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We are analyzing https://link.springer.com/article/10.1007/s00280-018-3549-0.

Title:
Influence of gemcitabine chemotherapy on the microbiota of pancreatic cancer xenografted mice | Cancer Chemotherapy and Pharmacology
Description:
Background and aims Pancreatic ductal adenocarcinoma (PDAC) represents the fourth cause of cancer-related death. We aimed to evaluate whether gemcitabine treatment shapes the gut microbiota in a model of PDAC xenografted mice. Materials and methods Pancreatic cancer xenograft mice were subjected to gemcitabine injection once per week for 3 weeks to assess the tumor volume as compared to control mice injected with normal saline solution. The composition of fecal microbiota, the activation of NF-kB pathway in cancer tissues and the serum metabolomics were further analyzed. Results Gemcitabine considerably decreases the proportion of Gram- positive Firmicutes (from about 39 to 17%) and the Gram- negative Bacteroidetes (from 38 to 17%) which are the two dominant phyla in the gut of tumor-bearing control mice. This downshift was replaced by an increase of Proteobacteria (Escherichia coli and Aeromonas hydrophila) from 15 up to 32% and Verrucomicrobia (Akkermansia muciniphila) from 5 to 33% in the gut of drug-receiving mice. An overall increase in inflammation-associated bacteria was observed upon gemcitabine. Consistently, activation of the NF-kB canonical pathway was found in cancer tissues from gemcitabine-treated mice. Serum metabolomics revealed a significant decrease of the purine compounds inosine and xanthine, and a decreasing trend for their metabolically-related molecule hypoxanthine. Discussion Understanding chemotherapy side effects may explain the lack of activity or the chemoresistant processes and it may help to set up strategies to improve the effectiveness of therapy.
Website Age:
28 years and 1 months (reg. 1997-05-29).

Matching Content Categories {📚}

  • Education
  • Health & Fitness
  • Science

Content Management System {📝}

What CMS is link.springer.com built with?

Custom-built

No common CMS systems were detected on Link.springer.com, and no known web development framework was identified.

Traffic Estimate {📈}

What is the average monthly size of link.springer.com audience?

🌠 Phenomenal Traffic: 5M - 10M visitors per month


Based on our best estimate, this website will receive around 5,000,016 visitors per month in the current month.

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How Does Link.springer.com Make Money? {💸}

We find it hard to spot revenue streams.

Many websites are intended to earn money, but some serve to share ideas or build connections. Websites exist for all kinds of purposes. This might be one of them. Link.springer.com might be earning cash quietly, but we haven't detected the monetization method.

Keywords {🔍}

pubmed, article, google, scholar, cas, cancer, central, pancreatic, microbiota, gut, chemotherapy, adamberg, intestinal, butyrate, gemcitabine, mice, inflammation, microbiome, human, research, treatment, access, role, panebianco, pazienza, gastroenterol, clin, pharmacol, author, privacy, cookies, content, data, kaarel, jaagura, model, review, med, disease, health, gastrointestinal, cells, inflammatory, tallinn, publish, search, vilu, valerio, adenocarcinoma, tumor,

Topics {✒️}

month download article/chapter contributed reagents/materials/analysis tools 5-fluorouracil-induced gastrointestinal mucositis reg deficiency-induced autoimmunity metabolically-related molecule hypoxanthine chemotherapy-induced gastrointestinal toxicity integrative view valerio pazienza tumor-bearing control mice gram-negative spore formers male sprague–dawley rats nf-kb canonical pathway article cancer chemotherapy full article pdf pancreatic cancer cells intestinal microbiota dysbiosis gemcitabine-treated mice chemotherapy-induced mucositis cancer-related death author correspondence privacy choices/manage cookies pancreatic cancer treated advanced pancreatic cancer van laethem jl pdac xenografted mice pancreatic ductal adenocarcinoma gemcitabine treatment shapes endotoxin-induced shock laboratory animal care drug-receiving mice institutional animal care article panebianco metastatic pancreatic adenocarcinoma institutional research funding control mice injected kaarel adamberg nf-kb pathway related subjects lactobacillus reuteri inhibits anti-inflammatory effects advanced pancreatic carcinoma chronic gastrointestinal disease cancer prev res gram- negative bacteroidetes gram-negative microbiome check access instant access inflammatory bowel disease european economic area microbial community imbalances

Questions {❓}

  • Bien J, Palagani V, Bozko P (2013) The intestinal microbiota dysbiosis and Clostridium difficile infection: is there a relationship with inflammatory bowel disease?
  • Nguyen TL, Vieira-Silva S, Liston A, Raes J (2015) How informative is the mouse for human gut microbiota research?
  • Scheppach W, Weiler F (2004) The butyrate story: old wine in new bottles?

