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Supramolecular arrangements in human amyloid tissues using SAXS

Amyloid diseases are characterized by the accumulation of misfolded protein aggregates in human tissues, pose significant challenges for both diagnosis and treatment. Protein aggregations known as amyloids are linked to several neurodegenerative conditions including Alzheimer's disease, Parkins...

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Published in:Biophysical chemistry 2025-01, Vol.316, p.107349, Article 107349
Main Authors: Ihsan, N.S. Mohd Nor, Abdul Sani, S.F., Looi, L.M., Pathmanathan, Dharini, Cheah, P.L., Chiew, S.F., Chio-Srichan, Sirinart, Soontaranon, Siriwat, Bradley, D.A.
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Language:English
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Summary:Amyloid diseases are characterized by the accumulation of misfolded protein aggregates in human tissues, pose significant challenges for both diagnosis and treatment. Protein aggregations known as amyloids are linked to several neurodegenerative conditions including Alzheimer's disease, Parkinson's disease, and systemic amyloidosis. The key goal of this research is to employ Small-Angle X-ray Scattering (SAXS) to examine the supramolecular structures of amyloid aggregates in human tissues. We present the structural analysis of amyloid using SAXS, which is employed directly to analyze thin tissue samples without damaging the tissues. This technique provides size and shape information of fibrils, which can be used to generate low-resolution 2D models. The present study investigates the structural changes in amyloid fibril axial d-spacing and scattering intensity in different human tissues, including kidney, heart, thyroid, and others, while also accounting for the presence of triglycerides in these tissues. Tissue structural components were examined at momentum transfer values between q = 0.2 nm−1 and 1.5 nm−1. The d-spacing is a critical parameter in SAXS that provides information about the periodic distances between structures within a sample. From the supramolecular SAXS patterns, the axial d-spacing of fibrils in amyloid tissues is prominent and exists within the 3rd to 10th order, compared to that of healthy tissues which do not have notable peak orders. The axial period of fibrils in amyloid tissues is within the scattering vector range 57.40–64.64 nm−1 while in normal tissues the range is between 60.68 and 61.41 nm−1, which is 3.0 nm−1 smaller than amyloid-containing tissues. Differences in d-spacing are often correlate with distinct pathological mechanisms or stages of disease progression. The application of SAXS to investigate amyloid structures in human tissues has enormous potential to further knowledge of amyloid disorders. This work will open the path for novel diagnostic instruments and therapeutic strategies meant to reduce the burden of amyloid-related diseases by offering a thorough structural examination of amyloid aggregates. [Display omitted] •SAXS differentiated amyloid tissues from healthy one with high resolution data•Amyloid tissue showed 3rd to 10th order SAXS peaks, revealing ordered fibril structures absent in normal tissues•SAXS identified axial d-spacing of 61.9 nm-1 in amyloid vs 61.01 nm-1 in healthy tissues, showing structural
ISSN:0301-4622
1873-4200
1873-4200
DOI:10.1016/j.bpc.2024.107349