Your search keyword '"Dorsomorphin"' showing total 121 results

1. Empagliflozin mitigates methotrexate-induced nephrotoxicity in male albino rats: insights on the crosstalk of AMPK/Nrf2 signaling pathway

Author

Amal Anwar Mishriki, Amira Karam Khalifa, Dina Anwar Ibrahim, Ghada Mohamed Abdel Zaher Hashem, Laila Ahmed Rashed, Sahar Samir Abdelrahman, and Hesham M. Mahmoud

Subjects

Empagliflozin, Methotrexate, Dorsomorphin, AMPK, Cytochrome c, Nrf2, Therapeutics. Pharmacology, RM1-950, Pharmacy and materia medica, RS1-441

Abstract

Abstract Background The anti-diabetic drug, empagliflozin (EMPA), has many pleiotropic actions and is challenged recently to possess renoprotective properties. This renoprotective potential is proposed to be mediated via the activation of AMP-activated protein kinase (AMPK)/nuclear factor erythroid 2-related factor 2 (Nrf2) signaling pathways. This research investigated the renoprotective potential and the mechanistic pathway of EMPA against methotrexate (MTX)-induced nephrotoxicity and evaluated the role of AMPK by utilizing an AMPK inhibitor, dorsomorphin (Dorso). Methods Thirty male Wistar rats, weighing 180–200 g, were divided equally into five groups. Group I represented the control group. Nephrotoxicity was induced in the remaining rats through the administration of a single intraperitoneal injection of MTX (20 mg/kg). Rats were then randomly assigned to: Group 2 (received MTX injection only); Group 3 (received MTX and EMPA 30 mg/kg/day); Group 4 (received MTX and Dorso 0.2 mg/kg/day), Group 5 (received MTX, Dorso, EMPA). After one week, blood samples were collected, the rats were euthanized, and renal tissues were harvested for biochemical and histomorphometric assessments. Results MTX produced a significant rise in serum creatinine and tissue MDA levels; an increase in BAX, p53, cytochrome-c expression; a reduction in Bcl2 level; and disruption of renal microarchitecture. In contrast, EMPA therapy in group 3, resulted in a significant improvement of all these parameters, correlated with significant increase in AMPK phosphorylation and Nrf2 expression. Importantly, the co-administration of Dorso, in group 5, prevented EMPA’s beneficial effects. Conclusion EMPA has a potential protective effect against MTX-induced toxicity through the activation of the AMPK/Nrf2 signaling pathway.

Published

2024

2. Empagliflozin mitigates methotrexate-induced nephrotoxicity in male albino rats: insights on the crosstalk of AMPK/Nrf2 signaling pathway.

Author

Mishriki, Amal Anwar, Khalifa, Amira Karam, Ibrahim, Dina Anwar, Hashem, Ghada Mohamed Abdel Zaher, Rashed, Laila Ahmed, Abdelrahman, Sahar Samir, and Mahmoud, Hesham M.

Subjects

*AMP-activated protein kinases, *PROTEIN kinases, *CYTOCHROME c, *LABORATORY rats, *INTRAPERITONEAL injections

Abstract

Background: The anti-diabetic drug, empagliflozin (EMPA), has many pleiotropic actions and is challenged recently to possess renoprotective properties. This renoprotective potential is proposed to be mediated via the activation of AMP-activated protein kinase (AMPK)/nuclear factor erythroid 2-related factor 2 (Nrf2) signaling pathways. This research investigated the renoprotective potential and the mechanistic pathway of EMPA against methotrexate (MTX)-induced nephrotoxicity and evaluated the role of AMPK by utilizing an AMPK inhibitor, dorsomorphin (Dorso). Methods: Thirty male Wistar rats, weighing 180–200 g, were divided equally into five groups. Group I represented the control group. Nephrotoxicity was induced in the remaining rats through the administration of a single intraperitoneal injection of MTX (20 mg/kg). Rats were then randomly assigned to: Group 2 (received MTX injection only); Group 3 (received MTX and EMPA 30 mg/kg/day); Group 4 (received MTX and Dorso 0.2 mg/kg/day), Group 5 (received MTX, Dorso, EMPA). After one week, blood samples were collected, the rats were euthanized, and renal tissues were harvested for biochemical and histomorphometric assessments. Results: MTX produced a significant rise in serum creatinine and tissue MDA levels; an increase in BAX, p53, cytochrome-c expression; a reduction in Bcl2 level; and disruption of renal microarchitecture. In contrast, EMPA therapy in group 3, resulted in a significant improvement of all these parameters, correlated with significant increase in AMPK phosphorylation and Nrf2 expression. Importantly, the co-administration of Dorso, in group 5, prevented EMPA's beneficial effects. Conclusion: EMPA has a potential protective effect against MTX-induced toxicity through the activation of the AMPK/Nrf2 signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2024

3. Dorsomorphin attenuates ABCG2-mediated multidrug resistance in colorectal cancer.

Author

Xiao-Peng Li, Liang-Qi Cao, Ze-Zhong Yu, Ke He, Peng-Bo Ding, Ji-Sheng Li, Yi-Yao Shan, Yu-Bin Su, Zhong-Min Yuan, and Zhi Shi

Subjects

COLORECTAL cancer, MULTIDRUG resistance, GENETIC overexpression, MOLECULAR docking, PROTEIN expression, RAS oncogenes

Abstract

Colorectal cancer is a common malignant tumor with high mortality, for which chemotherapy resistance is one of the main reasons. The high expression of ABCG2 in the cancer cells and expulsion of anticancer drugs directly cause multidrug resistance (MDR). Therefore, the development of new ABCG2 inhibitors that block the active causes of MDR may provide a strategy for the treatment of colorectal cancer. In this study, we find that dorsomorphin (also known as compound C or BML-275) potently inhibits the transporter activity of ABCG2, thereby preserving the chemotherapeutic agents mitoxantrone and doxorubicin to antagonize MDR in ABCG2-overexpressing colorectal cancer cells. Additionally, dorsomorphin does not alter ABCG2 protein expression. The results of molecular docking studies show that dorsomorphin is bound stably to the ABCG2-binding pocket, suggesting that dorsomorphin is a potent ABCG2 inhibitor that attenuates ABCG2-mediated MDR in colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2024

4. 5'AMP-activated protein kinase: an emerging target of phytochemicals to treat chronic inflammatory diseases.

Author

Abdul Khaliq, Hafiz, Alhouayek, Mireille, Quetin-Leclercq, Joëlle, and Muccioli, Giulio G.

Subjects

*PROTEIN kinases, *INFLAMMATORY bowel diseases, *SAPONINS, *PHYTOCHEMICALS, *AMP-activated protein kinases, *INFLAMMATORY mediators

Abstract

Inflammation is a defensive response of the organism to traumatic, infectious, toxic, ischemic, and autoimmune injury. Inflammatory mediators are released to effectively eliminate the inflammatory trigger and restore homeostasis. However, failure of these processes can lead to chronic inflammatory conditions and diseases such as inflammatory bowel diseases, rheumatoid arthritis, inflammatory lung diseases, atherosclerosis, and neurodegenerative diseases. The cure of chronic inflammatory diseases remains challenging as current therapies have various limitations, such as pronounced side effects, progressive loss of efficacy, and high cost especially for biologics. In this context, phytochemicals (such as alkaloids, flavonoids, lignans, phenolic acids, saponins, terpenoids, and other classes) are considered as an interesting alternative approach. Among the numerous targets of phytochemicals, AMP-activated protein kinase (AMPK) can be considered as an interesting target in the context of inflammation. AMPK regulates inflammatory response by inhibiting inflammatory pathways (NF-κB, JAK/STAT, and MAPK) and regulating several other processes of the inflammatory response (oxidative stress, autophagy, and apoptosis). In this review, we summarize and discuss the studies focusing on phytochemicals that showed beneficial effects by blocking different inflammatory pathways implicating AMPK activation in chronic inflammatory disease models. We also highlight elements to consider when investigating AMPK in the context of phytochemicals. [ABSTRACT FROM AUTHOR]

Published

2024

5. Adiponectin receptor 1 regulates endometrial receptivity via the adenosine monophosphate‑activated protein kinase/E‑cadherin pathway.

Author

Sarankhuu, Bolor-Erdene, Jeon, Hye Jin, Jeong, Da-Un, Park, Seok-Rae, Kim, Tae-Hyun, Lee, Sung Ki, Han, Ae Ra, Yu, Seong-Lan, and Kang, Jaeku

Subjects

*REVERSE transcriptase polymerase chain reaction, *EMBRYO implantation, *AMP-activated protein kinases, *PROTEIN kinases, *GENITALIA

Abstract

Endometrial receptivity is essential for successful embryo implantation and pregnancy initiation and is regulated via various signaling pathways. Adiponectin, an important adipokine, may be a potential regulator of reproductive system functions. The aim of the present study was to elucidate the regulatory role of adiponectin receptor 1 (ADIPOR1) in endometrial receptivity. The endometrial receptivity between RL95-2 and AN3CA cell lines was confirmed using an in vitro JAr spheroid attachment model. 293T cells were transfected with control or short hairpin (sh)ADIPOR1 vectors and RL95-2 cells were transduced with lentiviral particles targeting ADIPOR1. Reverse transcription-quantitative PCR and immunoblot assays were also performed. ADIPOR1 was consistently upregulated in the endometrium during the mid-secretory phase compared with that in the proliferative phase and in receptive RL95-2 cells compared with that in non-receptive AN3CA cells. Stable cell lines with diminished ADIPOR1 expression caused by shRNA showed reduced E-cadherin expression and attenuated in vitro endometrial receptivity. ADIPOR1 regulated AMP-activated protein kinase (AMPK) activity in endometrial epithelial cells. Regulation of AMPK activity via dorsomorphin and 5-aminoimidazole-4-carboxamide ribonucleotide affected E-cadherin expression and in vitro endometrial receptivity. The ADIPOR1/AMPK/E-cadherin axis is vital to endometrial receptivity. These findings can help improve fertility treatments and outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

6. Empagliflozin mitigates type 2 diabetes-associated peripheral neuropathy: a glucose-independent effect through AMPK signaling.

Author

Abdelkader, Noha F., Elbaset, Marawan A., Moustafa, Passant E., and Ibrahim, Sherehan M.

Abstract

Diabetic peripheral neuropathy (DPN) represents a severe microvascular condition that dramatically affects diabetic patients despite adequate glycemic control, resulting in high morbidity. Thus, recently, anti-diabetic drugs that possess glucose-independent mechanisms attracted attention. This work aims to explore the potentiality of the selective sodium-glucose cotransporter-2 inhibitor, empagliflozin (EMPA), to ameliorate streptozotocin-induced DPN in rats with insight into its precise signaling mechanism. Rats were allocated into four groups, where control animals received vehicle daily for 2 weeks. In the remaining groups, DPN was elicited by single intraperitoneal injections of freshly prepared streptozotocin and nicotinamide (52.5 and 50 mg/kg, respectively). Then EMPA (3 mg/kg/p.o.) was given to two groups either alone or accompanied with the AMPK inhibitor dorsomorphin (0.2 mg/kg/i.p.). Despite the non-significant anti-hyperglycemic effect, EMPA improved sciatic nerve histopathological alterations, scoring, myelination, nerve fibers' count, and nerve conduction velocity. Moreover, EMPA alleviated responses to different nociceptive stimuli along with improved motor coordination. EMPA modulated ATP/AMP ratio, upregulated p-AMPK while reducing p-p38 MAPK expression, p-ERK1/2 and consequently p-NF-κB p65 as well as its downstream mediators (TNF-α and IL-1β), besides enhancing SOD activity and lowering MDA content. Moreover, EMPA downregulated mTOR and stimulated ULK1 as well as beclin-1. Likewise, EMPA reduced miR-21 that enhanced RECK, reducing MMP-2 and -9 contents. EMPA's beneficial effects were almost abolished by dorsomorphin administration. In conclusion, EMPA displayed a protective effect against DPN independently from its anti-hyperglycemic effect, probably via modulating the AMPK pathway to modulate oxidative and inflammatory burden, extracellular matrix remodeling, and autophagy. [ABSTRACT FROM AUTHOR]

Published

2022

7. Neuroprotective effect of liraglutide in an experimental mouse model of multiple sclerosis: role of AMPK/SIRT1 signaling and NLRP3 inflammasome.

