Publications by authors named "Benjamin Podbilewicz"

Neurons display unique shapes and establish intricate networks, which may differ between sexes. In complex organisms, studying sex differences in structure and function of individual neurons is difficult. The nematode hermaphrodites and males present an exceptional model for studying neuronal morphogenesis in a simple, sexually dimorphic system.

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Dendrites are crucial for receiving information into neurons. Sensory experience affects the structure of these tree-like neurites, which, it is assumed, modifies neuronal function, yet the evidence is scarce, and the mechanisms are unknown. To study whether sensory experience affects dendritic morphology, we use the ' arborized nociceptor PVD neurons, under natural mechanical stimulation induced by physical contacts between individuals.

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Article Synopsis
  • The text introduces a protocol for using Neuronalyzer software to automatically reconstruct branched neuronal structures from noisy microscopy images.
  • It outlines steps including loading images, denoising, segmenting, tracing, and extracting features like branch curvature and junction angles.
  • The software is capable of batch processing and allows for statistical comparisons, making it versatile and effective in handling variations across different datasets.
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  • The interaction between IZUMO1 on sperm and JUNO on oocytes is essential for gamete fusion.
  • Ectopic expression of IZUMO1 can induce fusion between sperm and fibroblasts or epithelial cells that express JUNO, leading to the formation of syncytia, similar to the process seen in some animal viruses.
  • This sperm-induced fusion depends on having the correct JUNO type, can be inhibited by an IZUMO1 antibody, and provides a quick method for assessing sperm functionality in male infertility diagnosis.
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Article Synopsis
  • * Significant structural changes in cells led to the development of eukaryotic cells featuring internal membrane compartments.
  • * Key stages in eukaryotic evolution include the internalization of symbiotic partners and the emergence of sexual reproduction linked to a polyploid ancestor from cell-cell fusion.
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Entry of enveloped viruses into cells is mediated by viral fusogenic proteins that drive membrane rearrangements needed for fusion between viral and target membranes. Skeletal muscle development also requires membrane fusion events between progenitor cells to form multinucleated myofibers. Myomaker and Myomerger are muscle-specific cell fusogens but do not structurally or functionally resemble classical viral fusogens.

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Entry of enveloped viruses into cells is mediated by fusogenic proteins that form a complex between membranes to drive rearrangements needed for fusion. Skeletal muscle development also requires membrane fusion events between progenitor cells to form multinucleated myofibers. Myomaker and Myomerger are muscle-specific cell fusogens, but do not structurally or functionally resemble classical viral fusogens.

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Mammalian sperm-egg adhesion depends on the trans-interaction between the sperm-specific type I glycoprotein IZUMO1 and its oocyte-specific GPI-anchored receptor JUNO. However, the mechanisms and proteins (fusogens) that mediate the following step of gamete fusion remain unknown. Using live imaging and content mixing assays in a heterologous system and structure-guided mutagenesis, we unveil an unexpected function for IZUMO1 in cell-to-cell fusion.

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Cell fusion of female and male gametes is the climax of sexual reproduction. In many organisms, the Hapless 2 (HAP2) family of proteins play a critical role in gamete fusion. We find that Plasmodium falciparum, the causative agent of human malaria, expresses two HAP2 proteins: PfHAP2 and PfHAP2p.

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Article Synopsis
  • - Sexual reproduction in organisms involves meiosis for genome reduction and gamete fusion, with DNA repair mechanisms leading to meiotic recombination, but prokaryotes lack known fusogenic proteins like those used in eukaryotes.
  • - Researchers identified archaeal proteins homologous to eukaryotic fusexins, which are crucial for cell fusion, and studied the crystal structure of Fusexin1 showing a unique six-helix bundle design.
  • - Fusexin1 can facilitate the fusion of mammalian cells and is linked to genes in mobile elements, indicating potential roles in archaeal cell fusion and evolution of fusexin proteins.
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Successful gamete fusion requires species-specific membrane adhesion. However, the interaction of adhesion molecules in gametes is difficult to study in real time through low-throughput microscopic observation. Therefore, we developed a live imaging-based adhesion molecule (LIAM) assay to study gamete adhesion molecule interactions in cultured cells.

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Gamete fusion is the climax of fertilization in all sexually reproductive organisms, from unicellular fungi to humans. Similarly to other cell-cell fusion events, gamete fusion is mediated by specialized proteins, named fusogens, that overcome the energetic barriers during this process. In recent years, HAPLESS 2/GENERATIVE CELL-SPECIFIC 1 (HAP2/GCS1) was identified as the fusogen mediating sperm-egg fusion in flowering plants and protists, being both essential and sufficient for the membrane merger in some species.

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Complex dendritic trees are a distinctive feature of neurons. Alterations to dendritic morphology are associated with developmental, behavioral and neurodegenerative changes. The highly-arborized PVD neuron of C.

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During multicellular organism development, complex structures are sculpted to form organs and tissues, which are maintained throughout adulthood. Many of these processes require cells to fuse with one another, or with themselves. These plasma membrane fusions merge endoplasmic cellular content across external, exoplasmic, space.

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The structural and functional properties of neurons have intrigued scientists since the pioneering work of Santiago Ramón y Cajal. Since then, emerging cutting-edge technologies, including light and electron microscopy, electrophysiology, biochemistry, optogenetics, and molecular biology, have dramatically increased our understanding of dendritic properties. This advancement was also facilitated by the establishment of different animal model organisms, from flies to mammals.

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Cell-cell fusion remains the least understood type of membrane fusion process. However, the last few years have brought about major advances in understanding fusion between gametes, myoblasts, macrophages, trophoblasts, epithelial, cancer, and other cells in normal development and in diseases. While different cell fusion processes appear to proceed via similar membrane rearrangements, proteins that have been identified as necessary and sufficient for cell fusion (fusogens) use diverse mechanisms.

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Segev et al. introduce fusogens - the proteins that coordinate, execute and control membrane fusion - and discuss their various physiological functions.

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Cell-cell fusion is essential for fertilization and organ development. Dedicated proteins known as fusogens are responsible for mediating membrane fusion. However, until recently, these proteins either remained unidentified or were poorly understood at the mechanistic level.

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The aging brain undergoes structural changes that affect brain homeostasis, neuronal function and consequently cognition. The complex architecture of dendritic arbors poses a challenge to understanding age-dependent morphological alterations, behavioral plasticity and remodeling following brain injury. Here, we use the PVD polymodal neurons of as a model to study how aging affects neuronal plasticity.

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Injury triggers regeneration of axons and dendrites. Research has identified factors required for axonal regeneration outside the CNS, but little is known about regeneration triggered by dendrotomy. Here, we study neuronal plasticity triggered by dendrotomy and determine the fate of complex PVD arbors following laser surgery of dendrites.

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Cell-cell fusion is inherent to sexual reproduction. Loss of HAPLESS 2/GENERATIVE CELL SPECIFIC 1 (HAP2/GCS1) proteins results in gamete fusion failure in diverse organisms, but their exact role is unclear. In this study, we show that HAP2/GCS1 is sufficient to promote mammalian cell-cell fusion.

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