logo
0

EbookBell.com

Most ebook files are in PDF format, so you can easily read them using various software such as Foxit Reader or directly on the Google Chrome browser.
Some ebook files are released by publishers in other formats such as .awz, .mobi, .epub, .fb2, etc. You may need to install specific software to read these formats on mobile/PC, such as Calibre.

Please read the tutorial at this link:  https://ebookbell.com/faq 


We offer FREE conversion to the popular formats you request; however, this may take some time. Therefore, right after payment, please email us, and we will try to provide the service as quickly as possible.


For some exceptional file formats or broken links (if any), please refrain from opening any disputes. Instead, email us first, and we will try to assist within a maximum of 6 hours.

EbookBell Team

Genomic Risk Prediction For Depression In A Large Prospective Study Of Older Adults Of European Descent Chenglong Yu

  • SKU: BELL-239013146
Genomic Risk Prediction For Depression In A Large Prospective Study Of Older Adults Of European Descent Chenglong Yu
$ 35.00 $ 45.00 (-22%)

4.3

78 reviews

Genomic Risk Prediction For Depression In A Large Prospective Study Of Older Adults Of European Descent Chenglong Yu instant download after payment.

Publisher: x
File Extension: PDF
File size: 1.08 MB
Pages: 8
Author: Chenglong Yu, Andrew Bakshi, Bruno Agustini, Alicia Walker, Tian Lin, Mojtaba Lotfaliany, Lana J. Williams, John J. McNeil, Naomi R. Wray, Michael Berk, Paul Lacaze
ISBN: 10.1038/S41380-025-03145-3
Language: English
Year: 2025

Product desciption

Genomic Risk Prediction For Depression In A Large Prospective Study Of Older Adults Of European Descent Chenglong Yu by Chenglong Yu, Andrew Bakshi, Bruno Agustini, Alicia Walker, Tian Lin, Mojtaba Lotfaliany, Lana J. Williams, John J. Mcneil, Naomi R. Wray, Michael Berk, Paul Lacaze 10.1038/S41380-025-03145-3 instant download after payment.

The extent to which genetic predisposition contributes to late-life depression risk, particularly after age 70, remains unclear, despite the high prevalence of depression in this age group and the variability in risk factors by age. This study investigated the association between a polygenic score (PGS) and depression outcomes, including severity, trajectories of depression, and antidepressant medication use, in a longitudinal cohort of 12,029 genotyped older adults of European descent aged ≥70 years, with no history of diagnosed cardiovascular disease events, dementia, or permanent physical disability at baseline. Participants were followed for a median of 4.7 years. 

The PGS was derived using the latest Psychiatric Genomics Consortium data for major depression. Depression was defined by the CES-D-10 score thresholds of ≥8 (primary outcome), ≥10, and ≥12 (secondary outcomes), alongside1234567890();,:antidepressant medication use and four previously established longitudinal trajectories of depressive symptoms: low (nondepressed), moderate (sub-threshold), high (persistent), and initially low but increasing (emerging). Multivariable models were used to examine associations between the PGS (per standard deviation, SD) and outcomes, adjusting for covariates. At baseline, mean participant age was 75.1 years, 54.9% were female, and 9.1% had depression (CES-D-10 ≥ 8). 

The PGS was significantly associated with baseline depression (OR = 1.23 [1.15–1.31]), incident depression (HR = 1.18 [1.14–1.23]) and antidepressant medication use(OR = 1.39 [1.31–1.47]). Compared with non-depressed participants, the PGS was associated with increasing severity of depression trajectory classes (sub-threshold depression OR = 1.15 [1.11–1.20], emerging depression OR = 1.22 [1.13–1.31], persistent depression OR = 1.40 [1.31–1.49]). These findings suggest that the PGS may play an important role in risk stratification for late-life depression.