Your search keyword '"MepM"' showing total 16 results

1. Peptidoglycan endopeptidase MepM of uropathogenic Escherichia coli contributes to competitive fitness during urinary tract infections

Author

Wen-Chun Huang, Ida Bagus Nyoman Putra Dwija, Masayuki Hashimoto, Jiunn-Jong Wu, Ming-Cheng Wang, Cheng-Yen Kao, Wei-Hung Lin, Shuying Wang, and Ching-Hao Teng

Subjects

MepM, YebA, MepS, Spr, Peptidoglycan endopeptidase, Uropathogenic E. Coli, Microbiology, QR1-502

Abstract

Abstract Background Urinary tract infections (UTIs) are common bacterial infections, primarily caused by uropathogenic Escherichia coli (UPEC), leading to significant health issues and economic burden. Although antibiotics have been effective in treating UPEC infections, the rise of antibiotic-resistant strains hinders their efficacy. Hence, identifying novel bacterial targets for new antimicrobial approaches is crucial. Bacterial factors required for maintaining the full virulence of UPEC are the potential target. MepM, an endopeptidase in E. coli, is involved in the biogenesis of peptidoglycan, a major structure of bacterial envelope. Given that the bacterial envelope confronts the hostile host environment during infections, MepM’s function could be crucial for UPEC’s virulence. This study aims to explore the role of MepM in UPEC pathogenesis. Results MepM deficiency significantly impacted UPEC’s survival in urine and within macrophages. Moreover, the deficiency hindered the bacillary-to-filamentous shape switch which is known for aiding UPEC in evading phagocytosis during infections. Additionally, UPEC motility was downregulated due to MepM deficiency. As a result, the mepM mutant displayed notably reduced fitness in causing UTIs in the mouse model compared to wild-type UPEC. Conclusions This study provides the first evidence of the vital role of peptidoglycan endopeptidase MepM in UPEC’s full virulence for causing UTIs. MepM’s contribution to UPEC pathogenesis may stem from its critical role in maintaining the ability to resist urine- and immune cell-mediated killing, facilitating the morphological switch, and sustaining motility. Thus, MepM is a promising candidate target for novel antimicrobial strategies.

Published

2024

2. Peptidoglycan endopeptidase MepM of uropathogenic Escherichia coli contributes to competitive fitness during urinary tract infections.

Author

Huang, Wen-Chun, Dwija, Ida Bagus Nyoman Putra, Hashimoto, Masayuki, Wu, Jiunn-Jong, Wang, Ming-Cheng, Kao, Cheng-Yen, Lin, Wei-Hung, Wang, Shuying, and Teng, Ching-Hao

Subjects

*URINARY tract infections, *ESCHERICHIA coli, *URODYNAMICS, *BACTERIAL diseases, *LABORATORY mice

Abstract

Background: Urinary tract infections (UTIs) are common bacterial infections, primarily caused by uropathogenic Escherichia coli (UPEC), leading to significant health issues and economic burden. Although antibiotics have been effective in treating UPEC infections, the rise of antibiotic-resistant strains hinders their efficacy. Hence, identifying novel bacterial targets for new antimicrobial approaches is crucial. Bacterial factors required for maintaining the full virulence of UPEC are the potential target. MepM, an endopeptidase in E. coli, is involved in the biogenesis of peptidoglycan, a major structure of bacterial envelope. Given that the bacterial envelope confronts the hostile host environment during infections, MepM's function could be crucial for UPEC's virulence. This study aims to explore the role of MepM in UPEC pathogenesis. Results: MepM deficiency significantly impacted UPEC's survival in urine and within macrophages. Moreover, the deficiency hindered the bacillary-to-filamentous shape switch which is known for aiding UPEC in evading phagocytosis during infections. Additionally, UPEC motility was downregulated due to MepM deficiency. As a result, the mepM mutant displayed notably reduced fitness in causing UTIs in the mouse model compared to wild-type UPEC. Conclusions: This study provides the first evidence of the vital role of peptidoglycan endopeptidase MepM in UPEC's full virulence for causing UTIs. MepM's contribution to UPEC pathogenesis may stem from its critical role in maintaining the ability to resist urine- and immune cell-mediated killing, facilitating the morphological switch, and sustaining motility. Thus, MepM is a promising candidate target for novel antimicrobial strategies. [ABSTRACT FROM AUTHOR]

Published

2024

3. The Involvement of hormone-sensitive lipase in all-trans retinoic acid induced cleft palate.

Author

ZHENG, K. and YE, Q. N.

