Dysregulated expression of suppressor loop of circadian rhythm genes in colorectal cancer pathogenesis

Namood E. Sahar; Javeria Qadir; Syeda K. Riaz; Sali A. Bagabir; Zahid Muneer; Ahmareen K. Sheikh; Shahzad H. Waqar; Rinaldo Pellicano; Sharmila Fagoonee; Shafiul Haque; Muhammad F. Malik

doi:10.23736/S0026-4806.22.07981-2

Dysregulated expression of suppressor loop of circadian rhythm genes in colorectal cancer pathogenesis

Namood E. Sahar
, Javeria Qadir
, Syeda K. Riaz
, Sali A. Bagabir
, Zahid Muneer
, Ahmareen K. Sheikh
, Shahzad H. Waqar
, Rinaldo Pellicano
, Sharmila Fagoonee
, Shafiul Haque
, Muhammad F. Malik

COMSATS University Islamabad
Shaheed Zulfiqar Ali Bhutto Medical University
Jazan University
Azienda Sanitaria Ospedaliera Molinette San Giovanni Battista Di Torino
National Research Council of Italy

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

11 Scopus citations

Abstract

BACKGROUND: Colorectal cancer (CRC) is a heterogeneous disease and activation of WNT and TGFβ mediated oncogenic pathways is frequently observed in this pathology. However, to date, limited reports have been published addressing the association of circadian clock with CRC pathogenesis and stratification. The current study aims at assessing the expression of important circadian markers, PER2, PER3 and NR1D1, in independent crc cohorts and their associations with crc-related pathways. MeTHOdS: Gene expression analysis was performed using available GeO (GSe39582) and TcGa datasets. Quantitative real time polymerase chain reaction was used to quantify the expression levels of PER2, PER3 and NRID1 in FFPe (formalin fixed paraffin embedded) CRC tissue samples. Furthermore, enrichment of circadian markers in WNT and TGFβ pathways-activated tumors was assessed. RESULTS: Statistically significant downregulation of PER3 was found in tumor versus control samples in GeO (P<0.0001) and TcGa colon and rectal adenocarcinoma datasets (P<0.05). analysis of GeO dataset revealed a statistically significant upregulation of PER2 (P<0.01), and NR1D1 in colon adenocarcinoma, which was confirmed by qRTPcr in crc tumor samples versus controls in FFPe validation cohort. Higher expression of NR1D1 was associated with poor prognosis in colon adenocarcinoma. contrastingly, PER3 was significantly downregulated in tumors (P<0.001) compared to controls and was associated with high-grade crc tumors versus low-grade tumors. Tumors with WNT pathway activation had significantly low PER3 and slightly upregulated PER2 (<0.0001) expression. interestingly, differential expression of PER3 and NR1D1 was significantly correlated with TGFβ1-expressing tumors (P<0.0001). Moreover, MYC- amplified tumors exhibited decreased PER3 levels. cONcLUSiONS: Thus, low PER3 expression in crc and poor survival of patients with NR1D1-high tumors reveal that genes in the suppressor loop of circadian rhythm are dysregulated in crc, hence pointing out to the importance of dissecting the circadian pathway in cancer.

Original language	English
Pages (from-to)	497-505
Number of pages	9
Journal	Minerva Medica
Volume	113
Issue number	3
DOIs	https://doi.org/10.23736/S0026-4806.22.07981-2
State	Published - Jun 2022
Externally published	Yes

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

Circadian rhythm
Colorectal neoplasms
NR1D1 protein,human
PER2 protein,human
PER3 protein,human

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10.23736/S0026-4806.22.07981-2

