Two-hit model for progression of medulloblastoma preneoplasia in Patched heterozygous mice

Pazzaglia, Simonetta; Tanori, Mirella; Mancuso, Mariateresa; Gessi, Marco; Pasquali, Emanuela; Leonardi, Simona; Oliva, Maria Antonietta; Rebessi, Simonetta; Majo, V. Di; Covelli, Vincenzo; Giangaspero, Felice; Saran, Anna

doi:10.1038/sj.onc.1209544

Cited by 65 publications

(74 citation statements)

References 30 publications

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“…6A). Regardless of radiation dose, we found a marked heterogeneity of LOH patterns in MBs developed after embryonic irradiation (E13.5 and E16.5) compared to tumors developed in mice irradiated as newborns (typically showing large chr13 interstitial deletions [31]). In mice irradiated at E13.5 only 43% (3/7) of the tumors showed typical interstitial deletions, while 28% (2/7) displayed large terminal losses and 28% (2/7) showed loss of the whole chr13.…”

Section: Ptc1 Loss Of Heterozygosity Patterns In Mbmentioning

confidence: 86%

Developmental and oncogenic radiation effects on neural stem cells and their differentiating progeny in mouse cerebellum

et al. 2013

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Neural stem cells are highly susceptible to radiogenic DNA damage, however, little is known about their mechanisms of DNA damage response (DDR) and the long-term consequences of genotoxic exposure. Patched1 heterozygous mice (Ptc1 1/2 ) provide a powerful model of medulloblastoma (MB), a frequent pediatric tumor of the cerebellum. Irradiation of newborn Ptc1 1/2 mice dramatically increases the frequency and shortens the latency of MB. In this model, we investigated the mechanisms through which multipotent neural progenitors (NSCs) and faterestricted progenitor cells (PCs) of the cerebellum respond to DNA damage induced by radiation, and the long-term developmental and oncogenic consequences. These responses were assessed in mice exposed to low (0.25 Gy) or high (3 Gy) radiation doses at embryonic day 13.5 (E13.5), when NSCs giving rise to the cerebellum are specified but the external granule layer (EGL) has not yet formed, or at E16.5, during the expansion of granule PCs to form the EGL. We found crucial differences in DDR and apoptosis between NSCs and fate-restricted PCs, including lack of p21 expression in NSCs. NSCs also appear to be resistant to oncogenesis from low-dose radiation exposure but more vulnerable at higher doses. In addition, the pathway to DNA repair and the pattern of oncogenic alterations were strongly dependent on age at exposure, highlighting a differentiation-stage specificity of DNA repair pathways in NSCs and PCs. These findings shed light on the mechanisms used by NSCs and PCs to maintain genome integrity during neurogenesis and may have important implications for radiation risk assessment and for development of targeted therapies against brain tumors.

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Section: Ptc1 Loss Of Heterozygosity Patterns In Mbmentioning

confidence: 86%

Developmental and oncogenic radiation effects on neural stem cells and their differentiating progeny in mouse cerebellum

et al. 2013

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“…A slower repair kinetics may contribute to a residual low level of unrepaired DSBs, providing opportunity for loss of heterozygosity of critical genetic regions. Ptch1 loss of heterozygosity is indeed a crucial event for Ptch1-associated tumorigenesis in cerebellum (Pazzaglia et al, 2006).…”

Section: Ependymal Channelmentioning

confidence: 99%

Role of connexin43 and ATP in long-range bystander radiation damage and oncogenesis in vivo

et al. 2011

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Ionizing radiation is a genotoxic agent and human carcinogen. Recent work has questioned long-held dogmas by showing that cancer-associated genetic alterations occur in cells and tissues not directly exposed to radiation, questioning the robustness of the current system of radiation risk assessment. In vitro, diverse mechanisms involving secreted soluble factors, gap junction intercellular communication (GJIC) and oxidative metabolism are proposed to mediate these indirect effects. In vivo, the mechanisms behind long-range 'bystander' responses remain largely unknown. Here, we investigate the role of GJIC in propagating radiation stress signals in vivo, and in mediating radiation-associated bystander tumorigenesis in mouse central nervous system using a mouse model in which intercellular communication is downregulated by targeted deletion of the connexin43 (Cx43) gene. We show that GJIC is critical for transmission of oncogenic radiation damage to the non-targeted cerebellum, and that a mechanism involving adenosine triphosphate release and upregulation of Cx43, the major GJIC constituent, regulates transduction of oncogenic damage to unirradiated tissues in vivo. Our data provide a novel hypothesis for transduction of distant bystander effects and suggest that the highly branched nervous system, similar to the vascular network, has an important role.

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“…PTCH is a Sonic Hedgehog (SHH) receptor and negative regulator of the pathway causing predisposition to childhood medulloblastoma (43). Ptch1 +/-mutant mice develop cerebellar tumours resembling human medulloblastoma which is accelerated when irradiated as neonates (44). Partial body irradiation of neonatal Ptch1 +/-mice was shown to significantly increase the occurrence of medulloblastoma compared to control animals, accompanied with increased DNA damage and apoptosis in the cerebellum.…”

Section: New Experimental Approaches For Studying Ribesmentioning

confidence: 99%

Bystander Signalling: Exploring Clinical Relevance Through New Approaches and New Models

Butterworth¹,

McMahon²,

Hounsell³

et al. 2013

Clinical Oncology

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Classical radiation biology research has centred on nuclear DNA as the main target of radiation induced damage. Over the past two decades, this has been challenged by a significant amount of scientific evidence clearly demonstrating radiation induced cell signalling effects to have important roles in mediating overall radiobiological response. These effects, generally termed radiation induced bystander effects (RIBEs) have challenged the traditional DNA targeted theory in radiation biology Key wordsbystander effect, in vivo, ionising radiation, microbeam SearchesArticles cited in this manuscript were sourced through a literature search on the Medline/Pubmed database using the search terms 'radiation', bystander' 'in vivo' and 'microbeam'. Full articles were retrieved when the abstract was deemed relevant. The bibliographies of retrieved papers were also searched and relevant articles included.

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Two-hit model for progression of medulloblastoma preneoplasia in Patched heterozygous mice

Cited by 65 publications

References 30 publications

Developmental and oncogenic radiation effects on neural stem cells and their differentiating progeny in mouse cerebellum

Developmental and oncogenic radiation effects on neural stem cells and their differentiating progeny in mouse cerebellum

Role of connexin43 and ATP in long-range bystander radiation damage and oncogenesis in vivo

Bystander Signalling: Exploring Clinical Relevance Through New Approaches and New Models

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