2–5 Mar 2026
FIAS / OSZ
Europe/Zurich timezone

Biomolecular condensate architecture of an autophagic cargo at molecular resolution in situ

3 Mar 2026, 14:45
45m
Lecture Hall (FIAS / OSZ)

Lecture Hall

FIAS / OSZ

Campus Riedberg Ruth-Moufang-Str. 1 60438 Frankfurt am Main

Speaker

Dr Florian Wilfing (Max Planck Institute of Biophysics)

Description

Biomolecular condensates organise cellular biochemistry, yet their molecular architecture in situ remains poorly understood. During selective autophagy, macromolecules frequently accumulate into biomolecular condensates, forming discrete entities for autophagic engulfment and degradation – ideal systems for structural analysis. We employed in situ cryo-electron tomography to determine the near-atomic resolution structure of Aminopeptidase 1 condensates within cells. These condensates form densely packed, spherical assemblies with amorphous organisation and liquid-like properties, elucidating the requirements of a selective autophagic cargo for exclusive targeting. Structural analysis and multiscale simulations reveal that the short, transient α-helical structures in the disordered N-terminus of Aminopeptidase 1 enable site-specific, coiled-coil-like interactions required for condensate formation and properties. A single point mutation that increases α-helical propensity directly modulates condensate viscosity and dynamics from a liquid-like to a glass-like state, while preserving local molecular packing. Our results demonstrate that disordered regions encode both specificity and material properties through transiently structured motifs, linking sequence specificity to phase behaviour in cells and expanding the molecular logic of phase separation in cells.

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