Subjects

CLEFT palate, TRETINOIN, LIPASES, RNA interference, HEMATOXYLIN & eosin staining, RETINOIC acid receptors, NON-coding RNA

Abstract

Abnormally high concentrations of all-trans retinoic acid (atRA) induce cleft palate, which is accompanied by abnormal migration and proliferation of mouse embryonic palatal mesenchyme (MEPM) cells. Hormone-sensitive lipase (HSL) is involved in many embryonic development processes. The current study was designed to elucidate the mechanism of HSL in cleft palate induced by atRA. To establish a cleft palate model in Kunming mice, pregnant mice were administered atRA (70 mg/kg) by gavage at embryonic Day 10.5 (E10.5). Embryonic palates were obtained through the dissection of pregnant mice at E15.5. Hematoxylin and eosin (H&E) staining was used to evaluate growth changes in the palatal shelves. The levels of HSL in MEPM cells were detected by immunohistochemistry, quantitative real-time reverse transcription-polymerase chain reaction (qRT-PCR) and western blotting. RNAi was applied to construct vectors expressing HSL small interference RNAs (siRNAs). The vectors were transfected into MEPM cells. Cell proliferation and migration were evaluated by the cell counting kit-8 (CCK-8) assay and wound healing assay, respectively. The palatal shelves in the atRA group had separated at E15.5 without fusing. In MEPM cells, the expression of HSL was reversed after atRA treatment, which caused cleft palate in vivo. In the atRA group, the proliferation of HSL siRNA-transfected cells was remarkably promoted, and the migration rate significantly increased in the HSL siRNA-transfected MEPM cells. These results suggested that HSL may be involved in cleft palate induced by atRA and that atRA enhances HSL levels to inhibit embryonic palate growth. [ABSTRACT FROM AUTHOR]

Published

2022

4. The role of lncRNA Meg3 in the proliferation of all-trans retinoic acid-treated mouse embryonic palate mesenchymal cells involves the Smad pathway.

Author

Liu, Xiaozhuan, Liu, Hongyan, Wu, Yang, He, Zhidong, Shen, Lijun, Zhang, Huanhuan, Wan, Zhongxiao, Chen, Yao, Yue, Haodi, Zhang, Tingting, Gao, Suhua, and Yu, Zengli

Subjects

*PALATE, *LINCRNA, *MICE, *CELL proliferation, *PROTEIN expression

Abstract

The role of Meg3 in the proliferation of atRA-treated mouse embryonic palate mesenchymal cells involved the Smad pathway. [Display omitted] • MEPM-cell proliferation is regulated by atRA and exogenous TGF-β3. • The inhibition of Smad signaling is related to the reduction of MEPM-cell proliferation. • atRA enhance LncRNAMeg3 expression in MEPM cells. • Meg3 participates in the atRA-induced suppression of MEPM-cell proliferation. • Meg3 targets Smad2 and thereby mediates the TGF-β/Smad signaling inhibition. Mesenchymal cell proliferation is critical for the growth of the palate shelf. All-trans retinoic acid (atRA), as well as pathways associated with TGF-β/Smad signaling, play crucial roles in the proliferation of mouse embryonic palate mesenchymal (MEPM) cells. We have found that MEPM-cell proliferation was regulated by atRA and exogenous TGF-β3 could significantly antagonize the atRA-mediated suppression of MEPM cell proliferation, which is closely associated with the regulation of TGF-β/Smad signaling pathway. The long non-coding RNA (lncRNA) MEG3 has been reported to activate TGF-β/Smad signaling, thereby regulating cellular proliferation, differentiation, and related processes. Here, we found that Meg3 expression increased significantly in atRA-treated MEPM cells while TGF-β3 treatment markedly inhibited Meg3 expression and antagonized the effect of atRA on Meg3. Moreover, Smad2 was found to interact directly with Meg3, and atRA treatment significantly enriched Meg3 in Smad2-immunoprecipitated samples. After Meg3 deletion, the effects of atRA on the proliferation of MEPM cells and TGF-β3-dependent protein expression were lost. Hence, we speculate that Meg3 has a role in the RA-induced suppression of MEPM cell proliferation by targeting Smad2 and thereby mediating TGF-β/Smad signaling inhibition. [ABSTRACT FROM AUTHOR]

