Proto-Oncogene HRAS Transcript Level and Overall Survival in Stages II and III Colorectal Cancer

Donghyun Kim; Saima Sharif; Juan Antonio Raygoza Garay; Avanish S. Bhakta; Patrick M. Boland; Michael J. Cavnar; Michelle L. Churchman; Hassan Hatoum; Lyen C. Huang; Joseph Kim; Richard Kim; Robert W. Lentz; Sarbajit Mukherjee; Mary T. O'Donnell; Benjamin Quartey; Matthew J. Reilley; Robert J. Rounbehler; Bodour Salhia; Bryan P. Schneider; Carlos H. Chan

doi:10.1002/cam4.71114

Proto-Oncogene HRAS Transcript Level and Overall Survival in Stages II and III Colorectal Cancer

Donghyun Kim^*, Saima Sharif, Juan Antonio Raygoza Garay, Avanish S. Bhakta, Patrick M. Boland, Michael J. Cavnar, Michelle L. Churchman, Hassan Hatoum, Lyen C. Huang, Joseph Kim, Richard Kim, Robert W. Lentz, Sarbajit Mukherjee, Mary T. O'Donnell, Benjamin Quartey, Matthew J. Reilley, Robert J. Rounbehler, Bodour Salhia, Bryan P. Schneider, Carlos H. Chan^*

^*Corresponding author for this work

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Abstract

Background: Mutational landscape is prognostic in colorectal cancer (CRC). Rat sarcoma (RAS) oncogenes, such as KRAS and NRAS, with driver mutations, portend poor survival outcomes, whereas pathologic mutations in HRAS are extremely rare, and their prognostic value remains uncertain. Methods: This retrospective study analyzed the Oncology Research Information Exchange Network (ORIEN) alliance tumor RNA-Seq data in Stages II and III CRC to investigate the association between RAS gene expression and survival outcomes. Results: High transcript levels of HRAS were associated with superior overall survival (OS). The high HRAS-associated OS benefit was most pronounced in patients with right-sided primary expressing low KRAS transcript levels in the absence of pathologic KRAS mutations. Conclusions: Contrary to the notion that RAS family genes are proto-oncogenic, this study demonstrates that high HRAS transcript levels are associated with superior OS in Stages II and III CRC. The potential of HRAS as a prognostic biomarker should be explored further.

Original language	English
Article number	e71114
Journal	Cancer Medicine
Volume	14
Issue number	15
DOIs	https://doi.org/10.1002/cam4.71114
State	Published - Aug 2025

Keywords

biomarkers
colorectal cancer
gene expression regulation
survival

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10.1002/cam4.71114

Cite this

Kim, D., Sharif, S., Garay, J. A. R., Bhakta, A. S., Boland, P. M., Cavnar, M. J., Churchman, M. L., Hatoum, H., Huang, L. C., Kim, J., Kim, R., Lentz, R. W., Mukherjee, S., O'Donnell, M. T., Quartey, B., Reilley, M. J., Rounbehler, R. J., Salhia, B., Schneider, B. P., & Chan, C. H. (2025). Proto-Oncogene HRAS Transcript Level and Overall Survival in Stages II and III Colorectal Cancer. Cancer Medicine, 14(15), Article e71114. https://doi.org/10.1002/cam4.71114

@article{7b11cafe14884afba5c404d3e3b68357,

title = "Proto-Oncogene HRAS Transcript Level and Overall Survival in Stages II and III Colorectal Cancer",

abstract = "Background: Mutational landscape is prognostic in colorectal cancer (CRC). Rat sarcoma (RAS) oncogenes, such as KRAS and NRAS, with driver mutations, portend poor survival outcomes, whereas pathologic mutations in HRAS are extremely rare, and their prognostic value remains uncertain. Methods: This retrospective study analyzed the Oncology Research Information Exchange Network (ORIEN) alliance tumor RNA-Seq data in Stages II and III CRC to investigate the association between RAS gene expression and survival outcomes. Results: High transcript levels of HRAS were associated with superior overall survival (OS). The high HRAS-associated OS benefit was most pronounced in patients with right-sided primary expressing low KRAS transcript levels in the absence of pathologic KRAS mutations. Conclusions: Contrary to the notion that RAS family genes are proto-oncogenic, this study demonstrates that high HRAS transcript levels are associated with superior OS in Stages II and III CRC. The potential of HRAS as a prognostic biomarker should be explored further.",

keywords = "biomarkers, colorectal cancer, gene expression regulation, survival",

