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Heart regenerates after infarction -- first trials with mice
December 12, 2008Up until today scientists assumed that the adult heart is unable to regenerate. Now, researchers and cardiologists from the Max Delbrück Center for Molecular Medicine (MDC) Berlin-Buch and the Charité - Universitätsmedizin Berlin (Germany) have been able to show that this dogma no longer holds true. Dr. Laura Zelarayán and Assistant Professor Dr. Martin W. Bergmann were able to show that the body`s own heart muscle stem cells do generate new tissue and improve the pumping function of the heart considerably in an adult organism, when they suppress the activity of a gene regulator known as beta-catenin in the nucleus of the heart cells. (PNAS, online December 10, 2008, doi: 10.1073/pnas.0808393105)*.
The gene regulator beta-catenin plays an important role in the development of the heart in embyros. Dr. Zelarayán and Dr. Bergmann could now show that beta-catenin is also important for the regeneration of the adult heart. They suppressed this factor in the nucleus of the heart cells in mice.
This way they activated heart precursor cells (stem cells) to turn on the regeneration of heart in adult mice. Four weeks after blocking beta-catenin, the pumping function of the heart of the animals had improved and the mice survived an infarction much better than those animals with a functioning beta-catenin gene. An important contribution to this project has been a transgenic mouse line generated by Professor Walter Birchmeier`s (MDC) laboratory.
Markers identified for Heart Muscle Stem Cells
In addition, the researchers have proven that heart muscle stem cells exist. So far, these cells had not been characterized clearly. They could demonstrate that two markers for heart cells - the structural protein alpha myosin heavy chain and the transcriptionfactor Tbx5 - are also expressed on heart precursor cells. "The evidence of cells with these markers in the adult heart demonstrates that stem cells dating back from heart development survive in niches in the adult heart", Dr. Bergmann explains.
The researchers in Germany collaborated with scientists in the Netherlands and Belgium. For this research, Dr. Bergmann was awarded the Wilhelm P. Wintersteinpreis this summer. The research group of Dr. Bergmann, a guest researcher at the MDC who recently became Deputy of the Department of Cardiology at the Asklepios Clinic St. Georg in Hamburg, belongs to the research group of Professor Rainer Dietz (MDC and Charité).
Helmholtz Association of German Research Centres
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Beta-Catenin: Webster's Timeline History, 1992 - 2007 by Icon Group International (Author) Webster's bibliographic and event-based timelines are comprehensive in scope, covering virtually all topics, geographic locations and people. They do so from a linguistic point of view, and in the case of this book, the focus is on "Beta-Catenin," including when used in literature (e.g. all authors that might have Beta-Catenin in their name). As such, this book represents the largest compilation of timeline events associated with Beta-Catenin when it is used in proper noun form. Webster's timelines cover bibliographic citations, patented inventions, as well as non-conventional and alternative meanings which capture ambiguities in usage. These furthermore cover all parts of speech (possessive, institutional usage, geographic usage) and contexts, including pop culture, the arts, social... |
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$ beta$-Catenin and Ha-ras - Master Regulators of Zonal Gene Expression in Mouse Liver? by Albert Braeuning (Author) | |
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Citrus flavanone naringenin enhances melanogenesis through the activation of Wnt/[beta] -catenin signalling in mouse melanoma cells.(Report): An ... Journal of Phytotherapy & Phytopharmacology by Huang Yu-Chun (Author), Yang Chao-Hsun (Author), Chiou Yi-Ling (Author) | |
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Beta-catenin stabilization extends regulatory T cell survival and induces anergy in non-regulatory T cells. by Yi Ding (Author) In this dissertation I focus on the effect of beta-catenin on the function of regulatory T cells and non-regulatory T cells. beta-catenin is the key mediator of the canonical Wnt pathway, which is evolutionarily conserved and involved in a large variety of developmental process, including cell proliferation and cell fate decisions. Expression of a stable form of beta-catenin on CD4+CD25+ regulatory T cells (Tregs) resulted in a striking enhancement of survival of these cells in vitro. Furthermore, stable beta-catenin-expressing CD4+CD25+ Tregs out competed control Tregs in vivo, and the number of Tregs necessary for protection against inflammatory bowel disease (IBD) could be substantially reduced when stable beta-catenin-expressing CD4+CD25+ Tregs were used instead of control Tregs.... |