Author

Ammar, Reham A., Mohamed, Ahmed F., Kamal, Mohamed M., Safar, Marwa M., and Abdelkader, Noha F.

Subjects

*NLRP3 protein, *NATALIZUMAB, *MYELIN proteins, *LIRAGLUTIDE, *MYELIN basic protein, *MULTIPLE sclerosis, *OLIGODENDROGLIA, *INFLAMMASOMES

Abstract

The heterogeneous nature of multiple sclerosis (MS) and the unavailability of treatments addressing its intricate network and reversing the disease state is yet an area that needs to be elucidated. Liraglutide, a glucagon-like peptide-1 analogue, recently exhibited intriguing potential neuroprotective effects. The currents study investigated its potential effect against mouse model of MS and the possible underlying mechanisms. Demyelination was induced in C57Bl/6 mice by cuprizone (400 mg/kg/day p.o.) for 5 weeks. Animals received either liraglutide (25 nmol/kg/day i.p.) or dorsomorphin, an AMPK inhibitor, (2.5 mg/Kg i.p.) 30 min before the liraglutide dose, for 4 weeks (starting from the second week). Liraglutide improved the behavioral profile in cuprizone-treated mice. Furthermore, it induced the re-myelination process through stimulating oligodendrocyte progenitor cells differentiation via Olig2 transcription activation, reflected by increased myelin basic protein and myelinated nerve fiber percentage. Liraglutide elevated the protein content of p-AMPK and SIRT1, in addition to the autophagy proteins Beclin-1 and LC3B. Liraglutide halted cellular damage as manifested by reduced HMGB1 protein and consequently TLR-4 downregulation, coupled with a decrease in NF-κB. Liraglutide also suppressed NLRP3 transcription. Dorsomorphin pre-administration indicated a possible interplay between AMPK/SIRT1 and NLRP3 inflammasome activation as it partially reversed liraglutide's effects. Immunohistochemical examination of Iba+ microglia emphasized these findings. In conclusion, liraglutide exerts neuroprotection against cuprizone-induced demyelination via anti-inflammatory, autophagic flux activation, NLRP3 inflammasome suppression, and anti-apoptotic mechanisms, possibly mediated, at least in part, via AMPK/SIRT1, autophagy, TLR-4/ NF-κB/NLRP3 signaling. The potential mechanistic insight of Lira in alleviating Cup-induced neurotoxicity via: (1) AMPK/SIRT1 pathways activation resulting in the stimulation of brain autophagy flux (confirmed by lowering Beclin-1 and LC3-B protein expression). (2) Inhibition of NLRP3 inflammasome activation, as evidenced by reduced HMGB1, TLR-4, NF-κB and NLRP3 protein expression, alongside diminishing the activation of its downstream cascade as reflected by reduced levels of caspase-1 and IL-1β protein expression. (3) A possible modulating interplay between the previously mentioned two pathways. [ABSTRACT FROM AUTHOR]

Published

2022

8. Dorsomorphin induces cancer cell apoptosis and sensitizes cancer cells to HSP90 and proteasome inhibitors by reducing nuclear heat shock factor 1 levels

Author

Na Li, Ting Wang, Zongmeng Li, Xiaoli Ye, Bo Deng, Shu Zhuo, Pengle Yao, Mengmei Yang, Hong Mei, Xiaofang Chen, Tengfei Zhu, Shiting Chen, Hui Wang, Jiming Wang, and Yingying Le

Subjects

Dorsomorphin, heat shock factor 1, heat shock protein, apoptosis, cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Objective Heat shock factor 1 (HSF1), a transcriptional regulator of heat shock proteins (HSPs), is an attractive therapeutic target for cancer. However, only a few HSF1 inhibitors have been identified so far.Methods The mRNA and protein levels of HSF1, HSPs, cleaved PARP, and phosphorylated HSF1 were examined by real-time PCR and Western blot. Forced expression, RNA interference, and immunofluorescence assay were used for mechanistic studies. Cell viability and apoptosis were measured by WST-8 assay and flow cytometry, respectively. Xenograft studies were performed in nude mice to evaluate the effect of dorsomorphin and an HSP90 inhibitor on tumor growth.Results Dorsomorphin suppressed multiple stimuli-induced and constitutive HSPs expression in cancer cells. Mechanistic studies revealed that dorsomorphin reduced heat-induced HSP expression independent of adenosine monophosphate activated protein kinase. Dorsomorphin reduced heat-stimulated HSF1 Ser320 phosphorylation and nuclear translocation, as well as resting nuclear HSF1 levels in cancer cells. Dorsomorphin induced cancer cell apoptosis by inhibiting HSF1 expression. A structure-activity study revealed that the 4-pyridyl at the 3-site of the pyrazolo [1, 5-a]pyrimidine ring is critical for the anti-HSF1 activities of dorsomorphin. Dorsomorphin sensitized cancer cells to HSP90 and proteasome inhibitors and inhibited HSP70 expression induced by these inhibitors in vitro. In tumor-bearing nude mice, dorsomorphin enhanced HSP90 inhibitor-induced cancer cell apoptosis, tumor growth inhibition, and HSP70 expression.Conclusions Dorsomorphin is an HSF1 inhibitor. It induces cancer cell apoptosis, sensitizes cancer cells to both HSP90 and proteasome inhibitors, and suppresses HSP upregulation by these drugs, which may prevent the development of drug resistance. Hence, dorsomorphin and its derivates may serve as potential precursors for developing drugs against cancer.

Published

2019

9. AMPK activation does not enhance autophagy in neurons in contrast to MTORC1 inhibition: different impact on β-amyloid clearance.

Author

Benito-Cuesta, Irene, Ordóñez-Gutiérrez, Lara, and Wandosell, Francisco

Subjects

PROTEIN kinases, AUTOPHAGY, NEURONS, MTOR inhibitors, AMYLOID

Abstract

The physiological AKT-MTORC1 and AMPK signaling pathways are considered key nodes in the regulation of anabolism-catabolism, and particularly of macroautophagy/autophagy. Indeed, it is reported that these are altered processes in neurodegenerative proteinopathies such as Alzheimer disease (AD), mainly characterized by deposits of β-amyloid (Aβ) and hyperphosphorylated MAPT. These accumulations disrupt the optimal neuronal proteostasis, and hence, the recovery/enhancement of autophagy has been proposed as a therapeutic approach against these proteinopathies. The purpose of the present study was to characterize the modulation of autophagy by MTORC1 and AMPK signaling pathways in the highly specialized neurons, as well as their repercussions on Aβ production. Using a double transgenic mice model of AD, we demonstrated that MTORC1 inhibition, either in vivo or ex vivo (primary neuronal cultures), was able to reduce amyloid secretion through moderate autophagy induction in neurons. The pharmacological prevention of autophagy in neurons augmented the Aβ secretion and reversed the effect of rapamycin, confirming the anti-amyloidogenic effects of autophagy in neurons. Inhibition of AMPK with compound C generated the expected decrease in autophagy induction, though surprisingly did not increase the Aβ secretion. In contrast, increased activity of AMPK with metformin, AICAR, 2DG, or by gene overexpression did not enhance autophagy but had different effects on Aβ secretion: whereas metformin and 2DG diminished the secreted Aβ levels, AICAR and PRKAA1/AMPK gene overexpression increased them. We conclude that AMPK has a significantly different role in primary neurons than in other reported cells, lacking a direct effect on autophagy-dependent amyloidosis. Abbreviations: 2DG: 2-deoxy-D-glucose; Aβ: β-amyloid; ACACA: acetyl-CoA carboxylase alpha; ACTB: actin beta; AD: Alzheimer disease; AICAR: 5-aminoimidazole-4-carboxamide-1-β-riboside; AKT: AKT kinases group (AKT1 [AKT serine/threonine kinase 1], AKT2 and AKT3); AMPK: adenosine 5'-monophosphate (AMP)-activated protein kinase; APP: amyloid beta precursor protein; APP/PSEN1: B6.Cg-Tg (APPSwe, PSEN1dE9) 85Dbo/J; ATG: autophagy related; ATP: adenosine triphosphate; BafA1: bafilomycin A1; CA: constitutively active; CGN: cerebellar granule neuron; CoC/compound C: dorsommorphin dihydrochloride; ELISA: enzyme-linked immunosorbent assay; GAPDH: glyceraldehyde-3-phosphate dehydrogenase; GFP: green fluorescent protein; Gmax: GlutaMAX™; IN1: PIK3C3/VPS34-IN1; KI: kinase-inactive; MAP1LC3B/LC3: microtubule associated protein 1 light chain 3; MAPT/TAU: microtubule associated protein tau; Metf: metformin; MRT: MRT68921; MTORC1: mechanistic target of rapamycin kinase complex 1; NBR1: NBR1 autophagy cargo receptor; PRKAA: 5ʹ-AMP-activated protein kinase catalytic subunit alpha; PtdIns3K: phosphatidylinositol 3-kinase; Rapa: rapamycin; RPS6KB1/S6K: ribosomal protein S6 (RPS6) kinase polypeptide 1; SCR: scramble; SQSTM1/p62: sequestosome 1; ULK1/2: unc-51 like autophagy activating kinase 1/2; WT: wild type. [ABSTRACT FROM AUTHOR]

Published

2021

10. Dorsomorphin attenuates ABCG2-mediated multidrug resistance in colorectal cancer.

Author

Li XP, Cao LQ, Yu ZZ, He K, Ding PB, Li JS, Shan YY, Su YB, Yuan ZM, and Shi Z

Abstract

Colorectal cancer is a common malignant tumor with high mortality, for which chemotherapy resistance is one of the main reasons. The high expression of ABCG2 in the cancer cells and expulsion of anticancer drugs directly cause multidrug resistance (MDR). Therefore, the development of new ABCG2 inhibitors that block the active causes of MDR may provide a strategy for the treatment of colorectal cancer. In this study, we find that dorsomorphin (also known as compound C or BML-275) potently inhibits the transporter activity of ABCG2, thereby preserving the chemotherapeutic agents mitoxantrone and doxorubicin to antagonize MDR in ABCG2-overexpressing colorectal cancer cells. Additionally, dorsomorphin does not alter ABCG2 protein expression. The results of molecular docking studies show that dorsomorphin is bound stably to the ABCG2-binding pocket, suggesting that dorsomorphin is a potent ABCG2 inhibitor that attenuates ABCG2-mediated MDR in colorectal cancer., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Li, Cao, Yu, He, Ding, Li, Shan, Su, Yuan and Shi.)

Published

2024

11. Cercosporamide inhibits bone morphogenetic protein receptor type I kinase activity in zebrafish

Author

Jelmer Hoeksma, Gerard C. M. van der Zon, Peter ten Dijke, and Jeroen den Hertog

Subjects

bone morphogenetic protein, cercosporamide, dorsomorphin, kinase inhibitor, zebrafish, Medicine, Pathology, RB1-214

Abstract

Zebrafish models are well-established tools for investigating the underlying mechanisms of diseases. Here, we identified cercosporamide, a metabolite from the fungus Ascochyta aquiliqiae, as a potent bone morphogenetic protein receptor (BMPR) type I kinase inhibitor through a zebrafish embryo phenotypic screen. The developmental defects in zebrafish, including lack of the ventral fin, induced by cercosporamide were strikingly similar to the phenotypes caused by renowned small-molecule BMPR type I kinase inhibitors and inactivating mutations in zebrafish BMPRs. In mammalian cell-based assays, cercosporamide blocked BMP/SMAD-dependent transcriptional reporter activity and BMP-induced SMAD1/5-phosphorylation. Biochemical assays with a panel of purified recombinant kinases demonstrated that cercosporamide directly inhibited kinase activity of type I BMPRs [also called activin receptor-like kinases (ALKs)]. In mammalian cells, cercosporamide selectively inhibited constitutively active BMPR type I-induced SMAD1/5 phosphorylation. Importantly, cercosporamide rescued the developmental defects caused by constitutively active Alk2 in zebrafish embryos. We believe that cercosporamide could be the first of a new class of molecules with potential to be developed further for clinical use against diseases that are causally linked to overactivation of BMPR signaling, including fibrodysplasia ossificans progressiva and diffuse intrinsic pontine glioma. This article has an associated First Person interview with the first author of the paper.