author = "Donghyun Kim and Saima Sharif and Garay, {Juan Antonio Raygoza} and Bhakta, {Avanish S.} and Boland, {Patrick M.} and Cavnar, {Michael J.} and Churchman, {Michelle L.} and Hassan Hatoum and Huang, {Lyen C.} and Joseph Kim and Richard Kim and Lentz, {Robert W.} and Sarbajit Mukherjee and O'Donnell, {Mary T.} and Benjamin Quartey and Reilley, {Matthew J.} and Rounbehler, {Robert J.} and Bodour Salhia and Schneider, {Bryan P.} and Chan, {Carlos H.}",

note = "Publisher Copyright: {\textcopyright} 2025 The Author(s). Cancer Medicine published by John Wiley & Sons Ltd.",

year = "2025",

month = aug,

doi = "10.1002/cam4.71114",

language = "English",

volume = "14",

journal = "Cancer Medicine",

issn = "2045-7634",

publisher = "John Wiley and Sons Inc",

number = "15",

}

Kim, D, Sharif, S, Garay, JAR, Bhakta, AS, Boland, PM, Cavnar, MJ, Churchman, ML, Hatoum, H, Huang, LC, Kim, J, Kim, R, Lentz, RW, Mukherjee, S, O'Donnell, MT, Quartey, B, Reilley, MJ, Rounbehler, RJ, Salhia, B, Schneider, BP & Chan, CH 2025, 'Proto-Oncogene HRAS Transcript Level and Overall Survival in Stages II and III Colorectal Cancer', Cancer Medicine, vol. 14, no. 15, e71114. https://doi.org/10.1002/cam4.71114

TY - JOUR

T1 - Proto-Oncogene HRAS Transcript Level and Overall Survival in Stages II and III Colorectal Cancer

AU - Kim, Donghyun

AU - Sharif, Saima

AU - Garay, Juan Antonio Raygoza

AU - Bhakta, Avanish S.

AU - Boland, Patrick M.

AU - Cavnar, Michael J.

AU - Churchman, Michelle L.

AU - Hatoum, Hassan

AU - Huang, Lyen C.

AU - Kim, Joseph

AU - Kim, Richard

AU - Lentz, Robert W.

AU - Mukherjee, Sarbajit

AU - O'Donnell, Mary T.

AU - Quartey, Benjamin

AU - Reilley, Matthew J.

AU - Rounbehler, Robert J.

AU - Salhia, Bodour

AU - Schneider, Bryan P.

AU - Chan, Carlos H.

PY - 2025/8

Y1 - 2025/8

N2 - Background: Mutational landscape is prognostic in colorectal cancer (CRC). Rat sarcoma (RAS) oncogenes, such as KRAS and NRAS, with driver mutations, portend poor survival outcomes, whereas pathologic mutations in HRAS are extremely rare, and their prognostic value remains uncertain. Methods: This retrospective study analyzed the Oncology Research Information Exchange Network (ORIEN) alliance tumor RNA-Seq data in Stages II and III CRC to investigate the association between RAS gene expression and survival outcomes. Results: High transcript levels of HRAS were associated with superior overall survival (OS). The high HRAS-associated OS benefit was most pronounced in patients with right-sided primary expressing low KRAS transcript levels in the absence of pathologic KRAS mutations. Conclusions: Contrary to the notion that RAS family genes are proto-oncogenic, this study demonstrates that high HRAS transcript levels are associated with superior OS in Stages II and III CRC. The potential of HRAS as a prognostic biomarker should be explored further.

AB - Background: Mutational landscape is prognostic in colorectal cancer (CRC). Rat sarcoma (RAS) oncogenes, such as KRAS and NRAS, with driver mutations, portend poor survival outcomes, whereas pathologic mutations in HRAS are extremely rare, and their prognostic value remains uncertain. Methods: This retrospective study analyzed the Oncology Research Information Exchange Network (ORIEN) alliance tumor RNA-Seq data in Stages II and III CRC to investigate the association between RAS gene expression and survival outcomes. Results: High transcript levels of HRAS were associated with superior overall survival (OS). The high HRAS-associated OS benefit was most pronounced in patients with right-sided primary expressing low KRAS transcript levels in the absence of pathologic KRAS mutations. Conclusions: Contrary to the notion that RAS family genes are proto-oncogenic, this study demonstrates that high HRAS transcript levels are associated with superior OS in Stages II and III CRC. The potential of HRAS as a prognostic biomarker should be explored further.

KW - biomarkers

KW - colorectal cancer

KW - gene expression regulation

KW - survival

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U2 - 10.1002/cam4.71114

DO - 10.1002/cam4.71114

M3 - Article

C2 - 40879062

AN - SCOPUS:105012148668

SN - 2045-7634

VL - 14

JO - Cancer Medicine

JF - Cancer Medicine

IS - 15

M1 - e71114

ER -