Your search keyword '"PDE3A"' showing total 86 results

1. PDE3A Is a Highly Expressed Therapy Target in Myxoid Liposarcoma.

Author

Toivanen, Kirsi, Kilpinen, Sami, Ojala, Kalle, Merikoski, Nanna, Salmikangas, Sami, Sampo, Mika, Böhling, Tom, and Sihto, Harri

Subjects

*REVERSE transcriptase polymerase chain reaction, *IMMUNOHISTOCHEMISTRY, *RNA, *SOFT tissue tumors, *CELLULAR signal transduction, *IMMUNOBLOTTING, *CELL survival, *GENE expression profiling, *GENES, *CELL proliferation, *RESEARCH funding, *ESTERASES, *CELL lines, *SENSITIVITY & specificity (Statistics), *LIPOSARCOMA

Abstract

Simple Summary: Liposarcomas (LPSs) are common soft-tissue sarcoma subtypes. There is an unmet clinical need for targeting LPS-subtype-specific highly expressed genes. We investigated RNA sequence data from a large clinical LPS sample series and an in silico transcriptome database consisting of 201 tissue types. We discovered that the PDE3A gene is highly expressed in the myxoid LPS subtype. In addition, PDE3A served as a drug target for PDE3A modulators in LPS cell lines, warranting further studies toward its usage in clinical therapy. Liposarcomas (LPSs) are a heterogeneous group of malignancies that arise from adipose tissue. Although LPSs are among the most common soft-tissue sarcoma subtypes, precision medicine treatments are not currently available. To discover LPS-subtype-specific therapy targets, we investigated RNA sequenced transcriptomes of 131 clinical LPS tissue samples and compared the data with a transcriptome database that contained 20,218 samples from 95 healthy tissues and 106 cancerous tissue types. The identified genes were referred to the NCATS BioPlanet library with Enrichr to analyze upregulated signaling pathways. PDE3A protein expression was investigated with immunohistochemistry in 181 LPS samples, and PDE3A and SLFN12 mRNA expression with RT-qPCR were investigated in 63 LPS samples. Immunoblotting and cell viability assays were used to study LPS cell lines and their sensitivity to PDE3A modulators. We identified 97, 247, and 37 subtype-specific, highly expressed genes in dedifferentiated, myxoid, and pleomorphic LPS subtypes, respectively. Signaling pathway analysis revealed a highly activated hedgehog signaling pathway in dedifferentiated LPS, phospholipase c mediated cascade and insulin signaling in myxoid LPS, and pathways associated with cell proliferation in pleomorphic LPS. We discovered a strong association between high PDE3A expression and myxoid LPS, particularly in high-grade tumors. Moreover, myxoid LPS samples showed elevated expression levels of SLFN12 mRNA. In addition, PDE3A- and SLFN12-coexpressing LPS cell lines SA4 and GOT3 were sensitive to PDE3A modulators. Our results indicate that PDE3A modulators are promising drugs to treat myxoid LPS. Further studies are required to develop these drugs for clinical use. [ABSTRACT FROM AUTHOR]

Published

2023

2. Impact of Functional Polymorphisms on Drug Survival of Biological Therapies in Patients with Moderate-to-Severe Psoriasis.

Author

Membrive-Jiménez, Cristina, Pérez-Ramírez, Cristina, Arias-Santiago, Salvador, Richetta, Antonio Giovanni, Ottini, Laura, Pineda-Lancheros, Laura Elena, Ramírez-Tortosa, Maria del Carmen, and Jiménez-Morales, Alberto

Subjects

*BIOTHERAPY, *TUMOR necrosis factors, *PSORIASIS, *SINGLE nucleotide polymorphisms, *POLYMERASE chain reaction, *ANTIRHEUMATIC agents, *KILLER cell receptors, *ADALIMUMAB

Abstract

Biological therapies (BTs) indicated for psoriasis are highly effective; however, not all patients obtain good results, and loss of effectiveness is the main reason for switching. Genetic factors may be involved. The objective of this study was to evaluate the influence of single-nucleotide polymorphisms (SNPs) on the drug survival of tumor necrosis factor inhibitors (anti-TNF) medications and ustekinumab (UTK) in patients diagnosed with moderate-to-severe psoriasis. We conducted an ambispective observational cohort study that included 379 lines of treatment with anti-TNF (n = 247) and UTK (132) in 206 white patients from southern Spain and Italy. The genotyping of the 29 functional SNPs was carried out using real-time polymerase chain reaction (PCR) with TaqMan probes. Drug survival was evaluated with Cox regression and Kaplan–Meier curves. The multivariate analysis showed that the HLA-C rs12191877-T (hazard ratio [HR] = 0.560; 95% CI = 0.40–0.78; p = 0.0006) and TNF-1031 (rs1799964-C) (HR = 0.707; 95% CI = 0.50–0.99; p = 0.048) polymorphisms are associated with anti-TNF drug survival, while TLR5 rs5744174-G (HR = 0.589; 95% CI = 0.37–0.92; p = 0.02), CD84 rs6427528-GG (HR = 0.557; 95% CI = 0.35–0.88; p = 0.013) and PDE3A rs11045392-T together with SLCO1C1 rs3794271-T (HR = 0.508; 95% CI = 0.32–0.79; p = 0.002) are related to UTK survival. The limitations are the sample size and the clustering of anti-TNF drugs; we used a homogeneous cohort of patients from 2 hospitals only. In conclusion, SNPs in the HLA-C, TNF, TLR5, CD84, PDE3A, and SLCO1C1 genes may be useful as biomarkers of drug survival of BTs indicated for psoriasis, making it possible to implement personalized medicine that will reduce financial healthcare costs, facilitate medical decision-making and improve patient quality of life. However, further pharmacogenetic studies need to be conducted to confirm these associations. [ABSTRACT FROM AUTHOR]

Published

2023

3. Velcrin molecular glues induce apoptosis in glioblastomas with high PDE3A and SLFN12 expression.

Author

Aquilanti E, Goldoni S, Baker A, Kotynkova K, Andersen S, Bozinov V, Gao GF, Cherniack AD, Lange M, Lesche R, Kopitz C, Lienau P, Lewis TA, Garrido M, Gradl S, Seidel H, Tseng YY, Ligon KL, Wen PY, Meyerson M, and Greulich H

Abstract

Background: Velcrins are molecular glues that kill cells by inducing the formation of a protein complex between the RNase SLFN12 and the phosphodiesterase PDE3A. Formation of the complex activates SLFN12, which cleaves tRNA Leu (TAA) and induces apoptosis. Velcrins such as the clinical investigational compound, BAY 2666605, were found to have activity across multiple solid tumor cell lines from the cancer cell line encyclopedia, including glioblastoma cell lines. We therefore aim to characterize velcrins as novel therapeutic agents in glioblastoma., Materials and Methods: PDE3A and SLFN12 expression levels were measured in glioblastoma cell lines, the Cancer Genome Atlas (TCGA) tumor samples, and tumor neurospheres. Velcrin-treated cells were assayed for viability, induction of apoptosis, cell cycle phases, and global changes in translation. Transcriptional profiling of the cells was obtained. Xenograft-harboring mice treated with velcrins were also monitored for survival., Results: We identified several velcrin-sensitive glioblastoma cell lines and 4 velcrin-sensitive glioblastoma patient-derived models. We determined that BAY 2666605 crosses the blood-brain barrier and elicits full tumor regression in an orthotopic xenograft model of GB1 cells. We also determined that the velcrins BAY 2666605 and BRD3800 induce tumor regression in subcutaneous glioblastoma PDX models., Conclusions: Velcrins have antitumor activity in preclinical models of glioblastoma, warranting further investigation as potential therapeutic agents., Competing Interests: P.Y.W.: Research Support: Agios, Astra Zeneca/Medimmune, Beigene, Celgene, Eli Lily, Genentech/Roche, Kazia, MediciNova, Merck, Novartis, Nuvation Bio, Oncoceutics, Vascular Biogenics, VBI Vaccines. Advisory Board: Agios, Astra Zeneca, Bayer, Boston Pharmaceuticals, CNS Pharmaceuticals, Elevate Bio Immunomic Therapeutics, Imvax, Karyopharm, Merck, Novartis, Nuvation Bio, Vascular Biogenics, VBI Vaccines, Voyager, QED, Celularity, Sapience. J.G.D.: consults for Microsoft Research, Abata Therapeutics, Servier, Maze Therapeutics, BioNTech, Sangamo, and Pfizer; consults for and has equity in Tango Therapeutics; serves as a paid scientific advisor to the Laboratory for Genomics Research, funded in part by GSK; receives funding support from the Functional Genomics Consortium: Abbvie, Bristol Myers Squibb, Janssen, Merck, and Vir Biotechnology. M.M. is the scientific advisory board chair of Isabl; consults for Bayer, DelveBio, and Interline; is an inventor of patents licensed to LabCorp and Bayer; and receives research funding from Bayer and Janssen. M.M. and H.G. receive an inventor’s share of license revenue as part of their employment for certain patent filings, including US-2016-0016913 and US-2018-0235961, which relate to aspects of the work described in this manuscript. The co-owners of these patent filings are The Broad Institute, Inc., Dana-Farber Cancer Institute, Inc., and Bayer Pharma A.G., A.D.C, and H.G. also receive research funding from Bayer. A.D.C consults for KaryoVerse. K.L.L.: Research Support: BMS; Consulting: BMS, Travera, Integragen Equity: Travera., (© The Author(s) 2024. Published by Oxford University Press, the Society for Neuro-Oncology and the European Association of Neuro-Oncology.)