Published

2020

12. Compound C Reducing Interferon Expression by Inhibiting cGAMP Accumulation

Author

Junzhong Lai, Xuan Luo, Shuoran Tian, Xing Zhang, Shanlu Huang, Hanze Wang, Qiumei Li, Shaoli Cai, and Qi Chen

Subjects

compound C, dorsomorphin, cGAS, cGAMP, DNA sensing, type I interferon, Therapeutics. Pharmacology, RM1-950

Abstract

Cyclic GMP-AMP (cGAMP) synthase (cGAS) is a major DNA sensor responsible for cytosolic DNA-mediated innate immune response. Inhibition of cGAS may be an effective strategy for treating autoimmune diseases such as Aicardi-Goutieres syndrome and systemic lupus erythematosus. Compound C (also known as Dorsomorphin) has been annotated as a potent and reversible inhibitor for AMPKs as well as ALK protein kinases. Here, we report a new function of Compound C which can suppress dsDNA-dependent type I interferon induction. These effects were not dependent on the activities of AMPK proteins. In vitro assays and liquid chromatograph-mass spectrometry data show that Compound C has the capability of reducing cGAMP accumulation, suggesting that Compound C may function as a modulator involved in the cGAS-STING-mediated DNA sensing pathway. Furthermore, Compound C is able to rescue the autoimmune phenotypes in a mouse model carrying the Trex1 gene deficiency. These data demonstrate a new and inverse correlation between Compound C and type I interferon production in response to dsDNA signaling.

Published

2020

13. Inhibition of the BMP Signaling Pathway Ameliorated Established Clinical Symptoms of Experimental Autoimmune Encephalomyelitis.

Author

Eixarch, Herena, Calvo-Barreiro, Laura, Costa, Carme, Reverter-Vives, Gemma, Castillo, Mireia, Gil, Vanessa, Del Río, José Antonio, Montalban, Xavier, and Espejo, Carmen

Abstract

Bone morphogenetic proteins (BMPs) are secreted growth factors that belong to the transforming growth factor beta superfamily. BMPs have been implicated in physiological processes, but they are also involved in many pathological conditions. Multiple sclerosis (MS) is an immune-mediated disease of the central nervous system (CNS); however, its etiology remains elusive. Some evidence points to BMPs as important players in the pathogenesis of inflammatory and autoimmune disorders. In the present work, we studied the expression of BMP2, BMP4, BMP5, BMP6, BMP7, BMP type II receptor, and noggin in the immune system during different phases of experimental autoimmune encephalomyelitis (EAE). Major changes in the expression of BMPs took place in the initial phases of EAE. Indeed, those changes mainly affected BMP6 (whose expression was abrogated), BMP2, and BMP7 (whose expression was increased). In addition, we showed that in vivo inhibition of the BMP signaling pathway with small molecules ameliorated the already established clinical symptoms of EAE, as well as the CNS histopathological features. At the immune level, we observed an expansion of plasmacytoid dendritic cells (pDCs) in mice treated with small molecules that inhibit the BMP signaling pathway. pDCs could play an important role in promoting the expansion of antigen-specific regulatory T cells. Altogether, our data suggest a role for BMPs in early immune events that take place in myelin oligodendrocyte glycoprotein (MOG)-induced EAE. In addition, the clinical outcome of the disease was improved when the BMP signaling pathway was inhibited in mice that presented established EAE symptoms. [ABSTRACT FROM AUTHOR]

Published

2020

14. Cell death induced by dorsomorphin in adult T‐cell leukemia/lymphoma is AMPK‐independent.

Author

Aikawa, Akiyoshi, Kozako, Tomohiro, Uchida, Yuichiro, Yoshimitsu, Makoto, Ishitsuka, Kenji, Ohsugi, Takeo, and Honda, Shin‐ichiro

Subjects

*ADULT T-cell leukemia, *CELL death, *REACTIVE oxygen species, *APOPTOSIS, *INTRACELLULAR calcium

Abstract

Adult T‐cell leukemia/lymphoma (ATL) is an aggressive T‐cell neoplasm with poor prognosis that develops after chronic infection with human T‐cell leukemia virus type 1 (HTLV‐1). Although AMP‐activated protein kinase (AMPK) is a critical cellular energy sensor, it has recently become clear that AMPK can act as a tumor regulator. Here, we assessed the expression of AMPK in primary ATL cells and the effects of dorsomorphin, an AMPK inhibitor, on primary ATL cells and HTLV‐1‐infected T‐cell lines. AMPK expression in acute and chronic ATL patients was significantly higher than in asymptomatic HTLV‐1 carriers and healthy donors. Dorsomorphin induced apoptosis in peripheral blood mononuclear cells from ATL patients. Dorsomorphin also induced dose‐ and time‐dependent apoptosis in HTLV‐1‐infected T‐cell lines. Dorsomorphin increased the production of intracellular reactive oxygen species (ROS) and induced ataxia telangiectasia‐mutated Ser1981 phosphorylation and p53 accumulation. These results indicated that dorsomorphin induces apoptosis via ROS‐mediated DNA damage in HTLV‐1‐infected T‐cell lines. Furthermore, dorsomorphin suppressed the growth of human ATL tumor xenografts in NOD/SCID mice. Together, these data suggest that AMPK could be a candidate therapeutic target for ATL and that dorsomorphin could be a therapeutic agent for ATL. [ABSTRACT FROM AUTHOR]

Published

2020

15. Dorsomorphin: A novel inhibitor of Dickkopf-1 in breast cancer.

Author

Jaschke, Nikolai, Kleymann, Alexander, Hofbauer, Lorenz C., Göbel, Andy, and Rachner, Tilman D.

Subjects

*BREAST cancer, *BONE metastasis, *CANCER-related mortality, *PROTEIN kinases, *SMALL molecules

Abstract

Advanced stages of breast cancer are frequently complicated by bone metastases which cause substantial cancer-related morbidity and mortality. The Wnt-signaling antagonist Dickkopf-1 (DKK-1) has emerged as a crucial factor in the development and progression of osteolytic bone metastases. Although several signaling pathways have been implicated in promoting DKK-1 production in breast cancer cells, pharmacological interventions that interfere with tumor DKK-1 synthesis still remain scarce. In the current study, using an unbiased approach, we identified the small molecule Dorsomorphin as a potent suppressor of DKK-1 in several breast cancer cell lines (MDA-MB-231, MDA-Bone, MDA-MET and MCF7, respectively). Here, Dorsomorphin suppressed DKK-1 mRNA and protein production by 70 and 90%, respectively (p <0.001). Whereas bone morphogenic protein (BMP)- and AMP activated protein kinase (AMPK)-signaling are two well-established targets of Dorsomorphin, we show that neither pathway is essentially involved in facilitating its inhibitory effects on DKK-1. In summary, we identified Dorsomorphin as a potent pharmacological inhibitor of DKK-1 production in breast cancer cells. Whether Dorsomorphin reflects a valuable therapeutic agent in breast cancer warrants further investigations. • The small molecule Dorsomorphin acts as a potent suppressor of DKK-1 in multiple cancer cell lines. • Neither AMPK-, nor BMP-signaling are essentially involved in facilitating the effects of Dorsomorphin on DKK-1 in breast cancer. • Dorsomorphin elicits cytotoxicity at higher concentrations which might add anti-tumor potential to its clinical use. [ABSTRACT FROM AUTHOR]

Published

2020

16. Compound C Reducing Interferon Expression by Inhibiting cGAMP Accumulation.

Author

Lai, Junzhong, Luo, Xuan, Tian, Shuoran, Zhang, Xing, Huang, Shanlu, Wang, Hanze, Li, Qiumei, Cai, Shaoli, and Chen, Qi

Subjects

TYPE I interferons, INTERFERONS, SYSTEMIC lupus erythematosus, PROTEIN kinases, INVERSE relationships (Mathematics), AUTOIMMUNE diseases

Abstract

Cyclic GMP-AMP (cGAMP) synthase (cGAS) is a major DNA sensor responsible for cytosolic DNA-mediated innate immune response. Inhibition of cGAS may be an effective strategy for treating autoimmune diseases such as Aicardi-Goutieres syndrome and systemic lupus erythematosus. Compound C (also known as Dorsomorphin) has been annotated as a potent and reversible inhibitor for AMPKs as well as ALK protein kinases. Here, we report a new function of Compound C which can suppress dsDNA-dependent type I interferon induction. These effects were not dependent on the activities of AMPK proteins. In vitr o assays and liquid chromatograph-mass spectrometry data show that Compound C has the capability of reducing cGAMP accumulation, suggesting that Compound C may function as a modulator involved in the cGAS-STING-mediated DNA sensing pathway. Furthermore, Compound C is able to rescue the autoimmune phenotypes in a mouse model carrying the Trex1 gene deficiency. These data demonstrate a new and inverse correlation between Compound C and type I interferon production in response to dsDNA signaling. [ABSTRACT FROM AUTHOR]

Published

2020

17. Induction of apoptosis in hematological cancer cells by dorsomorphin correlates with BAD upregulation.

Author

Liu, Zhao, Zhang, Guizhong, Huang, Shiran, Cheng, Jian, Deng, Tian, Lu, Xiaoxu, Adeshakin, Funmilayo Oladunni, Chen, Qian, and Wan, Xiaochun

Subjects

*CANCER cells, *APOPTOSIS inhibition, *COCARCINOGENS, *BCL-2 genes, *RNA interference

Abstract

AMPK is generally a tumor suppressor. However, once cancer arises, AMPK becomes a tumor promoter instead, driving cancer development. For such AMPK-driven cancers, AMPK blockade may be a valuable therapeutic strategy. Here we show that AMPK is upregulated in a variety of hematological cancers and plays key roles in maintaining viability of tumor cells. Blockade of AMPK signaling by dorsomorphin markedly induces apoptosis in Jurkat, K562 cell lines as well as primary cancerous B cells. Mechanistically, dorsomorphin significantly upregulates the expression of BAD, a pro-apoptotic member of the Bcl-2 gene family involved in initiating apoptosis. Reduction of BAD expression by RNA interference prevents apoptosis in response to AMPK inhibition. Thus, our data found BAD integrates the pro-apoptotic effects of dorsomorphin and provided novel insights into the mechanisms by which AMPK facilitates survival signaling in hematologic tumor cells. • Bioinformatics analysis reveals AMPK is upregulated in a variety of hematological cancers. • AMPK activity is required for maintaining cell viability in hematological cancer cells. • AMPK inhibition induces apoptosis through upregulating BAD expression in hematological cancer cells. [ABSTRACT FROM AUTHOR]

Published

2020

18. AMP‐kinase inhibitor dorsomorphin reduces the proliferation and migration behavior of colorectal cancer cells by targeting the AKT/mTOR pathway.

