bims-agimec 2025-03-02 papers

bims-agimec

Biomed News

on Aging mechanisms

Issue of 2025–03–02
seven papers selected by
Metin Sökmen, Ankara Üniversitesi

Hallmarks of ovarian aging.
Hallmarks of aging and Alzheimer's Disease pathogenesis: Paving the route for new therapeutic targets.
The Anti-Aging Mechanism of Metformin: From Molecular Insights to Clinical Applications.
The Role of Cortisol and Dehydroepiandrosterone in Obesity, Pain, and Aging.
Cellular Senescence in Health, Disease, and Lens Aging.
Non-pharmacological treatment of Alzheimer's disease: an update.
Autophagy in Tissue Repair and Regeneration.

Trends Endocrinol Metab. 2025 Feb 24. pii: S1043-2760(25)00018-9. [Epub ahead of print]

Hallmarks of ovarian aging.

Chuqing Wu, Dan Chen, Michael B Stout, Meng Wu, Shixuan Wang.

  Ovarian aging is considered to be the pacemaker of female aging, and is linked to various comorbidities such as osteoporosis, cardiovascular diseases, and cognitive decline. Many efforts have been made to determine the mechanisms underlying ovarian aging, but their potential to act as hallmarks to predict and intervene in this process currently remains unclear. In this review we propose nine hallmarks as common features of ovarian aging: genomic instability, telomere attrition, epigenetic alterations, impaired autophagy, cellular senescence, deregulated nutrient-sensing, mitochondrial dysfunction, oxidative stress, and chronic inflammation. Understanding the interaction between these hallmarks poses a significant challenge but may also pave the way to the identification of pharmaceutical targets that can attenuate ovarian aging.

Keywords:  endocrine; fertility; hallmarks; oocyte; ovarian aging

DOI:  https://doi.org/10.1016/j.tem.2025.01.005
Ageing Res Rev. 2025 Feb 20. pii: S1568-1637(25)00045-5. [Epub ahead of print]106 102699

Hallmarks of aging and Alzheimer's Disease pathogenesis: Paving the route for new therapeutic targets.

Federico Bellelli, Davide Angioni, Beatrice Arosio, Bruno Vellas, Philipe De Souto Barreto.

  Aging is the leading risk factor for Alzheimer's Disease (AD). Understanding the intricate interplay between biological aging and the AD pathophysiology may help to discover innovative treatments. The relationship between aging and core pathways of AD pathogenesis (amyloidopathy and tauopathy) have been extensively studied in preclinical models. However, the potential discordance between preclinical models and human pathology could represent a limitation in the identification of new therapeutic targets. This narrative review aims to gather the evidence currently available on the associations of β-Amyloid and Tau pathology with the hallmarks of aging in human studies. Briefly, our review suggests that while several hallmarks exhibit a robust association with AD pathogenesis (e.g., epigenetic alterations, chronic inflammation, dysbiosis), others (e.g., telomere attrition, cellular senescence, stem cell exhaustion) demonstrate either no relationship or weak associations. This is often due to limitations such as small sample sizes and study designs, being either cross-sectional or with short follow-up intervals, limiting the generalizability of the findings. Distinct hallmarks play varying roles in different stages of AD pathology, emphasizing the need for longitudinal studies with longer follow-up periods. Considering the intricate interconnections across the hallmarks of aging, future research on AD pathology should focus on multiple hallmarks simultaneously.

Keywords:  AD pathogenesis; Aging hallmarks; Amyloid; Geroscience; Human studies; Tau

DOI:  https://doi.org/10.1016/j.arr.2025.102699
Molecules. 2025 Feb 10. pii: 816. [Epub ahead of print]30(4):

The Anti-Aging Mechanism of Metformin: From Molecular Insights to Clinical Applications.

Ting Zhang, Lijun Zhou, Meagan J Makarczyk, Peng Feng, Jianying Zhang.

  Aging represents a complex biological phenomenon marked by the progressive deterioration of physiological functions over time, reduced resilience, and increased vulnerability to age-related diseases, ultimately culminating in mortality. Recent research has uncovered diverse molecular mechanisms through which metformin extends its benefits beyond glycemic control, presenting it as a promising intervention against aging. This review delves into the anti-aging properties of metformin, highlighting its role in mitochondrial energy modulation, activation of the AMPK-mTOR signaling pathway, stimulation of autophagy, and mitigation of inflammation linked to cellular aging. Furthermore, we discuss its influence on epigenetic modifications that underpin genomic stability and cellular homeostasis. Metformin's potential in addressing age-associated disorders including metabolic, cardiovascular, and neurodegenerative diseases is also explored. The Targeting Aging with Metformin (TAME) trial aims to provide key evidence on its efficacy in delaying aging in humans. Despite these promising insights, significant challenges persist in gaining a more comprehensive understanding into its underlying mechanisms, determining optimal dosing strategies, and evaluating long-term safety in non-diabetic populations. Addressing these challenges is crucial to fully realizing metformin's potential as an anti-aging therapeutic.

Keywords:  anti-aging; autophagy; clinical trials; epigenetic regulation; inflammation; metformin; mitochondrial function; nutrient sensing

DOI:  https://doi.org/10.3390/molecules30040816
Diseases. 2025 Feb 01. pii: 42. [Epub ahead of print]13(2):

The Role of Cortisol and Dehydroepiandrosterone in Obesity, Pain, and Aging.

Nikolina Erceg, Miodrag Micic, Eli Forouzan, Nebojsa Nick Knezevic.

