Your search keyword '"NNMT"' showing total 9 results

1. Nicotinamide N-methyl transferase (NNMT): An emerging therapeutic target.

Author

Gao, Yongzhi, Martin, Nathaniel I., and van Haren, Matthijs J.

Subjects

*NICOTINAMIDE, *GENETIC overexpression, *ENZYME inhibitors, *METABOLIC disorders, *IN vivo studies

Abstract

• Nicotinamide N -methyltransferase (NNMT) methylates nicotinamide (vitamin B3). • Interest in NNMT as a therapeutic target has grown significantly in recent years. • NNMT overexpression is linked to cancer, metabolic disorders, and neurodegeneration. • Progress has been made in developing potent and selective NNMT inhibitors. • Most NNMT inhibitors described to date display limited in vivo activity. Nicotinamide N -methyltransferase (NNMT) methylates nicotinamide (NA) to generate 1-methyl nicotinamide. Since its discovery 70 years ago, the appreciation of the role of NNMT in human health has evolved from serving only metabolic functions to also being a driving force in diseases, including a variety of cancers. Despite the increasing evidence indicating NNMT as a viable therapeutic target, the development of cell-active inhibitors against this enzyme is lacking. In this review, we provide an overview of the current status of NNMT inhibitor development, relevant in vitro and in vivo studies, and a discussion of the challenges faced in the development of NNMT inhibitors. [ABSTRACT FROM AUTHOR]

Published

2021

2. Single-cell analysis reveals insights into epithelial abnormalities in ovarian endometriosis.

Author

Yan, Jia, Zhou, Ling, Liu, Mengya, Zhu, Honglan, Zhang, Xin, Cai, E., Xu, Xueqiang, Chen, Tinghan, Cheng, Hongyan, Liu, Jun'e, Wang, Shang, Dai, Lin, Chang, Xiaohong, and Tang, Fuchou

Abstract

Ovarian endometriosis is characterized by the growth of endometrial tissue within the ovary, causing infertility and chronic pain. However, its pathophysiology remains unclear. Utilizing high-precision single-cell RNA sequencing, we profile the normal, eutopic, and ectopic endometrium from 34 individuals across proliferative and secretory phases. We observe an increased proportion of ciliated cells in both eutopic and ectopic endometrium, characterized by a diminished expression of estrogen sulfotransferase, which likely confers apoptosis resistance. After translocating to ectopic lesions, endometrial epithelium upregulates nicotinamide N-methyltransferase expression that inhibits apoptosis by promoting deacetylation and subsequent nuclear exclusion of transcription factor forkhead box protein O1, thereby leading to the downregulation of the apoptotic gene BIM. Moreover, epithelial cells in ectopic lesions elevate HLA class II complex expression, which stimulates CD4+ T cells and consequently contributes to chronic inflammation. Altogether, our study provides a comprehensive atlas of ovarian endometriosis and highlights potential therapeutic targets for modulating apoptosis and inflammation. [Display omitted] • Eutopic and ectopic endometrium upregulate the percentage of ciliated cells • The ciliated cells in patients exhibit decreased SULT1E1 expression • Epithelial cells in endometriotic lesions resist apoptosis through NNMT-FOXO1-BIM pathway • Epithelial cells in endometriotic lesions stimulate CD4+ T cells via HLA class II complex Yan et al. generated a single-cell endometriosis atlas and revealed that ciliated cells in eutopic and ectopic endometrium suppress apoptosis through reduced estrogen sulfotransferase expression. In ectopic lesions, epithelial cells further adapted to survive by resisting apoptosis via NNMT and driving chronic inflammation through the HLA class II complex. [ABSTRACT FROM AUTHOR]

Published

2024

3. ER stress-induced upregulation of NNMT contributes to alcohol-related fatty liver development.

Author

Song, Qing, Chen, Yingli, Wang, Jun, Hao, Liuyi, Huang, Chuyi, Griffiths, Alexandra, Sun, Zhaoli, Zhou, Zhangxiang, and Song, Zhenyuan

Subjects

*FATTY liver, *ENZYME regulation, *METABOLIC regulation, *ALCOHOL drinking, *ENZYME metabolism, *NICOTINAMIDE, *CATECHOL-O-methyltransferase

