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Citations to this article

Deficiencies in Chfr and Mlh1 synergistically enhance tumor susceptibility in mice
Zheng Fu, … , Junjie Chen, Donald J. Tindall
Zheng Fu, … , Junjie Chen, Donald J. Tindall
Published August 17, 2009
Citation Information: J Clin Invest. 2009;119(9):2714-2724. https://doi.org/10.1172/JCI37405.
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Research Article Oncology

Deficiencies in Chfr and Mlh1 synergistically enhance tumor susceptibility in mice

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Abstract

Genetic instability, which leads to an accumulation of various genetic abnormalities, has been considered an essential component of the human neoplasic transformation process. However, the molecular basis of genomic instability during tumorigenesis remains incompletely understood. Growing evidence indicates that checkpoint with forkhead and ring finger domains (CHFR), a recently identified mitotic checkpoint protein, plays an important role in maintaining chromosome integrity and functions as a tumor suppressor. In this study, we used high-throughput technology to conduct gene expression profiling of human colon cancers and found that loss of CHFR expression frequently occurred in colon cancers with high microsatellite instability (MSI-H). Downregulation of CHFR expression was closely associated with overexpression of Aurora A, an important mitotic kinase. Mice with deficiencies in both Chfr and Mlh1 (the gene that encodes the DNA mismatch-repair protein Mlh1) displayed dramatically higher incidence of spontaneous tumors relative to mice deficient for only one of these genes. These results suggest that defects in both Chfr and Mlh1 synergistically increase predisposition to tumorigenesis.

Authors

Zheng Fu, Kevin Regan, Lizhi Zhang, Michael H. Muders, Stephen N. Thibodeau, Amy French, Yanhong Wu, Scott H. Kaufmann, Wilma L. Lingle, Junjie Chen, Donald J. Tindall

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Total citations by year

Year: 2022 2021 2016 2015 2013 2012 2011 2009 Total
Citations: 1 2 2 1 2 3 1 1 13
Citation information
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Citations to this article (13)

Title and authors Publication Year
Differential gene expression and network analysis in head and neck squamous cell carcinoma
I Habib, F Anjum, T Mohammad, N Sulaimani, A Shafie, M Almehmadi, D Yadav, S Sohal, I Hassan
Molecular and Cellular Biochemistry 2022
Deciphering CHFR Role in Pancreatic Ductal Adenocarcinoma
I González-Borja, E Alors-Pérez, I Amat, L Alonso, C Viyuela-García, S Goñi, JC Reyes, M Ceballos-Chávez, I Hernández-García, ME Sánchez-Frías, E Santamaría, S Razquin, Á Arjona-Sánchez, V Arrazubi, J Pérez-Sanz, R Vera, J Fernández-Irigoyen, JP Castaño, A Viúdez
Frontiers in Medicine 2021
CHFR and Paclitaxel Sensitivity of Ovarian Cancer.
Wahner Hendrickson AE, Visscher DW, Hou X, Goergen KM, Atkinson HJ, Beito TG, Negron V, Lingle WL, Bruzek AK, Hurley RM, Wagner JM, Flatten KS, Peterson KL, Schneider PA, Larson MC, Maurer MJ, Kalli KR, Oberg AL, Weroha SJ, Kaufmann SH
Cancers 2021
Polo-like kinase 1 induces epithelial-to-mesenchymal transition and promotes epithelial cell motility by activating CRAF/ERK signaling: ( A ) Cell lysates were prepared from the indicated PCa cell lines and subjected to Western blots in order to detect the level and activity of PLK1 protein using anti−PLK1 and anti−PLK1(pT210) antibodies, respectively. β-actin was used as a loading control. ( B ) RWPE-1 cells were infected with lentivirus encoding Flag-PLK1 (PLK1) or empty vector (EV). The protein levels of PLK1, AR, PSA, and β-actin were determined by Western blot. C4-2B cells with high endogenous PLK1 expression were included for comparison. ( C ) Control RWPE-1 and RWPE-1–PLK1 cells were subjected to a wound healing assay. The figure shows representative images as well as calculated percentage of wound closure during 48 hr of cell migration. Scale bar, 500 µm. ( D ) In vitro Matrigel invasion assay. The figure shows representative images of invaded cells and quantification of the relative number of cells that invaded over 48 hr. The data are presented as the mean ± s.e.m. *pt-test. Scale bar, 100 µm. ( E – G ) Time-lapse video microscopy motility experiments to monitor random migration of control and PLK1-overexpressing RWPE-1 cells. The trajectories of individual cells of different experimental groups ( E ), track distance ( F ), and velocity of cell migration ( G ) are shown. Horizontal bars in F-G represent median and interquartile range. Each dot represents a single-cell measurement. Thirty cells per experimental group were measured. *p
J Wu, AI Ivanov, PB Fisher, Z Fu
eLife 2016
High-definition CpG methylation of novel genes in gastric carcinogenesis identified by next-generation sequencing
JL Sepulveda, JL Gutierrez-Pajares, A Luna, Y Yao, JW Tobias, S Thomas, Y Woo, F Giorgi, EV Komissarova, A Califano, TC Wang, AR Sepulveda
Modern Pathology 2016
Aurora kinase A in gastrointestinal cancers: time to target
A Katsha, A Belkhiri, L Goff, W El-Rifai
Molecular Cancer 2015
Emerging evidence for CHFR as a cancer biomarker: from tumor biology to precision medicine
S Derks, AH Cleven, V Melotte, KM Smits, JC Brandes, N Azad, W Criekinge, AP de Bruïne, JG Herman, M Engeland
Cancer metastasis reviews 2013
Chromosome missegregation rate predicts whether aneuploidy will promote or suppress tumors
AD Silk, LM Zasadil, AJ Holland, B Vitre, DW Cleveland, BA Weaver
Proceedings of the National Academy of Sciences 2013
Acute sensitization of colon cancer cells to inflammatory cytokines by prophase arrest
A Kuratnik, VE Senapati, R Verma, BG Mellone, AT Vella, C Giardina
Biochemical Pharmacology 2012
Transcriptome Analysis of a Rotenone Model of Parkinsonism Reveals Complex I-Tied and -Untied Toxicity Mechanisms Common to Neurodegenerative Diseases
Y Cabeza-Arvelaiz, RH Schiestl
PloS one 2012
SINE retrotransposons cause epigenetic reprogramming of adjacent gene promoters
MR Estécio, J Gallegos, M Dekmezian, Y Lu, S Liang, JP Issa
Molecular cancer research : MCR 2012
CHFR: a key checkpoint component implicated in a wide range of cancers
S Sanbhnani, FM Yeong
Cellular and Molecular Life Sciences 2011
Pulmonary surfactant: an immunological perspective
ZC Chroneos, Z Sever-Chroneos, VL Shepherd
Cellular physiology and biochemistry : international journal of experimental cellular physiology, biochemistry, and pharmacology 2009

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