cohort series study of 52 cases in Taiwan

Kuo Sheng Wu; Donald Ming Tak Ho; Shiann Tarng Jou; Alice L. Yu; Huy Minh Tran; Muh Lii Liang; Hsin Hung Chen; Yi Yen Lee; Yi Wei Chen; Shih Chieh Lin; Feng Chi Chang; Min Lan Tsai; Yen Lin Liu; Hsin Lun Lee; Kevin Li Chun Hsieh; Wen Chang Huang; Shian Ying Sung; Che Chang Chang; Chun Austin Changou; Kung Hao Liang; Tsung Han Hsieh; Yun Ru Liu; Meng En Chao; Wan Chen; Shing Shung Chu; Er Chieh Cho; Tai Tong Wong

doi:10.3390/cancers12030653

Molecular-clinical correlation in pediatric medulloblastoma: A cohort series study of 52 cases in Taiwan

Kuo Sheng Wu, Donald Ming Tak Ho, Shiann Tarng Jou, Alice L. Yu, Huy Minh Tran, Muh Lii Liang, Hsin Hung Chen, Yi Yen Lee, Yi Wei Chen, Shih Chieh Lin, Feng Chi Chang, Min Lan Tsai, Yen Lin Liu, Hsin Lun Lee, Kevin Li Chun Hsieh, Wen Chang Huang, Shian Ying Sung, Che Chang Chang, Chun Austin Changou, Kung Hao LiangTsung Han Hsieh, Yun Ru Liu, Meng En Chao, Wan Chen, Shing Shung Chu, Er Chieh Cho, Tai Tong Wong

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9 Citations (Scopus)

Abstract

In 2016, a project was initiated in Taiwan to adopt molecular diagnosis of childhood medulloblastoma (MB). In this study, we aimed to identify a molecular-clinical correlation and somatic mutation for exploring risk-adapted treatment, drug targets, and potential genetic predisposition. In total, 52 frozen tumor tissues of childhood MBs were collected. RNA sequencing (RNA-Seq) and DNA methylation array data were generated. Molecular subgrouping and clinical correlation analysis were performed. An adjusted Heidelberg risk stratification scheme was defined for updated clinical risk stratification. We selected 51 genes for somatic variant calling using RNA-Seq data. Relevant clinical findings were defined. Potential drug targets and genetic predispositions were explored. Four core molecular subgroups (WNT, SHH, Group 3, and Group 4) were identified. Genetic backgrounds of metastasis at diagnosis and extent of tumor resection were observed. The adjusted Heidelberg scheme showed its applicability. Potential drug targets were detected in the pathways of DNA damage response. Among the 10 patients with SHH MBs analyzed using whole exome sequencing studies, five patients exhibited potential genetic predispositions and four patients had relevant germline mutations. The findings of this study provide valuable information for updated risk adapted treatment and personalized care of childhood MBs in our cohort series and in Taiwan.

Original language	English
Article number	653
Journal	Cancers
Volume	12
Issue number	3
DOIs	https://doi.org/10.3390/cancers12030653
Publication status	Published - Mar 2020

Keywords

Clinical correlation
DNA damage response
Genetic predisposition
Medulloblastoma
Molecular
Risk stratification
RNA-Seq
Somatic mutations

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3390/cancers12030653

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Wu, K. S., Ho, D. M. T., Jou, S. T., Yu, A. L., Tran, H. M., Liang, M. L., Chen, H. H., Lee, Y. Y., Chen, Y. W., Lin, S. C., Chang, F. C., Tsai, M. L., Liu, Y. L., Lee, H. L., Hsieh, K. L. C., Huang, W. C., Sung, S. Y., Chang, C. C., Changou, C. A., ... Wong, T. T. (2020). Molecular-clinical correlation in pediatric medulloblastoma: A cohort series study of 52 cases in Taiwan. Cancers, 12(3), Article 653. https://doi.org/10.3390/cancers12030653

Wu, KS, Ho, DMT, Jou, ST, Yu, AL, Tran, HM, Liang, ML, Chen, HH, Lee, YY, Chen, YW, Lin, SC, Chang, FC, Tsai, ML , Liu, YL , Lee, HL , Hsieh, KLC, Huang, WC, Sung, SY , Chang, CC, Changou, CA, Liang, KH, Hsieh, TH , Liu, YR, Chao, ME, Chen, W, Chu, SS, Cho, EC & Wong, TT 2020, 'Molecular-clinical correlation in pediatric medulloblastoma: A cohort series study of 52 cases in Taiwan', Cancers, vol. 12, no. 3, 653. https://doi.org/10.3390/cancers12030653

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title = "Molecular-clinical correlation in pediatric medulloblastoma: A cohort series study of 52 cases in Taiwan",

abstract = "In 2016, a project was initiated in Taiwan to adopt molecular diagnosis of childhood medulloblastoma (MB). In this study, we aimed to identify a molecular-clinical correlation and somatic mutation for exploring risk-adapted treatment, drug targets, and potential genetic predisposition. In total, 52 frozen tumor tissues of childhood MBs were collected. RNA sequencing (RNA-Seq) and DNA methylation array data were generated. Molecular subgrouping and clinical correlation analysis were performed. An adjusted Heidelberg risk stratification scheme was defined for updated clinical risk stratification. We selected 51 genes for somatic variant calling using RNA-Seq data. Relevant clinical findings were defined. Potential drug targets and genetic predispositions were explored. Four core molecular subgroups (WNT, SHH, Group 3, and Group 4) were identified. Genetic backgrounds of metastasis at diagnosis and extent of tumor resection were observed. The adjusted Heidelberg scheme showed its applicability. Potential drug targets were detected in the pathways of DNA damage response. Among the 10 patients with SHH MBs analyzed using whole exome sequencing studies, five patients exhibited potential genetic predispositions and four patients had relevant germline mutations. The findings of this study provide valuable information for updated risk adapted treatment and personalized care of childhood MBs in our cohort series and in Taiwan.",

