| Literature DB >> 30842675 |
Ayelet Alpert1, Yishai Pickman1, Michael Leipold2, Yael Rosenberg-Hasson2, Xuhuai Ji2, Renaud Gaujoux1,3, Hadas Rabani1, Elina Starosvetsky1, Ksenya Kveler1, Steven Schaffert2,4, David Furman2, Oren Caspi1,5, Uri Rosenschein1,6, Purvesh Khatri2,4, Cornelia L Dekker2,7, Holden T Maecker2,8, Mark M Davis9,10,11, Shai S Shen-Orr12.
Abstract
Immune responses generally decline with age. However, the dynamics of this process at the individual level have not been characterized, hindering quantification of an individual's immune age. Here, we use multiple 'omics' technologies to capture population- and individual-level changes in the human immune system of 135 healthy adult individuals of different ages sampled longitudinally over a nine-year period. We observed high inter-individual variability in the rates of change of cellular frequencies that was dictated by their baseline values, allowing identification of steady-state levels toward which a cell subset converged and the ordered convergence of multiple cell subsets toward an older adult homeostasis. These data form a high-dimensional trajectory of immune aging (IMM-AGE) that describes a person's immune status better than chronological age. We show that the IMM-AGE score predicted all-cause mortality beyond well-established risk factors in the Framingham Heart Study, establishing its potential use in clinics for identification of patients at risk.Entities:
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Year: 2019 PMID: 30842675 PMCID: PMC6686855 DOI: 10.1038/s41591-019-0381-y
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440