Real-time in vivo imaging of p16Ink4a reveals cross talk with p53

Yamakoshi, Kimi; Takahashi, Akiko; Hirota, Fumiko; Nakayama, Ryu; Ishimaru, Naozumi; Kubo, Yoshiaki; Mann, David J.; Ohmura, Masako; Hirao, Atsushi; Saya, Hideyuki; Arase, Seiji; Hayashi, Yoshio; Nakao, Kazuki; Matsumoto, Machiko; Ohtani, Naoko; Hara, Eiji

doi:10.1083/jcb.200904105

Cited by 143 publications

(161 citation statements)

References 67 publications

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“…Our data also showed that shikonin increased expression of p16, further contributing to inhibition of phosphorylation of Rb in both K1 and FTC133 cells, and NAC dramatically abolished this effect. These observations suggest that shikonin inhibits cell growth by modulating the activity of the p16/Rb/E2 factor (E2F) pathway, as supported by previous studies showing that ROS-induced upregulation of p16 is one of the mechanisms regulating senescence, which keeps the balance between regeneration and cancer (34,35). Given that metastasis is the major cause of cancer-related death, we investigated the effect of shikonin on cell migration and invasion in this study.…”

Section: Discussionmentioning

confidence: 71%

Shikonin Inhibits Thyroid Cancer Cell Growth and Invasiveness Through Targeting Major Signaling Pathways

Yang

Guan

et al. 2013

The Journal of Clinical Endocrinology & Metabolism

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Section: Discussionmentioning

confidence: 71%

Shikonin Inhibits Thyroid Cancer Cell Growth and Invasiveness Through Targeting Major Signaling Pathways

Yang

Guan

et al. 2013

The Journal of Clinical Endocrinology & Metabolism

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“…Despite these advantages, p16 INK4A also has apparent limitations as an in vivo biomarker of senescence. First, there are forms of in vitro senescence that are not characterized by p16 INK4A expression 18,[78][79][80] . At least under some circumstances, the absence of p16 INK4A expression might be compensated by upregulation of p15 INK4B (REFS [81][82][83] or by the expression of CDKN2C (also known as INK4C) 84 .…”

Section: Markers Of Senescencementioning

confidence: 98%

Forging a signature of in vivo senescence

2015

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'Cellular senescence', a term originally defining the characteristics of cultured cells that exceed their replicative limit, has been broadened to describe durable states of proliferative arrest induced by disparate stress factors. Proposed relationships between cellular senescence, tumour suppression, loss of tissue regenerative capacity and ageing suffer from lack of uniform definition and consistently applied criteria. Here, we highlight caveats in interpreting the importance of suboptimal senescence-associated biomarkers, expressed either alone or in combination. We advocate that more-specific descriptors be substituted for the now broadly applied umbrella term 'senescence' in defining the suite of diverse physiological responses to cellular stress.

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“…Another possibility implicates increased expression of DNMTs induced by the oncogene. 9 Although unlikely, oncogenes might also be able to increase DNMT enzymatic activity thus disrupting the balance that keeps specific gene loci active (Fig. 1).…”

Section: Philadelphia Chromosomementioning

confidence: 99%