Author

Ghanaatgar‐Kasbi, Sadaf, Amerizadeh, Forouzan, Rahmani, Farzad, Hassanian, Seyed Mahdi, Khazaei, Majid, Ferns, Gordon A., and Avan, Amir

Subjects

*REVERSE transcriptase polymerase chain reaction, *COLORECTAL cancer, *CANCER cells, *ANNEXINS, *CANCER-related mortality

Abstract

Colorectal cancer (CRC) is among the leading causes of cancer‐related mortality, despite extensive efforts in the identification of new treatment options. Hence, there is a need for the development of novel agents with therapeutic potential in treatment of CRC. Dorsomorphin has demonstrated antiproliferative activity against different malignancies. Here we have investigated the pharmaceutical potential of dorsomorphin in two‐dimensional and three‐dimensional cell‐culture models of CRC. The antiproliferative, antimigratory, apoptotic activity and effect of this agent on cell cycle was evaluated by 3‐(4,5‐Dimethylthiazol‐2‐yl)‐2,5‐diphenyltetrazolium bromide (MTT) assay, wound healing assay, and flow cytometry, respectively, while the expression of genes involved in Wnt/Pi3K pathways was assessed at mRNA and/or proteins by reverse transcription polymerase chain reaction (RT‐PCR) or western blot. Dorsomorphin inhibited CRC cell growth by modulating the cyclinD1, surviving and p‐Akt. This agent was able to reduce the migratory behaviors of CRC cells, compared to control cells, through perturbation of E‐cadherin. Also our data showed that dorsomorphin enhanced the percentage of the cells in sub‐G1 and induced apoptosis in both late/early stages, as detected by annexin V. Also the regulatory effect of dorsomorphin on oxidant/antioxidant balance was assessed by cellular reactive oxygen species (ROS) generation. In particular, these data showed that dorsomorphin markedly increased the ROS production in CRC cells. Our finding demonstrated that dorsomorphin antagonizes cell growth and migration, through perturbation of Akt/mTOR/Wnt pathways in CRC, supporting further studies on the therapeutic potential of this novel anticancer agent in treatment of CRC. [ABSTRACT FROM AUTHOR]

Published

2019

19. 5’AMP-activated protein kinase: an emerging target of phytochemicals to treat chronic inflammatory diseases

Author

Mireille Alhouayek, Hafiz Abdul Khaliq, Giulio Muccioli, Joëlle Leclercq, and UCL - SSS/LDRI - Louvain Drug Research Institute

Subjects

acute lung injury, curcuminoids, AICAR, ARDS, General Medicine, Industrial and Manufacturing Engineering, Dorsomorphin, stilbenoids, Food Science

Abstract

Inflammation is a defensive response of the organism to traumatic, infectious, toxic, ischemic, and autoimmune injury. Inflammatory mediators are released to effectively eliminate the inflammatory trigger and restore homeostasis. However, failure of these processes can lead to chronic inflammatory conditions and diseases such as inflammatory bowel diseases, rheumatoid arthritis, inflammatory lung diseases, atherosclerosis, and neurodegenerative diseases. The cure of chronic inflammatory diseases remains challenging as current therapies have various limitations, such as pronounced side effects, progressive loss of efficacy, and high cost especially for biologics. In this context, phytochemicals (such as alkaloids, flavonoids, lignans, phenolic acids, saponins, terpenoids, and other classes) are considered as an interesting alternative approach. Among the numerous targets of phytochemicals, AMP-activated protein kinase (AMPK) can be considered as an interesting target in the context of inflammation. AMPK regulates inflammatory response by inhibiting inflammatory pathways (NF-κB, JAK/STAT, and MAPK) and regulating several other processes of the inflammatory response (oxidative stress, autophagy, and apoptosis). In this review, we summarize and discuss the studies focusing on phytochemicals that showed beneficial effects by blocking different inflammatory pathways implicating AMPK activation in chronic inflammatory disease models. We also highlight elements to consider when investigating AMPK in the context of phytochemicals.

Published

2022

20. The adipokine orosomucoid alleviates adipose tissue fibrosis via the AMPK pathway

Author

Wang, Peng-yuan, Feng, Jia-yi, Zhang, Zhen, Chen, Yi, Qin, Zhen, Dai, Xian-min, Wei, Jie, Hu, Bo-han, Zhang, Wei-dong, Sun, Yang, and Liu, Xia

Published

2022

21. Effects of cellular energy homeostasis modulation through AMPK on regulation of protein translation and response to hypoxia.

Author

Gunaydin, Gurcan and Gedik, Mustafa Emre

Subjects

*HYPOXIA-inducible factor 1, *LIVER cancer, *PROTEIN expression, *HYPOXEMIA, *TREATMENT effectiveness, *PROTEINS

Abstract

Objective: AMP-activated-protein-kinase (AMPK) regulates cellular energy-homeostasis. Eukaryotic-elongationfactor- 2-kinase (eEF2K) plays important roles in regulating protein-synthesis, functions similarly to AMPK to protect cancer-cells from metabolic stress. Tumor-hypoxia induces angiogenesis with activation of hypoxia-inducible-factor- 1-alpha (HIF-1α). AMPK might be implicated both in regulation of protein-translation and response-to-hypoxia. We aimed to investigate the effects of AMPK modulation on regulation of protein translation and response-to-hypoxia by evaluating eEF2K and HIF-1α proteins in breast and hepatocellular cancers. Materials and methods: Hepatocellular (Huh-7, HepG2) and breast (SKBR-3, MDA-MB-453) cancer-cells were incubated with AMPK-activator (A769662) or inhibitor (dorsomorphin) for 8/24 h. Alterations in eEF2K/HIF-1α protein expressions were examined. Results: Cancer-cells slightly increased eEF2K expression after 24-h of AMPK-activation. Significant decreases in eEF2K expressions were observed with AMPK inhibition in all cancer-cells except Huh-7. Slight transient decrease in HIF-1α expression was observed after 8-h of AMPK-activation in all cancer-cells except MDA-MB-453. AMPK-inhibition decreased HIF-1α expression, especially in HepG2-cells. Conclusion: The effects of AMPK modulation on eEF2K/HIF-1α protein expressions were investigated. Cells with varying molecular-expression-profiles demonstrate different metabolic activities. AMPK-activation may provide adaptive advantage to cancers and such an advantage may be reverted with an AMPK-inhibitor. The current study contributes to the literature in determining the effects of therapeutic strategies targeting AMPK on cancer-cell metabolic- pathway regulation. [ABSTRACT FROM AUTHOR]

Published

2019

22. Crystal structure of Maternal Embryonic Leucine Zipper Kinase (MELK) in complex with dorsomorphin (Compound C).

Author

Rembacz, Krzysztof P., Zrubek, Karol M., Golik, Przemyslaw, Michalik, Kinga, Bogusz, Jozefina, Wladyka, Benedykt, Romanowska, Malgorzata, and Dubin, Grzegorz

Subjects

*LEUCINE zippers, *CRYSTAL structure, *PROTEIN kinase C, *LIGANDS (Biochemistry)

Abstract

Maternal Embryonic Leucine Zipper Kinase (MELK) is overexpressed in various tumors which has been convincingly linked to tumor cell survival. As such, MELK became an interesting target for pharmacological intervention. In this study we present the crystal structure of MELK in complex with dorsomorphin, an inhibitor of VEGFR and AMPK. By defining the mechanistic details of ligand recognition we identify a key residue (Cys89) at the hinge region of MELK responsible for positioning of the ligand at the catalytic pocket. This conclusion is supported by kinetic characterization of Cys89 mutants which show decreased affinity towards both ATP and dorsomorphin. The detailed binding mode of dorsomorphin characterized in this study defines a minimal requirement for MELK ligands, a valuable information for future rational design of inhibitors based on entirely new scaffolds. [ABSTRACT FROM AUTHOR]

Published

2019

23. Regulation of inositol 1,4,5-trisphosphate-induced Ca2+ release from the endoplasmic reticulum by AMP-activated kinase modulators.

Author

Arias-del-Val, Jessica, Santo-Domingo, Jaime, García-Casas, Paloma, Alvarez-Illera, Pilar, Núñez Galindo, Antonio, Wiederkehr, Andreas, Fonteriz, Rosalba I., Montero, Mayte, and Alvarez, Javier

Abstract

Graphical abstract Highlights • The AMPK activator A769662 inhibited ER-Ca2+-release mediated by the IP 3 R. • The AMPK inhibitor dorsomorphin activated ER-Ca2+-release mediated by the IP 3 R. • Our data suggest that AMPK negatively regulates IP 3 R. • Phosphoproteomic data suggests some candidates to mediate IP 3 R modulation. Abstract The 5' AMP-activated protein kinase (AMPK) is a nutrient-sensitive kinase that plays a key role in the control of cellular energy metabolism. We have explored here the relationship between AMPK and Ca2+ signaling by looking at the effect of an AMPK activator (A769662) and an AMPK inhibitor (dorsomorphin) on histamine-induced Ca2+-release from the endoplasmic reticulum (ER) in HeLa cells. Our data show that incubation with A769662 (EC 50 = 29 μM) inhibited histamine-induced Ca2+-release from the ER in intact cells, as well as inositol-1,4,5-trisphosphate (IP 3)-induced Ca2+ release in permeabilized cells. On the contrary, dorsomorphin (EC 50 = 0.4 μM) activated both histamine and IP 3 -induced Ca2+-release and reversed the effect of A769662. These results suggest a direct effect of AMPK regulation on IP 3 receptor (IP 3 R) function. A phosphoproteomic study did not reveal changes in IP 3 R phosphorylation, but showed significant changes in phosphorylation of proteins placed upstream in the IP 3 R interactome and in several proteins related with Ca2+ metabolism, which could be candidates to mediate the effects observed. In conclusion, our data suggest that AMPK negatively regulates IP 3 R. This effect constitutes a novel and very important link between Ca2+ signaling and the AMPK pathway. [ABSTRACT FROM AUTHOR]

Published

2019

24. GLIS3, a novel prognostic indicator of gastric adenocarcinoma, contributes to the malignant biological behaviors of tumor cells via modulating TGF-β1/TGFβR1/Smad1/5 signaling pathway.

Author

Zhang, Yue, Wang, Bo, Song, Hui, and Han, Min

Subjects

*BONE morphogenetic protein receptors, *TRANSFORMING growth factors-beta, *TRANSFORMING growth factors, *CELLULAR signal transduction, *ADENOCARCINOMA

Abstract

GLIS3 is highly expressed in multiple cancers, but it has not been studied in gastric adenocarcinoma (GAC). Based on bioinformatics analysis, the prognostic significance of GLIS3 in GAC was analyzed. GAC cells were transfected with small interfering (si)-GLIS3 and GLIS3 overexpression plasmid as well as treated with SB505124 [an inhibitor for transforming growth factor beta receptor 1 (TGFβR1)] and dorsomorphin [an inhibitor for bone morphogenetic protein receptor 1 (BMPR1)]. The GLIS3 expression was detected using qRT-PCR. The impacts of GLIS3 on the proliferation, invasion and migration of GAC cells were measured using cell function assays. The activation of phosphor (p)-Smad1/5 was tested by immunofluorescence. Western blot was utilized to measure the level of transforming growth factor (TGF)-β1/Smad1/5 signaling pathway-related proteins (TGF-β1, p-Smad1, Smad1, p-Smad5, Smad5). GLIS3 was expressed at high levels in GAC tissues and cell lines and its high expression could indicate the poor prognosis of GAC patients. GLIS3 inhibition declined the proliferative, invasive and migratory capabilities as well as TGF-β1 expression and phosphorylation of Smad1/5 in GAC cells. Overexpressed GLIS3 promoted proliferation, migration, invasion, TGF-β1 expression and Smad1/5 phosphorylation in GAC cells, with SB505124 reversing the effects of overexpressed GLIS3 on proliferation, migration, invasion and Smad1/5 phosphorylation whereas dorsomorphin exhibiting no influence on GLIS3-induced effects. GLIS3 facilitated the malignant phenotype of GAC cells via regulating TGF-β1/TGFβR1/Smad1/5 pathway, which may be a novel prognostic indicator of GAC and provided a target for GAC treatment. [ABSTRACT FROM AUTHOR]

Published

2023

25. Efficient retina formation requires suppression of both Activin and BMP signaling pathways in pluripotent cells

Author

Kimberly A. Wong, Michael Trembley, Syafiq Abd Wahab, and Andrea S. Viczian

Subjects

Noggin, Retina, Xenopus, Animal cap, BMP, Activin, R-SMAD, SMAD1, SMAD2, SB431542, Dorsomorphin, Science, Biology (General), QH301-705.5

Abstract

Retina formation requires the correct spatiotemporal patterning of key regulatory factors. While it is known that repression of several signaling pathways lead to specification of retinal fates, addition of only Noggin, a known BMP antagonist, can convert pluripotent Xenopus laevis animal cap cells to functional retinal cells. The aim of this study is to determine the intracellular molecular events that occur during this conversion. Surprisingly, blocking BMP signaling alone failed to mimic Noggin treatment. Overexpressing Noggin in pluripotent cells resulted in a concentration-dependent suppression of both Smad1 and Smad2 phosphorylation, which act downstream of BMP and Activin signaling, respectively. This caused a decrease in downstream targets: endothelial marker, xk81, and mesodermal marker, xbra. We treated pluripotent cells with dominant-negative receptors or the chemical inhibitors, dorsomorphin and SB431542, which each target either the BMP or Activin signaling pathway. We determined the effect of these treatments on retina formation using the Animal Cap Transplant (ACT) assay; in which treated pluripotent cells were transplanted into the eye field of host embryos. We found that inhibition of Activin signaling, in the presence of BMP signaling inhibition, promotes efficient retinal specification in Xenopus tissue, mimicking the affect of adding Noggin alone. In whole embryos, we found that the eye field marker, rax, expanded when adding both dominant-negative Smad1 and Smad2, as did treating the cells with both dorsomorphin and SB431542. Future studies could translate these findings to a mammalian culture assay, in order to more efficiently produce retinal cells in culture.

