Molecular analysis of gastric cancer identifies subtypes associated with distinct clinical outcomes

Razvan Cristescu; Jeeyun Lee; Michael Nebozhyn; Kyoung Mee Kim; Jason C. Ting; Swee Seong Wong; Jiangang Liu; Yong Gang Yue; Jian Wang; Kun Yu; Xiang S. Ye; In Gu Do; Shawn Liu; Lara Gong; Jake Fu; Jason Gang Jin; Min Gew Choi; Tae Sung Sohn; Joon Ho Lee; Jae Moon Bae; Seung Tae Kim; Se Hoon Park; Insuk Sohn; Sin Ho Jung; Patrick Tan; Ronghua Chen; James Hardwick; Won Ki Kang; Mark Ayers; Dai Hongyue; Christoph Reinhard; Andrey Loboda; Sung Kim; Amit Aggarwal

doi:10.1038/nm.3850

Molecular analysis of gastric cancer identifies subtypes associated with distinct clinical outcomes

Razvan Cristescu
, Jeeyun Lee
, Michael Nebozhyn
, Kyoung Mee Kim
, Jason C. Ting
, Swee Seong Wong
, Jiangang Liu
, Yong Gang Yue
, Jian Wang
, Kun Yu
, Xiang S. Ye
, In Gu Do
, Shawn Liu
, Lara Gong
, Jake Fu
, Jason Gang Jin
, Min Gew Choi
, Tae Sung Sohn
, Joon Ho Lee
, Jae Moon Bae

Seung Tae Kim, Se Hoon Park, Insuk Sohn, Sin Ho Jung, Patrick Tan, Ronghua Chen, James Hardwick, Won Ki Kang, Mark Ayers, Dai Hongyue, Christoph Reinhard, Andrey Loboda, Sung Kim, Amit Aggarwal

Research output: Contribution to journal › Article › peer-review

1792 Scopus citations

Abstract

Gastric cancer, a leading cause of cancer-related deaths, is a heterogeneous disease. We aim to establish clinically relevant molecular subtypes that would encompass this heterogeneity and provide useful clinical information. We use gene expression data to describe four molecular subtypes linked to distinct patterns of molecular alterations, disease progression and prognosis. The mesenchymal-like type includes diffuse-subtype tumors with the worst prognosis, the tendency to occur at an earlier age and the highest recurrence frequency (63%) of the four subtypes. Microsatellite-unstable tumors are hyper-mutated intestinal-subtype tumors occurring in the antrum; these have the best overall prognosis and the lowest frequency of recurrence (22%) of the four subtypes. The tumor protein 53 (TP53)-active and TP53-inactive types include patients with intermediate prognosis and recurrence rates (with respect to the other two subtypes), with the TP53-active group showing better prognosis. We describe key molecular alterations in each of the four subtypes using targeted sequencing and genome-wide copy number microarrays. We validate these subtypes in independent cohorts in order to provide a consistent and unified framework for further clinical and preclinical translational research.

Original language	English
Pages (from-to)	449-456
Number of pages	8
Journal	Nature Medicine
Volume	21
Issue number	5
DOIs	https://doi.org/10.1038/nm.3850
State	Published - 1 May 2015

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10.1038/nm.3850

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Cristescu, R., Lee, J., Nebozhyn, M., Kim, K. M., Ting, J. C., Wong, S. S., Liu, J., Yue, Y. G., Wang, J., Yu, K., Ye, X. S., Do, I. G., Liu, S., Gong, L., Fu, J., Jin, J. G., Choi, M. G., Sohn, T. S., Lee, J. H., ... Aggarwal, A. (2015). Molecular analysis of gastric cancer identifies subtypes associated with distinct clinical outcomes. Nature Medicine, 21(5), 449-456. https://doi.org/10.1038/nm.3850

@article{9c0cd08c22ed444cbb626f84c6c8e2ef,

title = "Molecular analysis of gastric cancer identifies subtypes associated with distinct clinical outcomes",

abstract = "Gastric cancer, a leading cause of cancer-related deaths, is a heterogeneous disease. We aim to establish clinically relevant molecular subtypes that would encompass this heterogeneity and provide useful clinical information. We use gene expression data to describe four molecular subtypes linked to distinct patterns of molecular alterations, disease progression and prognosis. The mesenchymal-like type includes diffuse-subtype tumors with the worst prognosis, the tendency to occur at an earlier age and the highest recurrence frequency (63\%) of the four subtypes. Microsatellite-unstable tumors are hyper-mutated intestinal-subtype tumors occurring in the antrum; these have the best overall prognosis and the lowest frequency of recurrence (22\%) of the four subtypes. The tumor protein 53 (TP53)-active and TP53-inactive types include patients with intermediate prognosis and recurrence rates (with respect to the other two subtypes), with the TP53-active group showing better prognosis. We describe key molecular alterations in each of the four subtypes using targeted sequencing and genome-wide copy number microarrays. We validate these subtypes in independent cohorts in order to provide a consistent and unified framework for further clinical and preclinical translational research.",