Published

2021

5. Distinct Amino Acid Availability-Dependent Regulatory Mechanisms of MepS and MepM Levels in Escherichia coli

Author

Yung Jae Kim, Byoung Jun Choi, Si Hyoung Park, Han Byeol Lee, Ji Eun Son, Umji Choi, Won-Jae Chi, and Chang-Ro Lee

Subjects

peptidoglycan hydrolase, peptidoglycan endopeptidase, MepS, MepM, Prc, NlpI, Microbiology, QR1-502

Abstract

Peptidoglycan (PG) hydrolases play important roles in various aspects of bacterial physiology, including cytokinesis, PG synthesis, quality control of PG, PG recycling, and antibiotic resistance. However, the regulatory mechanisms of their expression are poorly understood. In this study, we have uncovered novel regulatory mechanisms of the protein levels of the synthetically lethal PG endopeptidases MepS and MepM, which are involved in PG synthesis. A mutant defective for both MepS and MepM was lethal in an amino acid-rich medium, whereas it exhibited almost normal growth in a minimal medium, suggesting the expendability of MepS and MepM in a minimal medium. Protein levels of MepS and MepM dramatically decreased in the minimal medium. Although MepM was revealed as a substrate of Prc, a periplasmic protease involved in the proteolysis of MepS, only the decrease in the MepS level in the minimal medium was affected by the prc depletion. Phenotypic and biochemical analyses showed that the presence of aromatic amino acids in the medium induced the accumulation of MepS, but not MepM, while the presence of glutamate increased the level of MepM, but not MepS. Together, these results demonstrate that the protein levels of the two major PG endopeptidases are regulated in an amino acid availability-dependent manner, but their molecular mechanisms and signaling are significantly distinct.

Published

2021

6. Distinct Amino Acid Availability-Dependent Regulatory Mechanisms of MepS and MepM Levels in Escherichia coli.

Author

Kim, Yung Jae, Choi, Byoung Jun, Park, Si Hyoung, Lee, Han Byeol, Son, Ji Eun, Choi, Umji, Chi, Won-Jae, and Lee, Chang-Ro

Subjects

AMINO acids, ESCHERICHIA coli, BACTERIAL physiology, ENDOPEPTIDASES, PEPTIDOGLYCAN hydrolase, PROTEOLYTIC enzymes

Abstract

Peptidoglycan (PG) hydrolases play important roles in various aspects of bacterial physiology, including cytokinesis, PG synthesis, quality control of PG, PG recycling, and antibiotic resistance. However, the regulatory mechanisms of their expression are poorly understood. In this study, we have uncovered novel regulatory mechanisms of the protein levels of the synthetically lethal PG endopeptidases MepS and MepM, which are involved in PG synthesis. A mutant defective for both MepS and MepM was lethal in an amino acid-rich medium, whereas it exhibited almost normal growth in a minimal medium, suggesting the expendability of MepS and MepM in a minimal medium. Protein levels of MepS and MepM dramatically decreased in the minimal medium. Although MepM was revealed as a substrate of Prc, a periplasmic protease involved in the proteolysis of MepS, only the decrease in the MepS level in the minimal medium was affected by the prc depletion. Phenotypic and biochemical analyses showed that the presence of aromatic amino acids in the medium induced the accumulation of MepS, but not MepM, while the presence of glutamate increased the level of MepM, but not MepS. Together, these results demonstrate that the protein levels of the two major PG endopeptidases are regulated in an amino acid availability-dependent manner, but their molecular mechanisms and signaling are significantly distinct. [ABSTRACT FROM AUTHOR]

Published

2021

7. LncRNA Meg3-mediated regulation of the Smad pathway in atRA-induced cleft palate.

Author

Liu, Xiaozhuan, Zhang, Yuwei, Shen, Lijun, He, Zhidong, Chen, Yao, Li, Ning, Zhang, Xiuli, Zhang, Tingting, Gao, Suhua, Yue, Haodi, Li, Zhitao, and Yu, Zengli

Subjects

*CLEFT palate, *NON-coding RNA, *LINCRNA, *CELL proliferation, *RNA analysis, *TRETINOIN

