@phdthesis{Leikam2012,
  author    = {Leikam, Claudia},
  title     = {Oncogene-induced senescence in melanocytes},
  url       = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-79316},
  school      = {Universit{\"a}t W{\"u}rzburg},
  year      = {2012},
  abstract  = {Melanoma is the most aggressive skin cancer with very limited treatment options. Upon appearance of metastases chemotherapeutics are used to either kill or slow down the growth of cancer cells by inducing apoptosis or senescence, respectively. With melanomas originating from melanocytes, it is vital to elucidate the mechanisms that distinguish senescence induction from proliferation and tumourigenicity. Xmrk (Xiphophorus melanoma receptor kinase), the fish orthologue of the human epidermal growth factor receptor (EGFR), causes highly aggressive melanoma in fish. Using an inducible variant, HERmrk, I showed that high receptor levels result in melanocyte senescence, whereas low and medium expression allows for cell proliferation and tumourigenicity. Mechanistically, HERmrk leads to increased reactive oxygen species (ROS) levels, which trigger a DNA damage response. Consequently, multinucleated, senescent cells develop by both endomitosis and fusion. Furthermore, oncogenic N-RAS (N--RAS61K) induces a similar multinucleated phenotype in melanocytes. In addition, I found that both overexpression of C-MYC and the knockdown of miz­-1 (Myc­-interacting zinc finger protein 1) diminished HERmrk-induced senescence entry. C-MYC prevent ROS induction, DNA damage and senescence, while acting synergistically with HERmrk in conveying tumourigenic features to melanocytes. Further analyses identified cystathionase (CTH) as a novel target gene of Myc and Miz-­1 crucial for senescence prevention. CTH encodes an enzyme involved in the synthesis of cysteine from methionine, thereby allowing for increased ROS detoxification. Even though senescence was thought to be irreversible and hence tumour protective, I demonstrated that prolonged expression of the melanoma oncogene N­-RAS61K in pigment cells overcomes initial OIS by triggering the emergence of tumour-initiating, mononucleated stem-like cells from multinucleated senescent cells. This progeny is dedifferentiated, highly proliferative, anoikis­-resistant and induces fast­-growing, metastatic tumours upon transplantation into nude mice. Our data demonstrate that induction of OIS is not only a cellular failsafe mechanism, but also carries the potential to provide a source for highly aggressive, tumour­-initiating cells.},
  subject      = {Melanom},
  language  = {en}
}