Müllerian inhibiting substance regulates its receptor/SMAD signaling and causes mesenchymal transition of the coelomic epithelial cells early in Müllerian duct regression

Zhan, Yumei; Fujino, Akihiro; MacLaughlin, David T.; Manganaro, Thomas F.; Szotek, Paul P.; Arango, Nelson A.; Teixeira, Jose; Donahoe, Patricia K.

doi:10.1242/dev.02383

Cited by 71 publications

(79 citation statements)

References 60 publications

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“…2 A-C), which lends support to the dual epithelial/mesenchymal potential ascribed to the ovarian coelomic epithelium (34,35). Interestingly, whereas ovarian cancer cells express the surface marker EpCam (36,37), the CE LRCs were negative (see Fig.…”

Section: H2b-gfp 3 Month Chasementioning

confidence: 58%

Normal ovarian surface epithelial label-retaining cells exhibit stem/progenitor cell characteristics

Szotek

Chang

Brennand

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

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116

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Ovulation induces cyclic rupture and regenerative repair of the ovarian coelomic epithelium. This process of repeated disruption and repair accompanied by complex remodeling typifies a somatic stem/progenitor cell-mediated process. Using BrdU incorporation and doxycycline inducible histone2B-green fluorescent protein pulse–chase techniques, we identify a label-retaining cell population in the coelomic epithelium of the adult mouse ovary as candidate somatic stem/progenitor cells. The identified population exhibits quiescence with asymmetric label retention, functional response to estrous cycling in vivo by proliferation, enhanced growth characteristics by in vitro colony formation, and cytoprotective mechanisms by enrichment for the side population. Together, these characteristics identify the label-retaining cell population as a candidate for the putative somatic stem/progenitor cells of the coelomic epithelium of the mouse ovary.

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Section: H2b-gfp 3 Month Chasementioning

confidence: 58%

Normal ovarian surface epithelial label-retaining cells exhibit stem/progenitor cell characteristics

Szotek

Chang

Brennand

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

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116

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“…CTNNB1 seemed a particularly interesting candidate gene, since β-catenin is a downstream effector of both AMH and WNT signaling pathways, which may function cooperatively in mediating Müllerian duct regression [24]. Whether the effect of AMH involves WNT signaling in the Müllerian mesenchyme is unknown.…”

Section: Discussionmentioning

confidence: 99%

Molecular analysis of the β-catenin gene in patients with the Mayer-Rokitansky-Küster-Hauser syndrome

Drummond

Rezende

Peixoto

et al. 2008

J Assist Reprod Genet

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Purpose To study the β-catenin gene in a group of MayerRokitansky-Küster-Hauser patients. Methods Twelve patients with the Mayer-RokitanskyKüster-Hauser syndrome were included in this study. DNA was extracted from peripheral blood and the region codifying β-catenin GSK-3β phosphorylation sites on exon 3 was amplified. PCR products were purified and directly sequenced.Results No mutations were found in the GSK-3β phosphorylation sites on exon 3 of β-catenin gene in this group of patients with the MRKH syndrome. Conclusions β-catenin gene mutations are an unlikely cause of the MRKH syndrome.Keywords Mayer-Rokitansky-Küster-Hauser syndrome . β-catenin . molecular analysis . Müllerian ducts . anti-Müllerian hormone Mayer-Rokitansky-Küster-Hauser (MRKH) syndrome (MIM *277000), a congenital malformation of the Müllerian ducts, is the second most common cause of primary amenorrhea, occurring in one in every 4,000 to 5,000 female live births. The extent of MRKH anomaly is variable, ranging from upper vaginal atresia and rudimentary uterus to total uterine, fallopian tubes and upper vaginal agenesis. Additional congenital skeletal and renal abnormalities are present in approximately 30% of the patients [1]. Clinically, the diagnosis should be suspected if primary amenorrhea and infertility are present in 46, XX individuals with normal ovaries and normal secondary sexual characteristics.The cause of the MRKH syndrome remains unexplained. The presence of familial clustering described in previous studies suggests a genetic defect [2,3]. Nevertheless, the molecular basis of the MRKH syndrome has not yet been established. The putative defective gene could be either involved in the process of Müllerian duct formation, or associated with abnormal activation of the anti-Müllerian hormone (AMH) signaling pathway, leading to Müllerian duct regression. Indeed, both hypotheses could ultimately result in the MRKH syndrome phenotype.Comprising the first group, several genes encoding transcription factors and signaling molecules have been studied. WT1, PAX-2, WNT-7a, RXR-alpha, RXR-gamma, HOXA-7 to HOXA-13, and PBX-1 are genes required for Müllerian duct formation and differentiation, which have been evaluated in different groups of patients and were all excluded as causes of the MRKH syndrome [4][5][6][7][8]. Analysis of WNT4, a gene encoding a signaling molecule crucial for ovarian and uterine development, has provided us with interesting information. WNT4 gene mutations have been described in patients with Mullerian duct abnormalities and hyperandrogenism [9-11], but were not found in patients with the classic MRKH syndrome phenotype [6,[11][12][13]. These results suggest that WNT4 gene mutation is a clinical phenotype distinct from the isolated MRKH, and exclude it J Assist Reprod Genet (2008) 25:511-514 DOI 10.1007/s10815-008-9261-y Capsule β-catenin gene mutations were not detected in a group of twelve patients with the Mayer-Rokitansky Küster-Hauser (MRKH) anomaly.