Published

2024

4. Carbamazepine Induces Platelet Apoptosis and Thrombocytopenia Through Protein Kinase A

Author

Weiling Xiao, Kangxi Zhou, Mengnan Yang, Chenglin Sun, Lan Dai, Jian Gu, Rong Yan, and Kesheng Dai

Subjects

carbamazepine, thrombocytopenia, PKA, platelet apoptosis, PDE3A, Therapeutics. Pharmacology, RM1-950

Abstract

Carbamazepine is extensively used worldwide to treat a wide range of disorders such as epilepsy, peripheral neuralgia and bipolar disorder. Thrombocytopenia and hemorrhage have been identified in multiple carbamazepine-treated patients. However, the underlying mechanism remains poorly understood. Here, we show that platelets undergo apoptosis after carbamazepine treatment. The apoptotic platelets induced by carbamazepine are rapidly removed in vivo, which accounts for thrombocytopenia. We found that carbamazepine treatment attenuates the phosphorylation level of bcl-xl/bcl-2-associated death promoter (BAD), vasodilator-associated stimulated phosphoprotein (VASP) and GPIbβ in platelets, indicating an inhibition effect on protein kinase A (PKA). We further demonstrated that carbamazepine reduced PKA activity through PI3K/Akt/PDE3A signaling pathway. Pharmacological activation of PKA or inhibition of PI3K/Akt/PDE3A protects platelets from apoptosis induced by carbamazepine. Importantly, PDE3A inhibitors or PKA activator ameliorates carbamazepine-mediated thrombocytopenia in vivo. These findings shed light on a possible mechanism of carbamazepine-induced thrombocytopenia, designating PDE3A/PKA as a potential therapeutic target in the treatment of carbamazepine-induced thrombocytopenia.

Published

2021

5. Carbamazepine Induces Platelet Apoptosis and Thrombocytopenia Through Protein Kinase A.

Author

Xiao, Weiling, Zhou, Kangxi, Yang, Mengnan, Sun, Chenglin, Dai, Lan, Gu, Jian, Yan, Rong, and Dai, Kesheng

Subjects

PROTEIN kinases, CARBAMAZEPINE, THROMBOCYTOPENIA, BLOOD platelets, CELLULAR signal transduction, CELL death

Abstract

Carbamazepine is extensively used worldwide to treat a wide range of disorders such as epilepsy, peripheral neuralgia and bipolar disorder. Thrombocytopenia and hemorrhage have been identified in multiple carbamazepine-treated patients. However, the underlying mechanism remains poorly understood. Here, we show that platelets undergo apoptosis after carbamazepine treatment. The apoptotic platelets induced by carbamazepine are rapidly removed in vivo , which accounts for thrombocytopenia. We found that carbamazepine treatment attenuates the phosphorylation level of bcl-xl/bcl-2-associated death promoter (BAD), vasodilator-associated stimulated phosphoprotein (VASP) and GPIbβ in platelets, indicating an inhibition effect on protein kinase A (PKA). We further demonstrated that carbamazepine reduced PKA activity through PI3K/Akt/PDE3A signaling pathway. Pharmacological activation of PKA or inhibition of PI3K/Akt/PDE3A protects platelets from apoptosis induced by carbamazepine. Importantly, PDE3A inhibitors or PKA activator ameliorates carbamazepine-mediated thrombocytopenia in vivo. These findings shed light on a possible mechanism of carbamazepine-induced thrombocytopenia, designating PDE3A/PKA as a potential therapeutic target in the treatment of carbamazepine-induced thrombocytopenia. [ABSTRACT FROM AUTHOR]

Published

2021

6. Serum Proteomics of Older Patients Undergoing Major Cardiac Surgery: Identification of Biomarkers Associated With Postoperative Delirium.

Author

Rhee, James, Kuznetsov, Alexandra, McKay, Tina, Lyons, Margaret, Houstis, Nicholas, Mekkonen, Jennifer, Ethridge, Breanna, Ibala, Reine, Hahm, Eunice, Gitlin, Jacob, Guseh, J. Sawalla, Kitchen, Robert, Rosenzweig, Anthony, Shaefi, Shahzad, Flaczyk, Adam, Qu, Jason, and Akeju, Oluwaseun

Subjects

OLDER patients, CARDIAC surgery, PROTEOMICS, MYELOID cells, BLOOD proteins, BLOOD sampling, CARDIOPULMONARY bypass

Abstract

Background: Postoperative delirium (POD) is an acute altered mental state commonly encountered after cardiac surgery. The pathophysiological mechanisms underlying POD remain unclear. We aimed to identify circulating proteins significantly altered after major cardiac surgery with cardiopulmonary bypass (CPB). We also aimed to enable inferences on associations with POD. Methods: Serum and whole blood samples were collected before CPB (n = 16 patients; n = 8 with POD) and again from the same patients on postoperative day 1. All patients were clinically evaluated for POD on postoperative days 1–3. An aptamer-based proteomics platform (SOMAscan) was used to quantify serum protein abundance in patients with POD compared with non-POD controls. We also performed a lipopolysaccharide (LPS)-based in vitro functional analysis (TruCulture) on whole blood samples from patients with POD and non-POD controls to approximate surgical stress. Cytokine levels were determined using a Luminex immunoassay. Results: Cardiac surgery with CPB resulted in a significant (p adj < 0.01) change in 48.8% (637 out of 1,305) of proteins detected by SOMAscan. Gene set enrichment showed that the most impacted biological processes involved myeloid cell activation. Specifically, activation and degranulation of neutrophils were the top five highest-scoring processes. Pathway analyses with the Kyoto Encyclopedia of Genes and Genomes (KEGG) showed that metabolic enzymes, particularly those of glycolysis, were elevated in serum concentration after surgery. Several proteins were significantly increased postoperatively in patients diagnosed with POD relative to the non-POD controls, with interleukin-6 (IL-6) showing the greatest fold-change. LPS stimulation of whole blood samples confirmed these findings. Linear regression analysis showed a highly significant correlation between Confusion Assessment Method (CAM) scores and CPB-mediated changes in cGMP-inhibited 3′,5′-cyclic phosphodiesterase A (PDE3A). Conclusions: ardiac surgery with CPB resulted in inflammasome changes accompanied by unexpected increases in metabolic pathways. In exploratory analyses, we found that POD was associated with changes in the expression level of various proteins, most notably IL-6 and PDE3A. This study and ongoing protein biomarker studies will likely help quantify risk or confirm the diagnosis for POD and increase understanding of its pathophysiological mechanisms. [ABSTRACT FROM AUTHOR]

