Biological age and immunosenescence in Colombian centenarians

Juan Manuel Anaya; Edward A. Ruiz-Narváez; Ivan David Lozada-Martinez; Manuel Rojas; Diana M. Monsalve; Jesús Armando Álvarez-Álvarez; María José Díaz Gutiérrez; Olianis Pájaro; Brenda Guerra; Juan Esteban Gallo; Isaura Torres; Carolina Ramírez-Santana; Andres Angelo Cadena Bonfanti; Yeny Acosta-Ampudia

doi:10.1038/s41514-026-00340-6

Biological age and immunosenescence in Colombian centenarians

Juan Manuel Anaya
, Edward A. Ruiz-Narváez
, Ivan David Lozada-Martinez
, Manuel Rojas
, Diana M. Monsalve
, Jesús Armando Álvarez-Álvarez
, María José Díaz Gutiérrez
, Olianis Pájaro
, Brenda Guerra
, Juan Esteban Gallo
, Isaura Torres
, Carolina Ramírez-Santana
, Andres Angelo Cadena Bonfanti
, Yeny Acosta-Ampudia

Escuela de Medicina y Ciencias de la Salud

Producción científica: Contribución a revista › Artículo de Investigación › revisión exhaustiva

1 Cita (Scopus)

Resumen

Biological aging and immunosenescence are central to longevity, yet their interplay in centenarians remains unclear. We conducted a cross-sectional study in 160 Colombian centenarians to examine associations between biological age (PhenoAge), immunosenescence and age-related clinical variables. Cytokine profiling (n = 114) and lymphocyte immunophenotyping (n = 42) were assessed. It was observed that better QoL and well-being were significantly associated with lower biological age, while depressive symptoms, prior tobacco use, elevated levels of RANTES and G-CSF as well as a distinct CD8+ T cell phenotype including greater CD27− CD28+ central memory, effector memory, and KLRG1− CD57+ terminally differentiated effector memory T cells (TEMRA), and fewer KLRG1+ CD57+ TEMRA cells were linked to higher biological age. Centenarians were classified into three categories: vigorous (10%), resilient (46.25%), and vulnerable (43.75%). Cytokine levels were similar across the groups. These findings challenge the notion of immunosenescence in centenarians and highlight the value of translational research in geroscience.

Idioma original	Inglés estadounidense
Número de artículo	60
Publicación	npj Aging
Volumen	12
N.º	1
DOI	https://doi.org/10.1038/s41514-026-00340-6
Estado	Publicada - dic. 2026

ODS de las Naciones Unidas

Este resultado contribuye a los siguientes Objetivos de Desarrollo Sostenible

ODS 3: Salud y bienestar

Áreas temáticas de ASJC Scopus

Estudio del envejecimiento
Geriatría y gerontología

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Anaya, J. M., Ruiz-Narváez, E. A., Lozada-Martinez, I. D., Rojas, M., Monsalve, D. M., Álvarez-Álvarez, J. A., Gutiérrez, M. J. D., Pájaro, O., Guerra, B., Gallo, J. E., Torres, I., Ramírez-Santana, C., Bonfanti, A. A. C., & Acosta-Ampudia, Y. (2026). Biological age and immunosenescence in Colombian centenarians. npj Aging, 12(1), Artículo 60. https://doi.org/10.1038/s41514-026-00340-6

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title = "Biological age and immunosenescence in Colombian centenarians",

abstract = "Biological aging and immunosenescence are central to longevity, yet their interplay in centenarians remains unclear. We conducted a cross-sectional study in 160 Colombian centenarians to examine associations between biological age (PhenoAge), immunosenescence and age-related clinical variables. Cytokine profiling (n = 114) and lymphocyte immunophenotyping (n = 42) were assessed. It was observed that better QoL and well-being were significantly associated with lower biological age, while depressive symptoms, prior tobacco use, elevated levels of RANTES and G-CSF as well as a distinct CD8+ T cell phenotype including greater CD27− CD28+ central memory, effector memory, and KLRG1− CD57+ terminally differentiated effector memory T cells (TEMRA), and fewer KLRG1+ CD57+ TEMRA cells were linked to higher biological age. Centenarians were classified into three categories: vigorous (10\%), resilient (46.25\%), and vulnerable (43.75\%). Cytokine levels were similar across the groups. These findings challenge the notion of immunosenescence in centenarians and highlight the value of translational research in geroscience.",

