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Scientific Fields
Diseases
Organisms
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Technique

Published in Communications biology - 25 Nov 2025

Groen J, Gazi A, Kapishnikov S, Brelot A, Vos M, Enninga J, Pereiro E, Sartori-Rupp A

Link to Pubmed [PMID] – 41291257

Link to DOI – 10.1038/s42003-025-09072-x

Commun Biol 2025 Nov; 8(1): 1677

Cryo-imaging in cellular biology provides the means to visualize the cellular interior at close-to-native conditions. A cornerstone in the field has been cryo-correlative light and electron microscopy (cryo-CLEM), with cryo-visible light fluorescent microscopy (cryo-VLFM) providing the specificity by tagging macromolecules or structures and cryo-electron tomography (cryo-ET) for the structural details at molecular level. The large resolution gap between these techniques, however, is limiting this correlative workflow as cryo-ET targets are often smaller than the resolution limit of cryo-VLFM. Here we introduce cryo-soft X-ray tomography (cryo-SXT) as an intermediate step that can compensate for the partial view caused by the lost cellular material due to FIB-milling and limited resolution of cryo-VLFM by providing invaluable cellular context information in 3D to the cryo-ET dataset within an integrated workflow. This work shows that X-ray and electron imaging are not mutually exclusive, creating opportunities for further correlative imaging strategies.