Abstract

N-nicotinamide methyltransferase (NNMT) is emerging as an important enzyme in the regulation of metabolism. NNMT is highly expressed in the liver. However, the exact regulatory mechanism(s) underlying NNMT expression remains unclear and its potential involvement in alcohol-related liver disease (ALD) is completely unknown. Both traditional Lieber-De Carli and the NIAAA mouse models of ALD were employed. A small-scale chemical screening assay and a chromatin immunoprecipitation assay were performed. NNMT inhibition was achieved via both genetic (adenoviral short hairpin RNA delivery) and pharmacological approaches. Chronic alcohol consumption induces endoplasmic reticulum (ER) stress and upregulates NNMT expression in the liver. ER stress inducers upregulated NNMT expression in both AML12 hepatocytes and mice. PERK-ATF4 pathway activation is the main contributor to ER stress-mediated NNMT upregulation in the liver. Alcohol consumption fails to upregulate NNMT in liver-specific Atf4 knockout mice. Both adenoviral NNMT knockdown and NNMT inhibitor administration prevented fatty liver development in response to chronic alcohol feeding; this was also associated with the downregulation of an array of genes involved in de novo lipogenesis, including Srebf1 , Acaca , Acacb and Fasn. Further investigations revealed that activation of the lipogenic pathway by NNMT was independent of its NAD+-enhancing action; however, increased cellular NAD+, resulting from NNMT inhibition, was associated with marked liver AMPK activation. ER stress, specifically PERK-ATF4 pathway activation, is mechanistically involved in hepatic NNMT upregulation in response to chronic alcohol exposure. Overexpression of NNMT in the liver plays an important role in the pathogenesis of ALD. In this study, we show that nicotinamide methyltransferase (NNMT) – the enzyme that catalyzes nicotinamide degradation – is a pathological regulator of alcohol-related fatty liver development. NNMT inhibition protects against alcohol-induced fatty liver development and is associated with suppressed de novo lipogenic activity and enhanced AMPK activation. Thus, our data suggest that NNMT may be a potential therapeutic target for the treatment of alcohol-related liver disease. • Chronic alcohol consumption upregulates NNMT expression and activity in the liver. • The activation of the PERK-ATF4 pathway contributes to alcohol-induced hepatic NNMT upregulation. • Adenoviral knockdown of NNMT protects against fatty liver development in response to ER stress and chronic alcohol exposure. • NNMT inhibition enhances cellular NAD+ levels. • NNMT knockdown suppresses the de novo lipogenesis pathway in hepatocytes and the liver. [ABSTRACT FROM AUTHOR]

Published

2020

4. A systems-approach to NAD+ restoration.

Author

Conlon, Nichola and Ford, Dianne

Subjects

*NAD (Coenzyme), *NICOTINAMIDE, *BIOCOMPLEXITY, *DIETARY supplements

Abstract

[Display omitted] A decline in NAD+ is a feature of ageing and may play a causal role in the process. NAD+ plays a pivotal role in myriad processes important in cellular metabolism and is a cosubstrate for enzymes that play key roles in pathways that modify ageing. Thus, interventions that increase NAD+ may slow aspects of the ageing trajectory and there is great interest in pharmacological NAD+ restoration. Dietary supplementation with NAD+ precursors, particularly nicotinamide riboside, has increased NAD+ levels in several human intervention studies and arguably been the most robust approach to date. However, consistency and reliability of such approaches to increase NAD+, and also impact on markers of efficacy to slow or reverse features of ageing, has been inconsistent. We argue that a major element of this variability may arise from the use of single-target approaches that do not consider the underlying biological complexity leading to NAD+ decline. Thus, a systems approach – targeting multiple key nodes in the NAD+ interactome – is likely to be more efficacious and reliable. [ABSTRACT FROM AUTHOR]

Published

2022

5. Cancer stem cell overexpression of nicotinamide N-methyltransferase enhances cellular radiation resistance

Author

D’Andrea, Filippo P., Safwat, Akmal, Kassem, Moustapha, Gautier, Laurant, Overgaard, Jens, and Horsman, Michael R.