Abstract

The role of LncRNA Meg3 in atRA-induced cleft palate involved the Smad pathway. • All-trans retinoic acid (atRA) enhanced Meg3 expression in MEPM cells. • Meg3 was linked to the suppression of MEPM cell proliferation. • AtRA treatment was associated with the demethylation of CpG sites in the Meg3 promoter. • Smad2 is a Meg3 target in the context of atRA-induced cleft palate. Palatal mesenchymal cell proliferation is essential to the process of palatogenesis, and the proliferation of mouse embryonic palate mesenchymal (MEPM) cells is impacted by both all-trans retinoic acid (atRA) and the TGF-β/Smad signaling pathway. The long non-coding RNA (lncRNA) MEG3 has been shown to activate TGF-β/Smad signaling and to thereby regulate cell proliferation, differentiation, and related processes. Herein, we found that atRA treatment (100 mg/kg) promoted Meg3 upregulation in MEPM cells, and that such upregulation was linked to the suppression of MEPM cell proliferation in the context of secondary palate fusion on gestational day (GD) 13 and 14. Moreover, the demethylation of specific CpG sites within the lncRNA Meg3 promoter was detected in atRA-treated MEPM cells, likely explaining the observed upregulation of this lncRNA. Smad signaling was also suppressed by atRA treatment in these cells, and RNA immunoprecipitation analyses revealed that Smad2 can directly interact with Meg3 in MEPM cells following atRA treatment. Therefore, we propose a model wherein Meg3 is involved in the suppression of MEPM cell proliferation, functioning at least in part via interacting with the Smad2 protein and thereby suppressing Smad signaling in the context of atRA-induced cleft palate. [ABSTRACT FROM AUTHOR]

Published

2021

8. Genetic Evidence for Distinct Functions of Peptidoglycan Endopeptidases in Escherichia coli

Author

Si Hyoung Park, Yung Jae Kim, Han Byeol Lee, Yeong-Jae Seok, and Chang-Ro Lee

Subjects

peptidoglycan, peptidoglycan hydrolase, endopeptidase, MepM, MepS, LytM domain, Microbiology, QR1-502

Abstract

Peptidoglycan (PG) is an essential component of the bacterial exoskeleton that plays a pivotal role in the maintenance of cell shape and resistance to cell lysis under high turgor pressures. The synthesis and degradation of PG must be tightly regulated during bacterial cell elongation and division. Unlike enzymes involved in PG synthesis, PG hydrolases show high redundancy in many bacteria including Escherichia coli. In this study, we showed that PG endopeptidases have distinct roles in cell growth and division. Phenotypic analysis of mutants lacking one of seven PG endopeptidases identified a MepM-specific phenotype, salt sensitivity, and a MepS-specific phenotype, EDTA sensitivity. Complementation test in each phenotype showed that the phenotype of the mepM mutant was restored only by MepM, whereas the phenotype of the mepS mutant was restored by MepS or by overexpression of MepH, PbpG, or MepM. These distinct phenotypes depend on both the specific localizations and specific domains of MepM and MepS. Finally, using the identified phenotypes, we revealed that MepM and MepH were genetically associated with both penicillin-binding protein 1a (PBP1a) and PBP1b, whereas MepS and PbpG were genetically associated with only PBP1b. Notably, a defect in PBP1a or PBP1b phenocopied the mepM mutant, suggesting the importance of MepM on PG synthesis. Therefore, our results indicate that each PG endopeptidase plays a distinct role in cell growth and division, depending on its distinct domains and cellular localizations.

Published

2020

9. Genetic Evidence for Distinct Functions of Peptidoglycan Endopeptidases in Escherichia coli.

Author

Park, Si Hyoung, Kim, Yung Jae, Lee, Han Byeol, Seok, Yeong-Jae, and Lee, Chang-Ro

Subjects

PEPTIDOGLYCANS, ENDOPEPTIDASES, LYSIS, ESCHERICHIA coli, CELL morphology, CELL growth

