Do uterine PTGS2, PGFS, and PTGFR expression play a role in canine uterine inertia?

Rempel, L.; Lillevang, Karina Tietgen Andresen; Straten, Ann-Kirstine thor; Friðriksdóttir, Sólrún Barbara; Körber, H.; Wehrend, Axel; Kowalewski, Mariusz P.; Reichler, Iris M; Balogh, Orsolya; Goericke-Pesch, Sandra

doi:10.1007/s00441-021-03427-6

Cited by 8 publications

(34 citation statements)

References 66 publications

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“…Similar changes in uterine mRNA expression of smooth muscle γ-actin and myosin between PUI and OD bitches [8], or in oxytocin receptor expression between dogs in labor with dystocia and undergoing elective CS [16] were found before, but not for uterine expression of prostaglandin-endoperoxidase synthase 2 and the PGF2α pathway [14]. These differences seen here may be due to abnormal labor signaling, or protracted or inadequate uterine response in PUI bitches.…”

Section: Discussionsupporting

confidence: 65%

“…Recently, advances were made in identifying defects in the contractile properties of the uterus at the cellular and molecular level. Our group showed that bitches diagnosed with PUI had higher uterine mRNA expression levels of smooth muscle γ-actin and smooth muscle myosin than dogs in labor still showing strong contractions [8], while gene expression of members of the prostaglandin (PG) F2α and PGE pathway did not differ [14,15]. Changes in uterine oxytocin receptor expression also did not seem to be implicated in the development of PUI [16].…”

Section: Introductionmentioning

confidence: 93%

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Implications of the RhoA/Rho associated kinase pathway and leptin in primary uterine inertia in the dog

Frehner

Reichler

Kowalewski

et al. 2021

Journal of Reproduction and Development

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The underlying functional and molecular changes in canine primary uterine inertia (PUI) are still not clarified. Leptin (Lep) and obesity negatively affect uterine contractility in women, partly mediated by the RhoA/Rho kinase pathway, affecting myometrial calcium sensitization. We hypothesized that increased uterine Lep/Lep receptor (LepR) or decreased RhoA/Rho kinase expression contributes to PUI in dogs, independent of obesity. Dogs presented for dystocia were grouped into PUI (n = 11) or obstructive dystocia (OD, still showing strong labor contractions; n = 7). Interplacental full-thickness uterine biopsies were collected during Cesarean section for relative gene expression (RGE) of RhoA, its effector kinases (ROCK1, ROCK2), Lep and LepR by qPCR. Protein and/or mRNA expression was evaluated by immunohistochemistry and in situ hybridization. RGE was compared between groups by one-way ANOVA using body weight as covariate with statistical significance P < 0.05. Uterine ROCK1 and ROCK2 gene expression was significantly higher in PUI than OD, while RhoA and Lep did not differ. LepR RGE was below the detection limit in 5 PUI and all OD dogs. Litter size had no influence. Lep, LepR, RhoA, ROCK1, ROCK2 protein and/or mRNA were localized in the myometrium and endometrium. Uterine protein expression appeared similar between groups. LepR mRNA signals appeared stronger in PUI than OD. In conclusion, lasting, strong labor contractions in OD resulted in downregulation of uterine ROCK1 and ROCK2, contrasting the higher expression in PUI dogs with insufficient contractions. The Lep-LepR system may affect uterine contractility in nonobese PUI dogs in a paracrine-autocrine manner.

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Section: Discussionsupporting

confidence: 65%

Section: Introductionmentioning

confidence: 93%

Implications of the RhoA/Rho associated kinase pathway and leptin in primary uterine inertia in the dog

Frehner

Reichler

Kowalewski

et al. 2021

Journal of Reproduction and Development

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“…Despite the frequent occurrence of PUI in dogs and its severe consequences for maternal and offspring survival, the exact etiology is still unknown. Up to now, only few studies have investigated its pathophysiology from a molecular biology approach looking directly at the level of the uterus [ 16 , 17 , 32 , 45 , 46 ]. As both oxytocin and progesterone are crucial hormones during parturition, we hypothesized and identified altered expression of the respective receptors as potential causes for PUI.…”

Section: Discussionmentioning

confidence: 99%

“…The significantly higher OXTR mRNA expression (ratio) in IP samples obtained from PUI (and PUI-N) dams compared to OD might be a consequence of the absence of intracervical pressure due to the fact that no puppy had been born and, thus, having insufficient systemic OXT release, as previously postulated by Tamminen et al [ 32 ]. It is worth noting that comparison of the OD and PUI samples was shown to be suitable in previous studies to gain further insight into the pathophysiology of canine dystocia and specifically PUI [ 15 , 16 , 17 , 32 , 45 , 46 ].…”

Section: Discussionmentioning

confidence: 99%

“…In contrast to this, Gogny et al [ 61 ] described a greater contractile response to OXT in the longitudinal compared to the circular myometrial layer of cyclic healthy bitches in anestrus or metestrus with and without Aglepristone treatment. Recently, our working group investigating the role of prostaglandins in PUI identified a significant difference in PTGS2 staining between myometrial layers, with PTGS2 being higher-expressed in the longitudinal layer of the same samples [ 46 ]. Taken together, all studies suggest a complex regulation of myometrial contractile activity during parturition with coordinated action of the two myometrial layers in canine uterine tissues being essential for eutocia.…”

Section: Discussionmentioning

confidence: 99%

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Involvement of Oxytocin and Progesterone Receptor Expression in the Etiology of Canine Uterine Inertia

Jungmann

Houghton

Nielsen

et al. 2022

IJMS

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An altered oxytocin and progesterone receptor (OXTR and PGR, respectively) expression was postulated in canine uterine inertia (UI), which is the lack of functional myometrial contractions. OXTR and PGR expressions were compared in uterine tissue obtained during C-section due to primary UI (PUI; n = 12) and obstructive dystocia (OD, n = 8). In PUI, the influence of litter size was studied (small/normal/large litter: PUI-S/N/L: n = 5/4/3). Staining intensity in immunohistochemistry was scored for the longitudinal and circular myometrial layer and summarized per dog (IP-Myoscore). Mean P4 did not differ significantly between PUI (n = 9) and OD (n = 7). OXTR and PGR expressions (ratios) were significantly higher in PUI (OXTR: p = 0.0019; PGR: p = 0.0339), also for OXTR in PUI-N versus OD (p = 0.0034). A trend for a higher PGR IP-Myoscore was identified (PUI-N vs. OD, p = 0.0626) as well as an influence of litter size (lowest PGR-Myoscore in PUI-L, p = 0.0391). In conclusion, PUI was not related to higher P4, but potentially increased PGR availability compared to OD. It remains to be clarified whether OXTR is upregulated in PUI due to a counterregulatory mechanism to overcome myometrial quiescence or downregulated in OD due to physiological slow OXTR desensitization associated with an advanced duration of labor. Identified OXTR differences between myometrial layers indicate the need for further research.

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Investigations on the potential role of prostaglandin E2 in canine uterine inertia

et al. 2021

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Do uterine PTGS2, PGFS, and PTGFR expression play a role in canine uterine inertia?

Cited by 8 publications

References 66 publications

Implications of the RhoA/Rho associated kinase pathway and leptin in primary uterine inertia in the dog

Implications of the RhoA/Rho associated kinase pathway and leptin in primary uterine inertia in the dog

Involvement of Oxytocin and Progesterone Receptor Expression in the Etiology of Canine Uterine Inertia

Investigations on the potential role of prostaglandin E2 in canine uterine inertia

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