Pharmacotherapeutic Considerations on Telomere Biology: The Positive Effect of Pharmacologically Active Substances on Telomere Length

Author:

Apetroaei Miruna-Maria1,Fragkiadaki Persefoni23,Velescu Bruno Ștefan1,Baliou Stella23,Renieri Elisavet23ORCID,Dinu-Pirvu Cristina Elena1,Drăgănescu Doina1,Vlăsceanu Ana Maria1ORCID,Nedea Marina Ionela (Ilie)1ORCID,Udeanu Denisa Ioana1ORCID,Docea Anca Oana4ORCID,Tsatsakis Artistidis23ORCID,Arsene Andreea Letiția1ORCID

Affiliation:

1. Faculty of Pharmacy, Carol Davila University of Medicine and Pharmacy, 6 Traian Vuia Street, 020956 Bucharest, Romania

2. Laboratory of Toxicology and Forensic Sciences, Medical School, University of Crete, Voutes, 71003 Heraklion, Greece

3. Lifeplus S.A., Science & Technological Park of Crete, C Building, Vassilika Vouton, 70013 Heraklion, Greece

4. Department of Toxicology, University of Medicine and Pharmacy of Craiova, 200349 Craiova, Romania

Abstract

Telomeres are part of chromatin structures containing repeated DNA sequences, which function as protective caps at the ends of chromosomes and prevent DNA degradation and recombination, thus ensuring the integrity of the genome. While telomere length (TL) can be genetically inherited, TL shortening has been associated with ageing and multiple xenobiotics and bioactive substances. TL has been characterised as a reliable biomarker for the predisposition to developing chronic pathologies and their progression. This narrative review aims to provide arguments in favour of including TL measurements in a complex prognostic and diagnostic panel of chronic pathologies and the importance of assessing the effect of different pharmacologically active molecules on the biology of telomeres. Medicines used in the management of cardiovascular diseases, diabetes, schizophrenia, hormone replacement therapy at menopause, danazol, melatonin, and probiotics have been studied for their positive protective effects against TL shortening. All these classes of drugs are analysed in the present review, with a particular focus on the molecular mechanisms involved.

Funder

Carol Davila University of Medicine and Pharmacy Bucharest, Romania

Ministry of Research and Innovation within PNCDI III, Program 1—Development of the National RD system, Subprogram 1.2—Institutional Performance—RDI excellence funding projects

Publisher

MDPI AG

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