In what they labeled a โsurprisingโ finding, Johns Hopkins Medicine researchers studying bacteria from freshwater lakes and soil say they have determined a proteinโs essential role in maintaining the germโs shape. Because the integrity of a bacterial cellโs โenvelopeโ or enclosure is key to its survival, the finding could advance the search for new and better antibiotics.
The research, described August 15 in the journal mBio, suggests that loss of a protein called OpgH in a widely studied bacterium known as Caulobacter crescentus creates a cascade of activity that disrupts the bubble-like cell envelope protecting the bacterium, resulting in the cellโs death. OpgH is an enzyme that creates glucose-containing molecules known as osmoregulated periplasmic glucans, or OPGs, which fill up the gelatinous in-between spaces of the protective cell envelope.
โIn our experiments, when we get rid of the protein OpgH in Caulobacter bacteria, which halts production of OPG sugar molecules, the bacteria canโt survive,โ says senior study author Erin Goley, Ph.D., professor of biochemistry at the Johns Hopkins University School of Medicine.
While Caulobacter crescentus bacteria themselves are not generally thought to cause diseases, OPGs found abundantly in gram-negative bacteria โ bacteria in an enclosed shell-like membrane โ play a role in antibiotic resistance and disease outcomes.
As a result, efforts to better understand the role of the sugar molecules in gram-negative bacteria, including Caulobacter, are seen as a way to aid in the development of new drugs that target disease-causing bacteria that have OPGs, including Brucella, Pseudomonas, Salmonella and E.coli.
If itโs true that the proteins that make or modify these sugar molecules are essential to bacterial survival, Goley notes, they could be good drug targets for antibiotics themselves. Or, in organisms where OPGs are not essential, a drug that targets some part of the OPG pathway might sensitize the cells to existing antibiotics, she says.
Sign up for the Daily Dose Newsletter and get every morning’s best science news from around the web delivered straight to your inbox? It’s easy like Sunday morning.
In this study, scientists used a molecular tool called an inducible promoter, dialing down the presence of the OpgH protein in Caulobacter to observe the effects on the shape of the bacteria cell and how loss of the OpgH protein affects a signaling pathway known as CenKR, which identifies and repairs problems in the cell envelope. They also manipulated the cell to make too much of the protein CenR, thus hyperactivating the CenKR pathway responsible for regulating the shape of the cell envelope.
After dialing up or down the OpgH or CenR proteins, scientists placed the bacteria cells on a pad of gel that prevented them from moving. Then, researchers used a specialized microscope to observe their shapes and activities.
โWe found that they became misshapen as we dialed down the OpgH protein and halted production of sugar OPG molecules, or hyperactivated the CenKR signaling pathway that maintains the cell envelope,โ Goley says.
โThen we also looked at where some of the molecular players that helped to grow the cell and keep the shape of the cell were located,โ she says. โThe molecular players were not in the correct locations, suggesting that OpgH and CenR are integral to maintaining the cellโs shape.โ
Once the cell envelope loses its shape, all of the bacteria eventually burst open and die, Goley says.
โWe established a model for how either depleting OPGs or activating the signaling pathway affects cell shape and growth,โ Goley says.
While characterizing the sugar moleculeโs role in Caulobacterโs cell structure is an important first step, Goley cautioned that โit will take some time to develop a complete picture about how they function across gram-negative species of bacteria.โ
In Caulobacter, the sugar molecules resemble closed rings, and in E. Coli, they look like trees, with branches sticking off of chained structures. Understanding their shape and all of the decorations that associate with the molecules can help researchers characterize the cell envelope, she says.
โIn the next phase of research, we hope to investigate all of the enzymes that make, decorate and break down these molecules โ so we can get a full picture of their metabolism and how they maintain the cell envelope,โ Goley says. โOnce we uncover how these enzymes function, thatโs great, because those are things drugs can target.โ
IMAGE CREDIT: Erin Goley, Ph.D.
If you enjoy the content we create and would like to support us, please consider becoming a patron on Patreon! By joining our community, you’ll gain access to exclusive perks such as early access to our latest content, behind-the-scenes updates, and the ability to submit questions and suggest topics for us to cover. Your support will enable us to continue creating high-quality content and reach a wider audience.
Join us on Patreon today and let’s work together to create more amazing content! https://www.patreon.com/ScientificInquirer
Leave a Reply