Higher fibrotic content of endometriotic lesions is associated with diminished prostaglandin E2 signaling

Huang, Qingqing; Liu, Xishi; Guo, Sun‐Wei

doi:10.1002/rmb2.12423

Cited by 23 publications

(28 citation statements)

References 96 publications

(279 reference statements)

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“…Indeed, endometrial stromal cells cultured on a stiff matrix display reduced expression of COX‐2, EP2, and EP4 with or without TGF‐β1 stimulation. 28 Furthermore, the combined use of a recently established mouse model of adenomyosis 25 and a mouse model of simulated menstruation 49 lends further support for this proposal (Mao et al, in preparation).…”

Section: Discussionmentioning

confidence: 88%

“… 27 Indeed, we recently reported that, in the context of endometriosis, the expression of COX‐2 and E‐series receptor type 2 (EP2) and EP4 is reduced as endometriotic lesions became more fibrotic. 28 , 29 In addition, endometriotic stromal cells cultured in stiffer matrices demonstrate decreasing expression of COX‐2, EP2, and EP4, 28 suggesting reduced PGE 2 signaling as the extracellular matrix (ECM) becomes stiffer. As ectopic endometrium, both adenomyosis and endometriotic lesions share the same and defining hallmark of cyclic bleeding, 30 they also share similar, but not exactly identical molecular processes that underpin lesional progression owing to different microenvironment.…”

Section: Introductionmentioning

confidence: 99%

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How does the extent of fibrosis in adenomyosis lesions contribute to heavy menstrual bleeding?

Huang

Liu

Critchley

et al. 2022

Reprod Medicine & Biology

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Purpose To investigate how the extent of fibrosis in adenomyosis lesions contributes to heavy menstrual bleeding (HMB). Methods We recruited 57 women with histologically confirmed adenomyosis, 29 of whom reported moderate/heavy bleeding (MHB) (menstrual blood loss (MBL) ≥20 but <100 mL) and the remaining 28, excessive MBL (EXB; ≥100 mL). Lesional stiffness was measured by transvaginal elastosonography. Full‐thickness uterine tissue columns containing the lesion and its neighboring endometrial‐myometrial interface (EMI) and endometrial tissues were evaluated for tissue fibrosis and immunohistochemical analysis of HIF‐1α, COX‐2, EP2, and EP4. Results The lesional stiffness in the EXB group was significantly higher than that of MHB, and consistently, the extent of lesional fibrosis and the extent of tissue fibrosis in both EMI and eutopic endometrium were also significantly higher. In adenomyotic lesions and their neighboring EMI and eutopic endometrial tissues, the immunostaining of HIF‐1α, COX‐2, EP2, and EP4 was significantly reduced. The extent of fibrosis and the immunostaining levels of HIF‐1α, COX‐2, EP2, and EP4 were negatively correlated in all tissues. Conclusions Lesional fibrosis begets stiffening matrix, propagating fibrosis to neighboring EMI and eutopic endometrium, resulting in reduced PGE 2 and HIF‐1α signaling, and thus likely reduced hypoxia necessary for endometrial repair, leading to HMB.

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Section: Discussionmentioning

confidence: 88%

Section: Introductionmentioning

confidence: 99%

How does the extent of fibrosis in adenomyosis lesions contribute to heavy menstrual bleeding?

Huang

Liu

Critchley

et al. 2022

Reprod Medicine & Biology

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“…For example, on average the OE lesions in adolescents would be more likely to be cystic and less fibrotic than those in adults, which would mean that these patients would be more likely to respond to non‐steroid anti‐inflammatory drugs (NSAIDs) therapy since the PGE2 signaling is less likely to be attenuated. 97 They may also respond to therapies that target the EP2 and/or EP4 receptors. 139 In contrast, OE lesions in adults may not respond well to either NSAID treatment 97 or therapies that target the EP2 and/or EP4 receptors, 139 especially when the lesions are highly fibrotic.…”

Section: Discussionmentioning

confidence: 99%

“… 97 They may also respond to therapies that target the EP2 and/or EP4 receptors. 139 In contrast, OE lesions in adults may not respond well to either NSAID treatment 97 or therapies that target the EP2 and/or EP4 receptors, 139 especially when the lesions are highly fibrotic.…”

Section: Discussionmentioning

confidence: 99%

“… 96 As OE lesions in adolescent and adult patients display different fibrotic content, 52 older women with OE may have more reduced ovarian reserve. In addition, compared with adolescent patients, OE lesions in adult patients display reduced prostaglandin E2 (PGE2) signaling as manifested as expression of COX‐2, EP2, and EP4, concomitant with increased extent of lesional fibrosis, 97 suggesting that adolescent patients with OE may be more responsible to NSAID treatment.…”

Section: Adult Lifementioning

confidence: 99%

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Age‐dependent phenotypes of ovarian endometriomas

Benagiano

Guo

2022

Reprod Medicine & Biology

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Purpose To analyze the characteristics of the ovarian endometrioma (OE) across the life span of a woman. In the past, the OE has traditionally been viewed as a single, monolithic disease. Today, there are emerging data indicating that OE phenotypes differ according to the age of the woman. Method A narrative review of original articles on OE indexed by PubMed. Results When appearing in infancy and early adolescence , OE may be the consequence of endometrial cells retrogradely shed with neonatal uterine bleeding. The post ‐ menarcheal variant, manifesting itself during full adolescence, is singularly frequent in the presence of vaginal or uterine outflow obstructive anomalies. The typical and most frequent adult phenotype is characterized by increasing fibrosis and a tendency to progress; its mere presence exerts a detrimental effect on the surrounding healthy ovarian tissue. In postmenopause , an old lesion may be reactivated in the presence of exogenous or endogenous estrogens, or even be produced ex novo ; rarely, it can spread to a variety of organs and structures and even degenerate causing malignancies. Conclusions Given the existence of these variants, it is important to agree on management guidelines that take into consideration these different phenotypes.

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Endometriosis, the Silent Disease: Molecular Targets, Active Principles, and Drug Delivery Systems

Teworte

Luciani

2022

Helvetica Chimica Acta

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In this perspective, we provide a broad overview of pathophysiological processes involved in endometriosis, including the role of inflammation, fibrosis, angiogenesis, hormonal regulation, and genetic factors. For each of the functional changes involved with the etiology of the disease, we showcase a selection of active principles in various stages of preclinical and clinical development. Finally, we highlight the role of drug delivery for endometriosis, particularly oral vs. vaginal administration. In doing so, we wish to draw the community's attention to this debilitating disease and highlight the need for interdisciplinary approaches to endometriosis treatment development.

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Higher fibrotic content of endometriotic lesions is associated with diminished prostaglandin E2 signaling

Cited by 23 publications

References 96 publications

How does the extent of fibrosis in adenomyosis lesions contribute to heavy menstrual bleeding?

How does the extent of fibrosis in adenomyosis lesions contribute to heavy menstrual bleeding?

Age‐dependent phenotypes of ovarian endometriomas

Endometriosis, the Silent Disease: Molecular Targets, Active Principles, and Drug Delivery Systems

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