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. 2021 Mar 11;13(6):1231. doi: 10.3390/cancers13061231

Table 4.

Studies on animal models; KC mice: p48Cre; LSL-KrasG12D. KPC mice: Pdx1Cre; LSL-KrasG12D; p53R172H; Rag1. KO: C57BL/6J mice carrying a Rag1tm1Mom. WT: wild-type.

Ref. Experimental Model Microbiota Association Main Findings/Authors’ Conclusion
Geller et al., 2017 [65] Mouse model of colon cancer Increased Gammaproteobacteria in PDAC Gammaproteobacteria possessing a long isoform of cytidine deaminase can metabolize gemcitabine.
Pushalkar et al., 2018 [80] KC and KPC mice Bacteroidetes and Firmicutes and select Actinobacteria- and Deferribacteres-associated genera were more prevalent in the early-KPC and advanced-KPC cohorts compared with WT Gut microbiota migrates into the pancreas in mice models. Germ-free mice are protected against PDAC progression.
Modulation of gut microbiota influences PDAC tumor progression and has a potential to augment PDAC responsiveness to immune therapy.
Thomas et al.,
2018 [81]		 KrasG12D/PTENlox/+ mice Acinetobacter, Enterobacter, Pseudomonas,
Delftia, Enterococcus, Streptococcus,
Corynebacterium, Propionibacterium,
Klebsiella, Sphingomonas and Staphylococcus. Klebsiella as disproportionally overrepresented in PDAC versus HC		 Intestinal microbiota exerts long-distance modulation and enhances PDAC carcinogenesis in transgenic and xenograft mouse models of PDAC.
Sethi et al.,
2018 [82] 		Rag1 KO, KPC, Ptenfl/fl mice Antibiotics induced a significant decrease in α-diversity, decrease in the relative abundance of Bacteroidetes and Firmicutes in the stool of KPC-bearing mice as well as reversed Bacteroidales: Clostridiales abundance ratio and colonization of the gut by likely antibiotic-resistant Proteobacteria and Tenericutes Gut microbiome depletion significantly reduced tumor burden in all the models tested, except for Rag1-knockout mice, which lack mature T and B cells.
Aykut et al.,
2019 [69]		 KC, KPC and WT mice Malassezia, at about 20% abundance Malassezia spp., most prevalent genus in pancreata of KC mice and exerts a tumor-promoting effect. Ablation of the mycobiome with the antifungal drugs in mice protected against the PDAC progression and enhanced the effects of gemcitabine by 15 to 25 percent.