Telomere shortening in late‐life depression: A potential marker of depression severity

Telomere shortening in late‐life depression: A potential marker of depression severity

Objectives Telomeres are structures at the extremity of chromosomes that prevents genomic instability, and its shortening seems to be a hallmark of cellular aging. Past studies have shown contradictory results of telomere length (TL) in major depression, and are a few studies in late‐life depression...

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Veröffentlicht in:Brain and Behavior 2021-08, Vol.11 (8), p.e2255-n/a
Hauptverfasser: Mendes‐Silva, Ana Paula, Vieira, Erica Leandro Marciano, Xavier, Gabriela, Barroso, Lucelia Scarabeli Silva, Bertola, Laiss, Martins, Efrem Augusto Ribeiro, Brietzke, Elisa Macedo, Belangero, Sintia Iole Nogueira, Diniz, Breno Satler
Format: Artikel
Sprache:eng
Schlagworte:
Aging
Cell division
cellular senescence
Chromosomes
Cognitive ability
Comorbidity
Dementia
Depression, Mental
Diagnosis
Gerontology
late‐life depression
Mental depression
Mental disorders
Older people
Original Research
Senescence
telomere length
Telomeres
Variables
Young adults
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Zusammenfassung:Objectives Telomeres are structures at the extremity of chromosomes that prevents genomic instability, and its shortening seems to be a hallmark of cellular aging. Past studies have shown contradictory results of telomere length (TL) in major depression, and are a few studies in late‐life depression (LLD). This explores the association between TL as a molecular marker of aging and diagnosis of LLD, the severity of depressive symptoms, and cognitive performance in older adults. Methods/design We included 78 older adults (45 with LLD and 33 nondepressed controls, according to DSM‐V criteria), aged 60–90 years. TL was measured in leukocytes by a quantitative polymerase chain reaction, determining the relative ratio (T/S) between the telomere region copy number (T) and a single copy gene (S), using a relative standard curve. Results TL was significantly shorter in the LLD compared with control participants (p = .039). Comparing groups through the severity of depressive symptoms, we found a negative correlation with the severity of depressive symptoms (Hamilton Depression Rating Scale‐21, r = −0.325, p = .004) and medical burden (r = −0.271, p = .038). There was no significant correlation between TL and cognitive performance (Mattis Dementia Rating Scale, r = 0.152, p = .21). Conclusions We found that older adults with LLD have shorter telomere than healthy controls, especially those with a more severe depressive episode. Our findings suggest that shorter TL can be a marker of the severity of depressive episodes in older adults and indicate that these individuals may be at higher risk of age‐associated adverse outcomes linked to depression. Our study explores and examines the relationship between telomere length (TL) and Late‐Life Depression (LLD), considering the severity of depressive episodes. We found that TL was significantly shorter in the LLD than control participants and was negatively correlated with the severity of depressive symptoms and medical burden. Our findings suggest that shorter TL can be a marker of the severity of depressive episodes in older adults and indicate that these individuals may be at higher risk of age‐associated adverse outcomes linked to depression.
ISSN:2162-3279
2162-3279
DOI:10.1002/brb3.2255