Cite this

@article{2aa870bbd21744328935b97f1679695f,

title = "Dysregulated expression of suppressor loop of circadian rhythm genes in colorectal cancer pathogenesis",

abstract = "BACKGROUND: Colorectal cancer (CRC) is a heterogeneous disease and activation of WNT and TGFβ mediated oncogenic pathways is frequently observed in this pathology. However, to date, limited reports have been published addressing the association of circadian clock with CRC pathogenesis and stratification. The current study aims at assessing the expression of important circadian markers, PER2, PER3 and NR1D1, in independent crc cohorts and their associations with crc-related pathways. MeTHOdS: Gene expression analysis was performed using available GeO (GSe39582) and TcGa datasets. Quantitative real time polymerase chain reaction was used to quantify the expression levels of PER2, PER3 and NRID1 in FFPe (formalin fixed paraffin embedded) CRC tissue samples. Furthermore, enrichment of circadian markers in WNT and TGFβ pathways-activated tumors was assessed. RESULTS: Statistically significant downregulation of PER3 was found in tumor versus control samples in GeO (P<0.0001) and TcGa colon and rectal adenocarcinoma datasets (P<0.05). analysis of GeO dataset revealed a statistically significant upregulation of PER2 (P<0.01), and NR1D1 in colon adenocarcinoma, which was confirmed by qRTPcr in crc tumor samples versus controls in FFPe validation cohort. Higher expression of NR1D1 was associated with poor prognosis in colon adenocarcinoma. contrastingly, PER3 was significantly downregulated in tumors (P<0.001) compared to controls and was associated with high-grade crc tumors versus low-grade tumors. Tumors with WNT pathway activation had significantly low PER3 and slightly upregulated PER2 (<0.0001) expression. interestingly, differential expression of PER3 and NR1D1 was significantly correlated with TGFβ1-expressing tumors (P<0.0001). Moreover, MYC- amplified tumors exhibited decreased PER3 levels. cONcLUSiONS: Thus, low PER3 expression in crc and poor survival of patients with NR1D1-high tumors reveal that genes in the suppressor loop of circadian rhythm are dysregulated in crc, hence pointing out to the importance of dissecting the circadian pathway in cancer.",

keywords = "Circadian rhythm, Colorectal neoplasms, NR1D1 protein,human, PER2 protein,human, PER3 protein,human",

author = "Sahar, \{Namood E.\} and Javeria Qadir and Riaz, \{Syeda K.\} and Bagabir, \{Sali A.\} and Zahid Muneer and Sheikh, \{Ahmareen K.\} and Waqar, \{Shahzad H.\} and Rinaldo Pellicano and Sharmila Fagoonee and Shafiul Haque and Malik, \{Muhammad F.\}",

year = "2022",

month = jun,

doi = "10.23736/S0026-4806.22.07981-2",

language = "English",

volume = "113",

pages = "497--505",

journal = "Minerva Medica",

issn = "0026-4806",

publisher = "Edizioni Minerva Medica",

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TY - JOUR

T1 - Dysregulated expression of suppressor loop of circadian rhythm genes in colorectal cancer pathogenesis

AU - Sahar, Namood E.

AU - Qadir, Javeria

AU - Riaz, Syeda K.

AU - Bagabir, Sali A.

AU - Muneer, Zahid

AU - Sheikh, Ahmareen K.

AU - Waqar, Shahzad H.

AU - Pellicano, Rinaldo

AU - Fagoonee, Sharmila

AU - Haque, Shafiul

AU - Malik, Muhammad F.