Abstract

Peptidoglycan (PG) is an essential component of the bacterial exoskeleton that plays a pivotal role in the maintenance of cell shape and resistance to cell lysis under high turgor pressures. The synthesis and degradation of PG must be tightly regulated during bacterial cell elongation and division. Unlike enzymes involved in PG synthesis, PG hydrolases show high redundancy in many bacteria including Escherichia coli. In this study, we showed that PG endopeptidases have distinct roles in cell growth and division. Phenotypic analysis of mutants lacking one of seven PG endopeptidases identified a MepM-specific phenotype, salt sensitivity, and a MepS-specific phenotype, EDTA sensitivity. Complementation test in each phenotype showed that the phenotype of the mepM mutant was restored only by MepM, whereas the phenotype of the mepS mutant was restored by MepS or by overexpression of MepH, PbpG, or MepM. These distinct phenotypes depend on both the specific localizations and specific domains of MepM and MepS. Finally, using the identified phenotypes, we revealed that MepM and MepH were genetically associated with both penicillin-binding protein 1a (PBP1a) and PBP1b, whereas MepS and PbpG were genetically associated with only PBP1b. Notably, a defect in PBP1a or PBP1b phenocopied the mepM mutant, suggesting the importance of MepM on PG synthesis. Therefore, our results indicate that each PG endopeptidase plays a distinct role in cell growth and division, depending on its distinct domains and cellular localizations. [ABSTRACT FROM AUTHOR]

Published

2020

10. Upregulated LncRNA-Meg3 modulates the proliferation and survival of MEPM cells via interacting with Smad signaling in TCDD-induced cleft palate.

Author

Liu, Xiaozhuan, Song, Shuaixing, Wang, Guoxu, Zhang, Yaxin, Su, Hexin, Wu, Yang, Zhang, Yuwei, Liu, Hongyan, Wang, Xiangdong, and Yu, Zengli

Subjects

*CLEFT palate, *SMAD proteins, *CELL survival, *FETAL tissues, *CELL differentiation

Abstract

Exposure to the environmental contaminant 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) in utero can result in high rates of cleft palate (CP) formation, yet the underlying mechanisms remain to be characterized. In vivo, the lncRNA Meg3 was upregulated following TCDD treatment in CP-associated murine embryonic palatal tissue, with concomitant changes in proliferative and apoptotic activity in these murine embryonic palatal mesenchymal (MEPM) cells. Meg3 can modulate the TGF-β/Smad to control the proliferation, survival, and differentiation of cells. Accordingly, TCCD and TGF-β1 were herein used to treat MEPM cells in vitro, revealing that while TCDD exposure altered the proliferative activity and apoptotic death of these cells, exogenous TGF-β1 exposure antagonized these effects via TGF-β/Smad signaling. TCDD promoted Meg3 upregulation, whereas TGF-β1 suppressed TCDD-driven upregulation of this lncRNA. Meg3 was additionally determined to directly interact with Smad2, with significant Meg3 enrichment in Smad2-immunoprecipitates following TCDD treatment. When Meg3 was silenced, the impact of TCDD on Smad signaling, proliferative activity, and apoptosis were ablated, while the effects of exogenous TGF-β1 were unchanged. This supports a model wherein Meg3 is upregulated in TCDD-exposed palatal tissue whereupon it can interact with Smad2 to suppress Smad-dependent signaling, thus controlling MEPM cell proliferation and apoptosis, contributing to TCDD-induced CP, which provides a theoretical support for the precautions of cleft palate induced by TCDD. • LncRNA- Meg3 gene was upregulated by TCDD in mouse embryo palate cells. • The MEPM cell cellular proliferation and apoptosis were regulated by TCDD and TGF-β1. • The Smad-dependent signaling was inhibited by TCDD in MEPM cells • The effects of TCDD on the MEPM cells and Smad signaling were abolished after Meg3 deletion. • Meg3 mediated Smad signaling and thereby regulated the TCDD effects on MEPM cells. [ABSTRACT FROM AUTHOR]

Published

2024

11. Corrigendum: Muramyl Endopeptidase Spr Contributes to Intrinsic Vancomycin Resistance in Salmonella enterica Serovar Typhimurium

Author

Kim Vestö, Douglas L. Huseby, Iina Snygg, Helen Wang, Diarmaid Hughes, and Mikael Rhen

Subjects

vancomycin, antibiotic resistance, Spr, MepS, YebA, MepM, Microbiology, QR1-502

Published

2019

12. Associations between the proliferation of palatal mesenchymal cells, Tgfβ2 promoter methylation, Meg3 expression, and Smad signaling in atRA-induced cleft palate.

