A new angle for countering severe bacterial infections and sepsis

A new angle for countering severe bacterial infections and sepsis
During bacterial invasion, protein complexes called inflammasomes are activated. This in turn activates caspase enzymes, which cleave gasdermin D in two, releasing an active fragment known as gasdermin-D-NT. The fragments (shown as red ovals) perforate the membranes of the bacteria (in green) that are infecting cells, killing them, and also group together to form pores that punch holes in the membrane of the infected cell. This causes pyroptosis: The cell explodes open, releasing bacteria together with cytokines that sound an immune alarm. Outside the cell, gasdermin-D-NT fragments can also kill bacteria directly. Credit: Xing Liu, PhD, Boston Children's Hospital and Youdong Pan, PhD, Brigham & Women's Hospital

Bacterial infections that don't respond to antibiotics are of rising concern, as is sepsis—the immune system's last-ditch, failed attack on infection that ends up being lethal itself. Reporting online in Nature on July 7, researchers at Boston Children's Hospital describe new potential avenues for controlling both sepsis and the runaway bacterial infections that provoke it.

Sepsis kills a quarter million people each year in the U.S. and is the largest killer of newborns and children worldwide. Like antibiotic-resistant infections, it has no good treatment. Through meticulous experiments, scientists in Boston Children's Program in Cellular and Molecular Medicine (PCMM) reveal the final cellular events necessary for both and stemming the bacterial attack.

Recent research has shown that at any sign of bacterial invasion, protein complexes called inflammasomes are activated. This activation triggers a process called pyroptosis—the infected cells explode open, releasing as well as chemical signals that sound an alarm. But there's a balance: too strong an alarm can trigger sepsis, causing fatal blood-vessel and organ damage.

"The immune system is trying like hell to control the infection, but if the bacteria win out, the can kill the patient," explains Judy Lieberman, MD, PhD, senior investigator on the study together with Hao Wu, PhD, also in the PCMM. "Most attempts to quiet the immune response haven't worked in treating sepsis in the clinic, because the parts that trigger it haven't been well understood."

Once activated, inflammasomes activate enzymes called caspases that cut a molecule called gasdermin D in two. This cleavage unleashes gasdermin D's active fragment, known as gasdermin-D-NT. But how this causes pyroptosis hasn't been known.

Lieberman, Wu and their colleagues now show that gasdermin-D-NT packs a one-two punch. On the one hand, it perforates the membranes of the bacteria that are infecting cells and kills them. It also punches holes in the membrane of the host cell, causing pyroptosis—killing the cell and releasing bacteria and immune alarm signals. Nearby uninfected cells are left unscathed, the team found.

Second, the team discovered that gasdermin-D-NT directly kills bacteria outside of cells, including E. coli, S. aureus and Listeria. In a dish, this happened quickly—within five minutes.

The results now need to be replicated in animal models of infection and sepsis, but Lieberman believes that understanding how gasdermin-D-NT works could be harnessed to help treat highly dangerous bacterial infections.

"Because of widespread antibiotic resistance, we have to think about other strategies," Lieberman says. "Since the fragment kills bacteria but not uninfected host cells, one can imagine injecting the fragment directly, especially to treat a localized infection involving ."

For sepsis, Lieberman speculates about ways of inhibiting or blocking gasdermin-D-NT, such as with antibodies or strategies targeting caspase enzymes.


Explore further

New gene a key to fighting sepsis

More information: Inflammasome-activated gasdermin D causes pyroptosis by forming membrane pores, Nature, DOI: 10.1038/nature18629
Journal information: Nature

Citation: A new angle for countering severe bacterial infections and sepsis (2016, July 6) retrieved 17 October 2019 from https://medicalxpress.com/news/2016-07-angle-countering-severe-bacterial-infections.html
This document is subject to copyright. Apart from any fair dealing for the purpose of private study or research, no part may be reproduced without the written permission. The content is provided for information purposes only.
101 shares

Feedback to editors

User comments

Please sign in to add a comment. Registration is free, and takes less than a minute. Read more