Your search keyword '"Shahnazari, Shahab"' showing total 3 results

1. Bacterial toxins can inhibit host cell autophagy through cAMP generation

Author

Shahnazari, Shahab, Namolovan, Anton, Mogridge, Jeremy, Kim, Peter K., and Brumell, John H.

Abstract

Autophagy plays a significant role in innate and adaptive immune responses to microbial infection. Some pathogenic bacteria have developed strategies to evade killing by host autophagy. These include the use of ‘camouflage’ proteins to block targeting to the autophagy pathway and the use of pore-forming toxins to block autophagosome maturation. However, general inhibition of host autophagy by bacterial pathogens has not been observed to date. Here we demonstrate that bacterial cAMP-elevating toxins from B. anthracisand V. choleracan inhibit host anti-microbial autophagy, including autophagic targeting of S. Typhimuriumand latex bead phagosomes. Autophagy inhibition required the cAMP effector protein kinase A. Formation of autophagosomes in response to rapamycin and the endogenous turnover of peroxisomes was also inhibited by cAMP-elevating toxins. These findings demonstrate that cAMP-elevating toxins, representing a large group of bacterial virulence factors, can inhibit host autophagy to suppress immune responses and modulate host cell physiology.

Published

2011

2. Antibacterial autophagy occurs at PI(3)P-enriched domains of the endoplasmic reticulum and requires Rab1 GTPase

Author

Huang, Ju, Birmingham, Cheryl L., Shahnazari, Shahab, Shiu, Jessica, Zheng, Yiyu T., Smith, Adam C., Campellone, Kenneth G., Heo, Won Do, Gruenheid, Samantha, Meyer, Tobias, Welch, Matthew D., Ktistakis, Nicholas T., Kim, Peter K., Klionsky, Daniel J, and Brumell, John H.

Abstract

Autophagy mediates the degradation of cytoplasmic components in eukaryotic cells and plays a key role in immunity. The mechanism of autophagosome formation is not clear. Here we examined two potential membrane sources for antibacterial autophagy: the ER and mitochondria. DFCP1, a marker of specialized ER domains known as ‘omegasomes,’ associated with Salmonella-containing autophagosomes via its PtdIns(3)P and ER-binding domains, while a mitochondrial marker (cytochrome b5-GFP) did not. Rab1 also localized to autophagosomes, and its activity was required for autophagosome formation, clearance of protein aggregates and peroxisomes, and autophagy of Salmonella. Overexpression of Rab1 enhanced antibacterial autophagy. The role of Rab1 in antibacterial autophagy was independent of its role in ER-to-Golgi transport. Our data suggest that antibacterial autophagy occurs at omegasomes and reveal that the Rab1 GTPase plays a crucial role in mammalian autophagy.

Published

2011

3. A role for diacylglycerol in antibacterial autophagy

Author

Shahnazari, Shahab, Namolovan, Anton, Klionsky, Daniel J, and Brumell, John H.

Abstract

Antibacterial autophagy is understood to be a key cellular immune response to invading microbes. However, the mechanism(s) by which bacteria are selected as targets of autophagy remain unclear. We recently identified diacylglycerol as a novel signaling molecule that targets bacteria to the autophagy pathway, and show that it acts via protein kinase C activation. We also found that Pkc1 is required for autophagy in yeast, indicating that this kinase plays a conserved role in autophagy regulation.

Published

2011