New function of a key component in the immune system discovered
Autophagy is the basic mechanism that controls cells’ ability to break down their own material, i.e. dispose of cellular waste, and generate new energy by reusing their own components. Disruption of the autophagy mechanism is thought to contribute to the development of several diseases. Therefore, this knowledge can play an important role in our understanding of the onset and treatment of type 2 diabetes and other diseases.
A few years ago, the research teams led by immunologist Anna Blom and diabetes researcher Erik Renström at Lund University showed that the complement system, which consists of some 40 proteins in the blood, is also present within our beta cells in the pancreas.
One protein, CD59, was shown to be essential for enabling beta cells to secrete insulin. Another protein, C3, was produced in large amounts in the beta cells, but its exact role was unclear.
In a new study, which has now been published in Cell Metabolism, the researchers discovered that the complement protein C3 can protect the beta cells from stress (e.g. long-term high blood sugar levels) when diabetes is in progress.
When the researchers, using CRISPR/Cas 9, removed the gene that expresses the complement protein C3 from the beta cells, autophagy was disrupted and the cells died more easily from stress. They also found that C3 production in beta cells increases considerably in response to diabetes and inflammation, probably in an attempt to protect beta cells.
“C3 is a very old protein from an evolutionary perspective and we have now shown that it not only has a role in the relatively modern immune system in the blood, but also within cells, where it is needed for one of the most fundamental cellular functions, autophagy. In all likelihood, this applies to many cell types and opens the way for new principles in the treatment of diseases such as type 2 diabetes and certain neurodegenerative diseases for which there is a need to protect cells from stress”, concludes Anna Blom.
The study was funded with support from the Knut and Alice Wallenberg Foundation, the Swedish Diabetes Foundation, the Greta and John Kock Foundation, the Royal Physiographic Society of Lund, the Lars Hierta Memorial Foundation, the Albert Påhlsson Foundation for Research and Charity, the Crafoord Foundation, the Tore Nilsson Foundation for Medical Research, the Swedish Heart-Lung Foundation and the Swedish Foundation for Strategic Research.
Publication: Complement component C3 is highly expressed in human pancreatic islets and prevents β-cell death via ATG16L1 interaction and autophagy regulation