Published

2021

7. Shortened Fingers and Toes: GNAS Abnormalities are Not the Only Cause.

Author

Reyes, Monica, Silve, Caroline, and Jüppner, Harald

Subjects

*G protein coupled receptors, *GROWTH plate, *G proteins, *TOES, *GENETIC mutation, *BASAL cell nevus syndrome

Abstract

The PTH/PTHrP receptor (PTHR1) mediates the actions of parathyroid hormone (PTH) and PTH-related peptide (PTHrP) by coupling this G protein-coupled receptor (GPCR) to the alpha-subunit of the heterotrimeric stimulatory G protein (Gsα) and thereby to the formation of cAMP. In growth plates, PTHrP-dependent activation of the cAMP/PKA second messenger pathway prevents the premature differentiation of chondrocytes into hypertrophic cells resulting in delayed growth plate closure. Heterozygous mutations in GNAS , the gene encoding Gsα, lead to a reduction in cAMP levels in growth plate chondrocytes that is sufficient to cause shortening of metacarpals and/or -tarsals, i. e. typical skeletal aspects of Albright's Hereditary Osteodystrophy (AHO). However, heterozygous mutations in other genes, including those encoding PTHrP, PRKAR1A, PDE4D, and PDE3A, can lead to similar or even more pronounced acceleration of skeletal maturation that is particularly obvious in hands and feet, and reduces final adult height. Genetic mutations other than those resulting in Gsα haploinsufficiency thus reduce intracellular cAMP levels in growth plate chondrocytes to a similar extent and thereby accelerate skeletal maturation. [ABSTRACT FROM AUTHOR]

Published

2020

8. A severe inactivating PTH/PTHrP signaling disorder type 2 in a patient carrying a novel large deletion of the GNAS gene: a case report and review of the literature.

Author

Brancatella, Alessandro, Mantovani, Giovanna, Elli, Francesca M., Borsari, Simona, Marcocci, Claudio, and Cetani, Filomena

Abstract

Purpose: Pseudohypoparathyroidism (PHP), characterized by multihormone resistance and Albright's hereditary osteodystrophy (AHO), is caused by GNAS mutations. Whole or partial gene deletions are rare. All disorders due to inactivating mutations of the GNAS gene are now classified as "inactivating PTH/PTHrP signaling disorder type 2" (iPPSD2). This study reports a family harboring a large GNAS gene deletion in order to improve the knowledge of genotype–phenotype correlation of this disease. Methods: An 18-year-old man with severe diffuse soft ossifications and multihormone resistance underwent to clinical, biochemical, radiological, and genetic studies. A review of the literature of other cases of iPPSD2 due to GNAS large deletions was performed focusing on clinical and biochemical features. Results: The proband presented signs of hypocalcemia and marked AHO features. Laboratory tests revealed hypocalcemia, high levels of serum phosphate, PTH, TSH, and calcitonin despite therapy with calcium carbonate, calcitriol, and levothyroxine. Diffuse soft tissue ossifications and brain calcifications were shown by radiological exams. Family history was remarkable for hypocalcemia, neurocognitive impairment, and cerebral calcifications in his brother and AHO features in the maternal grandfather. The proband's mother showed short stature, whereas physical examination of the father was unremarkable. Genetic analysis of the GNAS gene revealed an unreported large deletion encompassing exons 1–7 in the proband, brother, and mother. By reviewing the literature, only six other cases were described. Conclusions: We report a kindred harboring a large GNAS deletion. A genotype–phenotype correlation was observed in term of severity of tissue ossifications in the siblings but not in the mother. [ABSTRACT FROM AUTHOR]

Published

2020

9. Impact of Functional Polymorphisms on Drug Survival of Biological Therapies in Patients with Moderate-to-Severe Psoriasis

Author

Cristina Membrive-Jiménez, Cristina Pérez-Ramírez, Salvador Arias-Santiago, Antonio Giovanni Richetta, Laura Ottini, Laura Elena Pineda-Lancheros, Maria del Carmen Ramírez-Tortosa, and Alberto Jiménez-Morales

Subjects

Inorganic Chemistry, Organic Chemistry, General Medicine, Physical and Theoretical Chemistry, adalimumab, etanercept, infliximab, ustekinumab, anti-TNF, TLR5, HLA-C, TNF-1031, PDE3A, CD84, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

Biological therapies (BTs) indicated for psoriasis are highly effective; however, not all patients obtain good results, and loss of effectiveness is the main reason for switching. Genetic factors may be involved. The objective of this study was to evaluate the influence of single-nucleotide polymorphisms (SNPs) on the drug survival of tumor necrosis factor inhibitors (anti-TNF) medications and ustekinumab (UTK) in patients diagnosed with moderate-to-severe psoriasis. We conducted an ambispective observational cohort study that included 379 lines of treatment with anti-TNF (n = 247) and UTK (132) in 206 white patients from southern Spain and Italy. The genotyping of the 29 functional SNPs was carried out using real-time polymerase chain reaction (PCR) with TaqMan probes. Drug survival was evaluated with Cox regression and Kaplan–Meier curves. The multivariate analysis showed that the HLA-C rs12191877-T (hazard ratio [HR] = 0.560; 95% CI = 0.40–0.78; p = 0.0006) and TNF-1031 (rs1799964-C) (HR = 0.707; 95% CI = 0.50–0.99; p = 0.048) polymorphisms are associated with anti-TNF drug survival, while TLR5 rs5744174-G (HR = 0.589; 95% CI = 0.37–0.92; p = 0.02), CD84 rs6427528-GG (HR = 0.557; 95% CI = 0.35–0.88; p = 0.013) and PDE3A rs11045392-T together with SLCO1C1 rs3794271-T (HR = 0.508; 95% CI = 0.32–0.79; p = 0.002) are related to UTK survival. The limitations are the sample size and the clustering of anti-TNF drugs; we used a homogeneous cohort of patients from 2 hospitals only. In conclusion, SNPs in the HLA-C, TNF, TLR5, CD84, PDE3A, and SLCO1C1 genes may be useful as biomarkers of drug survival of BTs indicated for psoriasis, making it possible to implement personalized medicine that will reduce financial healthcare costs, facilitate medical decision-making and improve patient quality of life. However, further pharmacogenetic studies need to be conducted to confirm these associations.

Published

2023

10. High cGMP and low PDE3A activity are associated with oocyte meiotic incompetence.

Author

Gershon, Eran, Maimon, Iris, Galiani, Dalia, Elbaz, Michal, Karasenti, Sharon, and Dekel, Nava

Subjects

CYCLIC guanylic acid, OVARIAN follicle, CYCLIC nucleotides, SOMATIC cells, LUTEINIZING hormone

Abstract

Resumption of meiosis in mammalian oocytes, defined as oocyte maturation, is stimulated by luteinizing hormone (LH). Fully grown oocytes can also mature spontaneously, upon their release from the ovarian follicle. However, growing oocytes fail to resume meiosis in vitro and the mechanism underlying their meiotic incompetence is unknown. It is commonly accepted that a drop in intraoocyte cyclic guanosine monophosphate (cGMP) resulting in the elevated activity of the oocyte-specific PDE3A leads to a decrease in cAMP content, essential for reinitiation of meiosis. We explored the regulation of these cyclic nucleotides and their degrading PDE3A in growing oocytes. Our research addressed the LH-induced rather than spontaneous oocyte maturation. We examined 16–21 as compared to 25-day-old, PMSG-primed rats, treated with the LH analog, hCG. The effect of LH was also examined ex vivo, in isolated ovarian follicles. We found that hCG failed to induce oocyte maturation and ovulation in the younger animals and that ovulation-associated genes were not upregulated in response to this gonadotropin. Furthemore, the drop of intraoocyte cGMP and cAMP observed in fully grown oocytes upon exposure of the ovary to LH, was not detected in growing oocytes. Interestingly, whereas the global expression of PDE3A in growing and fully grown oocytes is similar, a significantly lower activity of this enzyme was determined in growing oocytes. Our findings show that meiotic incompetence is associated with a relatively high oocyte cGMP concentration and a low activity of PDE3A, which in follicle-enclosed oocytes may represent the failure of the somatic follicle cells to respond to LH. [ABSTRACT FROM AUTHOR]

Published

2019

11. Phosphodiesterase type 3A (PDE3A), but not type 3B (PDE3B), contributes to the adverse cardiac remodeling induced by pressure overload.

