Aging is a complex biological process which is accompanied by an increasing number of toxic protein aggregates in the cells. Scientists consider them the cause of various neurodegenerative disorders, such as Alzheimer’s, Huntington’s and Parkinson’s disease.
Muscle cell of a long-lived nematode worm: chaperone-rich protein aggregates (green) accumulate and save the cell during aging. Photo Credit: Prasad Kasturi / © MPI of Biochemistry
However, their exact role remains poorly understood. A collaborative team headed by F.-Ulrich Hartl at the MPIB now used the tiny nematode worm Caenorhabditis elegans (short: C. elegans) as a model organism to analyze the changes that occur in the proteome (the entirety of all proteins) during a lifespan. “The study is the most extensive of its kind in a whole organism quantifying more than 5,000 different proteins at multiple time points during aging, explains Prasad Kasturi, equally contributing first author together with Dirk Walther.
The researchers were able to show that the proteome undergoes extensive changes as the worms age. About one third of the quantified proteins significantly change in abundance. The normal relation between different proteins, which is critical for proper cell function, is lost. This shift overwhelms the machinery of protein quality control and impairs the functionality of the proteins. This is reflected in the widespread aggregation of surplus proteins ultimately contributing to the death of the animals.
Based on these findings, the researchers also analyzed how genetically changed worms with a substantially longer or shorter lifespan manage these changes. “We found that proteome imbalance sets in earlier and is increased in short-lived worms. In contrast, long-lived worms coped much better and their proteome composition deviated less dramatically from that of young animals”, as Kasturi says. Surprisingly, the long-lived worms increasingly deposited surplus and harmful proteins in insoluble aggregates, thus relieving pressure on the soluble, functional proteome. However, in contrast to the aggregates found in short-lived animals, these deposits were enriched with helper proteins — the so-called molecular chaperones — which apparently prevented the toxic effects normally exerted by aggregates.
“These findings demonstrate that the cells specifically accumulate chaperone-rich protein aggregates as a safety mechanism. Therefore, the aggregates seem to be an important part of healthy aging”, Kasturi explains. Indeed, it is known that insoluble protein aggregates also accumulate in the brains of healthy elderly people. So far, researchers assumed that neurodegeneration and dementia appear to be mainly caused by aberrant protein species accumulating in aggregates. This assumption may now being tested again: “Clearly, aggregates are not always harmful. Finding ways to concentrate harmful proteins in insoluble deposits might be a useful strategy to avoid or postpone neurodegenerative diseases as we age”, F.-Ulrich Hartl classifies the results.
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The above story is based on materials provided by Max Planck Institute of Biochemistry .