☆ 4.8 Article

Endophilin-A coordinates priming and fusion of neurosecretory vesicles via intersectin

NATURE COMMUNICATIONS (2020)

Journal

NATURE COMMUNICATIONS

Volume 11, Issue 1, Pages -

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NATURE PUBLISHING GROUP

DOI: 10.1038/s41467-020-14993-8

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Multidisciplinary Sciences

Funding

Schram-Stiftung [T287/25457]
Deutsche Forschungsgemeinschaft (Emmy Noether Young Investigator Award) [MI-1702/1]
SySy fellowship
Lundbeck foundation
ERC [337327]
ZonMW [91111009]
Alzheimer's Associaton [AARG-17498856]
Novo Nordisk Foundation
Independent Research Fund Denmark

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Abstract

Endophilins-A are conserved endocytic adaptors with membrane curvature-sensing and-inducing properties. We show here that, independently of their role in endocytosis, endophilin-A1 and endophilin-A2 regulate exocytosis of neurosecretory vesicles. The number and distribution of neurosecretory vesicles were not changed in chromaffin cells lacking endophilin-A, yet fast capacitance and amperometry measurements revealed reduced exocytosis, smaller vesicle pools and altered fusion kinetics. The levels and distributions of the main exocytic and endocytic factors were unchanged, and slow compensatory endocytosis was not robustly affected. Endophilin-A's role in exocytosis is mediated through its SH3-domain, specifically via a direct interaction with intersectin-1, a coordinator of exocytic and endocytic traffic. Endophilin-A not able to bind intersectin-1, and intersectin-1 not able to bind endophilin-A, resulted in similar exocytic defects in chromaffin cells. Altogether, we report that two endocytic proteins, endophilin-A and intersectin-1, are enriched on neurosecretory vesicles and regulate exocytosis by coordinating neurosecretory vesicle priming and fusion.

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Article Oncology

Taxanes trigger cancer cell killing in vivo by inducing non-canonical T cell cytotoxicity

Claire Vennin, Chiara M. Cattaneo, Leontien Bosch, Serena Vegna, Xuhui Ma, Hugo G. J. Damstra, Moreno Martinovic, Efi Tsouri, Mila Ilic, Leyla Azarang, Jan R. T. van Weering, Emilia Pulver, Amber L. Zeeman, Tim Schelfhorst, Jeroen O. Lohuis, Anne C. Rios, Johanna F. Dekkers, Leila Akkari, Renee Menezes, Rene Medema, Serena R. Baglio, Anna Akhmanova, Sabine C. Linn, Simone Lemeer, Dirk M. Pegtel, Emile E. Voest, Jacco van Rheenen

Summary: Although treatment with taxanes may not always be effective, it carries the risk of side effects like peripheral neuropathy. A study found that taxanes can directly stimulate T cells to selectively kill cancer cells, independent of the T cell receptor. This mechanism involves the release of cytotoxic extracellular vesicles by T cells, inducing apoptosis specifically in tumor cells. These findings were utilized to develop a therapeutic approach using pre-treated T cells, avoiding systemic toxicity.

CANCER CELL (2023)

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Article Neurosciences

A novel role for MLC1 in regulating astrocyte-synapse interactions

Mandy S. J. Kater, Katharina F. Baumgart, Aina Badia-Soteras, Tim S. Heistek, Karen E. Carney, A. Jacob Timmerman, Jan R. T. van Weering, August B. Smit, Marjo S. van der Knaap, Huibert D. Mansvelder, Mark H. G. Verheijen, Rogier Min

Summary: Loss of function of the astrocyte membrane protein MLC1 is the main cause of Megalencephalic Leukoencephalopathy with subcortical Cysts (MLC), a rare white matter disease characterized by disrupted brain ion and water balance. MLC1 has been found to be present in astrocyte processes that closely interact with excitatory synapses, and its loss affects synaptic transmission, structural plasticity, and fear memory. This study uncovers a new role for MLC1 in regulating astrocyte-synapse interactions.

GLIA (2023)

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Article Biochemistry & Molecular Biology

Structurally and Morphologically Distinct Pathological Tau Assemblies Differentially Affect GVB Accumulation

Marta Jorge-Oliva, Jan R. T. van Weering, Wiep Scheper

Summary: Tau aggregation plays a central role in the pathogenesis of tauopathies, but the response of neurons to tau pathology and the mechanisms leading to neurodegeneration are still unclear. This study investigated the accumulation of granulovacuolar degeneration bodies (GVBs), lysosomal structures that respond to tau pathology, in different tau aggregation models in primary neurons. The results showed that the structure and subcellular localization of tau aggregates may be important factors affecting GVB accumulation. The findings provide insights into the relationship between tau pathology and neurodegeneration.

INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES (2023)

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