Author

Polidovitch, Nazari, Yang, Sibao, Sun, Huan, Lakin, Robert, Ahmad, Faiyaz, Gao, Xiaodong, Turnbull, Patrick C., Chiarello, Carmelina, Perry, Christopher G.R., Manganiello, Vincent, Yang, Ping, and Backx, Peter H.

Subjects

*CONTRACTILE proteins, *CARDIAC patients, *VENTRICULAR remodeling, *ARTERIAL pressure, *HEART diseases, *HEART failure

Abstract

Phosphodiesterase type 3 (PDE3) inhibitors block the cAMP hydrolyzing activity of both PDE3 isoforms, PDE3A and PDE3B, which have distinct roles in the heart. Although PDE3 inhibitors improve cardiac function in heart disease patients, they also increase mortality. Nevertheless, PDE3 inhibitors can provide benefit to non-ischemic heart disease patients and are used extensively to treat heart failure in dogs. Since the isoform-dependence of the complex cardiac actions of PDE3 inhibition in diseased hearts remains unknown, we assessed the effects of PDE3 inhibitors as well as gene ablation of PDE3A or PDEB in mice following the induction of non-ischemic heart disease by pressure-overload with transverse-aortic constriction (TAC). As expected, after 6 weeks of TAC, mice exhibited left ventricular contractile dysfunction, dilation, hypertrophy and interstitial fibrosis, in association with increased macrophage numbers, activation of p38 MAPK and elevated PDE3 activity. Chronic PDE3 inhibition with milrinone (MIL), at doses that did not affect either cardiac contractility or arterial blood pressure, profoundly attenuated the adverse ventricular remodeling, reduced macrophage number and diminished p38-MAPK activation induced by TAC. Surprisingly, whole-body ablation of PDE3A, but not PDE3B, provided similar protection against TAC-induced adverse ventricular remodeling, and the addition of MIL to mice lacking PDE3A provided no further protection. Our results support the conclusion that PDE3A plays an important role in adverse cardiac remodeling induced by chronic pressure overload in mice, although the underlying biochemical mechanisms remain to be fully elucidated. The implications of this conclusion on the clinical use of PDE3 inhibitors are discussed. • PDE3 inhibition protects against ventricular remodeling due to pressure-overload. • This protection is associated with reduced p38 MAPK, calcineurin/NFAT activation. • PDE3A, not PDE3B, ablation protects against adverse effects of pressure-overload. • Cardiac PDE3 activity, PDE3A expression are increased with pressure overload. [ABSTRACT FROM AUTHOR]

Published

2019

12. A PDE3A Promoter Polymorphism Regulates cAMP-Induced Transcriptional Activity in Failing Human Myocardium.

Author

Sucharov, Carmen C., Nakano, Stephanie J., Slavov, Dobromir, Schwisow, Jessica A., Rodriguez, Erin, Nunley, Karin, Medway, Allen, Stafford, Natalie, Nelson, Penny, McKinsey, Timothy A., Movsesian, Matthew, Minobe, Wayne, Carroll, Ian A., Taylor, Matthew R.G., and Bristow, Michael R.

Subjects

*REVERSE transcriptase polymerase chain reaction, *CELL metabolism, *CELLULAR signal transduction, *COMPARATIVE studies, *CYCLIC adenylic acid, *ESTERASES, *GENETIC polymorphisms, *CARDIAC contraction, *HEART failure, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *RESEARCH funding, *EVALUATION research, *PHOSPHODIESTERASE inhibitors, *PHARMACODYNAMICS

Abstract

Background: The phosphodiesterase 3A (PDE3A) gene encodes a PDE that regulates cardiac myocyte cyclic adenosine monophosphate (cAMP) levels and myocardial contractile function. PDE3 inhibitors (PDE3i) are used for short-term treatment of refractory heart failure (HF), but do not produce uniform long-term benefit.Objectives: The authors tested the hypothesis that drug target genetic variation could explain clinical response heterogeneity to PDE3i in HF.Methods: PDE3A promoter studies were performed in a cloned luciferase construct. In human left ventricular (LV) preparations, mRNA expression was measured by reverse transcription polymerase chain reaction, and PDE3 enzyme activity by cAMP-hydrolysis.Results: The authors identified a 29-nucleotide (nt) insertion (INS)/deletion (DEL) polymorphism in the human PDE3A gene promoter beginning 2,214 nt upstream from the PDE3A1 translation start site. Transcription factor ATF3 binds to the INS and represses cAMP-dependent promoter activity. In explanted failing LVs that were homozygous for PDE3A DEL and had been treated with PDE3i pre-cardiac transplantation, PDE3A1 mRNA abundance and microsomal PDE3 enzyme activity were increased by 1.7-fold to 1.8-fold (p < 0.05) compared with DEL homozygotes not receiving PDE3i. The basis for the selective up-regulation in PDE3A gene expression in DEL homozygotes treated with PDE3i was a cAMP response element enhancer 61 nt downstream from the INS, which was repressed by INS. The DEL homozygous genotype frequency was also enriched in patients with HF.Conclusions: A 29-nt INS/DEL polymorphism in the PDE3A promoter regulates cAMP-induced PDE3A gene expression in patients treated with PDE3i. This molecular mechanism may explain response heterogeneity to this drug class, and may inform a pharmacogenetic strategy for a more effective use of PDE3i in HF. [ABSTRACT FROM AUTHOR]

Published

2019

13. Precision Medicine for Heart Failure: Back to the Future.

Author

Feldman, Arthur M.

Subjects

*HEART failure, *INDIVIDUALIZED medicine

Abstract

Corresponding Author [ABSTRACT FROM AUTHOR]

Published

2019

14. Parathyroid hormone resistance syndromes – Inactivating PTH/PTHrP signaling disorders (iPPSDs).

Author

Elli, Francesca Marta, Pereda, Arrate, Linglart, Agnès, Perez de Nanclares, Guiomar, and Mantovani, Giovanna

Abstract

Metabolic disorders caused by impairments of the Gsα/cAMP/PKA pathway affecting the signaling of PTH/PTHrP lead to features caused by non-responsiveness of target organs, in turn leading to manifestations similar to the deficiency of the hormone itself. Pseudohypoparathyroidism (PHP) and related disorders derive from a defect of the α subunit of the stimulatory G protein (Gsα) or of downstream effectors of the same pathway, such as the PKA regulatory subunit 1A and the phosphodiesterase type 4D. The increasing knowledge on these diseases made the actual classification of PHP outdated as it does not include related conditions such as acrodysostosis (ACRDYS) or progressive osseous heteroplasia (POH), so that a new nomenclature and classification has been recently proposed grouping these disorders under the term "inactivating PTH/PTHrP signaling disorder" (iPPSD). This review will focus on the pathophysiology, clinical and molecular aspects of these rare, heterogeneous but closely related diseases. [ABSTRACT FROM AUTHOR]

Published

2018

15. Lack of microRNA‐155 ameliorates renal fibrosis by targeting PDE3A/TGF‐β1/Smad signaling in mice with obstructive nephropathy.

