论文信息 - Senescence‐escape in melanoma

Senescence‐escape in melanoma

Cellular senescence is an important defense against uncontrolled cellular replication and is a critical tumor suppressor mechanism. Although initially described as an in vitro phenomenon, in recent years, several lines of evidence have indicated that senescence also occurs in vivo. Disparate cellular stresses can provoke senescence including telomere shortening, activation of certain oncogenes, oxidative stress and stalled replication forks. These stresses are best known to engage the p16INK4a-RB and ARF-p53 pathways to effect growth arrest and prevent neoplasia. Among these, ‘oncogene-induced senescence’ (OIS) is particularly known for the prevention of melanoma, resulting from the expression of mutant B-RAF or N-RAS in this disease.

N. Sharpless | Wenjin Liu

[1] Michael Wigler,et al. Genome-wide copy number analysis of single cells , 2012, Nature Protocols.

[2] J. Troge,et al. Tumour evolution inferred by single-cell sequencing , 2011, Nature.

[3] Pier Paolo Pandolfi,et al. Tenets of PTEN Tumor Suppression , 2008, Cell.

[4] C. Johannessen,et al. A negative feedback signaling network underlies oncogene-induced senescence. , 2006, Cancer cell.

[5] J. Shay,et al. BRAFE600-associated senescence-like cell cycle arrest of human naevi , 2005, Nature.

[6] F. Haluska,et al. Genetic interaction between NRAS and BRAF mutations and PTEN/MMAC1 inactivation in melanoma. , 2004, The Journal of investigative dermatology.

[7] N. Hayward,et al. Nuclear PTEN expression and clinicopathologic features in a population‐based series of primary cutaneous melanoma , 2002, International journal of cancer.

[8] A. McCullough,et al. Intratumor Heterogeneity and Branched Evolution Revealed by Multiregion Sequencing , 2013 .

[9] F. Haluska,et al. Genetic Interaction Between NRAS and BRAF Mutations and PTEN / MMAC 1 Inactivation in Melanoma , 2010 .