Inactivation of p16<sup>INK4a</sup>(inhibitor of cyclin‐dependent kinase 4A) immortalizes primary human keratinocytes by maintaining cells in the stem cell compartment

Maurelli, Riccardo; Zambruno, Giovanna; Guerra, Liliana; Abbruzzese, Claudia; Dimri, Goberdhan P.; Gellini, Mara; Bondanza, Sergio; Dellambra, Elena

doi:10.1096/fj.05-4480fje

Cited by 46 publications

(69 citation statements)

References 65 publications

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“…Cellular senescence dependent on p16 may be induced in response to telomere erosion and/or by another as yet unidentified stimulus. Maurelli et al (42) report that, in primary human keratinocytes, senescence bypass is accomplished only when p16 is down-regulated in those cells endowed with a high proliferative potential. Moreover, elevated intracellular level of reactive oxygen species and protein kinase Cy activation has been found to maintain senescent human cell cycle arrest, resulting in blocking against immortalization, even after p16/pRb signals are inactivated (20).…”

Section: Discussionmentioning

confidence: 99%

Function of JunB in Transient Amplifying Cell Senescence and Progression of Human Prostate Cancer

Konishi¹,

Shimada²,

Nakamura³

et al. 2008

Clinical Cancer Research

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Purpose: Replicative senescence in cells acts as a barrier against excessive proliferation and carcinogenesis. Transient amplifying cells (TAC) are a subset of basal cell populations within the prostate from which cancers are thought to originate; therefore, we focused on prostate TAC to investigate the molecular mechanisms by which theTAC may be able to evade senescence. Experimental Design: TAC clones were isolated from each zone within the whole prostate and analyzed in flow cytometry. Prostate cancer cells were transfected with junB small interfering RNA (siRNA) and examined by chorioallantoic membrane assay for cancer invasion. Immunohistochemical analysis was done in primary and metastatic prostate cancer specimens. Results: TAC populations showed increased expression of p53, p21, p16, and pRb, resulting in senescence. TAC clones with reduced p16 expression successfully bypassed this phase. We further found close correlation between the levels of junB and p16 expression. Repeated transfection of junB siRNA in prostaticTAC allowed the cells to escape senescence presumably through inactivation of p16/pRb. The chorioallantoic membrane invasion assay showed much lower in invasive cancer cells with high expression of junB; conversely, silencing of junB by transfection with junB siRNA promoted invasion.We also found that metastatic prostate cancers, as well as cancers with high Gleason scores, showed significantly low junB immunopositivity. Conclusions: JunB is an essential upstream regulator of p16 and contributes to maintain cell senescence that blocks malignant transformation of TAC. JunB thus apparently plays an important role in controlling prostate carcinogenesis and may be a new target for cancer prevention and therapy.

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Section: Discussionmentioning

confidence: 99%

Function of JunB in Transient Amplifying Cell Senescence and Progression of Human Prostate Cancer

Konishi¹,

Shimada²,

Nakamura³

et al. 2008

Clinical Cancer Research

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“…p16 INK4a -deficient mice present with increased incidence of spontaneous and carcinogen-induced cancers (Kim and Sharpless, 2006). More recently p16 INK4a was associated with the clonal evolution of epidermal cells such that inactivation of p16 maintained epidermal cells in the stem cell compartment (Maurelli et al, 2006). In extension of these findings, knockout models have unveiled an age-dependent, tissue-specific function of p16 in limiting stem cell renewal (Kim and Sharpless, 2006).…”

