Differential effects of young and old hematopoietic stem cell niches on bone marrow-derived dendritic cells.

IF 5.6 2区医学 Q1 GERIATRICS & GERONTOLOGY

Immunity & Ageing Pub Date : 2025-07-03 DOI:10.1186/s12979-025-00517-9

Patrik Milić, Mojca Justin Kjuder, Katerina Jazbec Gradišar, Urban Švajger, Primož Rožman

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Abstract

Background: Aging is linked to various dysfunctions of the immune system, including the decline of its primary developmental source: the hematopoietic stem cell (HSC) niche. This decline leads to chronic inflammation, increased vulnerability to infections, cancer, autoimmune diseases, and reduced vaccine efficacy. As individuals age, the HSC niche undergoes significant changes, including greater adipocyte accumulation and alterations in the molecular microenvironment, which may influence the development and function of immune cells. Among these cells, the impact of the aging HSC niche on dendritic cell (DC) function is less understood. Heterochronic autologous HSC transplantation is a promising intervention to prevent age-related disorders, contributing to the extension of healthspan and longevity, however, several murine experiments failed to produce the expected results, which led us to presume that the problem lies within the old HSC niche. Therefore, we created in vitro models of young and old HSC niches and examined how these microenvironments affect the differentiation and maturation and functionality of BM-derived DCs (BMDCs).

Results: An analysis of the conditioned media from young and aged HSC niches revealed that the environment of aged niches exhibited an increased presence of adiponectin. This media was subsequently utilized in BMDC differentiation and maturation protocols, with their effects closely monitored. Our results indicate that the old HSC niche microenvironment promotes premature BMDC activation, characterized by elevated MHC class II expression and enhanced allostimulatory capacity of BMDCs at their immature stage. Additionally, LPS stimulation of BMDCs, used to induce DC maturation, significantly increased CD86 expression on BMDCs from the aged niche. However, these cells did not show superior allostimulatory capacity compared to their counterparts from the young niche environment. By analyzing the BMDC cytokine profile, we observed that when cultured in aged niche-conditioned media, the BMDCs secreted significantly higher levels of IL-6, indicating a heightened proinflammatory activation state.

Conclusions: Collectively, our findings suggest that aging-related changes within the HSC niche can considerably alter DC functionality by disrupting their normal development from BM precursors. These results emphasize the significance of this phenomenon and its implications for immunosenescence.

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年轻和年老造血干细胞壁龛对骨髓来源的树突状细胞的不同影响。

背景：衰老与免疫系统的各种功能障碍有关，包括其主要发育来源：造血干细胞（HSC）生态位的下降。这种下降会导致慢性炎症，增加对感染、癌症、自身免疫性疾病的易感性，并降低疫苗效力。随着个体年龄的增长，HSC生态位会发生显著变化，包括脂肪细胞的积累和分子微环境的改变，这可能会影响免疫细胞的发育和功能。在这些细胞中，老化的HSC生态位对树突状细胞（DC）功能的影响尚不清楚。异慢性自体HSC移植是一种很有前途的干预措施，可以预防年龄相关疾病，有助于延长健康寿命和寿命，然而，一些小鼠实验未能产生预期的结果，这使我们假设问题出在旧的HSC生态位上。因此，我们建立了年轻和年老HSC生态位的体外模型，并研究了这些微环境如何影响脑源性dc （bmdc）的分化、成熟和功能。结果：对来自年轻和老年HSC生态位的条件培养基的分析显示，老年生态位的环境显示出脂肪联素的增加。该培养基随后用于BMDC分化和成熟方案，并密切监测其效果。我们的研究结果表明，旧的HSC生态位微环境促进BMDC过早激活，其特征是MHC II类表达升高和BMDC在未成熟阶段的异源刺激能力增强。此外，用于诱导DC成熟的脂多糖刺激BMDCs显著增加了老年生态位BMDCs上CD86的表达。然而，与来自年轻生态位环境的细胞相比，这些细胞并没有表现出优越的异源刺激能力。通过分析BMDC细胞因子谱，我们观察到，当在年龄较大的壁龛条件培养基中培养时，BMDC分泌的IL-6水平显著升高，表明促炎激活状态升高。结论：总的来说，我们的研究结果表明，HSC生态位中与年龄相关的变化可以通过破坏它们从BM前体正常发育而显著改变DC功能。这些结果强调了这一现象的重要性及其对免疫衰老的影响。

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来源期刊

Immunity & Ageing GERIATRICS & GERONTOLOGY-IMMUNOLOGY

CiteScore

10.20

自引率

3.80%

发文量

期刊介绍： Immunity & Ageing is a specialist open access journal that was first published in 2004. The journal focuses on the impact of ageing on immune systems, the influence of aged immune systems on organismal well-being and longevity, age-associated diseases with immune etiology, and potential immune interventions to increase health span. All articles published in Immunity & Ageing are indexed in the following databases: Biological Abstracts, BIOSIS, CAS, Citebase, DOAJ, Embase, Google Scholar, Journal Citation Reports/Science Edition, OAIster, PubMed, PubMed Central, Science Citation Index Expanded, SCImago, Scopus, SOCOLAR, and Zetoc.