Testicular activin and follistatin levels are elevated during the course of experimental autoimmune epididymo–orchitis in mice

Nicolas, Nour; Michel, Vera; Bhushan, Sudhanshu; Wahle, Eva; Hayward, Susan; Ludlow, Helen; Kretser, David Morritz de; Loveland, Kate; Schuppe, Hans‐Christian; Meinhardt, Andreas; Hedger, Mark P.; Fijak, Monika

doi:10.1038/srep42391

Cited by 37 publications

(41 citation statements)

References 75 publications

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“…Interestingly, in our mouse model of EAO, highly elevated numbers of CD4+ T cells, while reduced numbers of CD8+ T cells were detected, confirmed by a higher ratio of CD4+/CD8+ T cells in the testis. Moreover, a new population of double positive CD4+CD8+ T cells was identified in mouse EAO testis, previously identified in different organs with autoimmune disorders ( Nicolas et al , 2017a ). Although, the increased accumulation of various immunoregulatory T cell subtypes, such as CD4+CD25+Foxp3+, CD4+Foxp3+ and CD8+Foxp3+ T cells, has been reported in chronically inflamed rat testes, these cells were not able to suppress inflammatory responses generated by the effector T cells during the onset of EAO ( Guazzone et al , 2009 ; Fijak et al , 2011 ).…”

Section: Animal Models Of Autoimmune-based Testicular Inflammationmentioning

confidence: 91%

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Infectious, inflammatory and ‘autoimmune’ male factor infertility: how do rodent models inform clinical practice?

Fijak

Pilatz

Hedger

et al. 2018

Human Reproduction Update

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210

176

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Section: Animal Models Of Autoimmune-based Testicular Inflammationmentioning

confidence: 91%

“…Later stages of the disease are characterized by disruption of the BTB, extensive necrosis and fibrosis of seminiferous tubules ( Doncel et al , 1989 ; Lustig et al , 1993 ; Tung and Teuscher, 1995 ; Perez et al , 2012 ; Nicolas et al , 2017a ) (Fig. 3 E and F).…”

Section: Animal Models Of Autoimmune-based Testicular Inflammationmentioning

confidence: 99%

Infectious, inflammatory and ‘autoimmune’ male factor infertility: how do rodent models inform clinical practice?

Fijak

Pilatz

Hedger

et al. 2018

Human Reproduction Update

Self Cite

210

176

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show abstract

“…Affected tubules show degeneration of the germinal epithelium sparing few spermatogonia and Sertoli cells; concomitant thickening of the lamina propria may result in complete fibrosis of the tubules accompanied by increased collagen production (“tubular shadows”) ( 123 ). Notably, these are typical morphological features of experimental autoimmune orchitis (EAO) ( 124 – 127 ). Consistent with relevant animal models, infiltrating lymphocytes are primarily effector memory T cells (CD45R0+; CD4+>CD8+), which are accompanied by increased numbers of non-resident CD68+ macrophages and mast cells ( 58 , 123 , 128 – 132 ).…”

Section: Cytokines In Testicular Pathologiesmentioning

confidence: 99%

“…Besides cytokines and chemokines, other pro-inflammatory molecules, such as high-mobility group box protein 1, are involved in the regulation of inflammatory reactions in rat and human testis and might serve as targets for therapeutic intervention ( 150 ). In addition, involvement of galectin-1, activins, and inhibin in the development of testicular immunopathology is documented ( 127 , 151 – 153 ).…”

Section: Cytokines In Testicular Pathologiesmentioning

confidence: 99%

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Cytokines in Male Fertility and Reproductive Pathologies: Immunoregulation and Beyond

et al. 2017

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Germline development in vivo is dependent on the environment formed by somatic cells and the differentiation cues they provide; hence, the impact of local factors is highly relevant to the production of sperm. Knowledge of how somatic and germline cells interact is central to achieving biomedical goals relating to restoring, preserving or restricting fertility in humans. This review discusses the growing understanding of how cytokines contribute to testicular function and maintenance of male reproductive health, and to the pathologies associated with their abnormal activity in this organ. Here we consider both cytokines that signal through JAKs and are regulated by SOCS, and those utilizing other pathways, such as the MAP kinases and SMADs. The importance of cytokines in the establishment and maintenance of the testis as an immune-privilege site are described. Current research relating to the involvement of immune cells in testis development and disease is highlighted. This includes new data relating to testicular cancer which reinforce the understanding that tumorigenic cells shape their microenvironment through cytokine actions. Clinical implications in pathologies relating to local inflammation and to immunotherapies are discussed.

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Activin A and CCR2 regulate macrophage function in testicular fibrosis caused by experimental autoimmune orchitis

Peng

Kepsch

Kracht

et al. 2022

Cell. Mol. Life Sci.

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Experimental autoimmune-orchitis (EAO), a rodent model of chronic testicular inflammation and fibrosis, replicates pathogenic changes seen in some cases of human spermatogenic disturbances. During EAO, increased levels of pro-inflammatory and pro-fibrotic mediators such as TNF, CCL2, and activin A are accompanied by infiltration of leukocytes into the testicular parenchyma. Activin A levels correlate with EAO severity, while elevated CCL2 acting through its receptor CCR2 mediates leukocyte trafficking and recruits macrophages. CCR2 + CXCR4 + macrophages producing extracellular matrix proteins contribute widely to fibrogenesis. Furthermore, testicular macrophages (TMs) play a critical role in organ homeostasis. Therefore, we aimed to investigate the role of the activin A/CCL2-CCR2/macrophage axis in the development of testicular fibrosis. Following EAO induction, we observed lower levels of organ damage, collagen deposition, and leukocyte infiltration (including fibronectin+, collagen I+ and CXCR4+ TMs) in Ccr2−/− mice than in WT mice. Furthermore, levels of Il-10, Ccl2, and the activin A subunit Inhba mRNAs were lower in Ccr2−/− EAO testes. Notably, fibronectin+ TMs were also present in biopsies from patients with impaired spermatogenesis and fibrotic alterations. Overexpression of the activin A antagonist follistatin reduced tissue damage and collagen I+ TM accumulation in WT EAO testes, while treating macrophages with activin A in vitro increased the expression of Ccr2, Fn1, Cxcr4, and Mmp2 and enhanced migration along a CCL2 gradient; these effects were abolished by follistatin. Taken together, our data indicate that CCR2 and activin A promote fibrosis during testicular inflammation by regulating macrophage function. Inhibition of CCR2 or activin A protects against damage progression, offering a promising avenue for therapeutic intervention.

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Testicular activin and follistatin levels are elevated during the course of experimental autoimmune epididymo–orchitis in mice

Cited by 37 publications

References 75 publications

Infectious, inflammatory and ‘autoimmune’ male factor infertility: how do rodent models inform clinical practice?

Infectious, inflammatory and ‘autoimmune’ male factor infertility: how do rodent models inform clinical practice?

Cytokines in Male Fertility and Reproductive Pathologies: Immunoregulation and Beyond

Activin A and CCR2 regulate macrophage function in testicular fibrosis caused by experimental autoimmune orchitis

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