1,955 results match your criteria: "Max-Planck Institute of Molecular Cell Biology and Genetics[Affiliation]"

Phenotypic characterization of liver tissue heterogeneity through a next-generation 3D single-cell atlas.

Sci Rep

February 2024

Department of Cell Biology, Faculty of Biological Sciences, Universidad de Concepción, Concepción, Chile.

Three-dimensional (3D) geometrical models are potent tools for quantifying complex tissue features and exploring structure-function relationships. However, these models are generally incomplete due to experimental limitations in acquiring multiple (> 4) fluorescent channels in thick tissue sections simultaneously. Indeed, predictive geometrical and functional models of the liver have been restricted to few tissue and cellular components, excluding important cellular populations such as hepatic stellate cells (HSCs) and Kupffer cells (KCs).

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Statistical integration of multi-omics and drug screening data from cell lines.

PLoS Comput Biol

January 2024

Dept. Data science & Biostatistics, UMC Utrecht, Utrecht, Netherlands.

Data integration methods are used to obtain a unified summary of multiple datasets. For multi-modal data, we propose a computational workflow to jointly analyze datasets from cell lines. The workflow comprises a novel probabilistic data integration method, named POPLS-DA, for multi-omics data.

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Article Synopsis
  • Recovery from the dauer state in C. elegans is crucial for understanding how metabolic changes influence developmental flexibility.
  • Cholesterol is stored in the gut during the dauer phase and is later released into intestinal cells through endocytosis, promoting various metabolic processes.
  • This release of cholesterol activates key signaling pathways that drive growth and protein synthesis, highlighting its role as a central factor in transitioning from dormancy to active development.
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We present an instrument-independent benchmark procedure and software (LFQ_bout) for the validation and comparative evaluation of the performance of LC-MS/MS and data processing workflows in bottom-up proteomics. The procedure enables a back-to-back comparison of common and emerging workflows, ., diaPASEF or ScanningSWATH, and evaluates the impact of arbitrary and inadequately documented settings or black-box data processing algorithms.

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Extracellular lipidosomes containing lipid droplets and mitochondria are released during melanoma cell division.

Cell Commun Signal

January 2024

Biotechnology Center (BIOTEC) and Center for Molecular and Cellular Bioengineering, Technische Universität Dresden, Tatzberg 47-49, Dresden, 01307, Germany.

Background: The incidence of melanoma is increasing worldwide. Since metastatic melanoma is highly aggressive, it is important to decipher all the biological aspects of melanoma cells. In this context, we have previously shown that metastatic FEMX-I melanoma cells release small (< 150 nm) extracellular vesicles (EVs) known as exosomes and ectosomes containing the stem (and cancer stem) cell antigenic marker CD133.

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Tissue Organoid Cultures Metabolize Dietary Carcinogens Proficiently and Are Effective Models for DNA Adduct Formation.

Chem Res Toxicol

February 2024

Department of Analytical, Environmental and Forensic Sciences, School of Cancer & Pharmaceutical Sciences, King's College London, London SE1 9NH, U.K.

Human tissue three-dimensional (3D) organoid cultures have the potential to reproduce the physiological properties and cellular architecture of the organs from which they are derived. The ability of organoid cultures derived from human stomach, liver, kidney, and colon to metabolically activate three dietary carcinogens, aflatoxin B (AFB), aristolochic acid I (AAI), and 2-amino-1-methyl-6-phenylimidazo[4,5-]pyridine (PhIP), was investigated. In each case, the response of a target tissue (liver for AFB; kidney for AAI; colon for PhIP) was compared with that of a nontarget tissue (gastric).

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The nucleus is highly organized to facilitate coordinated gene transcription. Measuring the rheological properties of the nucleus and its sub-compartments will be crucial to understand the principles underlying nuclear organization. Here, we show that strongly localized temperature gradients (approaching 1°C/µm) can lead to substantial intra-nuclear chromatin displacements (>1 µm), while nuclear area and lamina shape remain unaffected.

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Energy metabolism supports neuronal function. While it is well established that changes in energy metabolism underpin brain plasticity and function, less is known about how individual neurons modulate their metabolic states to meet varying energy demands. This is because most approaches used to examine metabolism in living organisms lack the resolution to visualize energy metabolism within individual circuits, cells, or subcellular regions.

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Agglomeration: when folded proteins clump together.

Biophys Rev

December 2023

Department of Structural and Molecular Biology, Institut de Biologia Molecular de Barcelona (IBMB-CSIC), Barcelona, Spain.

Protein self-association is a widespread phenomenon that results in the formation of multimeric protein structures with critical roles in cellular processes. Protein self-association can lead to finite protein complexes or open-ended, and potentially, infinite structures. This review explores the concept of protein agglomeration, a process that results from the infinite self-assembly of folded proteins.

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Neocortical neurogenesis in development and evolution-Human-specific features.

J Comp Neurol

February 2024

Neuroscience Center, HiLIFE - Helsinki Institute of Life Science, University of Helsinki, Helsinki, Finland.

In this review, we focus on human-specific features of neocortical neurogenesis in development and evolution. Two distinct topics will be addressed. In the first section, we discuss the expansion of the neocortex during human evolution and concentrate on the human-specific gene ARHGAP11B.

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Artificial Cells: From Basic Assembly to Directed Functionality.

Small Methods

December 2023

MIIT Key Laboratory of Critical Materials Technology for New Energy Conversion and Storage, School of Chemistry and Chemical Engineering, Harbin Institute of Technology, Harbin, 150001, China.

