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Post-correlation on-lamella cryo-CLEM reveals the membrane architecture of lamellar bodies

View ORCID ProfileSteffen Klein, View ORCID ProfileBenedikt H. Wimmer, View ORCID ProfileSophie L. Winter, Androniki Kolovou, View ORCID ProfileVibor Laketa, View ORCID ProfilePetr Chlanda
doi: https://doi.org/10.1101/2020.02.27.966739
Steffen Klein
1Membrane Biology of Viral Infection Group, Center for Integrative Infectious Diseases, University Hospital Heidelberg
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Benedikt H. Wimmer
1Membrane Biology of Viral Infection Group, Center for Integrative Infectious Diseases, University Hospital Heidelberg
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Sophie L. Winter
1Membrane Biology of Viral Infection Group, Center for Integrative Infectious Diseases, University Hospital Heidelberg
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Androniki Kolovou
1Membrane Biology of Viral Infection Group, Center for Integrative Infectious Diseases, University Hospital Heidelberg
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Vibor Laketa
2Infectious Diseases Imaging Platform (IDIP), Center for Integrative Infectious Diseases, University Hospital Heidelberg
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Petr Chlanda
1Membrane Biology of Viral Infection Group, Center for Integrative Infectious Diseases, University Hospital Heidelberg
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  • For correspondence: petr.chlanda@bioquant.uni-heidelberg.de
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Abstract

Lamellar bodies (LBs) are surfactant-rich organelles in alveolar cells. LBs disassemble into a lipid-protein network that reduces surface tension and facilitates gas exchange in the alveolar cavity. Current knowledge of LB architecture is predominantly based on electron microscopy studies using disruptive sample preparation methods. We established and validated a post-correlation on-lamella cryo-correlative light and electron microscopy approach for cryo-FIB milled cells to structurally characterize and validate the identity of LBs in their unperturbed state. Using deconvolution and 3D image registration, we were able to identify fluorescently labeled membrane structures analyzed by cryo-electron tomography. In situ cryo-electron tomography of A549 cells as well as primary Human Small Airway Epithelial Cells revealed that LBs are composed of membrane sheets frequently attached to the limiting membrane through “T”-junctions. We report a so far undescribed outer membrane dome protein complex (OMDP) on the limiting membrane of LBs. Our data suggest that LB biogenesis is driven by parallel membrane sheet import and by the curvature of the limiting membrane to maximize lipid storage capacity.

Competing Interest Statement

The authors have declared no competing interest.

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Posted August 14, 2020.
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Post-correlation on-lamella cryo-CLEM reveals the membrane architecture of lamellar bodies
Steffen Klein, Benedikt H. Wimmer, Sophie L. Winter, Androniki Kolovou, Vibor Laketa, Petr Chlanda
bioRxiv 2020.02.27.966739; doi: https://doi.org/10.1101/2020.02.27.966739
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Post-correlation on-lamella cryo-CLEM reveals the membrane architecture of lamellar bodies
Steffen Klein, Benedikt H. Wimmer, Sophie L. Winter, Androniki Kolovou, Vibor Laketa, Petr Chlanda
bioRxiv 2020.02.27.966739; doi: https://doi.org/10.1101/2020.02.27.966739

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