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通过光束传播对生物样本进行逆散射。

Inverse-scattering in biological samples via beam-propagation.

作者信息

Kim Jeongsoo, Bolton Blythe, Moshksayan Khashayar, Khanna Rishika, Swartz Mary E, Ziemczonok Michał, Kamra Mohini, Jorn Karin A, Parekh Sapun H, Kujawińska Małgorzata, Eberhart Johann, Cenik Elif Sarinay, Ben-Yakar Adela, Chowdhury Shwetadwip

出版信息

bioRxiv. 2025 Aug 22:2025.08.17.670744. doi: 10.1101/2025.08.17.670744.

Abstract

Multiple scattering limits optical imaging in thick biological samples by scrambling sample-specific information. Physics-based inverse-scattering methods aim to computationally recover this information, often using non-convex optimization to reconstruct the scatter-corrected sample. However, this non-convexity can lead to inaccurate reconstructions, especially in highly scattering samples. Here, we show that various implementation strategies for even the same inverse-scattering method significantly affect reconstruction quality. We demonstrate this using multi-slice beam propagation (MSBP), a relatively simple nonconvex inverse-scattering method that reconstructs a scattering sample's 3D refractive-index (RI). By systematically conducting MSBP-based inverse-scattering on both phantoms and biological samples, we showed that an amplitude-only cost function in the inverse-solver, combined with angular and defocus diversity in the scattering measurements, enabled high-quality, fully-volumetric RI imaging. This approach achieved subcellular resolution and label-free 3D contrast across diverse, multiple-scattering samples. These results lay the groundwork for robust use of inverse-scattering techniques to achieve biologically interpretable 3D imaging in increasingly thick, multicellular samples, introducing a new paradigm for deep-tissue computational imaging.

摘要

多重散射通过扰乱样本特定信息限制了厚生物样本中的光学成像。基于物理的逆散射方法旨在通过计算恢复此信息,通常使用非凸优化来重建散射校正后的样本。然而,这种非凸性可能导致重建不准确,尤其是在高散射样本中。在这里,我们表明,即使是相同的逆散射方法,各种实现策略也会显著影响重建质量。我们使用多切片光束传播(MSBP)来证明这一点,MSBP是一种相对简单的非凸逆散射方法,用于重建散射样本的三维折射率(RI)。通过在模型和生物样本上系统地进行基于MSBP的逆散射,我们表明,逆求解器中的仅幅度成本函数,与散射测量中的角度和离焦多样性相结合,能够实现高质量的全体积RI成像。这种方法在各种多重散射样本中实现了亚细胞分辨率和无标记的三维对比度。这些结果为在越来越厚的多细胞样本中稳健地使用逆散射技术以实现具有生物学可解释性的三维成像奠定了基础,为深部组织计算成像引入了一种新范式。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0180/12393416/a380a6b8810d/nihpp-2025.08.17.670744v1-f0001.jpg

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