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Ovarian follicles are resistant to monocyte perturbations—implications for ovarian health with immune disruption
journal contribution
posted on 2021-07-01, 00:00 authored by Luba SominskyLuba Sominsky, S Younesi, S N de Luca, S M Loone, K M Quinn, S J SpencerAbstract
Monocytes and macrophages are the most abundant immune cell populations in the adult ovary, with well-known roles in ovulation and corpus luteum formation and regression. They are activated and proliferate in response to immune challenge and are suppressed by anti-inflammatory treatments. It is also likely they have a functional role in the healthy ovary in supporting the maturing follicle from the primordial through to the later stages; however, this role has been unexplored until now. Here, we utilized a Cx3cr1-Dtr transgenic Wistar rat model that allows a conditional depletion of circulating monocytes, to investigate their role in ovarian follicle health. Our findings show that circulating monocyte depletion leads to a significant depletion of ovarian monocytes and monocyte-derived macrophages. Depletion of monocytes was associated with a transient reduction in circulating anti-Müllerian hormone (AMH) at 5 days postdepletion. However, the 50–60% ovarian monocyte/macrophage depletion had no effect on ovarian follicle numbers, follicle atresia, or apoptosis, within 5–21 days postdepletion. These data reveal that the healthy adult ovary is remarkably resistant to perturbations of circulating and ovarian monocytes despite acute changes in AMH. These data suggest that short-term anti-inflammatory therapies that transiently impact on circulating monocytes are unlikely to disrupt ovarian follicle health, findings that have significant implications for fertility planning relative to the experience of an immune challenge or immunosuppression.
Monocytes and macrophages are the most abundant immune cell populations in the adult ovary, with well-known roles in ovulation and corpus luteum formation and regression. They are activated and proliferate in response to immune challenge and are suppressed by anti-inflammatory treatments. It is also likely they have a functional role in the healthy ovary in supporting the maturing follicle from the primordial through to the later stages; however, this role has been unexplored until now. Here, we utilized a Cx3cr1-Dtr transgenic Wistar rat model that allows a conditional depletion of circulating monocytes, to investigate their role in ovarian follicle health. Our findings show that circulating monocyte depletion leads to a significant depletion of ovarian monocytes and monocyte-derived macrophages. Depletion of monocytes was associated with a transient reduction in circulating anti-Müllerian hormone (AMH) at 5 days postdepletion. However, the 50–60% ovarian monocyte/macrophage depletion had no effect on ovarian follicle numbers, follicle atresia, or apoptosis, within 5–21 days postdepletion. These data reveal that the healthy adult ovary is remarkably resistant to perturbations of circulating and ovarian monocytes despite acute changes in AMH. These data suggest that short-term anti-inflammatory therapies that transiently impact on circulating monocytes are unlikely to disrupt ovarian follicle health, findings that have significant implications for fertility planning relative to the experience of an immune challenge or immunosuppression.
History
Journal
Biology of ReproductionVolume
105Issue
1Pagination
100 - 112Publisher
OXFORD UNIV PRESS INCLocation
United StatesPublisher DOI
ISSN
0006-3363eISSN
1529-7268Language
EnglishPublication classification
C1 Refereed article in a scholarly journalUsage metrics
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Categories
Keywords
Science & TechnologyLife Sciences & BiomedicineReproductive BiologymonocytesmacrophagesCx3cr1-Dtr ratovaryfollicle healthAMHANTI-MULLERIAN-HORMONENONSTEROIDAL ANTIINFLAMMATORY DRUGSCORPUS-LUTEUMINFLAMMATORY PATHWAYSLEUKOCYTE SUBSETSGROWTH-FACTORSSHORT-TERMLOCALIZATIONEXPRESSIONRECRUITMENT\n Cx3cr1-Dtr rat