author = "Razvan Cristescu and Jeeyun Lee and Michael Nebozhyn and Kim, \{Kyoung Mee\} and Ting, \{Jason C.\} and Wong, \{Swee Seong\} and Jiangang Liu and Yue, \{Yong Gang\} and Jian Wang and Kun Yu and Ye, \{Xiang S.\} and Do, \{In Gu\} and Shawn Liu and Lara Gong and Jake Fu and Jin, \{Jason Gang\} and Choi, \{Min Gew\} and Sohn, \{Tae Sung\} and Lee, \{Joon Ho\} and Bae, \{Jae Moon\} and Kim, \{Seung Tae\} and Park, \{Se Hoon\} and Insuk Sohn and Jung, \{Sin Ho\} and Patrick Tan and Ronghua Chen and James Hardwick and Kang, \{Won Ki\} and Mark Ayers and Dai Hongyue and Christoph Reinhard and Andrey Loboda and Sung Kim and Amit Aggarwal",

year = "2015",

month = may,

day = "1",

doi = "10.1038/nm.3850",

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Cristescu, R, Lee, J, Nebozhyn, M, Kim, KM, Ting, JC, Wong, SS, Liu, J, Yue, YG, Wang, J, Yu, K, Ye, XS, Do, IG, Liu, S, Gong, L, Fu, J, Jin, JG, Choi, MG , Sohn, TS, Lee, JH, Bae, JM , Kim, ST , Park, SH, Sohn, I, Jung, SH, Tan, P, Chen, R, Hardwick, J, Kang, WK, Ayers, M, Hongyue, D, Reinhard, C, Loboda, A, Kim, S & Aggarwal, A 2015, 'Molecular analysis of gastric cancer identifies subtypes associated with distinct clinical outcomes', Nature Medicine, vol. 21, no. 5, pp. 449-456. https://doi.org/10.1038/nm.3850

TY - JOUR

T1 - Molecular analysis of gastric cancer identifies subtypes associated with distinct clinical outcomes

AU - Cristescu, Razvan

AU - Lee, Jeeyun

AU - Nebozhyn, Michael

AU - Kim, Kyoung Mee

AU - Ting, Jason C.

AU - Wong, Swee Seong

AU - Liu, Jiangang

AU - Yue, Yong Gang

AU - Wang, Jian

AU - Yu, Kun

AU - Ye, Xiang S.

AU - Do, In Gu

AU - Liu, Shawn

AU - Gong, Lara

AU - Fu, Jake

AU - Jin, Jason Gang

AU - Choi, Min Gew

AU - Sohn, Tae Sung

AU - Lee, Joon Ho

AU - Bae, Jae Moon

AU - Kim, Seung Tae

AU - Park, Se Hoon

AU - Sohn, Insuk

AU - Jung, Sin Ho

AU - Tan, Patrick

AU - Chen, Ronghua

AU - Hardwick, James

AU - Kang, Won Ki

AU - Ayers, Mark

AU - Hongyue, Dai

AU - Reinhard, Christoph

AU - Loboda, Andrey

AU - Kim, Sung

AU - Aggarwal, Amit

PY - 2015/5/1

Y1 - 2015/5/1

N2 - Gastric cancer, a leading cause of cancer-related deaths, is a heterogeneous disease. We aim to establish clinically relevant molecular subtypes that would encompass this heterogeneity and provide useful clinical information. We use gene expression data to describe four molecular subtypes linked to distinct patterns of molecular alterations, disease progression and prognosis. The mesenchymal-like type includes diffuse-subtype tumors with the worst prognosis, the tendency to occur at an earlier age and the highest recurrence frequency (63%) of the four subtypes. Microsatellite-unstable tumors are hyper-mutated intestinal-subtype tumors occurring in the antrum; these have the best overall prognosis and the lowest frequency of recurrence (22%) of the four subtypes. The tumor protein 53 (TP53)-active and TP53-inactive types include patients with intermediate prognosis and recurrence rates (with respect to the other two subtypes), with the TP53-active group showing better prognosis. We describe key molecular alterations in each of the four subtypes using targeted sequencing and genome-wide copy number microarrays. We validate these subtypes in independent cohorts in order to provide a consistent and unified framework for further clinical and preclinical translational research.

AB - Gastric cancer, a leading cause of cancer-related deaths, is a heterogeneous disease. We aim to establish clinically relevant molecular subtypes that would encompass this heterogeneity and provide useful clinical information. We use gene expression data to describe four molecular subtypes linked to distinct patterns of molecular alterations, disease progression and prognosis. The mesenchymal-like type includes diffuse-subtype tumors with the worst prognosis, the tendency to occur at an earlier age and the highest recurrence frequency (63%) of the four subtypes. Microsatellite-unstable tumors are hyper-mutated intestinal-subtype tumors occurring in the antrum; these have the best overall prognosis and the lowest frequency of recurrence (22%) of the four subtypes. The tumor protein 53 (TP53)-active and TP53-inactive types include patients with intermediate prognosis and recurrence rates (with respect to the other two subtypes), with the TP53-active group showing better prognosis. We describe key molecular alterations in each of the four subtypes using targeted sequencing and genome-wide copy number microarrays. We validate these subtypes in independent cohorts in order to provide a consistent and unified framework for further clinical and preclinical translational research.

UR - https://www.scopus.com/pages/publications/84937765053

U2 - 10.1038/nm.3850

DO - 10.1038/nm.3850

M3 - Article

C2 - 25894828

AN - SCOPUS:84937765053

SN - 1078-8956

VL - 21

SP - 449

EP - 456

JO - Nature Medicine

JF - Nature Medicine

IS - 5

ER -

Molecular analysis of gastric cancer identifies subtypes associated with distinct clinical outcomes

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