Site-specific gains and losses of heterochromatin accelerate the age-related neurodegeneration through the cascading destruction of KDM3B-centered epigenomic network

An, Mi-Jin; Kim, Jiyoung; Park, Jin‐Hong; Kim, Jin-Ho; Kim, Dae-Hyun; Shin, Geun-Seup; Lee, Hyun-Min; Jo, Ah-Ra; Kim, Chulhong; Kim, Mi Jin; Kim, Jeongkyu; Rhee, Sangmyung; Kim, Jung-Woong

doi:10.21203/rs.3.rs-1246914/v1

2022

DOI: 10.21203/rs.3.rs-1246914/v1

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Site-specific gains and losses of heterochromatin accelerate the age-related neurodegeneration through the cascading destruction of KDM3B-centered epigenomic network

Mi-Jin An

Jiyoung Kim²,

Jin‐Hong Park

et al.

Abstract: Epigenetic alterations explained by the “loss of heterochromatin” model have been proposed as a universal mechanism of aging, but the region-specific changes of heterochromatin during aging are unclear. Here, we examine age-dependent transcriptomic profiling of mouse retinal neurons to identify epigenetic regulators involved in heterochromatin loss. RNA sequencing analysis revealed gradual down-regulation of Kdm3b during retinal aging. Disruption of Kdm3b (Kdm3b+/-) in 12-month-old mouse retina decreased the n… Show more

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2024

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Integration of multi-modal datasets to estimate human aging

Ribeiro,

Moraes,

Moreno

et al. 2024

Mach Learn

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Aging involves complex biological processes leading to the decline of living organisms. As population lifespan increases worldwide, the importance of identifying factors underlying healthy aging has become critical. Integration of multi-modal datasets is a powerful approach for the analysis of complex biological systems, with the potential to uncover novel aging biomarkers. In this study, we leveraged publicly available epigenomic, transcriptomic and telomere length data along with histological images from the Genotype-Tissue Expression project to build tissue-specific regression models for age prediction. Using data from two tissues, lung and ovary, we aimed to compare model performance across data modalities, as well as to assess the improvement resulting from integrating multiple data types. Our results demostrate that methylation outperformed the other data modalities, with a mean absolute error of 3.36 and 4.36 in the test sets for lung and ovary, respectively. These models achieved lower error rates when compared with established state-of-the-art tissue-agnostic methylation models, emphasizing the importance of a tissue-specific approach. Additionally, this work has shown how the application of Hierarchical Image Pyramid Transformers for feature extraction significantly enhances age modeling using histological images. Finally, we evaluated the benefits of integrating multiple data modalities into a single model. Combining methylation data with other data modalities only marginally improved performance likely due to the limited number of available samples. Combining gene expression with histological features yielded more accurate age predictions compared with the individual performance of these data types. Given these results, this study shows how machine learning applications can be extended to/in multi-modal aging research. Code used is available at https://github.com/zroger49/multi_modal_age_prediction.

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Integration of multi-modal datasets to estimate human aging

Ribeiro,

Moraes,

Moreno

et al. 2024

Mach Learn

View full text Add to dashboard Cite

show abstract

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Site-specific gains and losses of heterochromatin accelerate the age-related neurodegeneration through the cascading destruction of KDM3B-centered epigenomic network

Cited by 1 publication

References 45 publications

Integration of multi-modal datasets to estimate human aging

Integration of multi-modal datasets to estimate human aging

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