Repeated social defeat stress differently affects arthritis-associated hypersensitivity in male and female mice.

La Porta, Carmen; Palme, Rupert; Tappe-Theodor, Anke; Plum, Thomas; Mack, Matthias

doi:10.1016/j.bbi.2024.04.025

Items
Marc 21

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024	7	_	\|a 10.1016/j.bbi.2024.04.025 \|2 doi
024	7	_	\|a pmid:38663771 \|2 pmid
024	7	_	\|a 0889-1591 \|2 ISSN
024	7	_	\|a 1090-2139 \|2 ISSN
037	_	_	\|a DKFZ-2024-00879
041	_	_	\|a English
082	_	_	\|a 150
100	1	_	\|a La Porta, Carmen \|b 0
245	_	_	\|a Repeated social defeat stress differently affects arthritis-associated hypersensitivity in male and female mice.
260	_	_	\|a Orlando, Fla. \|c 2024 \|b Academic Press
336	7	_	\|a article \|2 DRIVER
336	7	_	\|a Output Types/Journal article \|2 DataCite
336	7	_	\|a Journal Article \|b journal \|m journal \|0 PUB:(DE-HGF)16 \|s 1716371028_7220 \|2 PUB:(DE-HGF)
336	7	_	\|a ARTICLE \|2 BibTeX
336	7	_	\|a JOURNAL_ARTICLE \|2 ORCID
336	7	_	\|a Journal Article \|0 0 \|2 EndNote
500	_	_	\|a 2024 Apr 23:119:572-596
520	_	_	\|a Chronic stress enhances the risk of neuropsychiatric disorders and contributes to the aggravation and chronicity of pain. The development of stress-associated diseases, including pain, is affected by individual vulnerability or resilience to stress, although the mechanisms remain elusive. We used the repeated social defeat stress model promoting susceptible and resilient phenotypes in male and female mice and induced knee mono-arthritis to investigate the impact of stress vulnerability on pain and immune system regulation. We analyzed different pain-related behaviors, measured blood cytokine and immune cell levels, and performed histological analyses at the knee joints and pain/stress-related brain areas. Stress susceptible male and female mice showed prolonged arthritis-associated hypersensitivity. Interestingly, hypersensitivity was exacerbated in male but not female mice. In males, stress promoted transiently increased neutrophils and Ly6Chigh monocytes, lasting longer in susceptible than resilient mice. While resilient male mice displayed persistently increased levels of the anti-inflammatory interleukin (IL)-10, susceptible mice showed increased levels of the pro-inflammatory IL-6 at the early- and IL-12 at the late arthritis stage. Although joint inflammation levels were comparable among groups, macrophage and neutrophil infiltration was higher in the synovium of susceptible mice. Notably, only susceptible male mice, but not females, presented microgliosis and monocyte infiltration in the prefrontal cortex at the late arthritis stage. Blood Ly6Chigh monocyte depletion during the early inflammatory phase abrogated late-stage hypersensitivity and the associated histological alterations in susceptible male mice. Thus, recruitment of blood Ly6Chigh monocytes during the early arthritis phase might be a key factor mediating the persistence of arthritis pain in susceptible male mice. Alternative neuro-immune pathways that remain to be explored might be involved in females.
536	_	_	\|a 314 - Immunologie und Krebs (POF4-314) \|0 G:(DE-HGF)POF4-314 \|c POF4-314 \|f POF IV \|x 0
588	_	_	\|a Dataset connected to CrossRef, PubMed, , Journals: inrepo02.dkfz.de
650	_	7	\|a Arthritis \|2 Other
650	_	7	\|a Cytokines \|2 Other
650	_	7	\|a Microglia \|2 Other
650	_	7	\|a Monocytes \|2 Other
650	_	7	\|a Neutrophils \|2 Other
650	_	7	\|a Pain \|2 Other
650	_	7	\|a Social defeat \|2 Other
700	1	_	\|a Plum, Thomas \|0 P:(DE-He78)3e042037287d6871eec3dbd48556b0b4 \|b 1 \|u dkfz
700	1	_	\|a Palme, Rupert \|b 2
700	1	_	\|a Mack, Matthias \|b 3
700	1	_	\|a Tappe-Theodor, Anke \|b 4
773	_	_	\|a 10.1016/j.bbi.2024.04.025 \|g p. S0889159124003726 \|0 PERI:(DE-600)1462491-6 \|p 572-596 \|t Brain, behavior and immunity \|v 119 \|y 2024 \|x 0889-1591
909	C	O	\|p VDB \|o oai:inrepo02.dkfz.de:289800
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 1 \|6 P:(DE-He78)3e042037287d6871eec3dbd48556b0b4
913	1	_	\|a DE-HGF \|b Gesundheit \|l Krebsforschung \|1 G:(DE-HGF)POF4-310 \|0 G:(DE-HGF)POF4-314 \|3 G:(DE-HGF)POF4 \|2 G:(DE-HGF)POF4-300 \|4 G:(DE-HGF)POF \|v Immunologie und Krebs \|x 0
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Marc 21

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