Published

2015

26. An investigation of oyster TGF-β receptor genes and their potential roles in early molluscan development.

Author

Tan, Sujian, Huan, Pin, and Liu, Baozhong

Subjects

*MOLLUSCAN shell proteins, *TRANSFORMING growth factors, *MESSENGER RNA, *BONE morphogenetic proteins, *GASTRULATION

Abstract

Though the roles of BMP signaling in development is studied extensively in insects and vertebrates, our knowledge of BMP signaling in molluscan development is limited. In the present study, we performed a genome-based analysis of TGF-β receptors in the Pacific oyster Crassostrea gigas and revealed that C. gigas possessed all five canonical members of the gene family, including three type I and two type II receptors. Whole mount in situ hybridization revealed that four receptor genes exhibited universal expression at the gastrula stage but cgi-bmprII mRNA was only expressed at the anterior lip of blastopore, indicating the regulation of BMP signaling through restricted expression of TGF-β receptors. Treatment of oyster embryos using a BMP signaling inhibitor (dorsomorphin) resulted in obvious changes of the expression of developmental regulatory genes. In particular, three dorsally expressed genes were inhibited and two genes expressed at the opposite side showed increased expression, indicating BMP signaling may function in dorsal-ventral (DV) patterning. Some of the influenced genes were potential shell-formation (pSF) genes, including the well-accepted pSF gene engrailed , and thus this indicates the development of shell field was affected by dorsomorphin treatment. Subsequent scanning electronic observation revealed morphological change of the posterior margin of the shell field. Taken together, these results indicate the roles of BMP signaling in both DV patterning and development of shell field in oyster embryo, which expands our knowledge of early molluscan development. [ABSTRACT FROM AUTHOR]

Published

2018

27. Effects of the Small Molecule Dorsomorphin on Intracellular Signaling

Author

Kudo, Tada-aki, Kanetaka, Hiroyasu, Mizuno, Kazutoshi, Ryu, Yasuhiro, Zhang, Ye, Kano, Mitsuhiro, Shimizu, Yoshinaka, Hayashi, Haruhide, Sasaki, Keiichi, editor, Suzuki, Osamu, editor, and Takahashi, Nobuhiro, editor

Published

2012

28. Alcohol Exposure Causes Overexpression of Heart Development-Related Genes by Affecting the Histone H3 Acetylation via BMP Signaling Pathway in Cardiomyoblast Cells.

Author

Shi, Jin, Zhao, Weian, Pan, Bo, Zheng, Min, Si, Lina, Zhu, Jing, Liu, Lingjuan, and Tian, Jie

Subjects

*COMPLICATIONS of alcoholism, *ACETYLTRANSFERASES, *ANIMAL experimentation, *BIOLOGICAL assay, *BONE morphogenetic proteins, *CELL culture, *CELLULAR signal transduction, *CONGENITAL heart disease, *ETHANOL, *GENE expression, *HEART, *HETEROCYCLIC compounds, *HISTONES, *HYDROLASES, *MYOCARDIUM, *PHOSPHORYLATION, *POLYMERASE chain reaction, *PROBABILITY theory, *RATS, *RESEARCH funding, *RNA, *STEM cells, *WESTERN immunoblotting, *DATA analysis software, *DESCRIPTIVE statistics, *PRECIPITIN tests, *ONE-way analysis of variance, *CHEMICAL inhibitors, *PREGNANCY

Abstract

Background Abusive alcohol utilization of pregnant woman may cause congenital heart disease ( CHD) of fetus, where alcohol ignites histone H3 hyperacetylation leading to abnormal development of heart morphogenesis and associated genes. Knowledge about the regularized upstream genes is little, but bone morphogenetic protein ( BMP) signaling may actively and prominently take part in alteration in acetylation of histone H3. The supreme objective of this study was to unearth the involvement of BMP signaling pathway in alcohol-driven hyperacetylation of histone H3 in cardiomyoblast cells. Methods Cardiomyoblast cells (H9c2 cells) were addicted with alcohol (100 mM) for 24 hours. Dorsomorphin (5 μM) was used for the inhibition of BMP signaling pathway. We detected the phosphorylation activity of SMAD1/5/8, mRNA expression, histone acetyltransferases ( HAT)/histone deacetylase ( HDAC) activity, and acetylation of histone H3. Results Following alcohol exposure, phosphorylation of SMAD1/5/8 and HAT activities was increased to a significant extent, while histone H3 acetylation and expression of heart development-related genes were also increased. The said phenomenon influenced by alcohol was reverted upon dorsomorphin treatment to the cells without effecting HDAC activity. Conclusions The data clearly identified that BMP-mediated histone H3 acetylation of heart development-related genes might be one of the possible cellular mechanisms to control alcohol-induced expression of heart development-related genes. Dorsomorphin, on the other hand, may modulate alcohol-induced hyperacetylation of histone H3 through BMP targeting, which could be a potential way to block CHD. [ABSTRACT FROM AUTHOR]

Published

2017

29. Systemic administration of dorsomorphin relieves inflammatory nociception in the mouse formalin test.

Author

Xinqiang, Yin, Yuanyuan, Jing, Zhipeng, You, Jie, Ke, Xiao, Tan, Yumeng, Hu, Chenxi, Zhu, Shiyu, Duan, Mingpeng, Yi, Yanlin, Zhu, Sihan, Chen, and Hao, Yan

Subjects

*FORMALDEHYDE, *SPINAL cord, *MICE, *INFLAMMATORY mediators, *PAIN management

Abstract

• Dorsomorphin produced antinociceptive effect in a dose-dependent manner in the mouse formalin test. • Dorsomorphin regulated TNF-α, IL-1β, IFN-β, and COX-2 in the mouse serum, spinal cord, and inflamed paw. • Dorsomorphin suppressed formalin-induced P38, and NF-κB P65 phosphorylation in the spinal cord. • Dorsomorphin inhibited formalin-induced c-fos protein expression in the spinal cord. Inflammatory pain is the most important clinical symptom of inflammatory diseases. Despite intensive research into inflammatory pain mechanisms, the majority of analgesics available are based on mechanistic classes of compounds that have been known for many years, as a result, inflammatory pain control remains a challenge for drug design in the context of clinically unmet needs in terms of safety and efficacy. A growing literature supports that pro-inflammatory cytokine signaling plays a crucial role in the development of inflammatory pain. Modulation of the pro-inflammatory cytokine may hold the key to improved pain management. Previous studies have reported that dorsomorphin played key roles in inflammation. But the role of dorsomorphin in the formalin-induced inflammatory nociception in mice has never been reported. Here, we report a new function of dorsomorphin which can inhibit formalin-induced inflammatory nociception in mice. The antinociceptive effect of dorsomorphin mainly depended on inhibiting the p38 MAPK/c-fos signaling and regulating inflammatory mediators. [ABSTRACT FROM AUTHOR]

Published

2022

30. Boosting amygdaloid GABAergic and neurotrophic machinery via dapagliflozin-enhanced LKB1/AMPK signaling in anxious demented rats.

Author

Kamel, Ahmed S., Wahid, Ahmed, Abdelkader, Noha F., and Ibrahim, Weam W.

Subjects

*BRAIN-derived neurotrophic factor, *GABA receptors, *ALZHEIMER'S disease, *PHOSPHOLIPASE C, *AMP-activated protein kinases, *PHOSPHOLIPASES, *PROTEIN kinase C

Abstract

Anxiety is a neuropsychiatric disturbance that is commonly manifested in various dementia forms involving Alzheimer's disease (AD). The mechanisms underlying AD-associated anxiety haven't clearly recognized the role of energy metabolism in anxiety represented by the amygdala's autophagic sensors; liver kinase B1 (LKB1)/adenosine monophosphate kinase (AMPK). Dapagliflozin (DAPA), a SGLT2 inhibitor, acts as an autophagic activator through LKB1 activation in several diseases including AD. Herein, the propitious yet undetected anxiolytic potential of DAPA as an autophagic enhancer was investigated in AD animal model with emphasis on amygdala's GABAergic neurotransmission and brain-derived neurotrophic factor (BDNF). Alzheimer's disease was induced by ovariectomy (OVX) along with seventy-days-D-galactose (D-Gal) administration (150 mg/kg/day, i.p). On the 43rd day of D-Gal injection, OVX/D-Gal-subjected rats received DAPA (1 mg/kg/day, p.o) alone or with dorsomorphin the AMPK inhibitor (DORSO, 25 μg/rat, i.v.). In the amygdala, LKB1/AMPK were activated by DAPA inducing GABA B2 receptor stimulation; an effect that was abrogated by DORSO. Dapagliflozin also replenished the amygdala GABA, NE, and 5-HT levels along with glutamate suppression. Moreover, DAPA triggered BDNF production with consequent activation of its receptor, TrkB through activating GABA B2 -related downstream phospholipase C/diacylglycerol/protein kinase C (PLC/DAG/PKC) signaling. This may promote GABA A expression, verifying the crosstalk between GABA A and GABA B2. The DAPA's anxiolytic effect was visualized by improved behavioral traits in elevated plus maze together with amendment of amygdala' histopathological abnormalities. Thus, the present study highlighted DAPA's anxiolytic effect which was attributed to GABA B2 activation and its function to induce BDNF/TrkB and GABA A expression through PLC/DAG/PKC pathway in AMPK-dependent manner. [Display omitted] • Dapagliflozin exerts anxiolytic effect and amends the amygdala photomicrographs. • Dapagliflozin activates LKB1/AMPK and regulates neurotransmitters level. • GABA B2 activation by dapagliflozin triggers BDNF production and GABA A upleveling. • Activation of PLC/DAG/PKC is a crucial signaling in dapagliflozin-mediated effects. • Dapagliflozin is a promising nominee for anxiety accompanying Alzheimer's disease. [ABSTRACT FROM AUTHOR]

Published

2022

31. Membrane proteome functional characterization of breast cancer-initiating cells subjected to bone morphogenetic protein signaling inhibition by dorsomorphin.

