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dc.contributor.authorJackaman, Connie
dc.contributor.authorRadley-Crabb, Hannah
dc.contributor.authorSoffe, Z.
dc.contributor.authorShavlakadze, T.
dc.contributor.authorGrounds, M.
dc.contributor.authorNelson, Delia
dc.date.accessioned2017-01-30T15:15:40Z
dc.date.available2017-01-30T15:15:40Z
dc.date.created2013-08-01T20:00:19Z
dc.date.issued2013
dc.identifier.citationJackaman, Connie and Radley-Crabb, Hannah G. and Soffe, Zoe and Shavlakadze, Tea and Grounds, Miranda D. and Nelson, Delia J. 2013. Targeting macrophages rescues age-related immune deficiencies in C57BL/6J geriatric mice. Aging Cell. 12 (3): pp. 345-357.
dc.identifier.urihttp://hdl.handle.net/20.500.11937/44664
dc.identifier.doi10.1111/acel.12062
dc.description.abstract

Changes to innate cells, such as macrophages and myeloid-derived suppressor cells (MDSCs), during aging in healthy or tumor-bearing hosts are not well understood. We compared macrophage subpopulations and MDSCs from healthy young (6–8 weeks) C57BL/6J mice to those from healthy geriatric (24–28 months) mice. Spleens, lymph nodes, and bone marrow of geriatric hosts contained significantly more M2 macrophages and MDSCs than their younger counterparts. Peritoneal macrophages from geriatric, but not young, mice co-expressed CD40 and CX3CR1 that are usually mutually exclusively expressed by M1 or M2 macrophages. Nonetheless, macrophages from geriatric mice responded to M1 or M2 stimuli similarly to macrophages from young mice, although they secreted higher levels of TGF-β in response to IL-4. We mimicked conditions that may occur within tumors by exposing macrophages from young vs. geriatric mice to mesothelioma or lung carcinoma tumor cell–derived supernatants. While both supernatants skewed macrophages toward the M2-phenotype regardless of age, only geriatric-derived macrophages produced IL-4, suggesting a more immunosuppressive tumor microenvironment will be established in the elderly. Both geriatric- and young-derived macrophages induced allogeneic T-cell proliferation, regardless of the stimuli used, including tumor supernatant. However, only macrophages from young mice induced T-cell IFN-γ production. We examined the potential of an IL-2/agonist anti-CD40 antibody immunotherapy that eradicates large tumors in young hosts to activate macrophages from geriatric mice. IL-2-/CD40-activated macrophages rescued T-cell production of IFN-γ in geriatric mice. Therefore, targeting macrophages with IL-2/anti-CD40 antibody may improve innate and T-cell immunity in aging hosts.

dc.publisherWiley-Blackwell
dc.subjectinterleukin-2
dc.subjectcancer immunotherapy
dc.subjectmacrophage
dc.subjectCD40
dc.subjectaging
dc.titleTargeting macrophages rescues age-related immune deficiencies in C57BL/6J geriatric mice
dc.typeJournal Article
dcterms.source.volume12
dcterms.source.number3
dcterms.source.startPage345
dcterms.source.endPage357
dcterms.source.issn14749726
dcterms.source.titleAging Cell
curtin.department
curtin.accessStatusOpen access via publisher


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