Subjects

*CANCER cells, *STEM cells, *RADIOTHERAPY, *CANCER relapse, *PHENOTYPES, *GENE expression, *REVERSE transcriptase polymerase chain reaction, *DRUG resistance in cancer cells, *METHYLTRANSFERASES, *DNA repair

Abstract

Abstract: Background: Cancer stem cells are thought to be a radioresistant population and may be the seeds for recurrence after radiotherapy. Using tumorigenic clones of retroviral immortalized human mesenchymal stem cell with small differences in their phenotype, we investigated possible genetic expression that could explain cancer stem cell radiation resistance. Methods: Tumorigenic mesenchymal cancer stem cell clones BB3 and CE8 were irradiated at varying doses and assayed for clonogenic surviving fraction. Altered gene expression before and after 2Gy was assessed by Affymetric exon chip analysis and further validated with q-RT-PCR using TaqMan probes. Results: The CE8 clone was more radiation resistant than the BB3 clone. From a pool of 15 validated genes with altered expression in the CE8 clone, we found the enzyme nicotinamide N-methyltransferase (NNMT) more than 5-fold upregulated. In-depth pathway analysis found the genes involved in cancer, proliferation, DNA repair and cell death. Conclusions: The higher radiation resistance in clone CE8 is likely due to NNMT overexpression. The higher levels of NNMT could affect the cellular damage resistance through depletion of the accessible amounts of nicotinamide, which is a known inhibitor of cellular DNA repair mechanisms. [Copyright &y& Elsevier]

Published

2011

6. Adipose tissue as a source of nicotinamide N-methyltransferase and homocysteine

Author

Riederer, Monika, Erwa, Wolfgang, Zimmermann, Robert, Frank, Saša, and Zechner, Rudolf

Subjects

*ADIPOSE tissues, *NICOTINAMIDE, *METHYLTRANSFERASES, *HOMOCYSTEINE, *METABOLIC detoxification, *FAT cells, *MESSENGER RNA, *LABORATORY mice

Abstract

Abstract: Nicotinamide N-methyltransferase (NNMT) catalyses the conversion of nicotinamide to 1-methylnicotinamide and plays an important role in hepatic detoxification reactions. Here we show that, in addition to the liver, 3T3-L1 adipocytes as well as human and murine adipose tissue explants express high amounts of enzymatically active NNMT. NNMT mRNA levels and enzyme activity increased in 3T3-L1 cells in a differentiation-dependent manner. Homocysteine, the atherogenic product of the NNMT-catalyzed reaction, was secreted from 3T3-L1 cells or adipose tissue cultures. Homocysteine release increased during 3T3-L1 differentiation and was reduced when adipose tissue was treated with the NNMT inhibitor 1-methylnicotinamide. Nicotinic acid (NA), a widely used drug to lower elevated plasma lipid levels, induced NNMT enzyme activity in white adipose tissue of mice. In tissue culture nicotinamide treatment led to an increase in adipose tissue homocysteine secretion. These data support the concept that adipose tissue NNMT contributes to the increased plasma homocysteine levels in patients treated with NA. [Copyright &y& Elsevier]

Published

2009

7. Nicotinamide N-methyltransferase in endothelium protects against oxidant stress-induced endothelial injury.

Author

Campagna, Roberto, Mateuszuk, Łukasz, Wojnar-Lason, Kamila, Kaczara, Patrycja, Tworzydło, Anna, Kij, Agnieszka, Bujok, Robert, Mlynarski, Jacek, Wang, Yu, Sartini, Davide, Emanuelli, Monica, and Chlopicki, Stefan

Subjects

*NICOTINAMIDE, *ENDOTHELIAL cells, *ENDOTHELIUM, *SIRTUINS, *OXIDIZING agents, *GLYCOCALYX, *CELL nuclei, *CELL survival

