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Exploring the impact of diabetes on aging: insights from TERT and COL1A1 methylation.
Liamri, Jessica Nathania; Humardani, Farizky Martriano; Chandra, Giovani; Mulyanata, Lisa Thalia; Kok, Tjie; Irawati, Fenny; Sulistomo, Hikmawan Wahyu; Reichetzeder, Christoph; Dwi Putra, Sulistyo Emantoko.
Afiliação
  • Liamri JN; Faculty of Biotechnology, University of Surabaya, Surabaya, Indonesia.
  • Humardani FM; Faculty of Biotechnology, University of Surabaya, Surabaya, Indonesia.
  • Chandra G; Department of Biomedical Science, Faculty of Medicine, Universitas Brawijaya, Malang, Indonesia.
  • Mulyanata LT; Faculty of Medicine, University of Surabaya, Surabaya, Indonesia.
  • Kok T; Bioinformatics Research Center, Indonesia Bioinformatics and Biomolecular, Malang, Indonesia.
  • Irawati F; Faculty of Biotechnology, University of Surabaya, Surabaya, Indonesia.
  • Sulistomo HW; Faculty of Medicine, University of Surabaya, Surabaya, Indonesia.
  • Reichetzeder C; Faculty of Biotechnology, University of Surabaya, Surabaya, Indonesia.
  • Dwi Putra SE; Faculty of Biotechnology, University of Surabaya, Surabaya, Indonesia.
Turk J Biol ; 48(4): 257-266, 2024.
Article em En | MEDLINE | ID: mdl-39296334
ABSTRACT
Background/

aim:

Aging, a multifaceted biological process, leads to diminished physical performance, especially in older adults with diabetes, where a mismatch between biological and chronological age is noticeable. Numerous studies have demonstrated that diabetes accelerates aging at the cellular and organ levels. Notable aging markers are telomerase reverse transcriptase (TERT), related to telomere length, and type 1 chain collagen (COL1A1), a key component of skin collagen. Additionally, age-related methylation increases, as revealed through methylation analysis, augmenting aspects of aging. However, the detailed interplay between aging and diabetes, particularly regarding methylation, remains underexplored and warrants further study to elucidate the biological links between the two. Materials and

methods:

In this study, we elucidate the modulatory influence of diabetes on the aging process, focusing specifically on the modifications in TERT in the kidney and COL1A1 in the skin using mice of Swiss Webster strain as the diabetes model. Specimens were categorized into three distinct chronological cohorts chronologically young (16 weeks; n = 5), chronologically old (40 weeks; n = 5), and a periodically assessed group (16 weeks; n = 30), from which five mice were systematically sacrificed on a weekly basis.

Results:

Our findings reveal a marked impact of diabetes on the methylation statuses of TERT and COL1A1, characterized by an elevation in methylation levels within the periodic group (1st-6th week) and a simultaneous, progressive attenuation in the expression of TERT and COL1A1 genes.

Conclusion:

The observed alterations in the methylation levels of TERT and COL1A1 propound the hypothesis that diabetes potentially expedites the aging process, concomitantly impinging on the production of TERT and COL1A, ostensibly through the mechanism of promoter gene hypermethylation.
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Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2024 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2024 Tipo de documento: Article