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Interplay between Misplaced Müllerian-Derived Stem Cells and Peritoneal Immune Dysregulation in the Pathogenesis of Endometriosis

机译:子宫内膜异位症发病机制中错位的苗勒氏干细胞与腹膜免疫失调之间的相互作用

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摘要

In the genetic regulation of Müllerian structures development, a key role is played by Hoxa and Wnt clusters, because they lead the transcription of different genes according to the different phases of the organogenesis, addressing correctly cell-to-cell interactions, allowing, finally, the physiologic morphogenesis. Accumulating evidence is suggesting that dysregulation of Wnt and/or Hox genes may affect cell migration during organogenesis and differentiation of Müllerian structures of the female reproductive tract, with possible dislocation and dissemination of primordial endometrial stem cells in ectopic regions, which have high plasticity to differentiation. We hypothesize that during postpubertal age, under the influence of different stimuli, these misplaced and quiescent ectopic endometrial cells could acquire new phenotype, biological functions, and immunogenicity. So, these kinds of cells may differentiate, specializing in epithelium, glands, and stroma to form a functional ectopic endometrial tissue. This may provoke a breakdown in the peritoneal cavity homeostasis, with the consequent processes of immune alteration, documented by peripheral mononuclear cells recruitment and secretion of inflammatory cytokines in early phases and of angiogenic and fibrogenic cytokines in the late stages of the disease.
机译:在Müllerian结构发育的遗传调控中,Hoxa和Wnt簇发挥了关键作用,因为它们根据器官发生的不同阶段引导不同基因的转录,正确解决了细胞与细胞之间的相互作用,最终使生理形态发生。越来越多的证据表明,Wnt和/或Hox基因的失调可能影响女性生殖道穆勒结构的器官发生和分化过程中的细胞迁移,并可能在异位区域使原始子宫内膜干细胞移位和扩散,这对分化具有很高的可塑性。 。我们假设在青春期后,在不同刺激的影响下,这些错位和静止的异位子宫内膜细胞可以获得新的表型,生物学功能和免疫原性。因此,这些类型的细胞可能分化,专门从事上皮,腺体和间质形成功能性异位子宫内膜组织。这可能引起腹膜腔内稳态的破坏,随之而来的是免疫改变,其表现为早期外周血单个核细胞募集和炎性细胞因子的分泌以及疾病后期血管生成和纤维生成细胞因子的分泌。

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