Abstract

Nicotinamide N -methyltransferase (NNMT, EC 2.1.1.1.) plays an important role in the growth of many different tumours and is also involved in various non-neoplastic disorders. However, the presence and role of NNMT in the endothelium has yet to be specifically explored. Here, we characterized the functional activity of NNMT in the endothelium and tested whether NNMT regulates endothelial cell viability. NNMT in endothelial cells (HAEC, HMEC-1 and EA.hy926) was inhibited using two approaches: pharmacological inhibition of the enzyme by NNMT inhibitors (5-amino-1-methylquinoline – 5MQ and 6-methoxynicotinamide – JBSF-88) or by shRNA-mediated silencing. Functional inhibition of NNMT was confirmed by LC/MS/MS-based analysis of impaired MNA production. The effects of NNMT inhibition on cellular viability were analyzed in both the absence and presence of menadione. Our results revealed that all studied endothelial lines express relatively high levels of functionally active NNMT compared with cancer cells (MDA-MB-231). Although the aldehyde oxidase 1 enzyme was also expressed in the endothelium, the further metabolites of N1-methylnicotinamide (N1-methyl-2-pyridone-5-carboxamide and N1-methyl-4-pyridone-3-carboxamide) generated by this enzyme were not detected, suggesting that endothelial NNMT-derived MNA was not subsequently metabolized in the endothelium by aldehyde oxidase 1. Menadione induced a concentration-dependent decrease in endothelial viability as evidenced by a decrease in cell number that was associated with the upregulation of NNMT and SIRT1 expression in the nucleus in viable cells. The suppression of the NNMT activity either by NNMT inhibitors or shRNA-based silencing significantly decreased the endothelial cell viability in response to menadione. Furthermore, NNMT inhibition resulted in nuclear SIRT1 expression downregulation and upregulation of the phosphorylated form of SIRT1 on Ser47. In conclusion, our results suggest that the endothelial nuclear NNMT/SIRT1 pathway exerts a cytoprotective role that safeguards endothelial cell viability under oxidant stress insult. [Display omitted] • Endothelial lines express relatively high levels of functionally active Nicotinamide N -methyltransferase (NNMT) • Aldehyde oxidase 1 (AO-1) is expressed in the endothelium, but NNMT-derived MNA did not seem to be metabolized in by AO-1. • The suppression of the NNMT activity significantly decreased the endothelial cell viability in response to menadione. • Endothelial NNMT-SIRT1 –dependent pathway exerts a protective role that safeguards cells against oxidant stress insult. [ABSTRACT FROM AUTHOR]

Published

2021

8. Thiamethoxam induces nonalcoholic fatty liver disease in mice via methionine metabolism disturb via nicotinamide N-methyltransferase overexpression.

Author

Yang, Daqian, Zhang, Xiaoting, Yue, Lei, Hu, Hailong, Wei, Xiangjuan, Guo, Qian, Zhang, Boya, Fan, Xingpei, Xin, Yuan, Oh, Yuri, and Gu, Ning

Subjects

*METHIONINE metabolism, *FATTY liver, *METHIONINE, *NICOTINAMIDE, *THIAMETHOXAM, *NEONICOTINOIDS, *METABOLIC disorders, *MOUSE diseases

Abstract

Thiamethoxam (TMX) is one of the major compounds of neonicotinoids, the most widely used class of insecticides worldwide. Previously, TMX was considered a non-toxic neonicotinoid insecticide to mammals. However, the genotoxicity, cytotoxicity, and hepatotoxicity of TMX in mammals were recently reported. Thus far, the effects of TMX on the mouse liver and its detailed mechanism remain unclear. NNMT, strongly expressed in the liver, plays a critical role in body energy expenditure. To confirm the potential pathogenesis of liver dysfunction induced by TMX, ICR mice were exposed to TMX at a dose of 4 mg/kg and 20 mg/kg by gavage administration for 12 weeks. The data showed that chronic TMX exposure caused dyslipidemia and nonalcoholic fatty liver disease (NAFLD) in mice. Moreover, aggravated oxidative stress, dysfunction, and disorganized structure were also observed in TMX-treated mouse livers. In addition, increases of PPARγ, fatty acid synthase, and NNMT expression, as well as decreases of PPARα and GNMT expression, S-adenosylmethionine deficiency, and methionine metabolism disorder were also observed in TMX-treated mouse livers. These results suggest that chronic TMX exposure induces dyslipidemia and NAFLD in mice. Moreover, inhibition of NNMT in hepatocytes significantly reversed the effects of TMX. The molecular mechanism of TMX-induced NAFLD is mostly through NNMT-mediated methionine metabolism and methyl donor balance, which ultimately regulates PPARα signaling pathway. Inhibition of NNMT could be a potentially novel strategy for blocking the progression of NAFLD induced by TMX. [Display omitted] • Thiamethoxam (TMX) induces dyslipidemia and nonalcoholic fatty liver disease (NAFLD) in mice. • TMX alters various transcription factors related to lipid synthesis and lipid oxidation. • TMX upregulates nicotinamide N-methyltransferase (NNMT) expression and disturbs S-adenosylmethionine metabolism. • TMX induces NAFLD via NNMT overexpression-mediated methionine metabolism disorder. Thiamethoxam induces nonalcoholic fatty liver disease in mice via methionine metabolism disturb associated with NNMT overexpression. [ABSTRACT FROM AUTHOR]

Published

2021

9. Qian Yang Yu Yin Granule protects against hypertension-induced renal injury by epigenetic mechanism linked to Nicotinamide N-Methyltransferase (NNMT) expression.

