Your search keyword '"Kochetov, Kirill"' showing total 3 results

1. Blood Biochemistry Analysis to Detect Smoking Status and Quantify Accelerated Aging in Smokers

Author

Mamoshina, Polina, Kochetov, Kirill, Cortese, Franco, Kovalchuk, Anna, Aliper, Alexander, Putin, Evgeny, Scheibye-Knudsen, Morten, Cantor, Charles R., Skjodt, Neil M., Kovalchuk, Olga, and Zhavoronkov, Alex

Published

2019

2. DeepMAge: A Methylation Aging Clock Developed with Deep Learning.

Author

Galkin, Fedor, Mamoshina, Polina, Kochetov, Kirill, Sidorenko, Denis, and Zhavoronkov, Alex

Subjects

DNA methylation, AGING, METHYLATION, EPIGENETICS, ARTIFICIAL intelligence

Abstract

DNA methylation aging clocks have become an invaluable tool in biogerontology research since their inception in 2013. Today, a variety of machine learning approaches have been tested for the purpose of predicting human age based on molecular-level features. Among these, deep learning, or neural networks, is an especially promising approach that has been used to construct accurate clocks using blood biochemistry, transcriptomics, and microbiomics data-feats unachieved by other algorithms. In this article, we explore how deep learning performs in a DNA methylation setting and compare it to the current industry standard-the 353 CpG clock published in 2013. The aging clock we are presenting (DeepMAge) is a neural network regressor trained on 4,930 blood DNA methylation profiles from 17 studies. Its absolute median error was 2.77 years in an independent verification set of 1,293 samples from 15 studies. DeepMAge shows biological relevance by assigning a higher predicted age to people with various health-related conditions, such as ovarian cancer, irritable bowel diseases, and multiple sclerosis. [ABSTRACT FROM AUTHOR]

Published

2021

3. Population Specific Biomarkers of Human Aging: A Big Data Study Using South Korean, Canadian, and Eastern European Patient Populations.

Author

Mamoshina, Polina, Kochetov, Kirill, Putin, Evgeny, Cortese, Franco, Aliper, Alexander, Lee, Won-Suk, Ahn, Sung-Min, Uhn, Lee, Skjodt, Neil, Kovalchuk, Olga, Scheibye-Knudsen, Morten, and Zhavoronkov, Alex

Subjects

*AGING prevention, *BIOLOGICAL tags, *GERONTOLOGY, *BIOCHEMISTRY, *MACHINE learning

Abstract

Accurate and physiologically meaningful biomarkers for human aging are key to assessing antiaging therapies. Given ethnic differences in health, diet, lifestyle, behavior, environmental exposures, and even average rate of biological aging, it stands to reason that aging clocks trained on datasets obtained from specific ethnic populations are more likely to account for these potential confounding factors, resulting in an enhanced capacity to predict chronological age and quantify biological age. Here, we present a deep learning-based hematological aging clock modeled using the large combined dataset of Canadian, South Korean, and Eastern European population blood samples that show increased predictive accuracy in individual populations compared to population specific hematologic aging clocks. The performance of models was also evaluated on publicly available samples of the American population from the National Health and Nutrition Examination Survey (NHANES). In addition, we explored the association between age predicted by both population specific and combined hematological clocks and all-cause mortality. Overall, this study suggests (a) the population specificity of aging patterns and (b) hematologic clocks predicts all-cause mortality. The proposed models were added to the freely-available Aging.AI system expanding the range of tools for analysis of human aging. [ABSTRACT FROM AUTHOR]

Published

2018