Author

Yu, Zengli, Wang, Guoxu, Song, Shuaixing, Zhang, Yaxin, Wu, Yang, Zhang, Yuwei, Duan, Wenjing, and Liu, Xiaozhuan

Subjects

*CLEFT palate, *SMAD proteins, *METHYLATION, *DNA methylation, *CELL proliferation, *P16 gene, *RETINOIC acid receptors

Abstract

All-trans retinoic acid (atRA) is a teratogen that can induce cleft palate formation. During palatal development, murine embryonic palate mesenchymal (MEPM) cell proliferation is required for the appropriate development of the palatal frame, with Meg3 serving as a key regulator of the proliferative activity of these cells and the associated epithelial-mesenchymal transition process. DNA methylation and signaling via the TGFβ/Smad pathway are key in regulating embryonic development. Here, the impact of atRA on MEPM cell proliferation and associations between Tgfβ2 promoter methylation, Meg3 , and signaling via the Smad pathway were explored using C57BL/6 N mice treated with atRA (100 mg/kg) to induce fetal cleft palate formation. Immunohistochemistry and BrdU assays were used to detect MEPM proliferation and DNA methylation assays were performed to detect Tgfβ2 promoter expression. These analyses revealed that atRA suppressed MEPM cell proliferation, promoted the upregulation of Meg3 , and reduced the levels of Smad2 and Tgfβ2 expression phosphorylation, whereas Tgfβ2 promoter methylation was unaffected. RNA immunoprecipitation experiments indicated that the TgfβI receptor is directly targeted by Meg3 , suggesting that the ability of atRA to induce cleft palate may be mediated through the Tgfβ/Smad signaling pathway. [Display omitted] atRA treatment suppresses palatal mesenchymal cell proliferation. atRA exposure inhibits the expression of Tgfβ2 without altering its methylation. Exposure to atRA inhibits Smad protein signaling. Meg3 may be involved in regulation of the Tgfβ/Smad pathway. [ABSTRACT FROM AUTHOR]

Published

2023

13. Muramyl Endopeptidase Spr Contributes to Intrinsic Vancomycin Resistance in Salmonella enterica Serovar Typhimurium

Author

Kim Vestö, Douglas L. Huseby, Iina Snygg, Helen Wang, Diarmaid Hughes, and Mikael Rhen

Subjects

vancomycin, antibiotic resistance, Spr, MepS, YebA, MepM, Microbiology, QR1-502

Abstract

The impermeability barrier provided by the outer membrane of enteric bacteria, a feature lacking in Gram-positive bacteria, plays a major role in maintaining resistance to numerous antimicrobial compounds and antibiotics. Here we demonstrate that mutational inactivation of spr, coding for a muramyl endopeptidase, significantly sensitizes Salmonella enterica serovar Typhimurium to vancomycin without any accompanying apparent growth defect or outer membrane destabilization. A similar phenotype was not achieved by deleting the genes coding for muramyl endopeptidases MepA, PbpG, NlpC, YedA, or YhdO. The spr mutant showed increased autolytic behavior in response to not only vancomycin, but also to penicillin G, an antibiotic for which the mutant displayed a wild-type MIC. A screen for suppressor mutations of the spr mutant phenotype revealed that deletion of tsp (prc), encoding a periplasmic carboxypeptidase involved in processing Spr and PBP3, restored intrinsic resistance to vancomycin and reversed the autolytic phenotype of the spr mutant. Our data suggest that Spr contributes to intrinsic antibiotic resistance in S. Typhimurium without directly affecting the outer membrane permeability barrier. Furthermore, our data suggests that compounds targeting specific cell wall endopeptidases might have the potential to expand the activity spectrum of traditional Gram-positive antibiotics.

Published

2018

14. Excessive retinoic acid inhibit mouse embryonic palate mesenchymal cell growth through involvement of Smad signaling.

Author

Zhang, Huanhuan, Liu, Xiaozhuan, Gao, Zhan, Li, Zhitao, Yu, Zengli, Yin, Jun, Tao, Yuchang, and Cui, Lingling

