All About Chemistry... 2011 and beyond

Related Stories

Corrected Protein Structure Reveals Drug Targets for Cancer, Neurodegenerative Diseases

Released: 10-Aug-2015 3:05 PM EDT
Embargo expired: 13-Aug-2015 12:00 PM EDT
Source Newsroom: University of California, San Diego Health Sciences
Contact Information

Available for logged-in reporters only

Citations Cell Reports

Aug. 14, 2015 - Protein Kinase C (PKC) is a family of enzymes that controls the activity of other proteins in a cell by attaching chemical tags. That simple act helps determine cell survival or death. When it goes awry, a number of diseases may result. In a study published August 13 in Cell Reports, researchers at University of California, San Diego School of Medicine reveal a more accurate structure of PKC, providing new targets for fine-tuning the enzyme’s activity as needed to improve human health.

“By understanding how PKC clamps itself closed, we can now look for ways to wedge it open to keep it active,” said Alexandra C. Newton, PhD, professor of pharmacology. “This has great potential for developing therapies for cancer, in which keeping the enzyme in its ‘on’ position will promote tumor cell death. We also want to do the opposite in neurodegenerative diseases, in which we need treatments that keep neurons alive.”

Researchers typically use a technique called X-ray crystallography to determine the 3D structure of proteins. But sometimes they have to make assumptions in order to fit the data together as best they can. In a 2011 study, a different research group resolved most of PKC’s structure and made their best guess at how all the pieces fit together.

But that structure didn’t add up with the biology of how PKC works. In collaboration with the research team of Susan Taylor, PhD, professor of pharmacology at UC San Diego School of Medicine, Newton and researchers took another look at how to connect the parts, or domains, of the enzyme. They came up with a different structure and tested it using a sophisticated cellular imaging technique to visualize whether PKC was properly packed together or not.

The researchers found that PKC’s calcium-sensing (C2) domain interacts with its own tail and enzymatic domain (the part that does the chemical tagging, a process known as phosphorylation), locking the enzyme in an inactive pose. PKC begins to activate when calcium triggers the bridging of the C2 domain to the Cell-Membrane'>cell membrane, thus opening the enzyme for activity.

The team also validated this packing by mutating specific parts of the protein that hold the domains together, unlocking and relocking PKC between unpacked and correctly packed structures.

“Knowing the interfaces that hold PKC closed will now allow the design of small molecules that can either disrupt the interactions between PKC’s domains to open up and activate the enzyme, or clamp the domains closed to prevent its activation,” said first author Corina Antal, PhD, who was a graduate student in Newton’s lab at the time of the study.

Co-authors of this study also include Julia A. Callender, and Alexandr P. Kornev, UC San Diego.

This research was funded, in part, by the National Institutes of Health (grants GM43154, DK54441, T32GM007752) and National Science Foundation (grant DGE1144086).



Share this story with your friends!

Social Networking

Please recommend us on Facebook, Twitter and more:

Other social media tools

Global Partners

Tell us what you think of Chemistry 2011 -- we welcome both positive and negative comments. Have any problems using the site? Questions?

About us

Chemistry2011 is an informational resource for students, educators and the self-taught in the field of chemistry. We offer resources such as course materials, chemistry department listings, activities, events, projects and more along with current news releases.

Events & Activities

Are you interested in listing an event or sharing an activity or idea? Perhaps you are coordinating an event and are in need of additional resources? Within our site you will find a variety of activities and projects your peers have previously submitted or which have been freely shared through creative commons licenses. Here are some highlights: Featured Idea 1, Featured Idea 2.

About you

Ready to get involved? The first step is to sign up by following the link: Join Here. Also don’t forget to fill out your profile including any professional designations.

Global Partners