Higher order chromatin modulator cohesin SA1 is an early biomarker for colon carcinogenesis: Race-specific implications

Ramesh K. Wali; Navneet Momi; Mart Dela Cruz; Audrey H. Calderwood; Yolanda Stypula-Cyrus; Luay Almassalha; Anuj Chhaparia; Christopher R. Weber; Andrew Radosevich; Ashish K. Tiwari; Bilal Latif; Vadim Backman; Hemant K. Roy

doi:10.1158/1940-6207.CAPR-16-0054

Higher order chromatin modulator cohesin SA1 is an early biomarker for colon carcinogenesis: Race-specific implications

Ramesh K. Wali, Navneet Momi, Mart Dela Cruz, Audrey H. Calderwood, Yolanda Stypula-Cyrus, Luay Almassalha, Anuj Chhaparia, Christopher R. Weber, Andrew Radosevich, Ashish K. Tiwari, Bilal Latif, Vadim Backman, Hemant K. Roy^*

^*Corresponding author for this work

Biomedical Engineering

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

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Abstract

Alterations in high order chromatin, with concomitant modulation in gene expression, are one of the earliest events in the development of colorectal cancer. Cohesins are a family of proteins that modulate high-order chromatin, although the role in colorectal cancer remains incompletely understood. We, therefore, assessed the role of cohesin SA1 in colorectal cancer biology and as a biomarker focusing in particular on the increased incidence/mortality of colorectal cancer among African-Americans. Immunohistochemistry on tissue arrays revealed dramatically decreased SA1 expression in both adenomas (62%;P= 0.001) and adenocarcinomas (75%; P = 0.0001). RT-PCR performed in endoscopically normal rectal biopsies (n = 78) revealed a profound decrease in SA1 expression in adenoma-harboring patients (field carcinogenesis) compared with those who were neoplasia-free (47%; P = 0.03). From a racial perspective, colorectal cancer tissues from Caucasians had 56% higher SA1 expression than in African-Americans. This was mirrored in field carcinogenesis where healthy Caucasians expressed more SA1 at baseline compared with matched African-American subjects (73%; P = 0.003). However, asabiomarker for colorectal cancer risk, the diagnostic performance as assessed by area under ROC curve was greater in African-Americans (AUROC = 0.724) than in Caucasians (AUROC = 0.585). From a biologic perspective, SA1 modulation of high-order chromatin was demonstrated with both biophotonic (nanocytology) and chromatin accessibility [micrococcal nuclease (MNase)] assays in SA1-knockdown HT29 colorectal cancer cells. The functional consequences were underscored by increased proliferation (WST-1; P = 0.0002, colony formation; P = 0.001) in the SA1-knockdown HT29 cells. These results provide the first evidence indicating a tumor suppressor role of SA1 in early colon carcinogenesis and as a risk stratification biomarker giving potential insights into biologicbasis of racial disparities in colorectal cancer.

Original language	English (US)
Pages (from-to)	844-854
Number of pages	11
Journal	Cancer Prevention Research
Volume	9
Issue number	11
DOIs	https://doi.org/10.1158/1940-6207.CAPR-16-0054
State	Published - Nov 2016

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/1940-6207.CAPR-16-0054

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Wali, R. K., Momi, N., Dela Cruz, M., Calderwood, A. H., Stypula-Cyrus, Y., Almassalha, L., Chhaparia, A., Weber, C. R., Radosevich, A., Tiwari, A. K., Latif, B., Backman, V., & Roy, H. K. (2016). Higher order chromatin modulator cohesin SA1 is an early biomarker for colon carcinogenesis: Race-specific implications. Cancer Prevention Research, 9(11), 844-854. https://doi.org/10.1158/1940-6207.CAPR-16-0054

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title = "Higher order chromatin modulator cohesin SA1 is an early biomarker for colon carcinogenesis: Race-specific implications",

abstract = "Alterations in high order chromatin, with concomitant modulation in gene expression, are one of the earliest events in the development of colorectal cancer. Cohesins are a family of proteins that modulate high-order chromatin, although the role in colorectal cancer remains incompletely understood. We, therefore, assessed the role of cohesin SA1 in colorectal cancer biology and as a biomarker focusing in particular on the increased incidence/mortality of colorectal cancer among African-Americans. Immunohistochemistry on tissue arrays revealed dramatically decreased SA1 expression in both adenomas (62%;P= 0.001) and adenocarcinomas (75%; P = 0.0001). RT-PCR performed in endoscopically normal rectal biopsies (n = 78) revealed a profound decrease in SA1 expression in adenoma-harboring patients (field carcinogenesis) compared with those who were neoplasia-free (47%; P = 0.03). From a racial perspective, colorectal cancer tissues from Caucasians had 56% higher SA1 expression than in African-Americans. This was mirrored in field carcinogenesis where healthy Caucasians expressed more SA1 at baseline compared with matched African-American subjects (73%; P = 0.003). However, asabiomarker for colorectal cancer risk, the diagnostic performance as assessed by area under ROC curve was greater in African-Americans (AUROC = 0.724) than in Caucasians (AUROC = 0.585). From a biologic perspective, SA1 modulation of high-order chromatin was demonstrated with both biophotonic (nanocytology) and chromatin accessibility [micrococcal nuclease (MNase)] assays in SA1-knockdown HT29 colorectal cancer cells. The functional consequences were underscored by increased proliferation (WST-1; P = 0.0002, colony formation; P = 0.001) in the SA1-knockdown HT29 cells. These results provide the first evidence indicating a tumor suppressor role of SA1 in early colon carcinogenesis and as a risk stratification biomarker giving potential insights into biologicbasis of racial disparities in colorectal cancer.",

author = "Wali, {Ramesh K.} and Navneet Momi and {Dela Cruz}, Mart and Calderwood, {Audrey H.} and Yolanda Stypula-Cyrus and Luay Almassalha and Anuj Chhaparia and Weber, {Christopher R.} and Andrew Radosevich and Tiwari, {Ashish K.} and Bilal Latif and Vadim Backman and Roy, {Hemant K.}",

note = "Publisher Copyright: {\textcopyright} 2016 American Association for Cancer Research.",

year = "2016",

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doi = "10.1158/1940-6207.CAPR-16-0054",

