Pharmacomicrobiomics: exploiting the drug-microbiota interactions in anticancer therapies

Panebianco, Concetta; Andriulli, Angelo; Pazienza, Valerio

doi:10.1186/s40168-018-0483-7

Cited by 236 publications

(217 citation statements)

References 89 publications

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“…In the wild, due to food shortage, protein and fat intake decreased, and the Bacteroidetes content increased to help host to increase their nutrition. A disruption of the symbiosis between the microbiota and host is known as dysbiosis and is described in multiple chronic diseases, such as obesity and malnutrition (Castaner et al 2018;Zhang et al 2018;Jeong et al 2019), neurological disorders (Kurokawa et al 2018;Quagliariello et al 2018;Sun and Shen 2018), inflammatory bowel disease (IBD) (Costa et al 2012;Roche-Lima et al 2018), metabolic syndrome (Zhao et al 2018), cancer and other diseases (Katsimichas et al 2018;Lu et al 2018;Panebianco et al 2018;Pulikkan et al 2018;Zitvogel et al 2018). We presume that the health of the wild group of Tibetan wild asses was better than the captive group.…”

Section: Discussionmentioning

confidence: 99%

Comparison of the gut microbiota composition between the wild and captive Tibetan wild ass ( Equus kiang )

et al. 2019

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Aims The gut microbiota has a great effect on the health and nutrition of the host. Manipulation of the intestinal microbiota may improve animal health and growth performance. The objectives of our study were to characterize the faecal microbiota between wild and captive Tibetan wild asses and discuss the differences and their reasons. Methods and Results Through high‐throughput sequencing of the 16S rRNA V4‐V5 region, we studied the gut microbiota composition and structure of Tibetan wild asses in winter, and analysed the differences between wild and captive groups. The results showed that the most common bacterial phylum in Tibetan wild ass faeces samples was Bacteroidetes, while the phylum Firmicutes was dominant in captive Tibetan wild ass faecal samples. The relative abundance of Firmicutes, Tenericutes and Spirochaetes were significantly higher (P < 0·01) than in the wild groups. Conclusions Captivity reduces intestinal microbial diversity, evenness and operational taxonomic unit number due to the consumption of industrial food, therefore, increasing the risk of disease prevalence and affecting the health of wildlife. Significance and Impact of the Study We studied the effect of the captive environment on intestinal micro‐organisms. This article provides a theoretical basis for the ex‐situ conservation of wild animals in the future.

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Section: Discussionmentioning

confidence: 99%

Comparison of the gut microbiota composition between the wild and captive Tibetan wild ass ( Equus kiang )

et al. 2019

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“…The human gut microbiota is highly complex and exists in a dynamic balance between symbiosis and pathogenesis, which can influence almost any aspect of host physiology [28]. Growing evidence suggests that the gut microbiota not only plays a key role in carcinogenesis but also influences the efficacy and toxicity of anticancer therapy [29,30]. The microbiota modulates the host response to chemotherapy via numerous mechanisms, such as alteration of community structure and immune microenvironment.…”

Section: Discussionmentioning

confidence: 99%

Mutational signatures shift induced by chemotherapeutic agents, 5-Fluorouracil and Oxaliplatin, in the gut microbiome

Liu

Zou

et al. 2020

Preprint

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We developed a powerful framework for taxonomy composition and genomic variation analysis to investigate the mutagenesis effect and proliferation influence of chemotherapeutic agents, such as 5-Fluorouracil (5-FU) and Oxaliplatin (Oxi) on gut microbiota. Using the gut microbiome data of 68 time serial stool samples, we detected 1.45 million variations among the chemotherapy groups and found the drugs significantly affected mutation signatures of gut microbiota. About 786 faecal metagenomes of 755 individuals from 5 different cohorts were analyzed to build the mutation pattern of gut microbiota from health samples. Oxi notably increase transversion rate, while 5-FU reduced the rate. We also performed in vitro experiments to confirm that chemotherapeutic agents could disrupt the pattern of genetic variant in the intestinal microorganisms. Post-chemotherapy samples had specific gut microbiome signatures with higher abundance of Bacilli and a lack of anaerobic bacteria. In addition, drug-associated functional alterations were also found: metabolism changes in the 5-FU group implied that gut microbiota could provide additional NAD + to inhibit cancer cell autophagy; in the Oxi group, the ribosome and lysine biosynthesis genes were obviously enriched. According to molecular evolution analysis, traits related to protein secretion system showed evidence of strong selection pressure from the drugs, which could be a novel potential treatment strategy for chemotherapy-induced diarrhea. Our study provides a blueprint for characterizing the role of microbes and drug-microbe interaction in the gut microbiota response to chemotherapy.

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“…The study of the microbiota has attracted increasing attention during the last decade since it has become clear that the composition and function of this ecological community of commensal, symbiotic and pathogenic microorganisms affect several physiological and pathological processes, including cancer [13]. Although microbiota is relatively stable over time [14] it can be easily modi ed by a number of environmental factors, such as lifestyle, diet and drugs [15,16,17]. The current study shows that DCA treatment led to several shifts on the microbiota in particular at family, genus or species level in pancreatic cancer xenograft mice.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of pyruvate dehydrogenase kinase influence microbiota and metabolomic profile in pancreatic cancer xenograft mice

Adamberg

Vilu

Pazienza³

2020

Preprint

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Objective Despite recent advances in treatment options, pancreatic cancer remains the most deadly major cancer. Targeting metabolism represents an emerging anti-cancer strategy. Results Metagenomic 16S analysis was employed to explore the effect of Dichloroacetate (DCA) on the composition of the fecal microbiota and metabolomic profile was assessed on in vivo pancreatic cancer mouse xenograft model. Pancreatic cancer xenograft mice displayed a shift of microbiota’ profile as compared to control mice without DCA treatment and a significant decrease of the purine bases inosine xanthine together with their metabolically-related compound hypoxanthine were observed in the DCA treated group as compared to the control group. Two aminoacids methionine and aspartic acid resulted decreased and increased respectively. DCA affects tumor environment and studies are needed in order to understand whether DCA supplementation could be supportive as synergistic approach to enhance the efficacy of existing cancer treatments in pancreatic cancer patients.

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Pharmacomicrobiomics: exploiting the drug-microbiota interactions in anticancer therapies

Cited by 236 publications

References 89 publications

Comparison of the gut microbiota composition between the wild and captive Tibetan wild ass ( Equus kiang )

Comparison of the gut microbiota composition between the wild and captive Tibetan wild ass ( Equus kiang )

Mutational signatures shift induced by chemotherapeutic agents, 5-Fluorouracil and Oxaliplatin, in the gut microbiome

Inhibition of pyruvate dehydrogenase kinase influence microbiota and metabolomic profile in pancreatic cancer xenograft mice

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