Author

Xi, Weiwei, Zhao, Xuming, Wu, Meijun, Jia, Wenjuan, and Li, Hua

Subjects

*MESENCHYMAL stem cells, *MICRORNA, *CELL proliferation, *GENE expression, *GLOMERULONEPHRITIS

Abstract

Although microRNA‐155 (miR‐155) is implicated in the pathogenesis of several fibrotic diseases, information regarding its functional role in renal fibrosis is limited. The current study aims to investigate the effects of miR‐155 on renal fibrosis in unilateral ureteral occlusion (UUO) mice. MiR‐155 level was significantly increased in renal tissues of UUO mice and TGF‐β1‐treated HK2 cells. Masson's trichrome staining showed that delivery of adeno‐associated virus encoding miR‐155 inhibitor led to a decrease in renal fibrosis induced by UUO. The increased expression of plasminogen activator inhibitor type 1, collagen III and collagen IV was also inhibited after miR‐155 inhibition. In addition, miR‐155 knockdown also prevented TGF‐β1‐induced epithelial–mesenchymal transition, concomitantly with a restoration of E‐cadherin expression and a decrease of vimentin expression. Computational analysis revealed that miR‐155 directly targets at 3′UTR of PDE3A. Overexpression of miR‐155 suppressed the luciferase activity and protein expression of PDE3A, whereas inhibition of miR‐155 increased PDE3A luciferase activity and expression. Furthermore, miR‐155 inhibited TGF‐β1‐induced the increase of TGF‐β1 expression and Smad‐2/3 phosphorylation in HK2 cells. In contrast, knockdown of PDE3A reversed the effect of miR‐155 inhibition on TGF‐β1 expression. This study demonstrates that knockdown of miR‐155 attenuates renal fibrosis via inhibiting TGF‐β1/Smad signaling activation by targeting the upstream molecule PDE3A. This study suggests that miR‐155 inhibition may be a novel therapeutic approach for preventing fibrotic kidney diseases. [ABSTRACT FROM AUTHOR]

Published

2018

16. Targeting tumor cells based on Phosphodiesterase 3A expression.

Author

Nazir, Madiha, Senkowski, Wojciech, Nyberg, Frida, Blom, Kristin, Edqvist, Per-Henrik, Jarvius, Malin, Andersson, Claes, Gustafsson, Mats G., Nygren, Peter, Larsson, Rolf, and Fryknäs, Mårten

Subjects

*CANCER cells, *PHOSPHODIESTERASES, *IMMUNOFLUORESCENCE, *GASTROINTESTINAL stromal tumors, *IMMUNOSTAINING

Abstract

We and others have previously reported a correlation between high phosphodiesterase 3 A ( PDE3A ) expression and selective sensitivity to phosphodiesterase (PDE) inhibitors. This indicates that PDE3 A could serve both as a drug target and a biomarker of sensitivity to PDE3 inhibition. In this report, we explored publicly available mRNA gene expression data to identify cell lines with different PDE3A expression. Cell lines with high PDE3A expression showed marked in vitro sensitivity to PDE inhibitors zardaverine and quazinone, when compared with those having low PDE3A expression. Immunofluorescence and immunohistochemical stainings were in agreement with PDE3A mRNA expression, providing suitable alternatives for biomarker analysis of clinical tissue specimens. Moreover, we here demonstrate that tumor cells from patients with ovarian carcinoma show great variability in PDE3A protein expression and that level of PDE3A expression is correlated with sensitivity to PDE inhibition. Finally, we demonstrate that PDE3A is highly expressed in subsets of patient tumor cell samples from different solid cancer diagnoses and expressed at exceptional levels in gastrointestinal stromal tumor (GIST) specimens. Importantly, vulnerability to PDE3 inhibitors has recently been associated with co-expression of PDE3A and Schlafen family member 12 ( SLFN12). We here demonstrate that high expression of PDE3A in clinical specimens, at least on the mRNA level, seems to be frequently associated with high SLFN12 expression. In conclusion, PDE3A seems to be both a promising biomarker and drug target for individualized drug treatment of various cancers. [ABSTRACT FROM AUTHOR]

Published

2017

17. Synthesis and biological evaluation of 8-aryl-2-morpholino-7-O-substituted benzo[e][1,3]oxazin-4-ones against DNA-PK, PI3K, PDE3A enzymes and platelet aggregation.

Author

Saifuzzaman, Md., Morrison, Rick, Zheng, Zhaohua, Orive, Stephanie, Hamilton, Justin, Thompson, Philip E., and Al-Rawi, Jasim M.a.

Subjects

*BLOOD platelet aggregation, *ETHER synthesis, *SUZUKI reaction, *STERIC hindrance, *METHOXY compounds

Abstract

A series of 40 7-(O-substituted)-2-morpholino-8-aryl-4H-benzo[ e ][1,3]oxazin-4-one derivatives was synthesized. They were prepared via synthesis of a key precursor, 8-bromo-7-hydroxy-2-morpholino-4H-benzo[ e ][1,3]oxazin-4-one 13 which was amenable to ether synthesis at the 7-position and Suzuki coupling at the 8-position. The 2 protons of 7-OCH 2 in compounds 18g , 18h , 18i , 18l and 18m prove to be magnetically non-equivalent, atropisomerism (axial chirality), as result of sterically hindered rotation of the bulky 8-aryl-substituent. The products were evaluated for their activities against PI3K isoforms, DNA-PK and PDE3. The results showed that this substitution pattern has a deleterious effect on PI3K activities, which may arise from steric hindrance in the active site. PI3Kδ was somewhat more tolerant of this substitution particularly where 8-(4-methoxylphenyl) substituents were present (IC 50 s ∼ 2–3 μM). Good activities against PDE3 were also obtained for compounds, with particular members of the 7-(2-pyridinyl) methoxy series 19 showing good inhibition (IC 50 s ∼ 2–3 μM), comparable to previously described analogues. A piperazinyl derivative 26a effectively inhibited ADP-induced platelet aggregation with an IC 50 of 8 μM. [ABSTRACT FROM AUTHOR]

Published

2017

18. PDE3A is hypermethylated in cisplatin resistant non-small cell lung cancer cells and is a modulator of chemotherapy response.

Author

TIAN, F.-M., ZHONG, C.-Y., WANG, X.-N., and MENG, Y.

Abstract

OBJECTIVE: In this study, we aimed to investigate the mechanism of PDE3A downregulation in chemoresistant non-small cell lung cancer (NSCLC) cells, its functional role in chemotherapy response and association with survival outcomes. MATERIALS AND METHODS: The raw data of GDS5247 was downloaded from GEO datasets and reanalyzed. The expression of PDE3A in patients with NSCLC and its DNA methylation status were analyzed in NSCLC cohort in TCGA database. Cisplatin resistant A549/Cis cells and the parental A549 cells were used as the in vitro cell model. The association between PDE3A expression and overall survival (OS) and progression- free survival (PFS) in NSCLC patients with adenocarcinoma or squamous cell carcinoma, as well as the median OS and PFS, were assessed by Kaplan-Meier curves using Kaplan- Meier plotter. RESULTS: PDE3A was significantly downregulated in chemoresistant NSCLC cells. Heat map of PDE3A expression and methylation in NSCLC patient cohort in TCGA database indicated a negative association between PDE3A expression and DNA methylation in lung adenocarcinoma. A549/Cis cells treated with 5-AZA-dC, a demethylation reagent, had significantly restored PDE3A expression. High PDE3A expression was associated with favorable OS (HR: 0.53, 95% CI: 0.41-0.68, p<0.0001) and PFS (HR: 0.54, 95% CI: 0.39-0.75, p<0.001) in patients with adenocarcinoma. However, in patients with squamous cell carcinoma, high PDE3A expression was associated with unfavorable OS (HR: 1.56, 95% CI: 1.08- 2.24, p=0.017) and PFS (HR: 1.83, 95% CI: 1.02- 3.29, p=0.04). CONCLUSIONS: PDE3A is downregulated in chemoresistant NSCLC cells due to DNA hypermethylation. Enforced PDE3A expression can sensitize A549/Cis cells to cisplatin. High PDE3A expression is associated with better OS and PFS in patients with adenocarcinoma, but not in patients with squamous cell carcinoma. [ABSTRACT FROM AUTHOR]

Published

2017

19. cUMP hydrolysis by PDE3A.