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The escape of DNA from mitochondria into the nuclear genome (nuclear mitochondrial DNA, NUMT) is an ongoing process. Although pervasively observed in eukaryotic genomes, their evolutionary trajectories in a mammal-wide context are poorly understood. The main challenge lies in the orthology assignment of NUMTs across species due to their fast evolution and chromosomal rearrangements over the past 200 million years.

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Article Synopsis
  • Researchers are investigating how morphogenetic movements are coordinated during the development of the wing in pupae, focusing on the mechanical and cellular behaviors involved.
  • Previous studies indicated that wing morphogenesis includes behaviors for stress relaxation and other patterned actions, but this new research shows these active cellular behaviors do not rely on a key signaling pathway called core planar cell polarity (PCP).
  • Experiments demonstrated that while core PCP mutations could alter quick responses to certain disturbances, they do not significantly impact the overall mechanics of tissue shape changes during wing development.
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Protocol for precision editing of endogenous Chlamydomonas reinhardtii genes with CRISPR-Cas.

STAR Protoc

March 2024

Human Technopole, V.le Rita Levi-Montalcini, 1, 20017 Milan, Italy. Electronic address:

CRISPR-Cas genome engineering in the unicellular green algal model Chlamydomonas reinhardtii has until recently suffered from low integration efficiencies despite traditional genetics being well established. Here, we present a protocol for efficient homology-directed knockin mutagenesis in all commonly used strains of Chlamydomonas. We describe steps for scarless integration of fusion tags and sequence modifications of almost all proteins without the need for a preceding mutant line.

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Adherens junctions as molecular regulators of emergent tissue mechanics.

Nat Rev Mol Cell Biol

April 2024

Institute for Molecular Bioscience, The University of Queensland, St. Lucia, Queensland, Australia.

Tissue and organ development during embryogenesis relies on the collective and coordinated action of many cells. Recent studies have revealed that tissue material properties, including transitions between fluid and solid tissue states, are controlled in space and time to shape embryonic structures and regulate cell behaviours. Although the collective cellular flows that sculpt tissues are guided by tissue-level physical changes, these ultimately emerge from cellular-level and subcellular-level molecular mechanisms.

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Temperature can impact every reaction and molecular interaction essential to a cell. For organisms that cannot regulate their own temperature, a major challenge is how to adapt to temperatures that fluctuate unpredictability and on variable timescales. Biomolecular condensation offers a possible mechanism for encoding temperature-responsiveness and robustness into cell biochemistry and organization.

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Transcription factors are among the most attractive therapeutic targets but are considered largely 'undruggable' in part due to the intrinsically disordered nature of their activation domains. Here we show that the aromatic character of the activation domain of the androgen receptor, a therapeutic target for castration-resistant prostate cancer, is key for its activity as transcription factor, allowing it to translocate to the nucleus and partition into transcriptional condensates upon activation by androgens. On the basis of our understanding of the interactions stabilizing such condensates and of the structure that the domain adopts upon condensation, we optimized the structure of a small-molecule inhibitor previously identified by phenotypic screening.

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A local polynomial moment approximation for compartmentalized biochemical systems.

Math Biosci

January 2024

Max Planck Institute of Molecular Cell Biology and Genetics, Pfotenhauerstraße 108, 01307, Dresden, Germany; Center for Systems Biology Dresden, Pfotenhauerstraße 108, 01307, Dresden, Germany; Cluster of Excellence Physics of Life, TU Dresden, Arnoldstraße 18, 01307, Dresden, Germany. Electronic address:

Compartmentalized biochemical reactions are a ubiquitous building block of biological systems. The interplay between chemical and compartmental dynamics can drive rich and complex dynamical behaviors that are difficult to analyze mathematically - especially in the presence of stochasticity. We have recently proposed an effective moment equation approach to study the statistical properties of compartmentalized biochemical systems.

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Intracellular vesicular transport along cytoskeletal filaments ensures targeted cargo delivery. Such transport is rarely unidirectional but rather bidirectional, with frequent directional reversals owing to the simultaneous presence of opposite-polarity motors. So far, it has been unclear whether such complex motility pattern results from the sole mechanical interplay between opposite-polarity motors or requires regulators.

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Axis convergence in C. elegans embryos.

Curr Biol

December 2023

Max Planck Institute of Molecular Cell Biology and Genetics, Pfotenhauerstrase 108, Dresden 01037, Germany; Cluster of Excellence Physics of Life, Technische Universitӓt Dresden, Arnoldstrase 18, Dresden 01307, Germany; Center for Systems Biology Dresden, Pfotenhauerstrase 108, Dresden 01037, Germany. Electronic address:

Embryos develop in a surrounding that guides key aspects of their development. For example, the anteroposterior (AP) body axis is always aligned with the geometric long axis of the surrounding eggshell in fruit flies and worms. The mechanisms that ensure convergence of the AP axis with the long axis of the eggshell remain unresolved.

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Studying the role of molecularly distinct lipid species in cell signaling remains challenging due to a scarcity of methods for performing quantitative lipid biochemistry in living cells. We have recently used lipid uncaging to quantify lipid-protein affinities and rates of lipid trans-bilayer movement and turnover in the diacylglycerol signaling pathway. This approach is based on acquiring live-cell dose-response curves requiring light dose titrations and experimental determination of uncaging photoreaction efficiency.

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