New insights into metabolites that control aging and disease

In a significant advancement in the field of biochemistry, scientists at BTI and Cornell University have uncovered new insights into a family of metabolites, acylspermidines, that could change how we understand aging and fight diseases.

The study, recently published in Nature Chemical Biology, presents an unexpected connection between spermidine, a long-known compound present in all living cells, and sirtuins, an enzyme family that regulates many life-essential functions.

Sirtuins have been the subject of significant attention over the past two decades. Recent studies indicate that sirtuins play a crucial role in various age-related diseases. As a result, there is growing interest in the link between sirtuins and aging, making them a promising target for therapeutic interventions aimed at improving health span and longevity.

“We were excited to uncover this unexpected branch of cellular metabolism related to sirtuins,” said lead author Frank Schroeder, a professor at BTI and professor of chemistry and chemical biology in the College of Arts and Sciences. “Discovering these previously uncharacterized spermidine derivatives provides insight into the inner workings of this critical pathway and brings us a step closer to understanding the physiological functions of mitochondrial sirtuins.”

The researchers took an unbiased approach, comparative metabolomics, a methodology that the Schroeder lab has been developing for over a decade, to screen for sirtuin-dependent metabolic changes. The study revealed a novel family of metabolites called acylspermidines, which are derived from modifications of diverse proteins, many of which play essential roles in growth and cell survival.

Following the discovery of sirtuin-linked acylspermidines in the simple organism C. elegans, the researchers further demonstrated that the same compounds are also present in mammals (including humans). Lastly, the research team demonstrates the direct impact of these metabolites on lifespan in C. elegans and cell proliferation in mammals.

“Important physiological functions are reflected in many molecular fingerprints, including tens of thousands of small molecule metabolites that remain to be discovered. This work is a step towards uncovering the biological roles and functions of the vast space of chemical dark matter in our bodies,” says Bingsen Zhang, a graduate student in the Schroeder lab and first author of the study.

Future research will explore the mechanisms and pharmacological aspects of these findings, particularly how acylspermidines affect lifespan, cell growth, and their potential interactions with other metabolic pathways.

“Nearly 350 years after spermidine was isolated and 100 years after its structure was understood, our work further advances the collective knowledge of the spermidine family, connecting it to other vital biochemical processes, including central energy metabolism and amino acid metabolism,” added Zhang.

This is a collaborative study with researchers from the lab of Robert Weiss, senior associate dean at the Cornell Graduate School and professor of molecular genetics at the Cornell University College of Veterinary Medicine. This work was partly supported by the NIH and HHMI.

Aaron Callahan is Director of IT & Communications for BTI.

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