The aging common marmoset's immune system: From junior to senior

Matthias Mietsch; Kristina Paqué; Charis Drummer; Christiane Stahl-Hennig; Berit Roshani

doi:10.1002/ajp.23128

The aging common marmoset's immune system: From junior to senior

Am J Primatol. 2020 Jun;82(6):e23128. doi: 10.1002/ajp.23128. Epub 2020 Apr 4.

Authors

Matthias Mietsch^{1

2}, Kristina Paqué¹, Charis Drummer³, Christiane Stahl-Hennig¹, Berit Roshani¹

Affiliations

¹ Unit of Infection Models, German Primate Center, Goettingen, Germany.
² Department of Laboratory Animal Science, German Primate Center, Goettingen, Germany.
³ Platform Degenerative Diseases, German Primate Center, Goettingen, Germany.

PMID: 32246726
DOI: 10.1002/ajp.23128

Abstract

The social, health, and economic challenges of a steadily increasing aging population demand the use of appropriate translational animal models to address questions like healthy aging, vaccination strategies, or potential interventions during the aging process. Due to their genetic proximity to humans, especially nonhuman primates (NHPs) with a relatively short generation period compared to humans, qualify as excellent animal models for these purposes. The use of common marmosets (Callithrix jacchus) in gerontology research steadily increased over the last decades, yet important information about their aging parameters are still missing. We therefore aimed to characterize their aging immune system by comprehensive flow cytometric phenotyping of blood immune cells from juvenile, adult, aging, and geriatric animals. Aged and geriatric animals displayed clear signs of immunosenescence. A decline in CD4/CD8 ratio, increased expression of HLA-DR and PD-1, higher frequencies of CD95⁺ memory cells, alterations in cytokine secretion, and a decline in the proliferative capacity proved T cell senescence in aging marmosets. Also, the B cell compartment was affected by age-related changes: while overall B cell numbers remained stable with advancing age, expression of the activation marker CD80 increased and immunoglobulin M expression decreased. Interestingly, marmoset B cell memory subset distribution rather mirrored the human situation than that of other NHP. CD21⁺ CD27^- naïve B cell frequencies decreased while those of CD21^- CD27^- tissue memory B cells increased with age. Furthermore, frequencies and numbers of NK cells as part of the innate immune system declined with advancing age. Thus, the observed immunological changes in common marmosets over their life span revealed several similarities to age-related changes in humans and encourages further studies to strengthen the common marmoset as a potential aging model.

Keywords: aging; common marmoset; immune system; immunosenescence; innate and adaptive immunity; sex.

MeSH terms

Aging / immunology*
Animals
CD4-CD8 Ratio
Callithrix / physiology*
Female
Flow Cytometry / veterinary
Immune System / physiology*
Longevity
Male
Models, Animal
Sex Factors