  Obesity, chronic pain, and aging are prevalent global challenges with profound implications for health and well-being. Central to these processes are adrenal hormones, particularly cortisol and dehydroepiandrosterone (DHEA), along with its sulfated form (DHEAS). Cortisol, essential for stress adaptation, can have adverse effects on pain perception and aging when dysregulated, while DHEA/S possess properties that may mitigate these effects. This review explores the roles of cortisol and DHEA/S in the contexts of obesity, acute and chronic pain, aging, and age-related diseases. We examine the hormonal balance, specifically the cortisol-to-DHEA ratio (CDR), as a key marker of stress system functionality and its impact on pain sensitivity, neurodegeneration, and physical decline. Elevated CDR and decreased DHEA/S levels are associated with worsened outcomes, including increased frailty, immune dysfunction, and the progression of age-related conditions such as osteoporosis and Alzheimer's disease. This review synthesizes the current literature to highlight the complex interplay between these hormones and their broader implications for health. It aims to provide insights into potential future therapies to improve pain management and promote healthy weight and aging. By investigating these mechanisms, this work contributes to a deeper understanding of the physiological intersections between pain, aging, and the endocrine system.

Keywords:  DHEA; DHEAS; acute pain; aging; chronic pain; cortisol; cortisol-to-DHEA ratio; obesity

DOI:  https://doi.org/10.3390/diseases13020042
Pharmaceuticals (Basel). 2025 Feb 12. pii: 244. [Epub ahead of print]18(2):

Cellular Senescence in Health, Disease, and Lens Aging.

Ying Qin, Haoxin Liu, Hongli Wu.

  Background: Cellular senescence is a state of irreversible cell cycle arrest that serves as a critical regulator of tissue homeostasis, aging, and disease. While transient senescence contributes to development, wound healing, and tumor suppression, chronic senescence drives inflammation, tissue dysfunction, and age-related pathologies, including cataracts. Lens epithelial cells (LECs), essential for maintaining lens transparency, are particularly vulnerable to oxidative stress-induced senescence, which accelerates lens aging and cataract formation. This review examines the dual role of senescence in LEC function and its implications for age-related cataractogenesis, alongside emerging senotherapeutic interventions. Methods: This review synthesizes findings on the molecular mechanisms of senescence, focusing on oxidative stress, mitochondrial dysfunction, and the senescence-associated secretory phenotype (SASP). It explores evidence linking LEC senescence to cataract formation, highlighting key studies on stress responses, DNA damage, and antioxidant defense. Recent advances in senotherapeutics, including senolytics and senomorphics, are analyzed for their potential to mitigate LEC senescence and delay cataract progression. Conclusions: LEC senescence is driven by oxidative damage, mitochondrial dysfunction, and impaired redox homeostasis. These factors activate senescence path-ways, including p53/p21 and p16/Rb, resulting in cell cycle arrest and SASP-mediated inflammation. The accumulation of senescent LECs reduces regenerative capacity, disrupts lens homeostasis, and contributes to cataractogenesis. Emerging senotherapeutics, such as dasatinib, quercetin, and metformin, show promise in reducing the senescent cell burden and modulating the SASP to preserve lens transparency.

Keywords:  cataractogenesis; cellular senescence; lens epithelial cells; oxidative stress; senescence-associated secretory phenotype; senotherapeutics

DOI:  https://doi.org/10.3390/ph18020244
Front Aging Neurosci. 2025 ;17 1527242

Non-pharmacological treatment of Alzheimer's disease: an update.

Shaofen Wang, Haochen Xu, Guangdong Liu, Limei Chen.

  Alzheimer's disease (AD) is a neurodegenerative disorder that significantly impairs memory, cognitive function, and the ability to perform daily tasks. The pathological features of AD include β-amyloid plaques, neurofibrillary tangles, and neuronal loss. Current AD treatments target pathological changes but often fail to noticeably slow disease progression and can cause severe complications, limiting their effectiveness. In addition to therapies targeting the core pathology of AD, a more comprehensive approach may be needed for its treatment. In recent years, non-pharmacological treatments such as physical therapy, exercise therapy, cell therapy, and nanoparticles have shown great potential in mitigating disease progression and alleviating clinical symptoms. This article reviews recent advances in non-pharmacological treatment approaches for AD, highlighting their contributions to AD management and facilitating the exploration of novel therapeutic strategies.

Keywords:  Alzheimer’s disease; cell therapy; exercise therapy; nanoparticles; non-pharmacological treatment; physical therapy

DOI:  https://doi.org/10.3389/fnagi.2025.1527242
Cells. 2025 Feb 14. pii: 282. [Epub ahead of print]14(4):

Autophagy in Tissue Repair and Regeneration.

Daniel Moreno-Blas, Teresa Adell, Cristina González-Estévez.

  Autophagy is a cellular recycling system that, through the sequestration and degradation of intracellular components regulates multiple cellular functions to maintain cellular homeostasis and survival. Dysregulation of autophagy is closely associated with the development of physiological alterations and human diseases, including the loss of regenerative capacity. Tissue regeneration is a highly complex process that relies on the coordinated interplay of several cellular processes, such as injury sensing, defense responses, cell proliferation, differentiation, migration, and cellular senescence. These processes act synergistically to repair or replace damaged tissues and restore their morphology and function. In this review, we examine the evidence supporting the involvement of the autophagy pathway in the different cellular mechanisms comprising the processes of regeneration and repair across different regenerative contexts. Additionally, we explore how modulating autophagy can enhance or accelerate regeneration and repair, highlighting autophagy as a promising therapeutic target in regenerative medicine for the development of autophagy-based treatments for human diseases.

Keywords:  autophagy; injury; planarian; regeneration; senescence; stem cell; tissue repair

DOI:  https://doi.org/10.3390/cells14040282