A dual luciferase assay for evaluation of skin sensitizing potential of medical devices

Mertl, Elisabeth; Riegel, Elisabeth; Glück, Nicole; Ettenberger-Bornberg, Gabriele; Lin, Grace; Auer, Sabrina; Haller, Magdalena; Wlodarczyk, Angelika; Steurer, Christoph; Kirchnawy, Christian; Czerny, Thomas

doi:10.1007/s11033-019-04964-8

Cited by 6 publications

(1 citation statement)

References 49 publications

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“…X8-72 (single clone #1), X8-12H (single clone #2), and X9-12H (single clone #13) were generated by introducing pGVL8 (for X8 cell lines, Fig. 1 a) [ 39 ] or pGVL9 (for X9 cell line, Fig. 1 a) backbones containing either the HSPA1A promoter or 12 × repeated HSE sites [ 40 ] into HEK293 cells with the PiggyBac transposon system [ 41 ].…”

Section: Methodsmentioning

confidence: 99%

Quantitative Comparison of HSF1 Activators

et al. 2022

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The heat shock response (HSR) pathway is a highly conserved rescue mechanism, which protects the cells from harmful insults disturbing the cellular protein homeostasis via expression of chaperones. Furthermore, it was demonstrated to play crucial roles in various diseases like neurodegeneration and cancer. For neurodegenerative diseases, an overexpression of chaperones is a potential therapeutic approach to clear the cells from non-functional protein aggregates. Therefore, activators of the HSR pathway and its master regulator HSF1 are under close observation. There are numerous HSR activators published in the literature using different model systems, experimental designs, and readout assays. The aim of this work was to provide a quantitative comparison of a broad range of published activators using a newly developed HSF responsive dual-luciferase cell line. Contrary to natural target genes, which are regulated by multiple input pathways, the artificial reporter exclusively reacts to HSF activity. In addition, the results were compared to endogenous heat shock protein expression. As a result, great differences in the intensity of pathway activation were observed. In addition, a parallel viability assessment revealed high variability in the specificity of the drugs. Furthermore, the differences seen compared to published data indicate that some activators exhibit tissue-specific differences leading to interesting assumptions about the regulation of HSF1.

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Section: Methodsmentioning

confidence: 99%