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D-DT-dependent regulation of COX-2 expression by beta-catenin and JNK/c-Jun-dependent pathways. by Dan Xin (Author) The small cytokine/growth factor, migration inhibitory factor (MIF) is a central participant in pro-growth and metastatic tumor processes. To date, there is only one other known MIF family member, D-dopachrome tautomerase (D-DT). Despite the increasingly accepted importance of MIF in cancer progression and disease severity, very little work has been done to investigate what the biological function of this MIF family member is. We now report that D-DT regulates COX-2 expression via both stabilized beta-catenin and a JNK/c-Jun-dependent pathway in human adenocarcinoma cells. Additionally, our studies indicate that D-DT depletion by siRNA strongly increases tumor suppressor p53 protein levels and transcriptional activity. Interestingly, MIF depletion by siRNA results in a corresponding... |
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beta-catenin, TCF, and ICAT in T cell development, function, and aging. by Mohammad Zulfiquer Hossain (Author) Both T cell factor (TCF) and beta-catenin play important roles during different stages of T cell development. Most strikingly, deletion of TCF results in a block early in development, which becomes complete with TCF-LEF double deletion. Similarly, T-cell specific deletion of beta-catenin impairs T cell development at the beta-selection checkpoint. However, in addition to working together to drive expression of beta-catenin-TCF target genes, both TCF and beta-catenin have the potential to work independently of each other. To specifically study the role of beta-catenin-TCF interactions during T cell development, function, and aging, we generated transgenic mice that express ICAT, a naturally occurring inhibitor of beta-catenin-TCF interactions, in the T cell lineage. We found that... |
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Critical roles of Wnt/beta-catenin signaling during development of the retinal pigment epithelium. by Peter D Westenskow (Author) The RPE is a polarized pigmented epithelial monolayer that is critical for vision and development of the neural retina. Considering its diverse and required roles, it is surprising how little is known about how it develops. Two transcription factors Mitf and Otx2 have been identified. Both are required for RPE development by activating many RPE terminal differentiation genes. The loss of either factor is catastrophic and induces RPE cells to dedifferentiate and to instead express retina-specific genes in a process termed RPE-to-retina transdifferentiation. Therefore, it is imperative that Mitf and Otx2 expression levels be maintained during development. A few other intrinsic and extrinsic factors have been identified that regulate RPE fate, but only one gene family (Pax genes) has been... |
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Chemical-genetic screening identifies novel protein regulators of Wnt/beta-catenin signaling. by Travis Logan Biechele (Author) Wnt/beta-catenin signaling regulates many aspects of metazoan development and adult homeostasis. Aberrant Wnt signaling has been linked to numerous pathological conditions. A thorough understanding of the Wnt/beta-catenin signal transduction events is crucial to the development of therapies that may be therapeutic in these pathological conditions. In the last few years, high-throughput screening of both chemicals and siRNAs has identified several novel protein regulators of Wnt/beta-catenin signaling. The research outlined in this dissertation describes the construction and characterization of a robust reporter of Wnt/beta-catenin signaling and its application in both high-throughput small molecule and siRNA screens to identify, Bruton's tyrosine kinase (BTK), metabotropic glutamate... |
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Preferential activation of beta-catenin nuclear signaling in atherosclerosis susceptible vasculature and contributions to atherogenic gene expression. by Bradley David Unti Gelfand (Author) Shear stress represents a major contributor to vascular endothelial cell phenotype. The development of atherosclerosis tends to occur in vascular beds associated with low and reversing shear stress (atheroprone). In contrast, vascular beds exposed to relatively high and unidirectional shear stress tend to be resistant to atherosclerosis (atheroprotective). The identification of signaling pathways associated with atherogenic phenotypes presents an opportunity for the therapeutic intervention of a global health problem. To study the effect of regional hemodynamics on endothelial cell biology, a quantitative description of the forces present in the human body is required. Phase-contrast magnetic resonance imaging was used in order to measure shear stress in the carotid bifurcation. A new... |
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Targeting the BCL9/B9L binding interaction with beta-catenin as a potential anticancer strategy. by Steven Akira Kawamoto (Author) Wnt signaling plays a critical role in numerous cellular processes including embryonic development, cell proliferation and tissue homeostasis. The multifunctional protein beta-catenin is the primary mediator of canonical Wnt signaling and acts as a transcriptional activator in this context. Dysregulated Wnt signaling is a hallmark of many human cancers and results in the stabilization and accumulation of beta-catenin, leading to the increased transcription and expression of Wnt target genes. The transcriptional activation function of beta-catenin requires the formation of a nuclear super-complex with protein cofactors including BCL9/B9L, TCF and CBP. It has been demonstrated that binding to these cofactors is essential for transcriptional. Of these critical cofactors, BCL9 and its homolog... |
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