Publications by authors named "Ofer Moldavski"

Article Synopsis
  • The sympathetic nervous system (SNS) plays a significant role in regulating bone metabolism, with abundant SNS innervation found in the periosteum and bone marrow, consisting of specific nerve fibers.
  • Using a viral tracing method, researchers have identified 87 specific brain nuclei that send SNS signals to bone, revealing the complexity of this neural connection.
  • Certain brain areas, like the raphe magnus and periaqueductal gray, show higher levels of SNS activity, emphasizing the importance of these sites in understanding bone metabolism and pain regulation.
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Article Synopsis
  • The sympathetic nervous system (SNS) plays a significant role in bone metabolism, with nerves found in the periosteum and bone marrow showing evidence of noradrenergic fibers.
  • Recent research using pseudorabies (PRV) tracing has identified 87 brain nuclei that send efferent SNS signals to bone, highlighting the complexity of this communication.
  • Specific regions, like the raphe magnus and periaqueductal gray, exhibit varying levels of SNS activity, leading to new insights into how these neural pathways could be linked to bone health and pain management.
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  • Seasonal changes in food intake and body fat in animals are influenced by changes in light duration, regulated by melatonin from the pineal gland.
  • The mediobasal hypothalamus plays a key role in integrating these seasonal variations through the detection of the thyroid-stimulating hormone (TSH).
  • Tanycytes in the hypothalamus are involved in regulating energy balance and modulating the blood-hypothalamus barrier, with TSH having potential effects beyond traditional single-target actions.
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Article Synopsis
  • The last ten years have greatly improved our understanding of how bones stay healthy and how diseases can cause bone loss, focusing on genetic mutations and animal models.* -
  • Bone cells interact and influence each other's roles through various signaling systems and developmental pathways, highlighting their integrated function in maintaining bone health.* -
  • The skeleton communicates with other organs, affecting overall metabolism, and recent studies have revealed complex connections involving hormones and immune responses that are vital for bone remodeling and disease treatment.*
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Oxysterols are oxidized derivatives of cholesterol that play regulatory roles in lipid biosynthesis and homeostasis. How oxysterol signaling coordinates different lipid classes such as sterols and triglycerides remains incompletely understood. Here, we show that 4β-hydroxycholesterol (HC) (4β-HC), a liver and serum abundant oxysterol of poorly defined functions, is a potent and selective inducer of the master lipogenic transcription factor, SREBP1c, but not the related steroidogenic transcription factor SREBP2.

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A key step in nutrient sensing is activation of the master growth regulator, mTORC1 kinase, on the lysosomal membrane. Nutrients enable mTORC1 scaffolding by a complex composed of the Rag GTPases (Rags) and Ragulator, but the underlying mechanism of mTORC1 capture is poorly understood. Combining dynamic imaging in cells and reconstituted systems, we uncover an affinity switch that controls mTORC1 lifetime and activation at the lysosome.

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Functional heterogeneity within the lipid droplet (LD) pool of a single cell has been observed, yet the underlying mechanisms remain enigmatic. Here, we report on identification of a specialized LD subpopulation characterized by a unique proteome and a defined geographical location at the nucleus-vacuole junction contact site. In search for factors determining identity of these LDs, we screened ∼6,000 yeast mutants for loss of targeting of the subpopulation marker Pdr16 and identified Ldo45 (LD organization protein of 45 kD) as a crucial targeting determinant.

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The mechanistic target of rapamycin complex 1 (mTORC1) protein kinase is a master growth regulator that becomes activated at the lysosome in response to nutrient cues. Here, we identify cholesterol, an essential building block for cellular growth, as a nutrient input that drives mTORC1 recruitment and activation at the lysosomal surface. The lysosomal transmembrane protein, SLC38A9, is required for mTORC1 activation by cholesterol through conserved cholesterol-responsive motifs.

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Exposing cells to folding stress causes a subset of their proteins to misfold and accumulate in inclusion bodies (IBs). IB formation and clearance are both active processes, but little is known about their mechanism. To shed light on this issue, we performed a screen with over 4,000 fluorescently tagged yeast proteins for co-localization with a model misfolded protein that marks IBs during folding stress.

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Living organisms change their proteome dramatically to sustain a stable internal milieu in fluctuating environments. To study the dynamics of proteins during stress, we measured the localization and abundance of the Saccharomyces cerevisiae proteome under various growth conditions and genetic backgrounds using the GFP collection. We created a database (DB) called 'LoQAtE' (Localizaiton and Quantitation Atlas of the yeast proteomE), available online at http://www.

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The division of the S. cerevisiae budding yeast, which produces one mother cell and one daughter cell, is asymmetric with respect to aging. Remarkably, the asymmetry of yeast aging coincides with asymmetric inheritance of damaged and aggregated proteins by the mother cell.

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FtsH is an evolutionary conserved membrane-bound metalloprotease complex. While in most prokaryotes FtsH is encoded by a single gene, multiple FtsH genes are found in eukaryotes. Genetic and biochemical data suggest that the Arabidopsis chloroplast FtsH is a hetero-hexamer.

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