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  4. Isotropic multi-scale neuronal reconstruction from high-ratio expansion microscopy with contrastive unsupervised deep generative models
 
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Isotropic multi-scale neuronal reconstruction from high-ratio expansion microscopy with contrastive unsupervised deep generative models

Journal
Computer Methods and Programs in Biomedicine
Journal Volume
244
Date Issued
2024-02-01
Author(s)
GARY HAN CHANG  
Wu, Meng Yun
Yen, Ling Hui
Huang, Da Yu
Lin, Ya Hui
Luo, Yi Ru
Liu, Ya Ding
Xu, Bin
Leong, Kam W.
WEN-SUNG LAI  
Chiang, Ann Shyn
KUO-CHUAN WANG  
Wang, Shih Luen
Chu, Li An
CHIN-HSIEN LIN  
DOI
10.1016/j.cmpb.2023.107991
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/639755
URL
https://api.elsevier.com/content/abstract/scopus_id/85182450456
Abstract
Background and objective: Current methods for imaging reconstruction from high-ratio expansion microscopy (ExM) data are limited by anisotropic optical resolution and the requirement for extensive manual annotation, creating a significant bottleneck in the analysis of complex neuronal structures.

Methods: We devised an innovative approach called the IsoGAN model, which utilizes a contrastive unsupervised generative adversarial network to sidestep these constraints. This model leverages multi-scale and isotropic neuron/protein/blood vessel morphology data to generate high-fidelity 3D representations of these structures, eliminating the need for rigorous manual annotation and supervision. The IsoGAN model introduces simplified structures with idealized morphologies as shape priors to ensure high consistency in the generated neuronal profiles across all points in space and scalability for arbitrarily large volumes.

Results: The efficacy of the IsoGAN model in accurately reconstructing complex neuronal structures was quantitatively assessed by examining the consistency between the axial and lateral views and identifying a reduction in erroneous imaging artifacts. The IsoGAN model accurately reconstructed complex neuronal structures, as evidenced by the consistency between the axial and lateral views and a reduction in erroneous imaging artifacts, and can be further applied to various biological samples.

Conclusion: With its ability to generate detailed 3D neurons/proteins/blood vessel structures using significantly fewer axial view images, IsoGAN can streamline the process of imaging reconstruction while maintaining the necessary detail, offering a transformative solution to the existing limitations in high-throughput morphology analysis across different structures.
Subjects
Biomedical imaging
Deep learning
Expansion microscopy
Publisher
Elsevier Ireland Ltd
Type
journal article

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