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“…The present studies were undertaken to determine the agents with which MIS could be used most efficaciously. For example, MIS exerts its effect in the embryonic urogenital ridge by activating MISRII, Alk2 and Alk3, and the Smad 1͞5͞8 differentiation and growth inhibitory pathway (35). In addition, MIS up-regulates pocket proteins p130 and p107 in human ovarian (10) and endometrial cancer cell lines (9).…”

Section: Discussionmentioning

confidence: 99%

“…Comprehensive studies in our laboratory, and in those of many others, have shown that MIS downstream signal transduction pathways include MISRII (28)(29)(30), the type I receptors Alk2 (31) and Alk3 (32), Smads 1͞5͞8 (33)(34)(35), cyclin-dependent kinase inhibitors (4, 9, 10), and cytokine-inducible pathways (36)(37)(38)(39), suggesting mechanisms of action that are potentially different from those of most cytotoxic drugs.…”

Section: Ullerian Inhibiting Substance (Mis) May Have Its Most Im-mentioning

confidence: 93%

Mullerian Inhibiting Substance enhances subclinical doses of chemotherapeutic agents to inhibit human and mouse ovarian cancer

Pieretti-Vanmarcke¹,

Donahoe²,

Pearsall³

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

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Mullerian Inhibiting Substance (MIS), a biological modifier that causes regression of Mullerian ducts in male embryos, is effective as a single agent in vitro and in vivo against human and mouse ovarian cancer cell lines expressing MIS type II receptor; however, little is known about how recombinant human MIS (rhMIS), now being scaled for preclinical trials, could be used in combination with cytotoxic or targeted chemotherapeutic agents. Mouse serous and endometrioid ovarian carcinoma cell lines were tested in vitro against rhMIS alone and with doxorubicin, paclitaxel, or cisplatin as agents in clinical use. Because MIS releases FK506 binding protein (FKBP12), which activates the mammalian target of rapamycin (mTOR) downstream of Akt, rhMIS and rapamycin combinations were tested. MIS increases p16 protein levels, and 5 -Aza-2 -deoxycytidine (AzadC) induces p16 mRNA; therefore, they were used in combination in vitro and in vivo with a human ovarian cancer cell line. A paclitaxel-resistant human ovarian cancer cell line and its parental line both respond to rhMIS in vitro. Additivity, synergy, or competition was observed with MIS and rapamycin, AzadC, doxorubicin, cisplatin, and paclitaxel, suggesting that MIS in combination with selective targeted therapies might achieve greater activity against ovarian cancer than the use of each individual agent alone. These assays and statistical analyses could be useful in selecting rhMIS and chemotherapeutic agent combinations that enhance clinical efficacy and reduce toxicity. For example, granulosa cell tumors can produce serum MIS at concentrations 1,000-fold higher (1, 2), and normal baby boys can produce MIS concentrations at least 60-fold higher, than those found in normal females (3), without apparent adverse outcomes. It is anticipated that exogenous recombinant human MIS (rhMIS) will be nontoxic as a single agent and that it can be used effectively in combination with chemotherapy drugs to lower their toxicity. We originally hypothesized that cancers of Mullerian origin that expressed MISRII could be targets for MIS treatment (4-9), focusing first on ovarian cancers because they are derived from an MISsensitive surface or coelomic epithelium (10) and have the worst prognosis of all female reproductive tumors. Furthermore, ovarian ascites cells are also accessible ex vivo to examine biomarkers that may predict their response and mechanisms of biologic effect. The idea that MIS could be used to treat epithelial ovarian cancer is predicted by the fact that the histology of the embryonic Mullerian ducts is recapitulated in the common ovarian adenocarcinomas that arise from the surface or coelomic epithelium, which in the embryo invaginates to form the Mullerian duct (11)(12)(13)(14).The discovery that abdominal ascites cells from Ͼ50% of Stage III or IV ovarian cancer patients bound rhMIS, expressed MISRII mRNA, and were inhibited by rhMIS when treated in ex vivo proliferation assays (4), makes it compelling to study MIS as a potential therapeutic agent. The availabilit...

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Müllerian inhibiting substance regulates its receptor/SMAD signaling and causes mesenchymal transition of the coelomic epithelial cells early in Müllerian duct regression

Cited by 71 publications

References 60 publications

Normal ovarian surface epithelial label-retaining cells exhibit stem/progenitor cell characteristics

Normal ovarian surface epithelial label-retaining cells exhibit stem/progenitor cell characteristics

Molecular analysis of the β-catenin gene in patients with the Mayer-Rokitansky-Küster-Hauser syndrome

Mullerian Inhibiting Substance enhances subclinical doses of chemotherapeutic agents to inhibit human and mouse ovarian cancer

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