32 research outputs found

    Molecular Effects of Doxycycline Treatment on Pterygium as Revealed by Massive Transcriptome Sequencing

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    Pterygium is a lesion of the eye surface which involves cell proliferation, migration, angiogenesis, fibrosis, and extracellular matrix remodelling. Surgery is the only approved method to treat this disorder, but high recurrence rates are common. Recently, it has been shown in a mouse model that treatment with doxycycline resulted in reduction of the pterygium lesions. Here we study the mechanism(s) of action by which doxycycline achieves these results, using massive sequencing techniques. Surgically removed pterygia from 10 consecutive patients were set in short term culture and exposed to 0 (control), 50, 200, and 500 µg/ml doxycycline for 24 h, their mRNA was purified, reverse transcribed and sequenced through Illumina’s massive sequencing protocols. Acquired data were subjected to quantile normalization and analyzed using cytoscape plugin software to explore the pathways involved. False discovery rate (FDR) methods were used to identify 332 genes which modified their expression in a dose-dependent manner upon exposure to doxycycline. The more represented cellular pathways included all mitochondrial genes, the endoplasmic reticulum stress response, integrins and extracellular matrix components, and growth factors. A high correlation was obtained when comparing ultrasequencing data with qRT-PCR and ELISA results

    Processing of nanostructured polymers and advanced polymeric based nanocomposites

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    A digoxin derivative that potently reduces intraocular pressure : efficacy and mechanism of action in different animal models

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    202404 bcchVersion of RecordOthersThis work was funded by research grants from the YEDA corporation, and a donation from 788 Les.E and Cyndy Lederer, at the Weizmann Institute of Science (SJDK); Health and Medical 789 Research Fund (20212781), Region government (CWD). InnoHK initiative and the Hong Kong 790 Special Administrative Region Government (CWD), 1-CD65 (CWD).PublishedC
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