Author

Berrisch, Stefan, Ostermeyer, Jessica, Kaever, Volkhard, Kälble, Solveig, Hilfiker-Kleiner, Denise, Seifert, Roland, and Schneider, Erich

Abstract

As previously reported, the cardiac phosphodiesterase PDE3A hydrolyzes cUMP. Moreover, cUMP-degrading activity was detected in cow and dog hearts several decades ago. Our aim was to characterize the enzyme kinetic parameters of PDE3A-mediated cUMP hydrolysis and to investigate whether cUMP and cUMP-hydrolyzing PDEs are present in cardiomyocytes. PDE3A-mediated cUMP hydrolysis was characterized in time course, inhibitor, and Michaelis-Menten kinetics experiments. Intracellular cyclic nucleotide (cNMP) concentrations and the mRNAs of cUMP-degrading PDEs were quantitated in neonatal rat cardiomyocytes (NRCMs) and murine HL-1 cardiomyogenic cells. Moreover, we investigated cUMP degradation in HL-1 cell homogenates and intact cells. Educts (cNMPs) and products (NMPs) of the PDE reactions were detected by HPLC-coupled tandem mass spectrometry. PDE3A degraded cUMP (measurement of UMP formation) with a K value of ~143 μM and a V value of ~42 μmol/min/mg. PDE3A hydrolyzed cAMP with a K value of ~0.7 μM and a V of ~1.2 μmol/min/mg (determination of AMP formation). The PDE3 inhibitor milrinone inhibited cUMP hydrolysis (determination of UMP formation) by PDE3A ( K = 57 nM). Significant amounts of cUMP as well as of PDE3A mRNA (in addition to PDE3B and PDE9A transcripts) were detected in HL-1 cells and NRCMs. Although HL-1 cell homogenates contain a milrinone-sensitive cUMP-hydrolyzing activity, intact HL-1 cells may use additional PDE3-independent mechanisms for cUMP disposal. PDE3A is a low-affinity and high-velocity PDE for cUMP. Future studies should investigate biological effects of cUMP in cardiomyocytes and the role of PDE3A in detoxifying high intracellular cUMP concentrations under pathophysiological conditions. [ABSTRACT FROM AUTHOR]

Published

2017

20. Clinical and Molecular Perspectives of Monogenic Hypertension

Author

Peter Levanovich, Alexander Diaczok, and Noreen F. Rossi

Subjects

Epithelial sodium channel, medicine.medical_specialty, Heredity, medicine.drug_class, ENaC, Inheritance Patterns, Blood Pressure, 030204 cardiovascular system & hematology, Essential hypertension, Article, WNK, 03 medical and health sciences, 0302 clinical medicine, Mineralocorticoid receptor, Risk Factors, monogenic, Internal medicine, mineralocorticoid, Internal Medicine, medicine, Humans, Genetic Predisposition to Disease, Liddle's syndrome, 030212 general & internal medicine, aldosteronism, PDE3A, business.industry, Pseudohypoaldosteronism, Apical membrane, Prognosis, medicine.disease, Glucocorticoid remediable aldosteronism, Pedigree, Phenotype, Endocrinology, Mineralocorticoid, Hypertension, Mutation, liddle’s syndrome, business

Abstract

Advances in molecular research techniques have enabled a new frontier in discerning the mechanisms responsible for monogenic diseases. In this review, we discuss the current research on the molecular pathways governing blood pressure disorders with a Mendelian inheritance pattern, each presenting with a unique pathophysiology. Glucocorticoid Remediable Aldosteronism (GRA) and Apparent Mineralocorticoid Excess (AME) are caused by mutations in regulatory enzymes that induce increased production of mineralocorticoids or inhibit degradation of glucocorticoids, respectively. Geller syndrome is due to a point mutation in the hormone responsive element of the promotor for the mineralocorticoid receptor, rendering the receptor susceptible to activation by progesterone, leading to hypertension during pregnancy. Pseudohypoaldosteronism type II (PHA-II), also known as Gordon’s syndrome or familial hyperkalemic hypertension, is a more variable disorder typically characterized by hypertension, high plasma potassium and metabolic acidosis. Mutations in a variety of intracellular enzymes that lead to enhanced sodium reabsorption have been identified. In contrast, hypertension in Liddle’s syndrome, which results from mutations in the Epithelial sodium Channel (ENaC), is associated with low plasma potassium and metabolic alkalosis. In Liddle’s syndrome, truncation of one the ENaC protein subunits removes a binding site necessary protein for ubiquitination and degradation, thereby promoting accumulation along the apical membrane and enhanced sodium reabsorption. The myriad effects due to mutation in phosphodiesterase 3A (PDE3A) lead to severe hypertension underlying sodium-independent autosomal dominant hypertension with brachydactyly. How mutations in PDE3A result in the phenotypic features of this disorder are discussed. Understanding the pathologies of these monogenic hypertensive disorders may provide insight into the causes of the more prevalent essential hypertension and new avenues to unravel the complexities of blood pressure regulation.

Published

2020

21. A severe inactivating PTH/PTHrP signaling disorder type 2 in a patient carrying a novel large deletion of the GNAS gene: a case report and review of the literature

Author

Giovanna Mantovani, Francesca Elli, Claudio Marcocci, Simona Borsari, Alessandro Brancatella, and Filomena Cetani

Subjects

Male, musculoskeletal diseases, Proband, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, PHP, PDE4D, Short stature, Gs, 03 medical and health sciences, Exon, 0302 clinical medicine, Endocrinology, Internal medicine, PDE3A, PRKAR1A, Pseudohypoparathyroidism, Pseudopseudohypoparathyroidism, Chromogranins, GTP-Binding Protein alpha Subunits, Gs, Humans, Parathyroid Hormone-Related Protein, Hypocalcemia, medicine, GNAS complex locus, Osteodystrophy, biology, business.industry, medicine.disease, GTP-Binding Protein alpha Subunits, 030220 oncology & carcinogenesis, biology.protein, medicine.symptom, business

Abstract

Pseudohypoparathyroidism (PHP), characterized by multihormone resistance and Albright’s hereditary osteodystrophy (AHO), is caused by GNAS mutations. Whole or partial gene deletions are rare. All disorders due to inactivating mutations of the GNAS gene are now classified as “inactivating PTH/PTHrP signaling disorder type 2” (iPPSD2). This study reports a family harboring a large GNAS gene deletion in order to improve the knowledge of genotype–phenotype correlation of this disease. An 18-year-old man with severe diffuse soft ossifications and multihormone resistance underwent to clinical, biochemical, radiological, and genetic studies. A review of the literature of other cases of iPPSD2 due to GNAS large deletions was performed focusing on clinical and biochemical features. The proband presented signs of hypocalcemia and marked AHO features. Laboratory tests revealed hypocalcemia, high levels of serum phosphate, PTH, TSH, and calcitonin despite therapy with calcium carbonate, calcitriol, and levothyroxine. Diffuse soft tissue ossifications and brain calcifications were shown by radiological exams. Family history was remarkable for hypocalcemia, neurocognitive impairment, and cerebral calcifications in his brother and AHO features in the maternal grandfather. The proband’s mother showed short stature, whereas physical examination of the father was unremarkable. Genetic analysis of the GNAS gene revealed an unreported large deletion encompassing exons 1–7 in the proband, brother, and mother. By reviewing the literature, only six other cases were described. We report a kindred harboring a large GNAS deletion. A genotype–phenotype correlation was observed in term of severity of tissue ossifications in the siblings but not in the mother.

Published

2020

22. Identification of a direct interaction of protein kinase A with the L-type Ca2+ channel and characterization of effects of PDE3A mutations on cardiac myocytes

Author

Pallien, Tamara

Subjects

Cardiomyocytes, PDE3A, LTCC, PKA, 500 Naturwissenschaften und Mathematik::570 Biowissenschaften, Biologie::572 Biochemie, Excitation-Contraction Coupling