author = "Anaya, \{Juan Manuel\} and Ruiz-Narv{\'a}ez, \{Edward A.\} and Lozada-Martinez, \{Ivan David\} and Manuel Rojas and Monsalve, \{Diana M.\} and {\'A}lvarez-{\'A}lvarez, \{Jes{\'u}s Armando\} and Guti{\'e}rrez, \{Mar{\'i}a Jos{\'e} D{\'i}az\} and Olianis P{\'a}jaro and Brenda Guerra and Gallo, \{Juan Esteban\} and Isaura Torres and Carolina Ram{\'i}rez-Santana and Bonfanti, \{Andres Angelo Cadena\} and Yeny Acosta-Ampudia",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2026.",

year = "2026",

month = dec,

doi = "10.1038/s41514-026-00340-6",

language = "English (US)",

volume = "12",

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AU - Anaya, Juan Manuel

AU - Ruiz-Narváez, Edward A.

AU - Lozada-Martinez, Ivan David

AU - Rojas, Manuel

AU - Monsalve, Diana M.

AU - Álvarez-Álvarez, Jesús Armando

AU - Gutiérrez, María José Díaz

AU - Pájaro, Olianis

AU - Guerra, Brenda

AU - Gallo, Juan Esteban

AU - Torres, Isaura

AU - Ramírez-Santana, Carolina

AU - Bonfanti, Andres Angelo Cadena

AU - Acosta-Ampudia, Yeny

PY - 2026/12

Y1 - 2026/12

N2 - Biological aging and immunosenescence are central to longevity, yet their interplay in centenarians remains unclear. We conducted a cross-sectional study in 160 Colombian centenarians to examine associations between biological age (PhenoAge), immunosenescence and age-related clinical variables. Cytokine profiling (n = 114) and lymphocyte immunophenotyping (n = 42) were assessed. It was observed that better QoL and well-being were significantly associated with lower biological age, while depressive symptoms, prior tobacco use, elevated levels of RANTES and G-CSF as well as a distinct CD8+ T cell phenotype including greater CD27− CD28+ central memory, effector memory, and KLRG1− CD57+ terminally differentiated effector memory T cells (TEMRA), and fewer KLRG1+ CD57+ TEMRA cells were linked to higher biological age. Centenarians were classified into three categories: vigorous (10%), resilient (46.25%), and vulnerable (43.75%). Cytokine levels were similar across the groups. These findings challenge the notion of immunosenescence in centenarians and highlight the value of translational research in geroscience.

AB - Biological aging and immunosenescence are central to longevity, yet their interplay in centenarians remains unclear. We conducted a cross-sectional study in 160 Colombian centenarians to examine associations between biological age (PhenoAge), immunosenescence and age-related clinical variables. Cytokine profiling (n = 114) and lymphocyte immunophenotyping (n = 42) were assessed. It was observed that better QoL and well-being were significantly associated with lower biological age, while depressive symptoms, prior tobacco use, elevated levels of RANTES and G-CSF as well as a distinct CD8+ T cell phenotype including greater CD27− CD28+ central memory, effector memory, and KLRG1− CD57+ terminally differentiated effector memory T cells (TEMRA), and fewer KLRG1+ CD57+ TEMRA cells were linked to higher biological age. Centenarians were classified into three categories: vigorous (10%), resilient (46.25%), and vulnerable (43.75%). Cytokine levels were similar across the groups. These findings challenge the notion of immunosenescence in centenarians and highlight the value of translational research in geroscience.

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DO - 10.1038/s41514-026-00340-6

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Biological age and immunosenescence in Colombian centenarians

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