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confidence: 99%

Inducible re-expression of p16 in an orthotopic mouse model of pancreatic cancer inhibits lymphangiogenesis and lymphatic metastasis

et al. 2008

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Functional inactivation of the tumour suppressor protein p16 INK4a constitutes a key event in the multistep process of pancreatic ductal cell transformation. However, the significance of p16 inactivation for complex and tissue-specific aspects of pancreatic cancer progression, such as angiogenesis and metastasis, is less understood. Here, we inducibly re-expressed p16 in vivo in an orthotopic model of pancreatic cancer and examined the impact on these clinically relevant aspects of pancreatic cancer tumour biology. Consistent with previous work in subcutaneous xenograft models, we found p16 capable of reducing primary tumour growth. In addition, p16 restitution resulted in a marked reduction of tumour angiogenesis, largely accounted for by a p16-dependent inhibition of lymphangiogenesis. In excellent agreement with the antilymphangiogenic effect, re-expression of p16 almost completely prevented lymph node metastases of MiaPaca-2 pancreatic tumours. To our knowledge, this is the first report that experimentally links the tumour suppressor p16 to the process of lymphangiogenesis.

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“…4,7,11 It is undetectable in holoclones and well-expressed in meroclones and paraclones. 8 Bmi-1 is a component of Polycomb Repressive Complex 1 (PRC1) that regulate the balance of SC dormancy and activation by modifying chromatin and suppressing gene expression.…”

Section: -9 P16mentioning

confidence: 99%

“…8 What is more, inactivation of p16 INK4a in human epidermal SCs is necessary for maintaining their stemness and this process might be regulated by Bmi-1 expression. 7 Bmi-1 modulates p16 INK4a levels and delays clonal conversion even in primary keratinocytes from elderly donors and from young patients suffering from premature aged syndromes. 8 In addition, Cbx4, a PRC1 associated protein, maintains SCs in an undifferentiated state by regulating Polycomb Group (PcG) proteins (Ezh2, Dnmt1 and Bmi-1) and preventing the active SC state.…”

Section: -9 P16mentioning

confidence: 99%

Oncogenic Ras: A double-edged sword for human epidermal stem and transient amplifying cells

Dellambra¹

2016

Small GTPases

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The human epidermal clonal evolution, i.e. the transition from stem cells (SCs) to transient amplifying (TA)-cells and post-mitotic cells, is a continuous and tightly regulated process that ensures physiologic tissue homeostasis. The Ras family of small GTPases has a key role in skin homeostasis and tumorigenesis. Indeed, activating mutations in Ras genes have been found in human cutaneous squamous cell carcinomas (cSCCs) and in experimentally-induced murine cSCCs. In mouse models, the Ras signaling might lead to hyperproliferative phenotypes, including the development of cSCCs, depending on the nature of the founding cells. Tumor-initiating cells or Cancer Stem Cells (CSCs) have been demonstrated in murine and human cSCCs even if the mechanism of their development from normal SCs or TA-cells is not completely elucidated. Here, the relation between the Ras expression outcome and the clonogenic potential of the target keratinocyte is discussed.

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Inactivation of p16^INK4a(inhibitor of cyclin‐dependent kinase 4A) immortalizes primary human keratinocytes by maintaining cells in the stem cell compartment

Cited by 46 publications

References 65 publications

Function of JunB in Transient Amplifying Cell Senescence and Progression of Human Prostate Cancer

Function of JunB in Transient Amplifying Cell Senescence and Progression of Human Prostate Cancer

Inducible re-expression of p16 in an orthotopic mouse model of pancreatic cancer inhibits lymphangiogenesis and lymphatic metastasis

Oncogenic Ras: A double-edged sword for human epidermal stem and transient amplifying cells

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Inactivation of p16INK4a(inhibitor of cyclin‐dependent kinase 4A) immortalizes primary human keratinocytes by maintaining cells in the stem cell compartment

Cited by 46 publications

References 65 publications

Function of JunB in Transient Amplifying Cell Senescence and Progression of Human Prostate Cancer

Function of JunB in Transient Amplifying Cell Senescence and Progression of Human Prostate Cancer

Inducible re-expression of p16 in an orthotopic mouse model of pancreatic cancer inhibits lymphangiogenesis and lymphatic metastasis

Oncogenic Ras: A double-edged sword for human epidermal stem and transient amplifying cells

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Inactivation of p16^INK4a(inhibitor of cyclin‐dependent kinase 4A) immortalizes primary human keratinocytes by maintaining cells in the stem cell compartment