Publications by authors named "D Stroka"

The genome duplication program is affected by multiple factors in vivo, including developmental cues, genotoxic stress, and aging. Here, we monitored DNA replication initiation dynamics in regenerating livers of young and old mice after partial hepatectomy to investigate the impact of aging. In young mice, the origin firing sites were well defined; the majority were located 10-50 kb upstream or downstream of expressed genes, and their position on the genome was conserved in human cells.

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Sepsis causes millions of deaths per year worldwide and is a current global health priority declared by the WHO. Sepsis-related deaths are a result of dysregulated inflammatory immune responses indicating the need to develop strategies to target inflammation. An important mediator of inflammation is extracellular adenosine triphosphate (ATP) that is released by inflamed host cells and tissues, and also by bacteria in a strain-specific and growth-dependent manner.

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Article Synopsis
  • Enhancers play a key role in controlling gene expression specific to certain tissues, and variations within these regions may impact cancer progression and treatment resistance, though the exact ways they do this are not fully understood.
  • Researchers studied an enhancer linked to the DPD gene, which is important for how the body processes the cancer drug 5-FU.
  • They found that a common genetic variant affects how well 5-FU works by influencing the recruitment of a transcription factor and altering the interaction between the enhancer and promoter, providing new insights into drug resistance mechanisms.
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Enhancers are critical for regulating tissue-specific gene expression, and genetic variants within enhancer regions have been suggested to contribute to various cancer-related processes, including therapeutic resistance. However, the precise mechanisms remain elusive. Using a well-defined drug-gene pair, we identified an enhancer region for dihydropyrimidine dehydrogenase (DPD, gene) expression that is relevant to the metabolism of the anti-cancer drug 5-fluorouracil (5-FU).

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Background: The inducible Kras/p53 lung adenocarcinoma mouse model, which faithfully recapitulates human disease, is routinely initiated by the intratracheal instillation of a virus-based Cre recombinase delivery system. Handling virus-based delivery systems requires elevated biosafety levels, e.g.

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