Serratia Marcescens is Able to Survive and Proliferate in Autophagic-like Vacuoles Inside Non-phagocytic Cells

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2011 Sep 9

PMID 21901159

Citations 30

Authors

Griselda V Fedrigo

Emanuel M Campoy

Gisela Di Venanzio

Maria Isabel Colombo

Eleonora Garcia Vescovi

Affiliations

Soon will be listed here.

Abstract

Serratia marcescens is an opportunistic human pathogen that represents a growing problem for public health, particularly in hospitalized or immunocompromised patients. However, little is known about factors and mechanisms that contribute to S. marcescens pathogenesis within its host. In this work, we explore the invasion process of this opportunistic pathogen to epithelial cells. We demonstrate that once internalized, Serratia is able not only to persist but also to multiply inside a large membrane-bound compartment. This structure displays autophagic-like features, acquiring LC3 and Rab7, markers described to be recruited throughout the progression of antibacterial autophagy. The majority of the autophagic-like vacuoles in which Serratia resides and proliferates are non-acidic and have no degradative properties, indicating that the bacteria are capable to either delay or prevent fusion with lysosomal compartments, altering the expected progression of autophagosome maturation. In addition, our results demonstrate that Serratia triggers a non-canonical autophagic process before internalization. These findings reveal that S. marcescens is able to manipulate the autophagic traffic, generating a suitable niche for survival and proliferation inside the host cell.

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