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A thermo‐resistant and RNase‐sensitive cargo from Giardia duodenalis extracellular vesicles modifies the behaviour of enterobacteria
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Abstract
Extracellular vesicles (EVs) recently emerged as important players in the pathophysiology of parasitic infections. While the protist parasite
Giardia duodenalis
can produce EVs, their role in giardiasis remains obscure.
Giardia
can disrupt gut microbiota biofilms and transform commensal bacteria into invasive pathobionts at sites devoid of colonizing trophozoites via unknown mechanisms. We hypothesized that
Giardia
EVs could modify gut bacterial behaviour via a novel mode of trans‐kingdom communication. Our findings indicate that
Giardia
EVs exert bacteriostatic effects on
Escherichia coli
HB101 and
Enterobacter cloacae
TW1, increasing their swimming motility.
Giardia
EVs also decreased the biofilm‐forming ability of
E. coli
HB101 but not by
E. cloacae
TW1, supporting the hypothesis that these effects are, at least in part, bacteria‐selective.
E. coli
HB101 and
E. cloacae
TW1 exhibited increased adhesion/invasion onto small intestine epithelial cells when exposed to
Giardia
EVs. EVs labelled with PKH67 revealed colocalization with
E. coli
HB101 and
E. cloacae
TW1 bacterial cells. Small RNA sequencing revealed a high abundance of ribosomal RNA (rRNA)‐ and transfer RNA (tRNA)‐derived small RNAs, short‐interfering RNAs (siRNAs) and micro‐RNAs (miRNAs) within
Giardia
EVs. Proteomic analysis of EVs uncovered the presence of RNA chaperones and heat shock proteins that can facilitate the thermal stability of EVs and its sRNA cargo, as well as protein‐modifying enzymes. In vitro, RNase heat‐treatment assays showed that total RNAs in EVs, but not proteins, are responsible for modulating bacterial swimming motility and biofilm formation.
G. duodenalis
small RNAs of EVs, but not proteins, were responsible for the increased bacterial adhesion to intestinal epithelial cells induced upon exposure to
Giardia
EVs. Together, the findings indicate that
Giardia
EVs contain a heat‐stable, RNase‐sensitive cargo that can trigger the development of pathobiont characteristics in Enterobacteria, depicting a novel trans‐kingdom cross‐talk in the gut.
Title: A thermo‐resistant and RNase‐sensitive cargo from
Giardia duodenalis
extracellular vesicles modifies the behaviour of enterobacteria
Description:
Abstract
Extracellular vesicles (EVs) recently emerged as important players in the pathophysiology of parasitic infections.
While the protist parasite
Giardia duodenalis
can produce EVs, their role in giardiasis remains obscure.
Giardia
can disrupt gut microbiota biofilms and transform commensal bacteria into invasive pathobionts at sites devoid of colonizing trophozoites via unknown mechanisms.
We hypothesized that
Giardia
EVs could modify gut bacterial behaviour via a novel mode of trans‐kingdom communication.
Our findings indicate that
Giardia
EVs exert bacteriostatic effects on
Escherichia coli
HB101 and
Enterobacter cloacae
TW1, increasing their swimming motility.
Giardia
EVs also decreased the biofilm‐forming ability of
E.
coli
HB101 but not by
E.
cloacae
TW1, supporting the hypothesis that these effects are, at least in part, bacteria‐selective.
E.
coli
HB101 and
E.
cloacae
TW1 exhibited increased adhesion/invasion onto small intestine epithelial cells when exposed to
Giardia
EVs.
EVs labelled with PKH67 revealed colocalization with
E.
coli
HB101 and
E.
cloacae
TW1 bacterial cells.
Small RNA sequencing revealed a high abundance of ribosomal RNA (rRNA)‐ and transfer RNA (tRNA)‐derived small RNAs, short‐interfering RNAs (siRNAs) and micro‐RNAs (miRNAs) within
Giardia
EVs.
Proteomic analysis of EVs uncovered the presence of RNA chaperones and heat shock proteins that can facilitate the thermal stability of EVs and its sRNA cargo, as well as protein‐modifying enzymes.
In vitro, RNase heat‐treatment assays showed that total RNAs in EVs, but not proteins, are responsible for modulating bacterial swimming motility and biofilm formation.
G.
duodenalis
small RNAs of EVs, but not proteins, were responsible for the increased bacterial adhesion to intestinal epithelial cells induced upon exposure to
Giardia
EVs.
Together, the findings indicate that
Giardia
EVs contain a heat‐stable, RNase‐sensitive cargo that can trigger the development of pathobiont characteristics in Enterobacteria, depicting a novel trans‐kingdom cross‐talk in the gut.
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