Your search keyword '"Stambolic, Vuk"' showing total 2 results

1. Concerted roles of PTEN and ATM in controlling hematopoietic stem cell fitness and dormancy

Author

Fortin, Jerome, Bassi, Christian, Ramachandran, Parameswaran, Li, Wanda Y., Tian, Ruxiao, Zarrabi, Ida, Hill, Graham, Snow, Bryan E., Haight, Jillian, Tobin, Chantal, Hodgson, Kelsey, Wakeham, Andrew, Stambolic, Vuk, and Mak, Tak W.

Subjects

Genetic aspects, Health aspects, DNA damage -- Health aspects, Tumor suppressor genes -- Health aspects, Hematopoietic stem cells -- Genetic aspects, Stem cell research

Abstract

Introduction Life-long hematopoiesis is required to produce all the blood cell types that maintain vital functions such as immunity, tissue repair, and oxygen transport. Hematopoietic dysregulation can have severe consequences [...], In order to sustain proficient life-long hematopoiesis, hematopoietic stem cells (HSCs) must possess robust mechanisms to preserve their quiescence and genome integrity. DNA-damaging stress can perturb HSC homeostasis by affecting their survival, self-renewal, and differentiation. Ablation of the kinase ataxia telangiectasia mutated (ATM), a master regulator of the DNA damage response, impairs HSC fitness. Paradoxically, we show here that loss of a single allele of Atm enhances HSC functionality in mice. To explain this observation, we explored a possible link between ATM and the tumor suppressor phosphatase and tensin homolog (PTEN), which also regulates HSC function. We generated and analyzed a knockin mouse line ([Pten.sup.S398A/S398A]), in which PTEN cannot be phosphorylated by ATM. Similar to [Atm.sup.+/-], [Pten.sup.S398A/S398A] HSCs have enhanced hematopoietic reconstitution ability, accompanied by resistance to apoptosis induced by genotoxic stress. Single- cell transcriptomic analyses and functional assays revealed that dormant [Pten.sup.S398A/S398A] HSCs aberrantly tolerate elevated mitochondrial activity and the accumulation of reactive oxygen species, which are normally associated with HSC priming for self-renewal or differentiation. Our results unveil a molecular connection between ATM and PTEN, which couples the response to genotoxic stress and dormancy in HSCs.

Published

2021

2. Prkar1a is an osteosarcoma tumor suppressor that defines a molecular subclass in mice

Author

Molyneux, Sam D., Grappa, Marco A. Di, Beristain, Alexander G., McKee, Trevor D., Wai, Daniel H., Paderova, Jana, Kashyap, Meenakshi, Hu, Pingzhao, Maiuri, Tamara, Narala, Swami R., Stambolic, Vuk, Squire, Jeremy, Penninger, Josef, Sanchez, Otto, Triche, Timothy J., Wood, Geoffrey A., Kirschner, Lawrence S., and Khokha, Rama

Subjects

Care and treatment, Development and progression, Research, Methods, Cancer genetics -- Research -- Care and treatment -- Development and progression, Gene therapy -- Methods -- Research, Osteosarcoma -- Development and progression -- Care and treatment -- Research, Molecular genetics -- Research -- Methods, Cancer -- Genetic aspects

Abstract

Introduction Common mutational processes underpin the development of diverse cancers by perturbing key regulatory networks that have evolved to resist the emergence of neoplastic cells in normal tissues. Some human [...], Some cancers have been stratified into subclasses based on their unique involvement of specific signaling pathways. The mapping of human cancer genomes is revealing a vast number of somatic alterations; however, the identification of clinically relevant molecular tumor subclasses and their respective driver genes presents challenges. This information is key to developing more targeted and personalized cancer therapies. Here, we generate a new mouse model of genomically unstable osteosarcoma (OSA) that phenocopies the human disease. Integrative oncogenomics pinpointed cAMP-dependent protein kinase type I, α regulatory subunit (Prkar1a) gene deletions at 11qE1 as a recurrent genetic trait for a molecularly distinct subclass of mouse OSA featuring RANKL overexpression. Using mouse genetics, we established that Prkar1a is a bone tumor suppressor gene capable of directing subclass development and driving RANKL overexpression during OSA tumorigenesis. Finally, we uncovered evidence for a PRKAR1A-low subset of human OSA with distinct clinical behavior. Thus, tumor subclasses develop in mice and can potentially provide information toward the molecular stratification of human cancers.

Published

2010