A novel Foxn1<sup>eGFP/+</sup> mouse model identifies Bmp4‐induced maintenance of <i>Foxn1</i> expression and thymic epithelial progenitor populations

Barsanti, Marco; Lim, Joanna; Hun, Michael L.; Lister, Natalie; Wong, Kahlia; Hammett, Maree Vanessa; Lepletier, Ailin; Boyd, Richard; Giudice, Antonietta; Chidgey, Ann Patricia

doi:10.1002/eji.201646553

Cited by 28 publications

(32 citation statements)

References 46 publications

(111 reference statements)

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“…The post-pubertal increase in Bmp4 expression by supporting stromal cells was, however, greater in females, and implicates better progenitor maintenance. Its receptor, Bmpr2, is primarily expressed on cTEC lo and mTEC lo progenitors (42), and was proposed to have a role in maintaining progenitor populations at the expense of differentiation (10). However, Bmp4 induced self-renewal of progenitors may also have a role in thymus regeneration following damage, as demonstrated following irradiation (43).…”

Section: Discussionmentioning

confidence: 99%

Gender Disparity Impacts on Thymus Aging and LHRH Receptor Antagonist-Induced Thymic Reconstitution Following Chemotherapeutic Damage

et al. 2020

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One of the main consequences of thymus aging is the decrease in naïve T cell output. This condition accelerates at the onset of puberty, and presents as a major clinical complication for cancer patients who require cytoablative therapy. Specifically, the extensive use of chemotherapeutics, such as cyclophosphamide, in such treatments damage thymic structure and eliminate the existing naïve T cell repertoire. The resulting immunodeficiency can lead to increased incidence of opportunistic infections, tumor growth relapse and/or autoimmune diseases, particularly in older patients. Thus, strategies aimed at rejuvenating the aged thymus following chemotherapeutic damage are required. Previous studies have revealed that sex hormone deprivation in male mice is capable of regenerating the thymic microenvironment following chemotherapy treatment, however, further investigation is crucial to identify gender-based differences, and the molecular mechanisms involved during thymus regeneration. Through phenotypic analyzes, we identified gender-specific alterations in thymocytes and thymic epithelial cell (TEC) subsets from the onset of puberty. By middle-age, females presented with a higher number of thymocytes in comparison to males, yet a decrease in their Aire + medullary TEC/thymocyte ratio was observed. This reduction could be associated with an increased risk of autoimmune disease in middle-aged women. Given the concurrent increase in female Aire + cTEC/thymocyte ratio, we proposed that there may be an impediment in Aire + mTEC hi differentiation, and Aire + cTEC hi as its upstream precursor. The regenerative effects of LHRH receptor antagonist, degarelix, on TEC subsets was also less pronounced in middle-aged females compared to males, possibly due to slower progression of thymic involution in the former, which presented with greater TEC hi proportions. Furthermore, following cyclophosphamide treatment, degarelix enhanced thymocyte and mature TEC subset recovery, with faster recovery kinetics observed in females. These events were found to involve both reactivation and proliferation of thymic epithelial progenitor cells. Taken together, the findings from this study portray Hun et al. Gender Disparity in the Aging Thymus a relationship between gender disparity and thymus aging, and highlight the potential benefits of LHRH receptor antagonist treatment for thymic regeneration. Further research is required, however, to determine how gender may impact on the mechanisms underpinning these events.

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Section: Discussionmentioning

confidence: 99%

Gender Disparity Impacts on Thymus Aging and LHRH Receptor Antagonist-Induced Thymic Reconstitution Following Chemotherapeutic Damage

et al. 2020

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“…Furthermore, endogenous regeneration following thymic damage was shown to involve TEC stimulation by endothelial cell-derived BMP4, which subsequently increased FOXN1 expression (Wertheimer et al, 2018). TEC expression of the BMP4 receptor BMPR2 was predominantly in TEPCs, Sca-1 lo cTEC lo precursors, and mTEC lo precursors of 7-week-old mice (Barsanti et al, 2017). Although the majority of BMP4 production in the adult thymus is derived from fibroblasts and endothelial cells (Barsanti et al, 2017), in addition to an increase in fibroblast BMP4 expression with aging, we identified increased BMP4 expression by TECs ( Figure 3F).…”

