INTRACELLULAR SURVIVAL OF BIOFILM-FORMING MRSA OJ-1 BY ESCAPING FROM THE LYSOSOME AND AUTOPHAGOSOME IN J774A CELLS CULTURED IN OVERDOSED VANCOMYCIN
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Jimi, Shiro
Yoshimura, Michinobu
Mashima, Kota
Ueda, Yutaka
Miyazaki, Motoyasu
Saparov, Arman
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Microorganisms
Abstract
We investigated the drug-resistant mechanisms of intracellular survival of methicillin resistant S. aureus (MRSA). Our established MRSA clinical strain, OJ-1, with high biofilm-forming
ability, and a macrophage cell line, J774A, were used. After ingestion of OJ-1 by J774A, the cells
were incubated for ten days with vancomycin at doses 30 times higher than the minimum inhibitory
concentration. The number of phagocytosed intracellular OJ-1 gradually decreased during the study
but plateaued after day 7. In J774A cells with intracellular OJ-1, the expression of LysoTracker-positive
lysosomes increased until day 5 and then declined from day 7. In contrast, LysoTracker-negative and
OJ-1-retaining J774A cells became prominent from day 7, and intracellular OJ-1 also escaped from
the autophagosome. Electron microscopy also demonstrated that OJ-1 escaped the phagosomes and
was localized in the J774A cytoplasm. At the end of incubation, when vancomycin was withdrawn,
OJ-1 started to grow vigorously. The present results indicate that intracellular phagocytosed biofilm forming MRSA could survive for more than ten days by escaping the lysosomes and autophagosomes
in macrophages. Intracellular MRSA may survive in macrophages, and accordingly, they could be
resistant to antimicrobial drug treatments. However, the mechanisms their escape from the lysosomes
are still unknown. Additional studies will be performed to clarify the lysosome-escaping mechanisms
of biofilm-forming MRSA.
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Jimi, S., Yoshimura, M., Mashima, K., Ueda, Y., Miyazaki, M., & Saparov, A. (2022). Intracellular Survival of Biofilm-Forming MRSA OJ-1 by Escaping from the Lysosome and Autophagosome in J774A Cells Cultured in Overdosed Vancomycin. Microorganisms, 10(2), 348. https://doi.org/10.3390/microorganisms10020348
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