Alterations of cell cycle genes in cancer: unmasking the role of cancer stem cells

被引:39
作者
Caglar, Hasan Onur [1 ]
Biray Avci, Cigir [2 ]
机构
[1] Ege Univ, Hlth Sci Inst, Dept Stem Cell, TR-35100 Izmir, Turkey
[2] Ege Univ, Fac Med, Dept Med Biol, TR-35100 Izmir, Turkey
来源
MOLECULAR BIOLOGY REPORTS | 2020年 / 47卷 / 04期
关键词
Cell cycle; Cyclins; Cyclin-dependent kinases; Cyclin-dependent kinase inhibitors; Cancer; Bmi-1; Cancer stem cells; DOWN-REGULATION; OVARIAN-CANCER; SELF-RENEWAL; TUMOR-GROWTH; DNA-DAMAGE; GENOMIC INSTABILITY; PROMOTES INVASION; CDK INHIBITORS; AMPLIFICATION; EXPRESSION;
D O I
10.1007/s11033-020-05341-6
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The cell cycle is a complex and strictly controlled process, consisting of different phases. Cell cycle regulation depends on phase-specific transcriptions of cell cycle genes. The alterations of cell cycle genes can predispose normal cells to have a cancerous phenotype. Indeed, several mechanisms underlying the deregulation of the cell cycle have been identified in different types of cancer. Cancer stem cells (CSCs), a fraction of tumor cells, are selectively capable of initiating tumor development. However, the deregulation of the cell cycle progression in CSCs still remains incompletely understood. This review describes epigenetic alterations and aberrant transcriptional regulation of cell cycle genes in CSCs as well as cell cycle patterns of CSCs.
引用
收藏
页码:3065 / 3076
页数:12
相关论文
共 137 条
  • [1] The Polycomb Repressive Complex 1 Protein BMI1 Is Required for Constitutive Heterochromatin Formation and Silencing in Mammalian Somatic Cells
    Abdouh, Mohamed
    Hanna, Roy
    El Hajjar, Jida
    Flamier, Anthony
    Bernier, Gilbert
    [J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 2016, 291 (01) : 182 - 197
  • [2] Nuclear accumulation of cyclin D1 during S phase inhibits Cul4-dependent Cdt1 proteolysis and triggers p53-dependent DNA rereplication
    Aggarwal, Priya
    Lessie, Matthew D.
    Lin, Douglas I.
    Pontano, Laura
    Gladden, Andrew B.
    Nuskey, Beth
    Goradia, Ami
    Wasik, Mariusz A.
    Klein-Szanto, Andres J. P.
    Rustgi, Anil K.
    Bassing, Craig H.
    Diehl, J. Alan
    [J]. GENES & DEVELOPMENT, 2007, 21 (22) : 2908 - 2922
  • [3] Gene amplification in mesenchymal stem cells and during differentiation towards adipocytes or osteoblasts
    Altmayer, Nora Corinna
    Galata, Valentina
    Warschburger, Nadine
    Keller, Andreas
    Meese, Eckart
    Fischer, Ulrike
    [J]. ONCOTARGET, 2018, 9 (02) : 1803 - 1812
  • [4] Gene amplification and overexpression of CDK4 in sporadic breast carcinomas is associated with high tumor cell proliferation
    An, HX
    Beckmann, MW
    Reifenberger, G
    Bender, HG
    Niederacher, D
    [J]. AMERICAN JOURNAL OF PATHOLOGY, 1999, 154 (01) : 113 - 118
  • [5] The diverse functions of Dot1 and H3K79 methylation
    Anh Tram Nguyen
    Zhang, Yi
    [J]. GENES & DEVELOPMENT, 2011, 25 (13) : 1345 - 1358
  • [6] Loss of p16 expression is associated with the stem cell characteristics of surface markers and therapeutic resistance in estrogen receptor-negative breast cancer
    Arima, Yoshimi
    Hayashi, Naoki
    Hayashi, Hidemi
    Sasaki, Mikako
    Kai, Kazuharu
    Sugihara, Eiji
    Abe, Eriko
    Yoshida, Atsushi
    Mikami, Shuji
    Nakamura, Seigo
    Saya, Hideyuki
    [J]. INTERNATIONAL JOURNAL OF CANCER, 2012, 130 (11) : 2568 - 2579
  • [7] Permanent cell cycle exit in G2 phase after DNA damage in normal human fibroblasts
    Baus, F
    Gire, V
    Fisher, D
    Piette, J
    Dulic, V
    [J]. EMBO JOURNAL, 2003, 22 (15) : 3992 - 4002
  • [8] Loss of Function of the Tumor Suppressor DKC1 Perturbs p27 Translation Control and Contributes to Pituitary Tumorigenesis
    Bellodi, Cristian
    Krasnykh, Olya
    Haynes, Nikesha
    Theodoropoulou, Marily
    Peng, Guang
    Montanaro, Lorenzo
    Ruggero, Davide
    [J]. CANCER RESEARCH, 2010, 70 (14) : 6026 - 6035
  • [9] Botchkina Inna L., 2009, Cancer Genomics & Proteomics, V6, P19
  • [10] Brown VD, 1999, MOL CELL BIOL, V19, P3246
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