Issue 39, 2024, Issue in Progress

Soft X-ray spectromicroscopy of human fibroblasts with impaired sialin function

Abstract

Salla disease (SD) is a lysosomal storage disease where free sialic acid (SA) accumulates in lysosomes due to the impaired function of a membrane protein, sialin. Synchrotron radiation-based scanning transmission soft X-ray spectromicroscopy (STXM) was used to analyze both SD patients' fibroblasts and normal human dermal fibroblasts (NHDF) from healthy controls. Both cell lines were also cultured with N-acetyl-D-mannosamine monohydrate (ManNAc) to see if it increased SA concentration in the cells. The STXM technique was chosen to simultaneously observe the morphological and chemical changes in cells. It was observed that free SA did not remain in the lysosomes during the sample processing, leaving empty vacuoles to the fibroblasts. The total cytosol and entire cell spectra, however, showed systematic differences between the SD and NHDF samples, indicating changes in the relative macromolecular concentrations of the cells. The NHDF cell lines contained a higher relative protein concentration compared to the SD cell lines, and the addition of ManNAc increased the relative protein concentration in both cell lines. In this study, two sample preparation methods were compared, resin-embedded thin sections and cells grown directly on sample analysis grids. While the samples grown on the grids exhibited clean, well-resolved spectra not masked by embedding resin, the low penetration depth of soft X-rays hindered the analysis to only the thin region of the microfilaments away from the thick nucleus.

Graphical abstract: Soft X-ray spectromicroscopy of human fibroblasts with impaired sialin function

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Article information

Article type
Paper
Submitted
30 Jul 2024
Accepted
27 Aug 2024
First published
10 Sep 2024
This article is Open Access
Creative Commons BY license

RSC Adv., 2024,14, 28797-28806

Soft X-ray spectromicroscopy of human fibroblasts with impaired sialin function

T. Mansikkala, S. M. Kangas, I. Miinalainen, P. Angervaniva, N. Darin, M. Blomqvist, R. Hinttala, M. Huttula, J. Uusimaa and M. Patanen, RSC Adv., 2024, 14, 28797 DOI: 10.1039/D4RA05520A

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