Abstract

In the heart, the excitation-contraction coupling (ECC) pathway links excitation at the plasma membrane to contraction of the cardiomyocytes. The L-type Ca2+ channel (LTCC) and phosphodiesterase 3A (PDE3A) play important roles in this pathway by facilitating Ca2+ influx into the cytosol and hydrolysis of cAMP at subcellular compartments e.g. the sarcoplasmic reticulum (SR) and in the cytosol. Regulation of the LTCC opening is modulated by proteins found in its local environment, amongst them the catalytic subunit of PKA (PKA-CS). However, how PKA-CS is tethered to the channel is unclear. Recently, it was found that the GTP-binding protein Rad is associated with the LTCC and is blocking the pore-forming a1c subunit in the basal state (Liu et al., 2020). PKA phosphorylation of Rad in response to a-adrenergic stimulation leads to its dissociation from the channel complex, releasing the inhibitory effect. In the first part of this work, a novel interaction of PKA-CS with the C terminus of the a1c subunit is described. This interaction was mapped to two regulatory regions of a1c, the distal and the proximal regulatory domain (DCRD and PCRD). Mutating the DCRD and PCRD regions affected the interaction with PKA-CS in vitro but not in a cellular environment, pointing towards a complex regulatory mechanism involving several proteins or an alternative recruitment process. The two regions did not affect the enzymatic activity of PKA-CS. The LTCC and isoform 1 of PDE3A were found in a complex in HEK293 cells, however no further functional link could be found. In the second part of this thesis, effects of mutations in PDE3A were characterized. These mutations cause hypertension with brachydactyly type E (HTNB). Affected individuals experience progressive hypertension and have characteristic shorter metacarpals. If untreated, patients die before the age of 50. Surprisingly, their hearts do not show hypertension-induced cardiac damage. This points to a cardioprotective effect of PDE3A mutations. HiPSC-CMs expressing T445N or R862C PDE3A HTNB-causing substitutions were established and differentiated to cardiac myocytes as a model system to study Ca2+ cycling. The mutant cells showed lower PDE3A and the LTCC a1c subunit protein levels and a longer Ca2+ dwell time in the cytosol compared to the wild-type (WT) cells. This might be an adaptive mechanism to improve contractility of the cells that contributes to the cardioprotective effect of the mutations.

Published

2022

23. Serum Proteomics of Older Patients Undergoing Major Cardiac Surgery: Identification of Biomarkers Associated With Postoperative Delirium

Author

James Rhee, Alexandra Kuznetsov, Tina McKay, Margaret Lyons, Nicholas Houstis, Jennifer Mekkonen, Breanna Ethridge, Reine Ibala, Eunice Hahm, Jacob Gitlin, J. Sawalla Guseh, Robert Kitchen, Anthony Rosenzweig, Shahzad Shaefi, Adam Flaczyk, Jason Qu, and Oluwaseun Akeju

Subjects

Aging, medicine.medical_specialty, Surgical stress, Cognitive Neuroscience, medicine.medical_treatment, Neurosciences. Biological psychiatry. Neuropsychiatry, Gastroenterology, law.invention, postoperative delirium, proteomics, TIMP-1, law, Internal medicine, Cardiopulmonary bypass, Medicine, SOMAscan, Interleukin 6, Original Research, Whole blood, IL-6, PDE3A, biology, business.industry, Aging Neuroscience, TruCulture, Pathophysiology, Cardiac surgery, Cytokine, biology.protein, Biomarker (medicine), cardiopulmonary bypass, business, RC321-571

Abstract

BackgroundPostoperative delirium (POD) is an acute altered mental state commonly encountered after cardiac surgery. The pathophysiological mechanisms underlying POD remain unclear. We aimed to identify circulating proteins significantly altered after major cardiac surgery with cardiopulmonary bypass (CPB). We also aimed to enable inferences on associations with POD.MethodsSerum and whole blood samples were collected before CPB (n = 16 patients; n = 8 with POD) and again from the same patients on postoperative day 1. All patients were clinically evaluated for POD on postoperative days 1–3. An aptamer-based proteomics platform (SOMAscan) was used to quantify serum protein abundance in patients with POD compared with non-POD controls. We also performed a lipopolysaccharide (LPS)-based in vitro functional analysis (TruCulture) on whole blood samples from patients with POD and non-POD controls to approximate surgical stress. Cytokine levels were determined using a Luminex immunoassay.ResultsCardiac surgery with CPB resulted in a significant (padj < 0.01) change in 48.8% (637 out of 1,305) of proteins detected by SOMAscan. Gene set enrichment showed that the most impacted biological processes involved myeloid cell activation. Specifically, activation and degranulation of neutrophils were the top five highest-scoring processes. Pathway analyses with the Kyoto Encyclopedia of Genes and Genomes (KEGG) showed that metabolic enzymes, particularly those of glycolysis, were elevated in serum concentration after surgery. Several proteins were significantly increased postoperatively in patients diagnosed with POD relative to the non-POD controls, with interleukin-6 (IL-6) showing the greatest fold-change. LPS stimulation of whole blood samples confirmed these findings. Linear regression analysis showed a highly significant correlation between Confusion Assessment Method (CAM) scores and CPB-mediated changes in cGMP-inhibited 3′,5′-cyclic phosphodiesterase A (PDE3A).ConclusionsCardiac surgery with CPB resulted in inflammasome changes accompanied by unexpected increases in metabolic pathways. In exploratory analyses, we found that POD was associated with changes in the expression level of various proteins, most notably IL-6 and PDE3A. This study and ongoing protein biomarker studies will likely help quantify risk or confirm the diagnosis for POD and increase understanding of its pathophysiological mechanisms.

Published

2021

24. ETV1 inhibition depressed M2 polarization of tumor-associated macrophage and cell process in gastrointestinal stromal tumor via down-regulating PDE3A.

Author

Guo X, Li Y, Wan B, Lv Y, Wang X, Liu G, and Wang P

Abstract

M2-type polarization of tumor associated-macrophage (TAM) is involved in the malignancy of gastrointestinal stromal tumor (GIST) progression. ETS variant 1 (ETV1) has been previously validated to regulate GIST pathogenesis. Our study intended to explore the role and mechanism of ETV1 in mediating the M2-polarization of TAM in GIST progression. First, we analyzed the correlation between ETV1 expression and M2-polarization in GIST tissues. IL-4 was used to treat THP-1-derived TAM cells and IL-4-stimulated TAM were co-cultured with GIST-T1 cells to mimic the GIST microenvironment. A loss-of-function assay was performed to explore the role of ETV1. Results showed that ETV1 elevation was positively correlated with M2-polarization. IL-4-induced TAM promoted ETV1 expression, silencing ETV1 inhibited proliferation, invasion and KIT activation in IL-4-treated GIST cells, while cell apoptosis was enhanced. Besides, co-culture of ETV1-silenced GIST cells significantly depressed M2-polarization in TAM, presented as decreased levels of CD206, Agr-1 and cytokines, as well as the proportion of CD206-positive TAM. PDE3A was positively correlated with ETV1 and M2-polarization. Overexpressing PDE3A reversed the inhibitory effects of ETV1 silencing. Generally, ETV1 inhibition depressed M2-polarization of TAM in GIST and its promotion on pathological aggravation via down-regulating PDE3A. This evidence may provide a new target for GIST regulation., Competing Interests: No potential conflicts of interest were disclosed., (Copyright © 2023 JCBN.)

Published

2023

25. Effects of aging on gene expression and mitochondrial DNA in the equine oocyte and follicle cells.

Author

Campos-Chillon, Fernando, Farmerie, Todd A., Bouma, Gerrit J., Clay, Colin M., and Carnevale, Elaine M.

Subjects

*MARES, *MESSENGER RNA, *GRANULOSA cells, *PHOSPHODIESTERASES, *G protein coupled receptors, *GENE expression in mammals, *OVUM, *MITOCHONDRIAL DNA, *REPRODUCTION, *MAMMALS

Abstract

We hypothesised that advanced mare age is associated with follicle and oocyte gene alterations. The aims of the study were to examine quantitative and temporal differences in mRNA for LH receptor (LHR), amphiregulin (AREG) and epiregulin (EREG) in granulosa cells, phosphodiesterase (PDE) 4D in cumulus cells and PDE3A, G-protein-coupled receptor 3 (GPR3), growth differentiation factor 9 (GDF9), bone morphogenetic protein 15 (BMP15) and mitochondrial (mt) DNA in oocytes. Samples were collected from dominant follicles of Young (3-12 years) and Old (≥20 years) mares at 0, 6, 9 and 12 h after administration of equine recombinant LH. LHR mRNA declined after 0 h in Young mares, with no time effect in Old mares. For both ages, gene expression of AREG was elevated at 6 and 9 h and EREG was expression was elevated at 9 h, with higher expression in Old than Young mares. Cumulus cell PDE4D expression increased by 6 h (Old) and 12 h (Young). Oocyte GPR3 expression peaked at 9 and 12 h in Young and Old mares, respectively. Expression of PDE3A increased at 6 h, with the increase greater in oocytes from Old than Young mares at 6 and 9 h. Mean GDF9 and BMP15 transcripts were higher in Young than Old, with a peak at 6 h. Copy numbers of mtDNA did not vary over time in oocytes from Young mares, but a temporal decrease was observed in oocytes from Old mares. The results support an age-associated asynchrony in the expression of genes that are essential for follicular and oocyte maturation before ovulation. Maternal aging is related to reduced fertility in various species, including the mare. We compared gene expression in follicle cells and oocytes from Young and Old mares after an ovulation-induction signal. Differences were observed in the timing and amount of expression for key regulatory genes between Young and Old mares, suggesting age-associated changes in follicles and oocytes that could impact fertility. [ABSTRACT FROM AUTHOR]