Subjects

*TRETINOIN, *SMAD proteins, *EOSIN, *MESSENGER RNA, *PROTEIN expression

Abstract

All-trans retinoic acid (atRA), the oxidative metabolite of retinoic acid (RA), is essential for palatogenesis. Overdose RA is capable of inducing cleft palate in mice and humans. Normal embryonic palatal mesenchymal (EPM) cell growth is crucial for shelf growth. Smad signaling is involved in many biological processes. However, it is not much clear if atRA could affect Smad signaling during EPM cells growth. In this study, the timed pregnant mice with maternal administration of 100 mg/kg body weight of RA by gastric intubation were cervical dislocation executed to evaluate growth changes of palatal shelves by hematoxylin and eosin (H&E) staining. At the same time, a primary mouse EPM (MEPM) cell culture model was also established. MEPM cells were treated with atRA (0.1, 0.5, 1, 5 and 10 μM) for 24, 48 and 72 h. The results indicated that the sizes of the shelves were smaller than those in control. AtRA inhibited MEPM cell growth with both increasing concentration and increasing incubation time, especially at 72 h in vitro. Moreover, atRA significantly increased the mRNA and protein expression levels of Smad7 (P < .05), but the mRNA and protein expression levels of PCNA were reduced (P < .05). We also found atRA inhibited phosphorylation of Smad2 compared with untreated group (P < .05). However, the protein and mRNA levels of Smad2 did not change both in atRA-treated and untreated group (P > .05). We demonstrated that RA induced inhibition of MEPM cell growth that could cause cleft palate partly by down-regulation of Smad pathway. [ABSTRACT FROM PUBLISHER]

Published

2017

15. Correlation of proliferation, TGF-β3 promoter methylation, and Smad signaling in MEPM cells during the development of ATRA-induced cleft palate.

Author

Liu, Xiaozhuan, Qi, Jingjiao, Tao, Yuchang, Zhang, Huanhuan, Yin, Jun, Ji, Mengmeng, Gao, Zhan, Li, Zhitao, Li, Ning, and Yu, Zengli

Subjects

*TRANSFORMING growth factors, *CELL proliferation, *SMAD proteins, *CLEFT palate, *RETINOIC acid receptors, *MICE embryology

Abstract

Mesenchymal cell proliferation is one of the processes in shelf outgrowth. Both all-trans retinoic acid (atRA) and transforming growth factor-β3 (TGF-β3) play an important role in mouse embryonic palate mesenchymal (MEPM) cell proliferation. The cellular effects of TGF-β are mediated by Smad-dependent or Smad-independent pathways. In the present study, we demonstrate that atRA promotes TGF-β3 promoter demethylation and protein expression, but can cause depression of mesenchymal cell proliferation, especially at embryonic day 14 (E14). Moreover, the inhibition of MEPM cell proliferation by atRA results in the downregulation of Smad signaling mediated by transforming growth interacting factor (TGIF). We speculate that the effects of atRA on MEPM cell proliferation may be mediated by Smad pathways, which are regulated by TGIF but are not related to TGF-β3 expression. Finally, the cellular effects of TGF-β3 on MEPM cell proliferation may be mediated by Smad-independent pathways. [ABSTRACT FROM AUTHOR]

Published

2016

16. Negative Interplay of Retinoic Acid and TGF-β Signaling Mediated by TG-Interacting Factor to Modulate Mouse Embryonic Palate Mesenchymal-Cell Proliferation.

Author

Liu, Xiaozhuan, Zhang, Huanhuan, Gao, Liyun, Yin, Yanyan, Pan, Xinjuan, Li, Zhitao, Li, Ning, Li, Haozhe, and Yu, Zengli

Abstract

Mesenchymal-cell proliferation is the main process in shelf outgrowth. Both all-trans-retinoic acid (atRA) and transforming growth factor-β3 (TGF-β3) play an important role in mouse embryonic palate mesenchymal (MEPM) cell proliferation. In the present study, we investigated the crosstalk between RA and TGF-β signaling in MEPM-cell proliferation. We found that atRA inhibited MEPM-cell proliferation by downregulating TGF-β/Smad signaling and that TGF-β3 treatment was able to antagonize RA signaling. Transforming growth-interacting factor (TGIF) is a transcriptional repressor that suppresses both TGF-β- and retinoid-driven gene transcription. Furthermore, we investigated the role of TGIF in the interaction between both TGF-β and RA signaling in MEPM-cell proliferation. The results showed that both atRA and TGF-β3 significantly increased the expression level of TGIF, and TGIF mediated the negative interaction between TGF-β and RA signaling pathways, which depended on TGIF binding to Smad2 or RARβ (RA receptor beta). Moreover, after deletion of TGIF, both the effects of atRA on TGF-β-dependent protein expression and the effects of TGF-β on RA-dependent protein expression were lost. So we conclude that there is a negative functional interplay of RA and TGF-β signaling mediated by TGIF to modulate MEPM-cell proliferation [ABSTRACT FROM AUTHOR]

Published

2014