Abstract
Late-life depression (LLD), compared to depression at a young age, is more likely to have poor prognosis and high risk of progression to dementia. A recent systemic review and meta-analysis of the present antidepressants for LLD showed that the treatment response rate was 48% and the remission rate was only 33.7%, thus implying the need to improve the treatment with other approaches in the future. Recently, agents modulating the glutamatergic system have been tested for mental disorders such as schizophrenia, dementia, and depressive disorder. Ketamine, a noncompetitive NMDA receptor (NMDAR) antagonist, requires more evidence from randomized clinical trials (RCTs) to prove its efficacy and safety in treating LLD. The metabotropic receptors (mGluRs) of the glutamatergic system are family G-protein-coupled receptors, and inhibition of the Group II mGluRs subtypes (mGlu2 and mGlu3) was found to be as effective as ketamine in exerting rapid antidepressant activity in some animal studies. Inflammation has been thought to contribute to depression for a long time. The cytokine levels not only increase with age but also decrease serotonin. Regarding LLD, interleukin 6 (IL-6) and tumor necrosis factor α (TNF-α) released in vivo are likely to contribute to the reduced serotonin level. Brain-derived neurotrophic factor (BDNF), a growth factor and a modulator in the tropomyosin receptor kinase (Trk) family of tyrosine kinase receptors, probably declines quantitatively with age. Recent studies suggest that BDNF/TrkB decrement may contribute to learning deficits and memory impairment. In the process of aging, physiological changes in combination with geriatric diseases such as vascular diseases result in poorer prognosis of LLD in comparison with that of young-age depression. Treatments with present antidepressants have been generally unsatisfactory. Novel treatments such as anti-inflammatory agents or NMDAR agonists/antagonists require more studies in LLD. Last but not least, LLD and dementia, which share common pathways and interrelate reciprocally, are a great concern. If it is possible to enhance the treatment of LDD, dementia can be prevented or delated.
Highlights
The findings showed that the Brain-derived neurotrophic factor (BDNF) level in the Late-life depression (LLD) + MCI and LLD + NCD groups presented no significant difference at baseline
Late-life depression (LLD), unlike early-onset depression (EOD), is a geriatric disease caused by a variety of factors
The glutamatergic system, inflammatory markers, and brain-derived neurotrophic factors may contribute to LLD and dementia
Summary
(https://www.un.org/en/global-issues/ageing?fbclid= IwAR2ut7ufS5ULfFGf4HbXtijNmx2q0VFzzIyBy0Fonznzt87LeIMjJGK21nU (accessed on 9 July 2021). Depression has recently been identified as a pandemic, causing huge social cost and high financial load. Unlike depression at a young age, late-life depression (LLD), with high pathogenic complexity caused by physiological and psychosocial issues and chronic disease, can rarely be treated with one antidepressant. A recent systemic review and meta-analysis of the present antidepressants for LLD showed that the treatment response rate and the depression remission rate are 48% and 33.7% [2], respectively. In the process of aging, structural changes in the brain may be associated with depression. The causes of LLD may include neuroendocrine dysregulation and changes in neural circuitry, and genetic vulnerability and stress due to life events that interact reciprocally [4,5]
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