Author

Zhang, Shu-Fei, Mao, Xin-Jing, Jiang, Wei-Min, and Fang, Zhu-Yuan

Subjects

*KIDNEY disease prevention, *ENZYME metabolism, *CELL proliferation, *ALTERNATIVE medicine, *ANIMAL experimentation, *BIOLOGICAL assay, *CELL cycle, *CREATININE, *ENZYME-linked immunosorbent assay, *HERBAL medicine, *HISTONES, *HYPERTENSION, *LIQUID chromatography, *MASS spectrometry, *CHINESE medicine, *METHYLATION, *POLYMERASE chain reaction, *RATS, *WESTERN immunoblotting, *DNA methylation, *IN vitro studies, *EPIGENOMICS, *IN vivo studies, *DISEASE complications

Abstract

Qian Yang Yu Yin Granule (QYYY) is a Chinese herbal formulation. It is used to treat hypertensive nephropathy for decades in China, but it is unknown that the exact mechanism of QYYY on hypertensive nephropathy. The present study was to elucidate its epigenetic mechanism of QYYY on hypertensive nephropathy. In the current study, HEK293T cells' proliferation induced by Ang II was chosen to observe epigenetic mechanisms of QYYY on renal damage. The cell proliferation was examined by MTT assays and ethynyldeoxyuridine analysis. Cell cycle analysis was performed. After treatment with QYYY, expression of Nicotinamide N-methyltransferase (NNMT), sirtuin1(SIRT1), S-adenosylhomocysteine(SAH), histone H3K4 methylation, and cortactin acetylation(acetyl-cortactin,ac-cortactin) were further investigated by western-blotting and real time PCR. DNA methylation was detected by ELISA. The study also observed the changes of SIRT1, SAH, H3K4 methylation, acetyl-cortactin when NNMT over-expressed by lentivirus transfection. Angiotensin II(Ang II) induced renal damage in spontaneously hypertensive rats(SHR). After eight weeks treatment of QYYY, blood pressure, serum and urine creatinine, and urinary microalbumin(mAlb) were assessed. The concentration of N1 -methylnicotinamide were detected by liquid chromatography with tandem mass spectrometry. The protein of NNMT, ac-cortactin, H3K3me3 were also assessed in vivo. QYYY inhibited HEK293T cells' proliferation, down-regulated the expression of NNMT, SAH, acetyl-cortactin and DNA methylation, up-regulated the expression of SIRT1, histone H3K4 trimethylation(H3K4me3). Over-expression of NNMT increased the expression of SAH and acetyl-cortactin, and reduced the expression of SIRT1 and H3K4me3. The study also demonstrated that QYYY promoted urinary creatinine excretion and reduced serum creatinine and urinary mAlb in SHR. QYYY decreased the concentration of N1 -methylnicotinamide in Ang II group. QYYY decreased the protein of NNMT, ac-cortactin and increased H3K4me3 in vivo. The results showed that QYYY alleviated renal impairment of SHR and inhibited HEK293T cells' proliferation induced by Ang II through the pathway of epigenetic mechanism linked to Nicotinamide N-Methyltransferase (NNMT) expression, including histone methylation, DNA methylation and acetyl-cortactin. This study unveiled a novel molecular mechanism by which QYYY controlled the progression of hypertensive nephropathy. NNMT, as a methyltransferase --is one of the most abundant human methyltransferases in the epigenetics. NNMT catalyzes the transfer of a methyl-group from S-adenosylmethionine(SAM) to nicotinamide (NAM), histone, and DNA, forming N1 -methylnicotinamide(ME-NaM), SAH and other methylated pyridine.NAM is a precursor of nicotinamide adenine dinucleotide (NAD+) and NAD+ is a cofactor of SIRT1 deacetylase activity. Epigenetic phenomena are also being recognized as potential contributors to hypertensive nephropathy.Qian Yang Yu Yin Granule protects against hypertensive nephropathy through NNMT -mediated epigenetic mechanism. Image 1 [ABSTRACT FROM AUTHOR]

Published

2020