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Wali, RK, Momi, N, Dela Cruz, M, Calderwood, AH, Stypula-Cyrus, Y, Almassalha, L, Chhaparia, A, Weber, CR, Radosevich, A, Tiwari, AK, Latif, B, Backman, V & Roy, HK 2016, 'Higher order chromatin modulator cohesin SA1 is an early biomarker for colon carcinogenesis: Race-specific implications', Cancer Prevention Research, vol. 9, no. 11, pp. 844-854. https://doi.org/10.1158/1940-6207.CAPR-16-0054

TY - JOUR

T1 - Higher order chromatin modulator cohesin SA1 is an early biomarker for colon carcinogenesis

T2 - Race-specific implications

AU - Wali, Ramesh K.

AU - Momi, Navneet

AU - Dela Cruz, Mart

AU - Calderwood, Audrey H.

AU - Stypula-Cyrus, Yolanda

AU - Almassalha, Luay

AU - Chhaparia, Anuj

AU - Weber, Christopher R.

AU - Radosevich, Andrew

AU - Tiwari, Ashish K.

AU - Latif, Bilal

AU - Backman, Vadim

AU - Roy, Hemant K.

PY - 2016/11

Y1 - 2016/11

N2 - Alterations in high order chromatin, with concomitant modulation in gene expression, are one of the earliest events in the development of colorectal cancer. Cohesins are a family of proteins that modulate high-order chromatin, although the role in colorectal cancer remains incompletely understood. We, therefore, assessed the role of cohesin SA1 in colorectal cancer biology and as a biomarker focusing in particular on the increased incidence/mortality of colorectal cancer among African-Americans. Immunohistochemistry on tissue arrays revealed dramatically decreased SA1 expression in both adenomas (62%;P= 0.001) and adenocarcinomas (75%; P = 0.0001). RT-PCR performed in endoscopically normal rectal biopsies (n = 78) revealed a profound decrease in SA1 expression in adenoma-harboring patients (field carcinogenesis) compared with those who were neoplasia-free (47%; P = 0.03). From a racial perspective, colorectal cancer tissues from Caucasians had 56% higher SA1 expression than in African-Americans. This was mirrored in field carcinogenesis where healthy Caucasians expressed more SA1 at baseline compared with matched African-American subjects (73%; P = 0.003). However, asabiomarker for colorectal cancer risk, the diagnostic performance as assessed by area under ROC curve was greater in African-Americans (AUROC = 0.724) than in Caucasians (AUROC = 0.585). From a biologic perspective, SA1 modulation of high-order chromatin was demonstrated with both biophotonic (nanocytology) and chromatin accessibility [micrococcal nuclease (MNase)] assays in SA1-knockdown HT29 colorectal cancer cells. The functional consequences were underscored by increased proliferation (WST-1; P = 0.0002, colony formation; P = 0.001) in the SA1-knockdown HT29 cells. These results provide the first evidence indicating a tumor suppressor role of SA1 in early colon carcinogenesis and as a risk stratification biomarker giving potential insights into biologicbasis of racial disparities in colorectal cancer.

AB - Alterations in high order chromatin, with concomitant modulation in gene expression, are one of the earliest events in the development of colorectal cancer. Cohesins are a family of proteins that modulate high-order chromatin, although the role in colorectal cancer remains incompletely understood. We, therefore, assessed the role of cohesin SA1 in colorectal cancer biology and as a biomarker focusing in particular on the increased incidence/mortality of colorectal cancer among African-Americans. Immunohistochemistry on tissue arrays revealed dramatically decreased SA1 expression in both adenomas (62%;P= 0.001) and adenocarcinomas (75%; P = 0.0001). RT-PCR performed in endoscopically normal rectal biopsies (n = 78) revealed a profound decrease in SA1 expression in adenoma-harboring patients (field carcinogenesis) compared with those who were neoplasia-free (47%; P = 0.03). From a racial perspective, colorectal cancer tissues from Caucasians had 56% higher SA1 expression than in African-Americans. This was mirrored in field carcinogenesis where healthy Caucasians expressed more SA1 at baseline compared with matched African-American subjects (73%; P = 0.003). However, asabiomarker for colorectal cancer risk, the diagnostic performance as assessed by area under ROC curve was greater in African-Americans (AUROC = 0.724) than in Caucasians (AUROC = 0.585). From a biologic perspective, SA1 modulation of high-order chromatin was demonstrated with both biophotonic (nanocytology) and chromatin accessibility [micrococcal nuclease (MNase)] assays in SA1-knockdown HT29 colorectal cancer cells. The functional consequences were underscored by increased proliferation (WST-1; P = 0.0002, colony formation; P = 0.001) in the SA1-knockdown HT29 cells. These results provide the first evidence indicating a tumor suppressor role of SA1 in early colon carcinogenesis and as a risk stratification biomarker giving potential insights into biologicbasis of racial disparities in colorectal cancer.

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Higher order chromatin modulator cohesin SA1 is an early biomarker for colon carcinogenesis: Race-specific implications

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UN SDGs

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