Schema {🗺️}

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         description:Pancreatic ductal adenocarcinoma (PDAC) represents the fourth cause of cancer-related death. We aimed to evaluate whether gemcitabine treatment shapes the gut microbiota in a model of PDAC xenografted mice. Pancreatic cancer xenograft mice were subjected to gemcitabine injection once per week for 3 weeks to assess the tumor volume as compared to control mice injected with normal saline solution. The composition of fecal microbiota, the activation of NF-kB pathway in cancer tissues and the serum metabolomics were further analyzed. Gemcitabine considerably decreases the proportion of Gram- positive Firmicutes (from about 39 to 17%) and the Gram- negative Bacteroidetes (from 38 to 17%) which are the two dominant phyla in the gut of tumor-bearing control mice. This downshift was replaced by an increase of Proteobacteria (Escherichia coli and Aeromonas hydrophila) from 15 up to 32% and Verrucomicrobia (Akkermansia muciniphila) from 5 to 33% in the gut of drug-receiving mice. An overall increase in inflammation-associated bacteria was observed upon gemcitabine. Consistently, activation of the NF-kB canonical pathway was found in cancer tissues from gemcitabine-treated mice. Serum metabolomics revealed a significant decrease of the purine compounds inosine and xanthine, and a decreasing trend for their metabolically-related molecule hypoxanthine. Understanding chemotherapy side effects may explain the lack of activity or the chemoresistant processes and it may help to set up strategies to improve the effectiveness of therapy.
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      headline:Influence of gemcitabine chemotherapy on the microbiota of pancreatic cancer xenografted mice
      description:Pancreatic ductal adenocarcinoma (PDAC) represents the fourth cause of cancer-related death. We aimed to evaluate whether gemcitabine treatment shapes the gut microbiota in a model of PDAC xenografted mice. Pancreatic cancer xenograft mice were subjected to gemcitabine injection once per week for 3 weeks to assess the tumor volume as compared to control mice injected with normal saline solution. The composition of fecal microbiota, the activation of NF-kB pathway in cancer tissues and the serum metabolomics were further analyzed. Gemcitabine considerably decreases the proportion of Gram- positive Firmicutes (from about 39 to 17%) and the Gram- negative Bacteroidetes (from 38 to 17%) which are the two dominant phyla in the gut of tumor-bearing control mice. This downshift was replaced by an increase of Proteobacteria (Escherichia coli and Aeromonas hydrophila) from 15 up to 32% and Verrucomicrobia (Akkermansia muciniphila) from 5 to 33% in the gut of drug-receiving mice. An overall increase in inflammation-associated bacteria was observed upon gemcitabine. Consistently, activation of the NF-kB canonical pathway was found in cancer tissues from gemcitabine-treated mice. Serum metabolomics revealed a significant decrease of the purine compounds inosine and xanthine, and a decreasing trend for their metabolically-related molecule hypoxanthine. Understanding chemotherapy side effects may explain the lack of activity or the chemoresistant processes and it may help to set up strategies to improve the effectiveness of therapy.
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      name:Department of Chemistry and Biotechnology, Tallinn University of Technology, Tallinn, Estonia
      name:Center of Food and Fermentation Technologies, University of Tallinn, Tallinn, Estonia
      name:Department of Chemistry and Biotechnology, Tallinn University of Technology, Tallinn, Estonia
      name:Center of Food and Fermentation Technologies, University of Tallinn, Tallinn, Estonia
      name:Biostatistics Unit, I.R.C.C.S. “Casa Sollievo della Sofferenza” Hospital, San Giovanni Rotondo, Italy
      name:Biostatistics Unit, I.R.C.C.S. “Casa Sollievo della Sofferenza” Hospital, San Giovanni Rotondo, Italy
      name:Department of Chemistry and Biotechnology, Tallinn University of Technology, Tallinn, Estonia
      name:Department of Chemistry and Biotechnology, Tallinn University of Technology, Tallinn, Estonia
      name:Department of Chemistry and Biotechnology, Tallinn University of Technology, Tallinn, Estonia
      name:Center of Food and Fermentation Technologies, University of Tallinn, Tallinn, Estonia
      name:Gastroenterology Unit, I.R.C.C.S. “Casa Sollievo della Sofferenza” Hospital, San Giovanni Rotondo, Italy
      name:Gastroenterology Unit, I.R.C.C.S. “Casa Sollievo della Sofferenza” Hospital, San Giovanni Rotondo, Italy
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