In-depth human immune cellular profiling from newborn to frail

Author:

Li Wangchun1,Liu Hangyu23,Gao Lijuan23,Hu Yang4,Zhang Anna1,Li Wenfeng1,Liu Guolong5ORCID,Bai Weibin6,Xu Yudai23,Xiao Chanchan23,Deng Jieping37,Lei Wen38,Chen Guobing239ORCID

Affiliation:

1. Intensive Care Unit, Affiliated Shunde Hospital, Jinan University , No.50, East Guizhou Avenue, Foshan 528000 , China

2. Institute of Geriatric Immunology, Department of Microbiology and Immunology, School of Medicine, Jinan University , No.601, West Huangpu Avenue, Tianhe District, Guangzhou 510632 , China

3. Guangdong-Hong Kong-Macau Great Bay Area Geroscience Joint Laboratory, Jinan University , No.601, West Huangpu Avenue, Tianhe District, Guangzhou 510632 , China

4. NHC Key Laboratory of Male Reproduction and Genetics, Guangdong Provincial Reproductive Science Institute, Guangdong Provincial Fertility Hospital , No.17, Meidong Road, Yuexiu District, Guangzhou 510632 , China

5. Department of Medical Oncology, the Second Affiliated Hospital, School of Medicine, South China University of Technology , No.1, Panfu Road, Yuexiu District, Guangzhou 510180 , China

6. Department of Food Science and Engineering, Guangdong Engineering Technology Center of Food Safety Molecular Rapid Detection, Institute of Food Safety and Nutrition, Jinan University, No.601, West Huangpu Avenue, Tianhe District , Guangzhou 510632 , China

7. Department of Systems Biomedical Sciences, School of Medicine, Jinan University, No.601, West Huangpu Avenue, Tianhe District , Guangzhou 510632 , China

8. Integrated Chinese and Western Medicine Postdoctoral Research Station, Guangdong Second Provincial General Hospital, School of Medicine, Jinan University , No.466, Xingang Middle Road, Haizhu District, Guangzhou 510632 , China

9. Key Laboratory of Viral Pathogenesis and Infection Prevention and Control, Jinan University, Ministry of Education, No.601, West Huangpu Avenue, Tianhe District , Guangzhou, 510632 , China

Abstract

Abstract Immune functional decline and remodeling accompany aging and frailty. It is still largely unknown how changes in the immune cellular composition differentiate healthy individuals from those who become frail at a relatively early age. Our aim in this exploratory study was to investigate immunological changes from newborn to frailty and the association between health statute and various immune cell subtypes. The participants analyzed in this study covered human cord blood cells and peripheral blood cells collected from young adults and healthy and frail old individuals. A total of 30 immune cell subsets were performed by flow cytometry based on the surface markers of immune cells. Furthermore, frailty was investigated for its relations with various leukocyte subpopulations. Frail individuals exhibited a higher CD4/CD8 ratio; a higher proportion of CD4+ central memory T cells, CD8+ effector memory T cells, CD27− switched memory B (BSM) cells, CD27+ BSM cells, age-associated B cells, and CD38−CD24− B cells; and a lower proportion of naïve CD8+ T cells and progenitor B cells. The frailty index score was found to be associated with naïve T cells, CD4/CD8 ratio, age-associated B cells, CD27− BSM cells, and CD4+ central memory T cells. Our findings conducted a relatively comprehensive and extensive atlas of age- and frailty-related changes in peripheral leukocyte subpopulations from newborn to frailty. The immune phenotypes identified in this study can contribute to a deeper understanding of immunosenescence in frailty and may provide a rationale for future interventions and diagnosis.

Publisher

Oxford University Press (OUP)

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