Author: Xiong, Ye; Zhong, Qiong; Palmer, Tsvi; Benner, Alison; Wang, Lan; Suresh, Karthik; Damico, Rachel; D’Alessio, Franco R.
Title: Estradiol resolves pneumonia via ERβ in regulatory T cells Cord-id: pbhwqdfh Document date: 2021_2_8
ID: pbhwqdfh
Snippet: Current treatments for pneumonia (PNA) are focused on the pathogens. Mortality from PNA-induced acute lung injury (PNA-ALI) remains high, underscoring the need for additional therapeutic targets. Clinical and experimental evidence exists for potential sex differences in PNA survival, with males having higher mortality. In a model of severe pneumococcal PNA, when compared with male mice, age-matched female mice exhibited enhanced resolution characterized by decreased alveolar and lung inflammatio
Document: Current treatments for pneumonia (PNA) are focused on the pathogens. Mortality from PNA-induced acute lung injury (PNA-ALI) remains high, underscoring the need for additional therapeutic targets. Clinical and experimental evidence exists for potential sex differences in PNA survival, with males having higher mortality. In a model of severe pneumococcal PNA, when compared with male mice, age-matched female mice exhibited enhanced resolution characterized by decreased alveolar and lung inflammation and increased numbers of Tregs. Recognizing the critical role of Tregs in lung injury resolution, we evaluated whether improved outcomes in female mice were due to estradiol (E2) effects on Treg biology. E2 promoted a Treg-suppressive phenotype in vitro and resolution of PNA in vivo. Systemic rescue administration of E2 promoted resolution of PNA in male mice independent of lung bacterial clearance. E2 augmented Treg expression of Foxp3, CD25, and GATA3, an effect that required ERβ, and not ERα, signaling. Importantly, the in vivo therapeutic effects of E2 were lost in Treg-depleted mice (Foxp3(DTR) mice). Adoptive transfer of ex vivo E2-treated Tregs rescued Streptococcus pneumoniae–induce PNA-ALI, a salutary effect that required Treg ERβ expression. E2/ERβ was required for Tregs to control macrophage proinflammatory responses. Our findings support the therapeutic role for E2 in promoting resolution of lung inflammation after PNA via ERβ Tregs.
Search related documents:
Co phrase search for related documents- absence presence and active process: 1, 2, 3
- absence presence and acute ali lung injury: 1, 2, 3
- absence presence and acute ards respiratory distress syndrome: 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11
- absence presence and acute lung injury: 1, 2, 3
- absence presence and additional therapeutic target: 1
- absence presence and adoptive transfer: 1, 2
- absence presence and low expression: 1, 2, 3
- absolute number and acute ali lung injury: 1
- absolute number and acute ards respiratory distress syndrome: 1
- absolute number and acute lung injury: 1
- absolute number and adoptive transfer: 1, 2
- active process and acute ards respiratory distress syndrome: 1
- acute ali lung injury and adoptive transfer: 1
- acute ards respiratory distress syndrome and adoptive transfer: 1, 2
- acute ards respiratory distress syndrome and low expression: 1, 2, 3, 4, 5, 6, 7
- acute lung injury and adoptive transfer: 1, 2, 3
Co phrase search for related documents, hyperlinks ordered by date