AI Article Synopsis
- Understanding cellular aging is essential for extending lifespan and studying age-related diseases, with yeast cells serving as a key model due to their genetics and lifespan.
- Recent experiments identified two distinct aging modes in yeast, focusing on declines in nucleolar and mitochondrial functions and showed different behaviors in young cells.
- A developed chemical-mechanical model revealed that bud morphogenesis during aging is influenced by material insertion at the bud tip and changes in signaling, indicating that aging can impair these processes.
Article Abstract
Understanding the mechanisms of cellular aging processes is crucial for attempting to extend organismal lifespan and for studying age-related degenerative diseases. Yeast cells divide through budding, providing a classical biological model for studying cellular aging. With their powerful genetics, relatively short lifespan and well-established signaling pathways also found in animals, yeast cells offer valuable insights into the aging process. Recent experiments suggested the existence of two aging modes in yeast characterized by nucleolar and mitochondrial declines, respectively. In this study, by analyzing experimental data it was shown that cells evolving into those two aging modes behave differently when they are young. While buds grow linearly in both modes, cells that consistently generate spherical buds throughout their lifespan demonstrate greater efficacy in controlling bud size and growth rate at young ages. A three-dimensional chemical-mechanical model was developed and used to suggest and test hypothesized mechanisms of bud morphogenesis during aging. Experimentally calibrated simulations showed that tubular bud shape in one aging mode could be generated by locally inserting new materials at the bud tip guided by the polarized Cdc42 signal during the early stage of budding. Furthermore, the aspect ratio of the tubular bud could be stabilized during the late stage, as observed in experiments, through a reduction on the new cell surface material insertion or an expansion of the polarization site. Thus model simulations suggest the maintenance of new cell surface material insertion or chemical signal polarization could be weakened due to cellular aging in yeast and other cell types.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10925247 | PMC |
| http://dx.doi.org/10.1101/2024.02.29.582376 | DOI Listing |
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