keywords = "Clinical correlation, DNA damage response, Genetic predisposition, Medulloblastoma, Molecular, Risk stratification, RNA-Seq, Somatic mutations",

author = "Wu, {Kuo Sheng} and Ho, {Donald Ming Tak} and Jou, {Shiann Tarng} and Yu, {Alice L.} and Tran, {Huy Minh} and Liang, {Muh Lii} and Chen, {Hsin Hung} and Lee, {Yi Yen} and Chen, {Yi Wei} and Lin, {Shih Chieh} and Chang, {Feng Chi} and Tsai, {Min Lan} and Liu, {Yen Lin} and Lee, {Hsin Lun} and Hsieh, {Kevin Li Chun} and Huang, {Wen Chang} and Sung, {Shian Ying} and Chang, {Che Chang} and Changou, {Chun Austin} and Liang, {Kung Hao} and Hsieh, {Tsung Han} and Liu, {Yun Ru} and Chao, {Meng En} and Wan Chen and Chu, {Shing Shung} and Cho, {Er Chieh} and Wong, {Tai Tong}",

note = "Publisher Copyright: {\textcopyright} 2020 by the authors. Licensee MDPI, Basel, Switzerland.",

year = "2020",

month = mar,

doi = "10.3390/cancers12030653",

language = "English",

volume = "12",

journal = "Cancers",

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T1 - Molecular-clinical correlation in pediatric medulloblastoma

T2 - A cohort series study of 52 cases in Taiwan

AU - Wu, Kuo Sheng

AU - Ho, Donald Ming Tak

AU - Jou, Shiann Tarng

AU - Yu, Alice L.

AU - Tran, Huy Minh

AU - Liang, Muh Lii

AU - Chen, Hsin Hung

AU - Lee, Yi Yen

AU - Chen, Yi Wei

AU - Lin, Shih Chieh

AU - Chang, Feng Chi

AU - Tsai, Min Lan

AU - Liu, Yen Lin

AU - Lee, Hsin Lun

AU - Hsieh, Kevin Li Chun

AU - Huang, Wen Chang

AU - Sung, Shian Ying

AU - Chang, Che Chang

AU - Changou, Chun Austin

AU - Liang, Kung Hao

AU - Hsieh, Tsung Han

AU - Liu, Yun Ru

AU - Chao, Meng En

AU - Chen, Wan

AU - Chu, Shing Shung

AU - Cho, Er Chieh

AU - Wong, Tai Tong

PY - 2020/3

Y1 - 2020/3

N2 - In 2016, a project was initiated in Taiwan to adopt molecular diagnosis of childhood medulloblastoma (MB). In this study, we aimed to identify a molecular-clinical correlation and somatic mutation for exploring risk-adapted treatment, drug targets, and potential genetic predisposition. In total, 52 frozen tumor tissues of childhood MBs were collected. RNA sequencing (RNA-Seq) and DNA methylation array data were generated. Molecular subgrouping and clinical correlation analysis were performed. An adjusted Heidelberg risk stratification scheme was defined for updated clinical risk stratification. We selected 51 genes for somatic variant calling using RNA-Seq data. Relevant clinical findings were defined. Potential drug targets and genetic predispositions were explored. Four core molecular subgroups (WNT, SHH, Group 3, and Group 4) were identified. Genetic backgrounds of metastasis at diagnosis and extent of tumor resection were observed. The adjusted Heidelberg scheme showed its applicability. Potential drug targets were detected in the pathways of DNA damage response. Among the 10 patients with SHH MBs analyzed using whole exome sequencing studies, five patients exhibited potential genetic predispositions and four patients had relevant germline mutations. The findings of this study provide valuable information for updated risk adapted treatment and personalized care of childhood MBs in our cohort series and in Taiwan.

AB - In 2016, a project was initiated in Taiwan to adopt molecular diagnosis of childhood medulloblastoma (MB). In this study, we aimed to identify a molecular-clinical correlation and somatic mutation for exploring risk-adapted treatment, drug targets, and potential genetic predisposition. In total, 52 frozen tumor tissues of childhood MBs were collected. RNA sequencing (RNA-Seq) and DNA methylation array data were generated. Molecular subgrouping and clinical correlation analysis were performed. An adjusted Heidelberg risk stratification scheme was defined for updated clinical risk stratification. We selected 51 genes for somatic variant calling using RNA-Seq data. Relevant clinical findings were defined. Potential drug targets and genetic predispositions were explored. Four core molecular subgroups (WNT, SHH, Group 3, and Group 4) were identified. Genetic backgrounds of metastasis at diagnosis and extent of tumor resection were observed. The adjusted Heidelberg scheme showed its applicability. Potential drug targets were detected in the pathways of DNA damage response. Among the 10 patients with SHH MBs analyzed using whole exome sequencing studies, five patients exhibited potential genetic predispositions and four patients had relevant germline mutations. The findings of this study provide valuable information for updated risk adapted treatment and personalized care of childhood MBs in our cohort series and in Taiwan.

KW - Clinical correlation

KW - DNA damage response

KW - Genetic predisposition

KW - Medulloblastoma

KW - Molecular

KW - Risk stratification

KW - RNA-Seq

KW - Somatic mutations

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U2 - 10.3390/cancers12030653

DO - 10.3390/cancers12030653

M3 - Article

AN - SCOPUS:85081261359

SN - 2072-6694

VL - 12

JO - Cancers

JF - Cancers

IS - 3

M1 - 653

ER -

Molecular-clinical correlation in pediatric medulloblastoma: A cohort series study of 52 cases in Taiwan

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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