Blue, red and yellow colors show where emerin clusters locate in a cell’s nucleus

A “heat map” shows the distribution of the protein emerin within a cell nucleus, from highly dispersed (blue) to dense nanoclusters (red), as determined with experiments (left) and computer modeling (right). (Photo: Courtesy of Carlos Alas.)

Scientists unlock clues to new treatments for muscular dystrophy

ByUSC Dornsife News Staff March 5, 2025

A new discovery about how tiny protein clusters form in cells could pave the way for treatments for Emery-Dreifuss muscular dystrophy (EDMD), a rare genetic disorder that causes muscle weakness and heart problems.

Researchers at the USC Dornsife College of Letters, Arts and Sciences combined advanced imaging techniques and theoretical physics to observe and explain how nanoclusters of the protein emerin form inside living cells. These clusters — about 100,000 times smaller than a human hair’s width — play a crucial role in how cells sense and respond to mechanical forces like stretching or pressure, a process known as mechanotransduction. When this process fails, it can contribute to diseases like muscular dystrophy.

The study, published in Physical Review Research, uncovers the molecular “rules” driving the arrangement of emerin into nanoclusters and the mechanisms leading to their defective assembly in people with EDMD. By identifying the physical principles behind those defects and why they disrupt mechanotransduction and trigger disease symptoms, scientists hope to develop new strategies to correct them.

Fascinatingly, the researchers, led by Christoph Haselwandter, professor of physics and astronomy and quantitative and computational biology, and Fabien Pinaud, associate professor of biological sciences and physics and astronomy, applied principles first proposed by Alan Turing — the famed WWII codebreaker and computing pioneer — to understand how these nanoclusters form. Turing’s work on pattern formation in nature(such as zebra stripes and leopard spots) revealed mathematical rules that also appear to govern protein assembly at a nanoscale level.

“This research opens up exciting possibilities,” said study first author Carlos Alas, who earned his physics PhD in 2023 from USC Dornsife. “By applying physics-based approaches, we can start thinking about ways to correct these defects and potentially help people with this debilitating disease.”

While the findings focus on muscular dystrophy, understanding how proteins like emerin function could also lead to breakthroughs in other diseases linked to cellular mechanics.

About the study

In addition to Haselwandter, Pinaud and Alas, USC Dornsife PhD student Liying Wu also contributed to the research.

The study was supported by National Science Foundation awards MCB-2202087 and DMR-2051681.