Dual effect of hormones on mare reproductive physiology and dysfunction

Rebordão, Maria Rosa; Amaral, Ana; Galvão, Ana Cecília de Menezes; Szótek, A Z; Pinto‐Bravo, Pedro; Skarzynski, Dariusz J.; Ferreira‐Dias, Graça

doi:10.21836/pem20160106

Cited by 4 publications

(3 citation statements)

References 22 publications

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“…The pro‐fibrotic role ascribed to PGF 2α in lung (Olman, ), and in mare endometrium (Rebordão et al., ) was also detected in the present work. In FP, this effect was reduced by sivelestat, which was able to inhibit both COL1 transcription and pro‐fibrotic PGF 2α production.…”

Section: Discussionsupporting

confidence: 85%

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Elastase inhibition affects collagen transcription and prostaglandin secretion in mare endometrium during the estrous cycle

Amaral

Fernandes

Łukasik

et al. 2018

Reprod Domestic Animals

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Contents We have shown that bacteria induce neutrophil extracellular traps (NETs) in mare endometrium. Besides killing pathogens, NETs may contribute for endometrosis (chronic endometrium fibrosis). Since elastase (ELA) is a NETs component that regulates fibrosis and prostaglandin (PG) output, the aim was to evaluate if inhibition of ELA would affect collagen 1 (COL1) transcription and PGs secretion by endometrium explants, in different estrous cycle phases. Follicular‐FP (n = 8) and mid luteal–MLP (n = 7) phases explants were cultured for 24–48 hr with medium alone (Control), ELA (0.5 μg/ml,1 μg/ml), sivelestat ‐ ELA inhibitor (INH,10 μg/ml), or ELA (0.5 μg/ml,1 μg/ml) + INH (10 μg/ml). COL1 gene transcription was done by qRT‐PCR and PGE2 and PGF2α determination in culture medium by EIA. In FP, at 24 hr, ELA0.5 increased COL1 transcription (p < 0.001) but its inhibition (ELA0.5 + INH10) decreased COL1 transcription (p < 0.01) and PGF2α production (p < 0.05). Also, ELA0.5 + INH10 or ELA1 + INH10 raised PGE2 production (p < 0.01). At 48 hr, ELA1 increased COL1 transcription (p < 0.01) and PGF2α production (p < 0.001), but its inhibition (ELA1 + INH10) decreased these actions (p < 0.01; p < 0.05, respectively). Besides, ELA1 + INH10 incubation increased PGE2 (p < 0.05). PGF2α also augmented with ELA0.5 (p < 0.001), but lowered with ELA0.5 + INH10 (p < 0.01). In MLP, ELA0.5 up‐regulated COL1 transcription (24 hr, p < 0.01; 48 hr, p < 0.001), but ELA0.5 + INH10 decreased it (24 hr, p < 0.05; 48 hr, p < 0.001). At 48 hr, incubation with ELA1 also increased COL1 transcription and PGF2α production (p < 0.05), but PGF2α production decreased with ELA1 + INH10 incubation (p < 0.05). PGE2 production was higher in ELA1 + INH10 incubation (p < 0.05). Therefore, ELA inhibition may reduce the establishment of mare endometrial fibrosis by stimulating the production of anti‐fibrotic PGE2 and inhibiting pro‐fibrotic PGF2α.

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Section: Discussionsupporting

confidence: 85%

“…In lungs, an anti‐fibrotic effect of PGE 2 has been described (Bozyk & Moore, ), as well as in mare endometrium (Rebordão et al., ). Sivelestat increased PGE 2 and lowered COL1 transcripts in FP endometrium.…”

Section: Discussionmentioning

confidence: 99%

Elastase inhibition affects collagen transcription and prostaglandin secretion in mare endometrium during the estrous cycle

Amaral

Fernandes

Łukasik

et al. 2018

Reprod Domestic Animals

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“…In the mare, it has been long recognized the luteolytic physiological role of PGF 2α on a well-established corpus luteum. However, to the best of our knowledge no in vivo evidence of PGF 2α fibrogenic pathological effect has been reported in mare endometrium [ 68 ]. While multiple low doses of PGF 2α in early luteal phase (ELP) have antiluteogenic effects, a single dose of PGF 2α can interrupt luteal function in the MLP [ 69 ].…”

Section: Discussionmentioning

confidence: 99%

Enzymes Present in Neutrophil Extracellular Traps May Stimulate the Fibrogenic PGF2α Pathway in the Mare Endometrium

Rebordão

Amaral

Fernandes

et al. 2021

Animals

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Endometrosis, a fibrotic disease of mare endometrium, impairs uterine function. Prostaglandins (PG), despite modulating reproductive physiological functions, may also cause local pathological collagen deposition (fibrogenesis). We have previously shown that neutrophil extracellular traps (NETs) may also favor mare endometrosis. The aim of this study was to investigate the effect of enzymes present in NETs on PGF2α-pathway activation. Kenney and Doig’s type I/IIA and IIB/III mare endometria, from follicular phase (FLP) and mid-luteal (MLP) phase, were cultured in vitro in the presence of NETs enzymes (elastase, cathepsin-G or myeloperoxidase). Production of PGF2α (EIA) and transcription (qPCR) of its synthases (PTGS2, AKR1C3) and receptor (PTGFR) genes were evaluated. PGF2α and PTGFR were influenced by endometrial category and estrous cycle phase. In FLP endometrium, NETs enzymes induced both high PGF2α production and/or PTGFR transcription. In MLP type I/IIA tissues, down-regulation of PTGFR transcripts occurred. However, in MLP type IIB/III endometrium, high levels of PTGFR transcripts were induced by NETs enzymes. As PGF2α-pathway activation facilitates fibrogenesis in other tissues, PGF2α may be involved in endometrosis pathogenesis. In the mare, the endocrine microenvironment of healthy and pathological endometrium might modulate the PGF2α pathway, as well as fibrosis outcome on endometrium challenged by NETs enzymes.

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