Publications by authors named "V Ruppert"

Article Synopsis
  • A study examined the HDL proteome of 16 patients experiencing post-COVID-19 symptoms, including those with post-acute sequelae (PCS) and post-vaccination syndrome (PVS), who were treated with statins and ARBs for 6 weeks.
  • Results showed that patients with PCS and PVS had no significant differences in their HDL proteins compared to each other, but both groups exhibited significant alterations in proteins related to metabolism and cell structure when compared to healthy controls.
  • Treatment with statins and ARBs improved clinical symptoms and led to changes in the HDL proteome that reduced inflammation in human endothelial cells, indicating that HDL analysis could reveal insights into the disease mechanisms of post-COVID-19 conditions.
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Background: The role of gut microbiota in human health has been intensively studied and more recently shifted from emphasis on composition towards function. Function is partly mediated through formed metabolites. Short-chain fatty acids (SCFAs) such as acetate, propionate, and butyrate as well as their branched analogues represent major products from gut fermentation of dietary fibre and proteins, respectively.

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Aims: The conditions of hypoxia are suggested to induce permanent atrial fibrillation (AF). The regulation of COX4I2 and COX4I1 depends on oxygen availability in tissues. A role of COX4I2 in the myocardium of AF patients is supposed for pathogenesis of AF and subsequent alterations in the electron transfer chain (ETC) under hypoxia.

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Next-generation sequencing has revolutionized the field of microbiology research and greatly expanded our knowledge of complex bacterial communities. Nanopore sequencing provides distinct advantages, combining cost-effectiveness, ease of use, high throughput, and high taxonomic resolution through its ability to process long amplicons, such as the entire 16s rRNA genome. We examine the performance of the conventional 27F primer (27F-I) included in the 16S Barcoding Kit distributed by Oxford Nanopore Technologies (ONT) and that of a more degenerate 27F primer (27F-II) in the context of highly complex bacterial communities in 73 human fecal samples.

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Familial hypercholesterolemia (FH) is an autosomal dominant lipid metabolism disorder characterized by severely elevated plasma low-density lipoprotein cholesterol levels. The disease is caused by mutations in 3 genes (, and ) while over 90% of the mutations are located within the gene. Thus, genetic analysis of the gene is the first step in the genetic diagnosis of FH.

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