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Microautophagy is essential for preventing aging

November 21, 2023
Osaka University
Researchers have shown that lysosomes, key organelles for maintaining cellular stability, can be repaired once damaged by a process termed microautophagy. They identified molecules called STK38 and GABARAPs as key regulators of this process. Depletion of microautophagy regulators lead to increased cellular senescence and a shorter lifespan, indicating the importance of this process. This study is highly significant for the achievement of healthy aging and points toward new therapies for age-related diseases.

To age or not to age! How does aging affect organisms on a cellular level? What mechanisms help cells survive self-inflicted or external harm? It is known that lysosomes -- critically important cellular structures -- are crucial for digesting damaged cellular components and pathogens, and maintain stability within cells and tissues. But can they also be repaired, and if so, how?

In a study published this month in EMBO Reports, researchers from Osaka University and Nara Medical University have shown that damaged lysosomes are repaired by a mechanism called "microautophagy" and have identified two key regulators of this process.

Microautophagy is one of the three main types of autophagy in most higher organisms. It is a regulated process by which cellular components that have become dysfunctional or are no longer required are broken down. Although it is assumed to be involved in defense mechanisms collectively called lysosomal damage responses, the details remain unknown.

Lysosomes frequently become damaged and lysosomal dysfunction has been linked to accelerated aging and a shortened lifespan. In this study, the researchers tried to understand the repair mechanisms. To identify a novel regulator of lysosomal damage response, they focused a signaling pathway called Hippo pathway which controls multiple processes such as cellular growth. They knocked down individual components of the Hippo pathway in the human cells, and then observed whether the cells could respond to induced lysosomal damage. This screening revealed that a protein called Serine-threonine kinase 38 (STK38) is essential for the lysosomal damage response.

They then found that STK38 works with a protein complex called the "endosomal sorting complex required for transport (ESCRT) machinery," which was already known to be linked to lysosomal repair. "STK38 recruits the protein 'vacuolar protein sorting 4' (VPS4) to damaged lysosomes and is crucial for disassembling the ESCRT machinery at the end of the repair process," explains lead author of the study Monami Ogura. They further found that lysosomal membrane repair by ESCRT machinery is mediated by microautophagy.

They also identified that non-canonical lipidation of a subfamily of autophagy-related protein 8 (ATG8s) molecules -- the key autophagy proteins -- known as Gamma-aminobutyric acid receptor-associated proteins (GABARAPs) is required for this process. Lipidation, the process of modifying ATG8s with lipid extensions, is the main process involved in autophagy. In non-canonical lipidation ATG8s are lipidated into single-membrane endolysosomes, instead of double-membrane phagophore seen in canonical lipidation.

The researchers showed that the GABARAPs are essential for the first step of the process of lysosomal repair. "We showed that non-canonical lipidation of ATG8s is crucial for the initial recruitment of the ESCRT machinery to damaged lysosomes and their subsequent repair," explains senior author Shuhei Nakamura.

The team showed that depletion of the regulators of microautophagy increased the rate of senescent cells and shortened lifespan in C. elegans. Both STK38 and GABARAPs also have evolutionarily conserved roles, indicating the significance of this pathway in maintaining lysosomal integrity, healthy cellular function, and the prevention of cellular senescence and organismal aging. The detailed understanding provided by this study paves the way for increasing healthy aging and has great therapeutic value for the treatment of age-related diseases.

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Materials provided by Osaka University. Note: Content may be edited for style and length.

Journal Reference:

  1. Monami Ogura, Tatsuya Kaminishi, Takayuki Shima, Miku Torigata, Nao Bekku, Keisuke Tabata, Satoshi Minami, Kohei Nishino, Akiko Nezu, Maho Hamasaki, Hidetaka Kosako, Tamotsu Yoshimori, Shuhei Nakamura. Microautophagy regulated by STK38 and GABARAPs is essential to repair lysosomes and prevent aging. EMBO reports, 2023; DOI: 10.15252/embr.202357300

Cite This Page:

Osaka University. "Microautophagy is essential for preventing aging." ScienceDaily. ScienceDaily, 21 November 2023. <>.
Osaka University. (2023, November 21). Microautophagy is essential for preventing aging. ScienceDaily. Retrieved February 23, 2024 from
Osaka University. "Microautophagy is essential for preventing aging." ScienceDaily. (accessed February 23, 2024).

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