PY - 2022/6

Y1 - 2022/6

N2 - BACKGROUND: Colorectal cancer (CRC) is a heterogeneous disease and activation of WNT and TGFβ mediated oncogenic pathways is frequently observed in this pathology. However, to date, limited reports have been published addressing the association of circadian clock with CRC pathogenesis and stratification. The current study aims at assessing the expression of important circadian markers, PER2, PER3 and NR1D1, in independent crc cohorts and their associations with crc-related pathways. MeTHOdS: Gene expression analysis was performed using available GeO (GSe39582) and TcGa datasets. Quantitative real time polymerase chain reaction was used to quantify the expression levels of PER2, PER3 and NRID1 in FFPe (formalin fixed paraffin embedded) CRC tissue samples. Furthermore, enrichment of circadian markers in WNT and TGFβ pathways-activated tumors was assessed. RESULTS: Statistically significant downregulation of PER3 was found in tumor versus control samples in GeO (P<0.0001) and TcGa colon and rectal adenocarcinoma datasets (P<0.05). analysis of GeO dataset revealed a statistically significant upregulation of PER2 (P<0.01), and NR1D1 in colon adenocarcinoma, which was confirmed by qRTPcr in crc tumor samples versus controls in FFPe validation cohort. Higher expression of NR1D1 was associated with poor prognosis in colon adenocarcinoma. contrastingly, PER3 was significantly downregulated in tumors (P<0.001) compared to controls and was associated with high-grade crc tumors versus low-grade tumors. Tumors with WNT pathway activation had significantly low PER3 and slightly upregulated PER2 (<0.0001) expression. interestingly, differential expression of PER3 and NR1D1 was significantly correlated with TGFβ1-expressing tumors (P<0.0001). Moreover, MYC- amplified tumors exhibited decreased PER3 levels. cONcLUSiONS: Thus, low PER3 expression in crc and poor survival of patients with NR1D1-high tumors reveal that genes in the suppressor loop of circadian rhythm are dysregulated in crc, hence pointing out to the importance of dissecting the circadian pathway in cancer.

AB - BACKGROUND: Colorectal cancer (CRC) is a heterogeneous disease and activation of WNT and TGFβ mediated oncogenic pathways is frequently observed in this pathology. However, to date, limited reports have been published addressing the association of circadian clock with CRC pathogenesis and stratification. The current study aims at assessing the expression of important circadian markers, PER2, PER3 and NR1D1, in independent crc cohorts and their associations with crc-related pathways. MeTHOdS: Gene expression analysis was performed using available GeO (GSe39582) and TcGa datasets. Quantitative real time polymerase chain reaction was used to quantify the expression levels of PER2, PER3 and NRID1 in FFPe (formalin fixed paraffin embedded) CRC tissue samples. Furthermore, enrichment of circadian markers in WNT and TGFβ pathways-activated tumors was assessed. RESULTS: Statistically significant downregulation of PER3 was found in tumor versus control samples in GeO (P<0.0001) and TcGa colon and rectal adenocarcinoma datasets (P<0.05). analysis of GeO dataset revealed a statistically significant upregulation of PER2 (P<0.01), and NR1D1 in colon adenocarcinoma, which was confirmed by qRTPcr in crc tumor samples versus controls in FFPe validation cohort. Higher expression of NR1D1 was associated with poor prognosis in colon adenocarcinoma. contrastingly, PER3 was significantly downregulated in tumors (P<0.001) compared to controls and was associated with high-grade crc tumors versus low-grade tumors. Tumors with WNT pathway activation had significantly low PER3 and slightly upregulated PER2 (<0.0001) expression. interestingly, differential expression of PER3 and NR1D1 was significantly correlated with TGFβ1-expressing tumors (P<0.0001). Moreover, MYC- amplified tumors exhibited decreased PER3 levels. cONcLUSiONS: Thus, low PER3 expression in crc and poor survival of patients with NR1D1-high tumors reveal that genes in the suppressor loop of circadian rhythm are dysregulated in crc, hence pointing out to the importance of dissecting the circadian pathway in cancer.

KW - Circadian rhythm

KW - Colorectal neoplasms

KW - NR1D1 protein,human

KW - PER2 protein,human

KW - PER3 protein,human

UR - https://www.scopus.com/pages/publications/85134633756

U2 - 10.23736/S0026-4806.22.07981-2

DO - 10.23736/S0026-4806.22.07981-2

M3 - Article

C2 - 35856182

AN - SCOPUS:85134633756

SN - 0026-4806

VL - 113

SP - 497

EP - 505

JO - Minerva Medica

JF - Minerva Medica

IS - 3

ER -

Dysregulated expression of suppressor loop of circadian rhythm genes in colorectal cancer pathogenesis

Abstract

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