Author

Piovesana, Susy, Capriotti, Anna, Colapicchioni, Valentina, Ferraris, Francesca, La Barbera, Giorgia, and Ventura, Salvatore

Abstract

In this study, A17 cells, which are an invasive mesenchymal cell line with cancer stem cell properties, were exploited for the study of the role of bone morphogenetic protein pathways in cancer-initiating cells employing a proteomics-based approach. A17 cells were treated with the bone morphogenetic protein signaling inhibitor dorsomorphin for 3 days. After that, subcellular fractionation of cell samples was performed and the membrane fraction analyzed by shotgun proteomics. The extracted membrane proteins were enzymatically digested and the resulting peptide mixture was analyzed by nano liquid chromatography coupled to tandem mass spectrometry and relative label-free quantitation. Protein profiles of A17 membrane fractions before and after dorsomorphin treatment were compared, and further mined by Gene Ontology search. The protein profile of untreated A17 samples correlated with the mesenchymal phenotype, whereas changes were observed in dorsomorphin-treated samples, further supporting a mesenchymal to epithelial transition upon bone morphogenetic protein signaling pathway inhibition and the importance of this pathway in breast cancer cell malignancy. [ABSTRACT FROM AUTHOR]

Published

2016

32. Dorsomorphin induces cancer cell apoptosis and sensitizes cancer cells to HSP90 and proteasome inhibitors by reducing nuclear heat shock factor 1 levels

Author

Yingying Le, Xiaoli Ye, Hong Mei, Shu Zhuo, Mengmei Yang, Pengle Yao, Hui Wang, Na Li, Tengfei Zhu, Shiting Chen, Ji-Ming Wang, Bo Deng, Zongmeng Li, Xiaofang Chen, and Ting Wang

Subjects

0301 basic medicine, Cancer Research, heat shock protein, lcsh:RC254-282, Hsp90 inhibitor, 03 medical and health sciences, 0302 clinical medicine, Heat shock protein, medicine, cancer, HSF1, biology, Chemistry, fungi, apoptosis, Cancer, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Hsp90, 030104 developmental biology, heat shock factor 1, Oncology, Proteasome, Apoptosis, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, biology.protein, Original Article, Dorsomorphin

Abstract

Objective Heat shock factor 1 (HSF1), a transcriptional regulator of heat shock proteins (HSPs), is an attractive therapeutic target for cancer. However, only a few HSF1 inhibitors have been identified so far.Methods The mRNA and protein levels of HSF1, HSPs, cleaved PARP, and phosphorylated HSF1 were examined by real-time PCR and Western blot. Forced expression, RNA interference, and immunofluorescence assay were used for mechanistic studies. Cell viability and apoptosis were measured by WST-8 assay and flow cytometry, respectively. Xenograft studies were performed in nude mice to evaluate the effect of dorsomorphin and an HSP90 inhibitor on tumor growth.Results Dorsomorphin suppressed multiple stimuli-induced and constitutive HSPs expression in cancer cells. Mechanistic studies revealed that dorsomorphin reduced heat-induced HSP expression independent of adenosine monophosphate activated protein kinase. Dorsomorphin reduced heat-stimulated HSF1 Ser320 phosphorylation and nuclear translocation, as well as resting nuclear HSF1 levels in cancer cells. Dorsomorphin induced cancer cell apoptosis by inhibiting HSF1 expression. A structure-activity study revealed that the 4-pyridyl at the 3-site of the pyrazolo [1, 5-a]pyrimidine ring is critical for the anti-HSF1 activities of dorsomorphin. Dorsomorphin sensitized cancer cells to HSP90 and proteasome inhibitors and inhibited HSP70 expression induced by these inhibitors in vitro. In tumor-bearing nude mice, dorsomorphin enhanced HSP90 inhibitor-induced cancer cell apoptosis, tumor growth inhibition, and HSP70 expression.Conclusions Dorsomorphin is an HSF1 inhibitor. It induces cancer cell apoptosis, sensitizes cancer cells to both HSP90 and proteasome inhibitors, and suppresses HSP upregulation by these drugs, which may prevent the development of drug resistance. Hence, dorsomorphin and its derivates may serve as potential precursors for developing drugs against cancer.

Published

2019

33. Regulation of inositol 1,4,5-trisphosphate-induced Ca2+ release from the endoplasmic reticulum by AMP-activated kinase modulators

Author

Andreas Wiederkehr, Jessica Arias-del-Val, Rosalba I. Fonteriz, Javier Alvarez, Antonio Núñez Galindo, Pilar Alvarez-Illera, Mayte Montero, Paloma García-Casas, Jaime Santo-Domingo, Ministerio de Economía y Competitividad (España), European Commission, Junta de Castilla y León, and National Institutes of Health (US)

Subjects

AMPK, 0301 basic medicine, Physiology, Inositol-1,4,5-trisphosphate receptor, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Inositol, Protein kinase A, Ca2+ signaling, Molecular Biology, Activator (genetics), Kinase, A769662, Endoplasmic reticulum, Cell Biology, Inositol trisphosphate receptor, Cell biology, 030104 developmental biology, chemistry, Phosphorylation, 030217 neurology & neurosurgery, Dorsomorphin

Abstract

The 5' AMP-activated protein kinase (AMPK) is a nutrient-sensitive kinase that plays a key role in the control of cellular energy metabolism. We have explored here the relationship between AMPK and Ca2+ signaling by looking at the effect of an AMPK activator (A769662) and an AMPK inhibitor (dorsomorphin) on histamine-induced Ca2+-release from the endoplasmic reticulum (ER) in HeLa cells. Our data show that incubation with A769662 (EC50 = 29 μM) inhibited histamine-induced Ca2+-release from the ER in intact cells, as well as inositol-1,4,5-trisphosphate (IP3)-induced Ca2+ release in permeabilized cells. On the contrary, dorsomorphin (EC50 = 0.4 μM) activated both histamine and IP3-induced Ca2+-release and reversed the effect of A769662. These results suggest a direct effect of AMPK regulation on IP3 receptor (IP3R) function. A phosphoproteomic study did not reveal changes in IP3R phosphorylation, but showed significant changes in phosphorylation of proteins placed upstream in the IP3R interactome and in several proteins related with Ca2+ metabolism, which could be candidates to mediate the effects observed. In conclusion, our data suggest that AMPK negatively regulates IP3R. This effect constitutes a novel and very important link between Ca2+ signaling and the AMPK pathway., This work was supported by grants from the Spanish Ministerio de Economía y Competitividad [BFU2014-55731-R and BFU2017-83509-R], projects co-financed by the European Union through the European Regional Development Fund. JA-d-V has a fellowship from Junta de Castilla y León (JCyL), cofinanced by the Fondo Social Europeo (FSE). PG-C has a FPI fellowship from Ministerio de Economía y Competitividad. We also thank Löic Dayon (NIHS) for his support to address the phospho-proteomic experiment.

Published

2019

34. Modulation of AMPK Significantly Alters Uveal Melanoma Tumor Cell Viability.

Author

Deliktas O, Gedik ME, Koc I, Gunaydin G, and Kiratli H

Subjects

Humans, Cell Line, Tumor, Cell Proliferation, Cell Survival, AMP-Activated Protein Kinases pharmacology, AMP-Activated Protein Kinases therapeutic use, Melanoma drug therapy, Melanoma genetics

Abstract

Introduction: Uveal melanoma (UM) responds poorly to targeted therapies or immune checkpoint inhibitors. Adenosine monophosphate-activated protein kinase (AMPK) is a pivotal serine/threonine protein kinase that coordinates vital processes such as cell growth. Targeting AMPK pathway, which represents a critical mechanism mediating the survival of UM cells, may prove to be a novel treatment strategy for UM. We aimed to demonstrate the effects of AMPK modulation on UM cells., Methods: In silico analyses were performed to compare UM and normal melanocyte cells via Kyoto Encyclopedia of Genes and Genomes (KEGG) and Gene Set Enrichment Analysis (GSEA). The effects of AMPK modulation on cell viability and proliferation in UM cell lines with different molecular profiles (i.e., 92-1, MP46, OMM2.5, and Mel270) were investigated via XTT cell viability and proliferation assays after treating the cells with varying concentrations of A-769662 (AMPK activator) or dorsomorphin (AMPK inhibitor)., Results: KEGG/GSEA studies demonstrated that genes implicated in the AMPK signaling pathway were differentially regulated in UM. Gene sets comprising genes involved in AMPK signaling and genes involved in energy-dependent regulation of mammalian target of rapamycin by liver kinase B1-AMPK were downregulated in UM. We observed gradual decreases in the numbers of viable UM cells as the concentration of A-769662 treatment increased. All UM cells demonstrated statistically significant decreases in cell viability when treated with 200 µm A-769662. Moreover, the effects of AMPK inhibition on UM cells were potent, since low doses of dorsomorphin treatment resulted in significant decreases in viabilities of UM cells. The half maximal inhibitory concentration (IC50) values confirmed the potency of dorsomorphin treatment against UM in vitro., Conclusion: AMPK may act like a friend or a foe in cancer depending on the context. As such, the current study contributes to the literature in determining the effects of therapeutic strategies targeting AMPK in several UM cells. We propose a new perspective in the treatment of UM. Targeting AMPK pathway may open up new avenues in developing novel therapeutic approaches to improve overall survival in UM., (© 2023 The Author(s). Published by S. Karger AG, Basel.)

Published

2023

35. Anti-Trypanosoma cruzi Activity of Metabolism Modifier Compounds

Author

Joaquim Gascon, Clara Martori, Julian Sherman, Jordi Alberola, María-Jesús Pinazo, Julio Alonso-Padilla, Ana Rodriguez, Alhelí Rodríguez-Cortés, Nuria Cortes-Serra, and Nieves Martinez-Peinado

Subjects

0301 basic medicine, Chagas disease, Trypanosoma cruzi, 030106 microbiology, Catalysis, Microbiology, Inorganic Chemistry, lcsh:Chemistry, 03 medical and health sciences, chemistry.chemical_compound, dorsomorphin, Heat shock protein, 17-DMAG, parasitic diseases, medicine, Parasite hosting, Physical and Theoretical Chemistry, Amastigote, phenotypic assays, Molecular Biology, IC50, lcsh:QH301-705.5, Spectroscopy, biology, Organic Chemistry, Metabolism drugs, In vitro toxicology, General Medicine, biology.organism_classification, medicine.disease, Computer Science Applications, cytotoxicity assays, Phenotypic assays, 030104 developmental biology, chemistry, lcsh:Biology (General), lcsh:QD1-999, Cytotoxicity assays, Chronic in vivo model, metabolism drugs, Growth inhibition, chronic in vivo model, Dorsomorphin

Abstract

Chagas disease is caused by the protozoan parasite Trypanosoma cruzi and affects over 6 million people worldwide. Development of new drugs to treat this disease remains a priority since those currently available have variable efficacy and frequent adverse effects, especially during the long regimens required for treating the chronic stage of the disease. T. cruzi modulates the host cell-metabolism to accommodate the cell cytosol into a favorable growth environment and acquire nutrients for its multiplication. In this study we evaluated the specific anti-T. cruzi activity of nine bio-energetic modulator compounds. Notably, we identified that 17-DMAG, which targets the ATP-binding site of heat shock protein 90 (Hsp90), has a very high (sub-micromolar range) selective inhibition of the parasite growth. This inhibitory effect was also highly potent (IC50 = 0.27 &mu, mol L&minus, 1) against the amastigote intracellular replicative stage of the parasite. Moreover, molecular docking results suggest that 17-DMAG may bind T. cruzi Hsp90 homologue Hsp83 with good affinity. Evaluation in a mouse model of chronic T. cruzi infection did not show parasite growth inhibition, highlighting the difficulties encountered when going from in vitro assays onto preclinical drug developmental stages.

Published

2021

36. Anti

Author

Nieves, Martinez-Peinado, Clara, Martori, Nuria, Cortes-Serra, Julian, Sherman, Ana, Rodriguez, Joaquim, Gascon, Jordi, Alberola, Maria-Jesus, Pinazo, Alheli, Rodriguez-Cortes, and Julio, Alonso-Padilla

Subjects

Chagas disease, Dose-Response Relationship, Drug, Trypanosoma cruzi, Molecular Conformation, Trypanocidal Agents, Article, cytotoxicity assays, Disease Models, Animal, Mice, Structure-Activity Relationship, dorsomorphin, 17-DMAG, parasitic diseases, Animals, Humans, HSP90 Heat-Shock Proteins, metabolism drugs, Energy Metabolism, phenotypic assays, Biomarkers, Metabolic Networks and Pathways, chronic in vivo model

Abstract

Chagas disease is caused by the protozoan parasite Trypanosoma cruzi and affects over 6 million people worldwide. Development of new drugs to treat this disease remains a priority since those currently available have variable efficacy and frequent adverse effects, especially during the long regimens required for treating the chronic stage of the disease. T. cruzi modulates the host cell-metabolism to accommodate the cell cytosol into a favorable growth environment and acquire nutrients for its multiplication. In this study we evaluated the specific anti-T. cruzi activity of nine bio-energetic modulator compounds. Notably, we identified that 17-DMAG, which targets the ATP-binding site of heat shock protein 90 (Hsp90), has a very high (sub-micromolar range) selective inhibition of the parasite growth. This inhibitory effect was also highly potent (IC50 = 0.27 μmol L−1) against the amastigote intracellular replicative stage of the parasite. Moreover, molecular docking results suggest that 17-DMAG may bind T. cruzi Hsp90 homologue Hsp83 with good affinity. Evaluation in a mouse model of chronic T. cruzi infection did not show parasite growth inhibition, highlighting the difficulties encountered when going from in vitro assays onto preclinical drug developmental stages.

