Macrophages inhibit and enhance endometriosis depending on their origin

Hogg, Chloe; Panir, Kavita; Dhami, Priya; Rosser, Matthew; Mack, Matthias; Soong, Daniel; Pollard, Jeffrey W.; Jenkins, Stephen J.; Horne, Andrew W; Greaves, Erin

doi:10.1073/pnas.2013776118

Cited by 59 publications

(76 citation statements)

References 44 publications

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“…Our previous study showed that SPMs polarize to M2 macrophages, whereas LPMs tend to polarize to M1 macrophages (22). Consistent with these findings, Hogg et al illustrated the protective effects of monocyte-derived LPM when the peritoneal cavity is challenged with ectopic endometrium (46). In this study, we observed that M2 macrophages were mainly differentiated from SPMs, and these macrophages were susceptible to M1NVs, whereas M2 macrophages differentiated from LPMs were not easily affected by M1NVs.…”

Section: Discussionsupporting

confidence: 89%

M1 Macrophage-Derived Nanovesicles Repolarize M2 Macrophages for Inhibiting the Development of Endometriosis

Yuan

Xue

et al. 2021

Front. Immunol.

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BackgroundEndometriosis is a common nonmalignant gynecological disorder that affects 10–15% women of reproductive age and causes several symptoms that result in decreased quality of life and a huge social burden. In recent decades, extracellular vesicles (EVs) have gained attention as a potential therapeutic tool; however, the therapeutic effects of EVs against endometriosis have not been reported. Accordingly, in this study, we investigated the feasibility of nanovesicles (NVs) derived from M1 macrophages (M1NVs) in treating endometriosis.MethodsM1NVs were prepared by serial extrusion. Co-culture assays were performed to investigate changes in tube formation and migration/invasion of eutopic endometrial stroma cells (ESCs) obtained from patients with endometriosis (EM-ESCs). A mouse model of endometriosis was established, and mice were treated with phosphate-buffered saline, M0NVs, or M1NVs to evaluate the efficacy and safety of M1NV for treating endometriosis.ResultsM1NVs directly or indirectly inhibited the migration and invasion of EM-ESCs and reduced tube formation. In the mouse model, M1NVs suppressed the development of endometriosis through reprogramming of M2 macrophages, without causing damage to the organs.ConclusionsM1NVs inhibit the development of endometriosis directly, or through repolarizing macrophages from M2 to M1 phenotype. Hence, administration of M1NVs may represent a novel method for the treatment of endometriosis.

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Section: Discussionsupporting

confidence: 89%

M1 Macrophage-Derived Nanovesicles Repolarize M2 Macrophages for Inhibiting the Development of Endometriosis

Yuan

Xue

et al. 2021

Front. Immunol.

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“…It remains unknown what is different about the lesions that progress or are maintained long-term, and future work should draw comparisons between resolving versus non-resolving mice. Recently, we identified a ‘protective’ population of monocyte-derived large peritoneal macrophages (LpM) in our menses mouse model of endometriosis that limit the development of lesions ( Hogg et al, 2021 ). Using gain- and loss-of-function experiments, we demonstrated that depletion of this population increases development of lesions, whereas reprogramming the peritoneal niche such that embryo-derived LpM are ablated and the niche is repopulated afresh with monocyte-derived LpM, leads to decreased lesion development.…”

Section: Discussionmentioning

confidence: 99%

Bioluminescent imaging in induced mouse models of endometriosis reveals differences in four model variations

Dorning

Dhami

Panir

et al. 2021

Disease Models &Amp; Mechanisms

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Our understanding of the etiology and pathophysiology of endometriosis remains limited. Disease modelling in the field is problematic as many versions of induced mouse models of endometriosis exist. We integrated bioluminescent imaging of ‘lesions’ generated using luciferase-expressing donor mice. We compared longitudinal bioluminescence and histology of lesions, sensory behavior of mice with induced endometriosis and the impact of the GnRH antagonist Cetrorelix on lesion regression and sensory behavior. Four models of endometriosis were tested. We found that the nature of the donor uterine material was a key determinant of how chronic the lesions were as well as their cellular composition. The severity of pain-like behavior also varied across models. Whilst Cetrorelix significantly reduced lesion bioluminescence in all models, it had varying impacts on pain-like behavior. Collectively, our results demonstrate key differences in the progression of the ‘disease’ across different mouse models of endometriosis. We propose that validation and testing in multiple models, each of which may be representative of the different subtypes / heterogeneity observed in women should become a standard approach to discovery science in the field of endometriosis.

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“…Among myeloid cell subpopulations, macrophages and DCs have been described as key players in endometriosis pathology 1,2,4 with reports showing endometriosis-related alterations of macrophages 26,52 and DCs 32,33 . However, a comprehensive description of myeloid sub-types that scRNAseq provides was lacking up until now.…”

Section: Discussionmentioning

confidence: 99%

Single cell analysis of endometriosis reveals a coordinated transcriptional program driving immunotolerance and angiogenesis across eutopic and ectopic tissues.

Courtois

Tan

Flynn

et al. 2021

Preprint

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Endometriosis is characterized by growth of endometrial-like tissue outside of the uterus affecting many women in their reproductive age, causing years of pelvic pain and potential infertility. Its pathophysiology remains largely unknown, limiting diagnosis and treatment. We characterized peritoneal and ovarian lesions at single-cell transcriptome resolution and compared to matched eutopic endometrium, control endometrium, and organoids derived from these tissues, generating data on over 100,000 cells across 12 individuals. We spatially localized many of the cell types using imaging mass cytometry. We identify a perivascular mural cell unique to the peritoneal lesions with dual roles in angiogenesis promotion and immune cell trafficking. We define an immunotolerant peritoneal niche, fundamental differences in eutopic endometrium and between lesions microenvironments, and a novel progenitor-like epithelial cell subpopulation. Altogether, this study provides a holistic view of the endometriosis microenvironment representing the first comprehensive cell atlas of the disease, essential information for advancing therapeutics and diagnostics.

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Macrophages inhibit and enhance endometriosis depending on their origin

Cited by 59 publications

References 44 publications

M1 Macrophage-Derived Nanovesicles Repolarize M2 Macrophages for Inhibiting the Development of Endometriosis

M1 Macrophage-Derived Nanovesicles Repolarize M2 Macrophages for Inhibiting the Development of Endometriosis

Bioluminescent imaging in induced mouse models of endometriosis reveals differences in four model variations

Single cell analysis of endometriosis reveals a coordinated transcriptional program driving immunotolerance and angiogenesis across eutopic and ectopic tissues.

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