Section: Reduction In Medullary Epithelia and Tepc Differentiation Wimentioning

confidence: 86%

“…We have previously shown that BMP4 supplementation of in vitro 3D postnatal TEC cultures maintained cTEC lo and mTEC lo precursors at the expense of differentiation into their mature counterparts (Barsanti et al, 2017). Furthermore, endogenous regeneration following thymic damage was shown to involve TEC stimulation by endothelial cell-derived BMP4, which subsequently increased FOXN1 expression (Wertheimer et al, 2018).…”

Section: Reduction In Medullary Epithelia and Tepc Differentiation Wimentioning

confidence: 98%

Interplay between Follistatin, Activin A and Bmp4 Signaling Regulates Postnatal Thymic Epithelial Progenitor Cell Differentiation During Aging

et al. 2018

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“…Transgenic expression of Noggin under the control of a FoxN1 promoter leads to a hypoplastic spheric thymus always containing big cystic structures [125]. These structural alterations seem to be the result of a branching defect in consonance with the known role of BMP signaling in regulating branching morphogenesis of different organs [26] and to affect Foxn1 expression [147]. Figure 2.…”

Section: After Acquisition Of Thymus Fate Thymic Primordium Undergoementioning

confidence: 98%

Epithelial Development Based on a Branching Morphogenesis Program: The Special Condition of Thymic Epithelium

Múñoz¹,

Zapata²

2019

Histology

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Numerous epithelia undergo tubulogenesis and branching morphogenesis during their development (i.e., lung, salivary gland, pancreas) in order to establish sufficient available surface for their proper functioning. The thymus is a primary lymphoid organ constituted by pharyngeal-derived epithelium necessary to produce immunocompetent lymphocytes whose mechanisms of development are not fully known. In the current chapter, we review histological, cellular, and molecular mechanisms governing early thymic epithelium development emphasizing its resemblance with the process of branching morphogenesis and tubulogenesis occurring in other epithelial organs in which epithelial-mesenchyme interactions determine the tissue patterning through specific combinations of common molecular signaling pathways.

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A novel Foxn1^eGFP/+ mouse model identifies Bmp4‐induced maintenance of Foxn1 expression and thymic epithelial progenitor populations

Cited by 28 publications

References 46 publications

Gender Disparity Impacts on Thymus Aging and LHRH Receptor Antagonist-Induced Thymic Reconstitution Following Chemotherapeutic Damage

Gender Disparity Impacts on Thymus Aging and LHRH Receptor Antagonist-Induced Thymic Reconstitution Following Chemotherapeutic Damage

Interplay between Follistatin, Activin A and Bmp4 Signaling Regulates Postnatal Thymic Epithelial Progenitor Cell Differentiation During Aging

Epithelial Development Based on a Branching Morphogenesis Program: The Special Condition of Thymic Epithelium

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A novel Foxn1eGFP/+ mouse model identifies Bmp4‐induced maintenance of Foxn1 expression and thymic epithelial progenitor populations

Cited by 28 publications

References 46 publications

Gender Disparity Impacts on Thymus Aging and LHRH Receptor Antagonist-Induced Thymic Reconstitution Following Chemotherapeutic Damage

Gender Disparity Impacts on Thymus Aging and LHRH Receptor Antagonist-Induced Thymic Reconstitution Following Chemotherapeutic Damage

Interplay between Follistatin, Activin A and Bmp4 Signaling Regulates Postnatal Thymic Epithelial Progenitor Cell Differentiation During Aging

Epithelial Development Based on a Branching Morphogenesis Program: The Special Condition of Thymic Epithelium

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A novel Foxn1^eGFP/+ mouse model identifies Bmp4‐induced maintenance of Foxn1 expression and thymic epithelial progenitor populations