Published

2020

37. Autocrine activation of canonical BMP signaling regulates PD- L1 and PD- L2 expression in human dendritic cells.

Author

Martínez, Víctor G., Hidalgo, Laura, Valencia, Jaris, Hernández‐López, Carmen, Entrena, Ana, Amo, Beatriz G., Zapata, Agustín G., Vicente, Angeles, Sacedón, Rosa, and Varas, Alberto

Abstract

Bone morphogenetic proteins ( BMPs) are multifunctional growth factors regulating differentiation and proliferation in numerous systems including the immune system. Previously, we described that the BMP signaling pathway is functional in human monocyte-derived dendritic cells ( Mo DCs), which were found to express both the specific receptors and the Smad proteins required for signal transduction. In this study, we provide evidence that human Mo DCs produce BMP-4 and that this production is increased over the maturation process as is BMP signal transduction. When DCs are matured in the presence of an inhibitor of the BMP pathway, the expression of the maturation markers PD- L1 and PD- L2 is reduced, while cytokine production is not affected. As a result, these mature DCs present an augmented ability to stimulate both T cells and NK cells. Eventually, the inhibition of BMP signaling during maturation causes a reduced expression of IRF-1, a transcription factor that positively regulates the expression of PD-L1 and PD-L2. The present study indicates that the BMP signaling pathway regulates PD-L1 and PD-L2 expression in human Mo DCs during the maturation process, probably through the IRF-1 transcription factor, and also points out that the manipulation of BMP signaling might considerably improve the immunogenicity of Mo DCs used in immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2014

38. Dorsomorphin reverses the mesenchymal phenotype of breast cancer initiating cells by inhibition of bone morphogenetic protein signaling.

Author

Garulli, Chiara, Kalogris, Cristina, Pietrella, Lucia, Bartolacci, Caterina, Andreani, Cristina, Falconi, Maurizio, Marchini, Cristina, and Amici, Augusto

Subjects

*MESENCHYMAL stem cells, *PHENOTYPES, *BONE morphogenetic proteins, *CELLULAR signal transduction, *BREAST cancer, *TUMOR growth, *CANCER relapse

Abstract

Abstract: Increasing evidence supports the theory that tumor growth, homeostasis, and recurrence are dependent on a small subset of cells with stem cell properties, redefined cancer initiating cells (CICs) or cancer stem cells. Bone morphogenetic proteins (BMPs) are involved in cell-fate specification during embryogenesis, in the maintenance of developmental potency in adult stem cells and may contribute to sustain CIC populations in breast carcinoma. Using the mouse A17 cell model previously related to mesenchymal cancer stem cells and displaying properties of CICs, we investigated the role of BMPs in the control of breast cancer cell plasticity. We showed that an autocrine activation of BMP signaling is crucial for the maintenance of mesenchymal stem cell phenotype and tumorigenic potential of A17 cells. Pharmacological inhibition of BMP signaling cascade by Dorsomorphin resulted in the acquisition of epithelial-like traits by A17 cells, including expression of Citokeratin-18 and E-cadherin, through downregulation of Snail and Slug transcriptional factors and Cyclooxygenase-2 (COX2) expression, and in the loss of their stem-features and self-renewal ability. This phenotypic switch compromised A17 cell motility, invasiveness and in vitro tumor growth. These results reveal that BMPs are key molecules at the crossroad between stemness and cancer. [Copyright &y& Elsevier]

Published

2014

39. BMP2 and GDF5 induce neuronal differentiation through a Smad dependant pathway in a model of human midbrain dopaminergic neurons.

Author

Hegarty, Shane V., Sullivan, Aideen M., and O'Keeffe, Gerard W.

Subjects

*SMAD proteins, *MESENCEPHALON, *DOPAMINERGIC neurons, *PARKINSON'S disease treatment, *NEURODEGENERATION, *BONE morphogenetic proteins

Abstract

Abstract: Parkinson's disease is the second most common neurodegenerative disease, and is characterised by the progressive degeneration of the nigrostriatal dopaminergic (DA) system. Current treatments are symptomatic, and do not protect against the DA neuronal loss. One of the most promising treatment approaches is the application of neurotrophic factors to rescue the remaining population of nigrostriatal DA neurons. Therefore, the identification of new neurotrophic factors for midbrain DA neurons, and the subsequent elucidation of the molecular bases of their effects, are important. Two related members of the bone morphogenetic protein (BMP) family, BMP2 and growth differentiation factor 5 (GDF5), have been shown to have neurotrophic effects on midbrain DA neurons both in vitro and in vivo. However, the molecular (signalling pathway(s)) and cellular (direct neuronal or indirect via glial cells) mechanisms of their effects remain to be elucidated. Using the SH-SH5Y human neuronal cell line, as a model of human midbrain DA neurons, we have shown that GDF5 and BMP2 induce neurite outgrowth via a direct mechanism. Furthermore, we demonstrate that these effects are dependent on BMP type I receptor activation of canonical Smad 1/5/8 signalling. [Copyright &y& Elsevier]

Published

2013

40. Bioanalytical method development, validation and quantification of dorsomorphin in rat plasma by LC-MS/MS.

Author

Karthikeyan, K., Mahat, Mahamad Yunnus A., Chandrasekaran, S., Gopal, K., Franklin, P. X., Sivakumar, Balasubramanian Jaganatha, Singh, Gajendra, Narayanan, Shridhar, Gopalan, B., and Khan, Ansar A.

Abstract

ABSTRACT The present investigation describes the development and validation of a sensitive liquid chromatography-mass spectrometry/mass spectrometry (LC-MS/MS) method for the estimation of dorsomorphin in rat plasma. A sensitive LC-MS/MS method was developed using multiple reaction monitoring mode, with the transition of m/ z (Q1/Q3) 400.2/289.3 for dorsomorphin and m/ z (Q1/Q3) 306.2/236.3 for zaleplon. Chromatographic separation was achieved on a reverse phase Agilent XDB C18 column (100 × 4.6 mm, 5 µm). The mobile phase consisted of acetonitrile and 5 m m ammonium acetate buffer (pH 6.0) 90:10 v/v, at a flow rate of 0.8 mL/min. The effluence was ionized in positive ion mode by electrospray ionization (ESI) and quantitated by mass spectrometry. The retention times of dorsomorphin and internal standard were found to be 2.13 and 1.13 min, respectively. Mean extraction recovery of dorsomorphin and internal standard in rat plasma was above 80%. Dorsomorphin calibration curve in rat plasma was linear ( r2 ≥ 0.99) ranging from 0.005 to 10 µg/mL. Inter-day and intra-day precision and accuracy were found to be within 85-115% (coefficient of variation). This method was successfully applied for evaluation of the oral pharmacokinetic profile of dorsomorphin in male Wistar rats. Copyright © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2013

41. A gene network that coordinates preplacodal competence and neural crest specification in zebrafish

Author

Bhat, Neha, Kwon, Hye-Joo, and Riley, Bruce B.

Subjects

*ECTODERM, *NEURAL crest, *ZEBRA danio, *PERIPHERAL nervous system, *BLASTULA, *TRANSCRIPTION factors

Abstract

Abstract: Preplacodal ectoderm (PPE) and neural crest (NC) are specified at the interface of neural and nonneural ectoderm and together contribute to the peripheral nervous system in all vertebrates. Bmp activates early steps for both fates during late blastula stage. Low Bmp activates expression of transcription factors Tfap2a and Tfap2c in the lateral neural plate, thereby specifying neural crest fate. Elevated Bmp establishes preplacodal competence throughout the ventral ectoderm by coinducing Tfap2a, Tfap2c, Foxi1 and Gata3. PPE specification occurs later at the end of gastrulation and requires complete attenuation of Bmp, yet expression of PPE competence factors continues well past gastrulation. Here we show that competence factors positively regulate each other''s expression during gastrulation, forming a self-sustaining network that operates independently of Bmp. Misexpression of Tfap2a in embryos blocked for Bmp from late blastula stage can restore development of both PPE and NC. However, Tfap2a alone is not sufficient to activate any other competence factors nor does it rescue individual placodes. On the other hand, misexpression of any two competence factors in Bmp-blocked embryos can activate the entire transcription factor network and support the development of NC, PPE and some individual placodes. We also show that while these factors are partially redundant with respect to PPE specification, they later provide non-redundant functions needed for development of specific placodes. Thus, we have identified a gene regulatory network that coordinates development of NC, PPE and individual placodes in zebrafish. [Copyright &y& Elsevier]

Published

2013

42. BMP signaling is responsible for serum-induced Id2 expression

Author

Kurooka, Hisanori, Nakahiro, Takeshi, Mori, Kentaro, Sano, Kazuo, and Yokota, Yoshifumi

Subjects

*BONE morphogenetic proteins, *CELLULAR signal transduction, *SERUM, *GENE expression, *TRANSCRIPTION factors, *MESSENGER RNA, *LABORATORY mice

Abstract

Abstract: Ids function as negative regulators of basic helix–loop–helix transcription factors and their expression is rapidly induced by serum stimulation in various cell types. In this study, we investigated the molecular basis of serum-induced expression of the mouse Id2 gene in NIH3T3 cells. A small-molecule inhibitor of bone morphogenetic protein (BMP) type I receptor kinases blocked the serum induction of Id2 mRNA. The chemical compound and several inhibitory proteins specific for BMP signaling suppressed the serum-induced activation of the luciferase construct with the mouse Id2 4.6-kb promoter region. Importantly, serum stimulation evoked rapid phosphorylation of Smad1/5/8 and significant activation of the reporter plasmid containing the recently identified BMP-responsive element (BRE) of the mouse Id2. Mutation analysis demonstrated that the binding sites for Smad proteins in the Id2 BRE were critical for serum response of the 4.6-kb whole construct. Gel shift and chromatin immunoprecipitation (ChIP) assays confirmed the serum-inducible binding of Smad1/5/8 and Smad4 to the Id2 BRE in vitro and in vivo. Finally, a knockdown experiment revealed the functional importance of Smad1 in the serum induction of Id2 expression. Thus, we concluded that BMP signaling is primarily responsible for the serum-induced Id2 expression. Our results also suggest that some of the cellular effects caused by serum are mediated through BMP signaling. [Copyright &y& Elsevier]

Published

2012

43. Structural basis for specificity of TGFβ family receptor small molecule inhibitors

Author

Ogunjimi, Abiodun A., Zeqiraj, Elton, Ceccarelli, Derek F., Sicheri, Frank, Wrana, Jeffrey L., and David, Laurent

Subjects

*TRANSFORMING growth factors, *ENZYME inhibitors, *ACTIVIN, *CRYSTAL structure, *GENETIC mutation, *CELL receptors, *MOLECULAR structure

Abstract

Abstract: Transforming growth factor-β (TGFβ) receptor kinase inhibitors have a great therapeutic potential. SB431542 is one of the mainly used kinase inhibitors of the TGFβ/Activin pathway receptors, but needs improvement of its EC50 (EC50 =1μM) to be translated to clinical use. A key feature of SB431542 is that it specifically targets receptors from the TGFβ/Activin pathway but not the closely related receptors from the bone morphogenic proteins (BMP) pathway. To understand the mechanisms of this selectivity, we solved the crystal structure of the TGFβ type I receptor (TβRI) kinase domain in complex with SB431542. We mutated TβRI residues coordinating SB431542 to their counterparts in activin-receptor like kinase 2 (ALK2), a BMP receptor kinase, and tested the kinase activity of mutated TβRI. We discovered that a Ser280Thr mutation yielded a TβRI variant that was resistant to SB431542 inhibition. Furthermore, the corresponding Thr283Ser mutation in ALK2 yielded a BMP receptor sensitive to SB431542. This demonstrated that Ser280 is the key determinant of selectivity for SB431542. This work provides a framework for optimising the SB431542 scaffold to more potent and selective inhibitors of the TGFβ/Activin pathway. [Copyright &y& Elsevier]

Published

2012

44. The canonical BMP signaling pathway is involved in human monocyte-derived dendritic cell maturation.

Author

Martínez, Víctor G., Hernández-López, Carmen, Valencia, Jaris, Hidalgo, Laura, Entrena, Ana, Zapata, Agustín G., Vicente, Angeles, Sacedón, Rosa, and Varas, Alberto

Subjects

*BONE morphogenetic proteins, *DENDRITIC cells, *PEPTIDES, *TISSUES, *IMMUNITY

Abstract

Bone morphogenetic proteins (BMPs), members of the transforming growth factor-β superfamily, are multifunctional polypeptides regulating a broad spectrum of functions in embryonic and adult tissues. Recent reports have demonstrated that BMPs regulate the survival, proliferation and differentiation of several cell types in the immune system. In this study, we investigate the effects of BMP signaling activation on the capacity of human dendritic cells (DCs) to stimulate immune responses. Human DCs express type I and type II BMP receptors (BMPRIA, BMPRIB, type IA activin receptor, BMPRII) and BMP signal transduction molecules (Smad1, 5, and 8, as well as Smad4). On BMP stimulation, Id1-3 (inhibitor of differentiation 1-3/DNA binding) mRNA expression is upregulated and this effect can be blocked with the inhibitor dorsomorphin, showing that the canonical BMP signal transduction pathway is functionally active in DCs. BMP signaling activation promotes the phenotypic maturation of human DCs by increasing the expression of co-stimulatory molecules and also CD83, programmed cell death ligand 1 (PD-L1) and PD-L2, and stimulates cytokine secretion, mainly interleukin-8 and tumor necrosis factor-α. Accordingly, BMP-treated DCs exhibit an enhanced T-cell stimulatory capacity. BMP signaling also enhances the survival of human DCs increasing the Bcl-2/Bax ratio. Finally, the expression of Runx transcription factors is increased in mature DCs, and the mRNA levels of Runx1-3 are upregulated in response to BMP stimulation, indicating that Runx transcription factor family may mediate the effects of BMP signaling in human DC maturation. [ABSTRACT FROM AUTHOR]

Published

2011

45. Biomechanical forces exert anabolic effects on osteoblasts by activation of SMAD 1/5/8 through type 1 BMP receptor.

Author

Rath, B., Nam, J., Deschner, J., Schaumburger, J., Tingart, M., Grässel, S., Grifka, J., and Agarwal, S.

Abstract

Osteoblasts are mechanosensitive cells, which respond to biomechanical stimuli to regulate the bone structure through anabolic and catabolic gene regulation. To examine the effects of mechanical forces on the osteogenic responses through the SMAD signaling in osteoblasts, the cells were cultured in well-characterized mechanoresponsive 3-D scaffolds and exposed to 10% dynamic compressive strain (Cmp) at 1 Hz. Subsequently, SMAD phosphorylation and osteogenic gene induction was examined. Osteoblasts cultured in 3-D scaffolds exhibited increased constitutive SMAD 1/5/8 phosphorylation, as compared to monolayers cultures. This SMAD 1/5/8 phosphorylation was further upregulated after 10, 30 and 60 min in response to Cmp, exhibiting a peak activation at 30 min. No significant changes in SMAD2 phosphorylation were observed, suggesting signals generated by Cmp may not activate the Transforming Growth Factor-β signaling cascade. Subsequently, biomechanical stimulation-induced SMAD 1/5/8 phosphorylation upregulated the expression of osteogenic genes such as Osteoprotegrin, Msx2 and Runx2. Dorsomorphin, a selective inhibitor of the bone morphogenetic protein (BMP) receptor type 1 (BMPR1), blocked Cmp-induced SMAD 1/5/8 phosphorylation, as well as Osteoprotegrin, Msx2 and Runx2 gene expression. Collectively, the present findings demonstrate that biomechanical stimulation of osteoblasts activates SMAD 1/5/8 in the BMP signaling pathway through BMPR1 and may enhance osteogenesis by upregulating SMAD-dependent osteogenic genes. [ABSTRACT FROM AUTHOR]

Published

2011

46. Laminins, via heparan sulfate proteoglycans, participate in zebrafish myotome morphogenesis by modulating the pattern of Bmp responsiveness.

Author

Dolez, Morgane, Nicolas, Jean-François, and Hirsinger, Estelle

Subjects

*PROTEOGLYCANS, *ZEBRA danio, *MORPHOGENESIS, *HEDGEHOG signaling proteins, *EXTRACELLULAR matrix

Abstract

In zebrafish, Hedgehog-induced Engrailed expression defines a muscle fibre population that includes both slow and fast fibre types and exhibits an organisational role on myotome and surrounding tissues, such as motoneurons and lateral line. This Engrailed-positive population is restricted in the myotome to a central domain. To understand how this population is established, we have analysed the phenotype of the sly/lamc1 mutation in the Laminin γ1 chain that was shown to specifically affect Engrailed expression in pioneers. We find that the sly mutation affects Engrailed expression in the entire central domain and that Hedgehog signalling does not mediate this effect. We show that Bmp-responding cells are excluded from the central domain and that this pattern is modulated by laminins, but not by Hedgehog signalling. Knockdown of Bmp signalling rescues Engrailed expression in the sly mutant and ectopically activates Engrailed expression in slow and fast lineages in wild-type embryos. Last, extracellular matrix-associated heparan sulfate proteoglycans are absent in sly and their enzymatic removal mimics the sly phenotype. Our results therefore show that laminins, via heparan sulfate proteoglycans, are instrumental in patterning Bmp responsiveness and that Bmp signalling restricts Engrailed expression to the central domain. This study underlines the importance of extracellular cues for the precise spatial modulation of cell response to morphogens. [ABSTRACT FROM AUTHOR]

Published

2011

47. Dorsomorphin and LDN-193189 inhibit BMP-mediated Smad, p38 and Akt signalling in C2C12 cells

Author

Boergermann, J.H., Kopf, J., Yu, P.B., and Knaus, P.

Subjects

*BONE morphogenetic proteins, *CELLULAR signal transduction, *CELL lines, *MITOGEN-activated protein kinases, *CELL receptors, *TRANSFORMING growth factors

Abstract

Abstract: Bone morphogenetic proteins (BMPs) are key regulators of cell fate decisions during embryogenesis and tissue homeostasis. BMPs signal through a coordinated assembly of two types of transmembrane serine/threonine kinase receptors to induce Smad1/5/8 plus non-Smad pathways, such as MAPK and Akt. The recent discovery of BMP receptor inhibitors opened new avenues to study specific BMP signalling and to delineate this effect from TGF-β and Activin signalling. Here we present comprehensive and quantitative analyses on both canonical and non-Smad mediated BMP signalling under Dorsomorphin (DM) and LDN-193189 (LDN) treatment conditions. We demonstrate for the first time, that both compounds affect not only the Smad but also the non-Smad signalling pathways induced by either BMP2, BMP6 or GDF5. The activation of p38, ERK1/2 and Akt in C2C12 cells was inhibited by DM and LDN. In addition “off-target” effects on all branches of BMP non-Smad signalling are presented. From this we conclude that the inhibition of BMP receptors by DM and more efficiently by LDN-193189 affects all known BMP induced signalling cascades. [ABSTRACT FROM AUTHOR]

Published

2010

48. Bone morphogenetic protein 4 mediates myocardial ischemic injury through JNK-dependent signaling pathway

Author

Pachori, Alok S., Custer, Laura, Hansen, Don, Clapp, Shannon, Kemppa, Erica, and Klingensmith, John

Subjects

*BONE morphogenetic proteins, *MYOCARDIAL infarction, *ISCHEMIA, *JNK mitogen-activated protein kinases, *CELLULAR signal transduction, *LABORATORY mice, *MOLECULAR cardiology, *APOPTOSIS

Abstract

Abstract: Bone morphogenetic protein (BMP) signaling regulates embryonic development of many organ systems and defective BMP signaling has been implicated in adult disorders of many of these systems. However, its relevance in cardiac disease has not been reported. Here we demonstrate for the first time that Bmp4 activity promotes cellular apoptosis following ischemia-reperfusion (I/R) injury induced myocardial infarction (MI). Bmp4 heterozygous null mice (Bmp4 +/ −) demonstrated reduced infarct size, less myocardial apoptosis and down-regulation of pro-apoptotic proteins relative to wild-type mice following I/R injury. This was associated with reduction in I/R induced BMP4 levels in the left ventricular infarcted region. Furthermore, treatment of neonatal cardiomyocytes with BMP4 resulted in time and dose-dependent increase in cellular apoptosis and activation of the JNK MAP kinase pathway. In contrast, while JNK activation was significantly attenuated in Bmp4 +/ − mice and following Smad1 inhibition in myocytes, inhibition of JNK with a specific inhibitory peptide, TAT-JBD20, blocked BMP4 induced apoptosis. In vivo treatment of mice with Noggin, an endogenous extracellular BMP antagonist, or dorsomorphin, a small molecule inhibitor of BMP signaling, reduced infarct size, and inhibited pro-apoptotic signaling accompanied by an inhibition of Smad1 phosphorylation and JNK activation. These studies identify a novel role for Bmp4 in the pathogenesis of myocardial infarction and illustrate the use of a small molecule inhibitor of BMP signaling for treatment of acute I/R injury. [Copyright &y& Elsevier]

Published

2010

49. BMP Inhibition with Dorsomorphin Limits Adipogenic Potential of Preadipocytes.

Author

SUENAGA, Masashi, MATSUI, Tohru, and FUNABA, Masayuki

Subjects

TRANSFORMING growth factors-beta, TRANSFORMING growth factors, ACTIVIN, BONE morphogenetic proteins, GROWTH factors, FAT cells

Abstract

The article focuses on a study which explored the role of endogenous bone morphogenetic protein (BMP) activity in 3T3-L1 preadipocytes. Because BMP transmits its signal through Smad 1/5/8 phosphorylation, the expression of phospho-Smad 1/5/8 was monitored. Dorsomorphin predominantly inhibits the BMP pathway but not the structurally related transforming growth factor (TGF)-β/activin pathway as revealed by reported assays. Results indicated that activation of BMP signaling in preadipocytes is required for these cells to initiate the adipogenic program.

Published

2010

50. Ambivalent effects of compound C (dorsomorphin) on inflammatory response in LPS-stimulated rat primary microglial cultures.

Author

Łabuzek, Krzysztof, Liber, Sebastian, Gabryel, Bożena, Bułdak, Łukasz, and Okopień, Bogusław

Abstract

It was proven that compound C displays beneficial effects in models of inflammatory-induced anemia, ischemic stroke, and fibrodysplasia ossificans progressiva. Compound C influence on microglia, playing a major role in neuroinflammation, has not been evaluated yet. The aim of the present study was to determine the effect of compound C on cytokine release, NO, and reactive oxygen species (ROS) production. The rat microglial cultures were obtained by shaking the primary mixed glial cultures. Cytokine and nitrite concentrations were assayed using ELISA kits. ROS were assayed with nitroblue tetrazolium chloride. AMPK activity was assayed using the SAMS peptide. The expression of arginase I, NF-κB p65, and hypoxia-inducible factor-1 alpha (HIF-1 alpha) was evaluated using Western blot. Compound C displayed ambivalent effect depending on microglia basal activity. It up-regulated the release of TNF alpha and NO production and increased the expression of arginase I in non-stimulated microglia. However, compound C down-regulated IL-1 beta, IL-6 and TNF alpha release, NO, ROS production, and AMPK activity, diminished NF-κB and HIF-1 alpha expression, as well as increased arginase I expression in lipopolysaccharide (LPS)-stimulated microglia. Compound C did not affect iNOS expression and IL-10 and TGF-beta release in non-stimulated and LPS-stimulated microglia. The observed alterations in the release or production of inflammatory mediators may be explained by the changes in NF-κB, HIF-1 alpha, and arginase I expression and 3-(4,5-dimethylthazol-2-yl)-2,5-diphenyltetrazolinum bromide values in response to LPS, whereas the basis for the compound C effect on non-stimulated microglia remains to be investigated. [ABSTRACT FROM AUTHOR]

Published

2010