Published

2015

26. Di (2-ethylhexyl) phthalate impairs primordial follicle assembly by increasing PDE3A expression in oocytes

Author

Hong-Chen Yan, Jing-Cai Liu, Zi-Hui Yan, Bo Li, Wei Shen, and Massimo De Felici

Subjects

Oocyte, endocrine system, Health, Toxicology and Mutagenesis, Granulosa cell, Phthalic Acids, 010501 environmental sciences, Toxicology, 01 natural sciences, Oogenesis, Primordial follicle assembly, Transcriptome, 03 medical and health sciences, chemistry.chemical_compound, Follicle, Mice, FIGLA, Ovarian Follicle, cAMP, Diethylhexyl Phthalate, medicine, Animals, 030304 developmental biology, 0105 earth and related environmental sciences, 0303 health sciences, Settore BIO/17, DEHP, Chemistry, Phthalate, General Medicine, Pollution, Cyclic Nucleotide Phosphodiesterases, Type 3, Cell biology, Pde3a, medicine.anatomical_structure, Oocytes, Female, Reproductive toxicology, Folliculogenesis

Abstract

It is known that Di (2-ethylhexyl) phthalate (DEHP) may impact mammalian reproduction and that in females one target of the drug’s action is follicle assembly. Here we revisited the phthalate’s action on the ovary and from bioinformatics analyses of the transcriptome performed on newborn mouse ovaries exposed in vitro to DEHP, up-regulation of PDE3A, as one of the most important alterations caused by DEHP on early folliculogenesis, was identified. We obtained some evidence suggesting that the decrease of cAMP level in oocytes and the parallel decrease of PKA expression, consequent on the PDE3A increase, were a major cause of the reduction of follicle assembly in the DEHP-exposed ovaries. In fact, Pde3a RNAi on cultured ovaries reducing cAMP and PKA decrease counteracted the primordial follicle assembly impairment caused by the compound. Moreover, RNAi normalized the level of Kit, Nobox, Figla mRNA and GDF9, BMP15, CX37, γH2AX proteins in oocytes, and KitL transcripts in granulosa cells as well as their proliferation rate altered by DEHP exposure. Taken together, these results identify PDE3A as a new critical target of the deleterious effects of DEHP on early oogenesis in mammals and highlight cAMP-dependent pathways as major regulators of oocyte and granulosa cell activities crucial for follicle assembly. Moreover, we suggest that the level of intracellular cAMP in the oocytes may be an important determinant for their capability to repair DNA lesions caused by DNA damaging compounds including DEHP.

Published

2020

27. Multiple PDE3A modulators act as molecular glues promoting PDE3A-SLFN12 interaction and induce SLFN12 dephosphorylation and cell death.

Author

Yan, Bo, Ding, Zhangcheng, Zhang, Wenbin, Cai, Gaihong, Han, Hui, Ma, Yan, Cao, Yang, Wang, Jiawen, Chen, She, and Ai, Youwei

Subjects

*CELL death, *DEPHOSPHORYLATION, *CYCLIC guanylic acid, *GLUE, *CYCLIC adenylic acid, *PROTEIN stability

Abstract

The canonical function of phosphodiesterase 3A (PDE3A) is to hydrolyze the phosphodiester bonds in second messenger molecules, such as cyclic AMP (cAMP) and cyclic guanosine monophosphate (cGMP). Recently, a phosphodiesterase-activity-independent role for PDE3A was reported. In this noncanonical function, PDE3A physically interacts with Schlafen 12 (SLFN12) upon treatment of cells with cytotoxic PDE3A modulators. Here, we confirmed that the cytotoxic PDE3A modulators act as molecular glues to initiate the association of PDE3A and SLFN12. The PDE3A-SLFN12 interaction increases the protein stability of SLFN12 located in the cytoplasm, while at the same time also inducing SLFN12 dephosphorylation (including serines 368 and 573). Mutational analysis demonstrates that dephosphorylation is required for cell death induced by cytotoxic PDE3A modulators. Finally, we found that dephosphorylation promoted the rRNA RNase activity of SLFN12 and show that this nucleolytic activity is essential for SLFN12's cell-death-inducing function. Thus, our study deepens the understanding of the biochemical mechanisms underlying SLFN12-mediated cell death. [Display omitted] • Multiple cytotoxic PDE3A modulators act as molecular glues • PDE3A-SLFN12 interaction reduces the phosphorylation of SLFN12 • Dephosphorylation of SLFN12 increases SLFN12's RNase activity Yan et al. find that multiple PDE3A modulators act as molecular glues that promote PDE3A-SLFN12 interaction, which results in dephosphorylation of SLFN12. Mutational analyses demonstrate that dephosphorylation of SLFN12 is required for SLFN12's cell-death-inducing function, which is mediated through SLFN12's RNase activity against rRNAs. [ABSTRACT FROM AUTHOR]

Published

2022

28. Cyclic nucleotide phosphodiesterase 3A1 protects the heart against ischemia-reperfusion injury.

Author

Oikawa, Masayoshi, Wu, Meiping, Lim, Soyeon, Knight, Walter E., Miller, Clint L., Cai, Yujun, Lu, Yan, Blaxall, Burns C., Takeishi, Yasuchika, Abe, Jun-ichi, and Yan, Chen

Subjects

*CYCLIC nucleotide phosphodiesterases, *ISCHEMIA, *REPERFUSION injury, *PHOSPHODIESTERASE inhibitors, *HEART cells, *ARRHYTHMIA

Abstract

Phosphodiesterase 3A (PDE3A) is a major regulator of cAMP in cardiomyocytes. PDE3 inhibitors are used for acute treatment of congestive heart failure, but are associated with increased incidence of arrhythmias and sudden death with long-term use. We previously reported that chronic PDE3A downregulation or inhibition induced myocyte apoptosis in vitro. However, the cardiac protective effect of PDE3A has not been demonstrated in vivo in disease models. In this study, we examined the role of PDE3A in regulating myocardial function and survival in vivo using genetically engineered transgenic mice with myocardial overexpression of the PDE3A1 isozyme (TG). TG mice have reduced cardiac function characterized by reduced heart rate and ejection fraction (52.5±7.8% vs. 83.9±4.7%) as well as compensatory expansion of left ventricular diameter (4.19±0.19mm vs. 3.10±0.18mm). However, there was no maladaptive increase of fibrosis and apoptosis in TG hearts compared to wild type (WT) hearts, and the survival rates also remained the same. The diminution of cardiac contractile function is very likely attributed to a decrease in beta-adrenergic receptor (β-AR) response in TG mice. Importantly, the myocardial infarct size (4.0±1.8% vs. 24.6±3.8%) and apoptotic cell number (1.3±1.0% vs. 5.6±1.5%) induced by ischemia/reperfusion (I/R) injury were significantly attenuated in TG mice. This was associated with decreased expression of inducible cAMP early repressor (ICER) and increased expression of anti-apoptotic protein BCL-2. To further verify the anti-apoptotic effects of PDE3A1, we performed in vitro apoptosis study in isolated adult TG and WT cardiomyocytes. We found that the apoptotic rates stimulated by hypoxia/reoxygenation or H2O2 were indeed significantly reduced in TG myocytes, and the differences between TG and WT myocytes were completely reversed in the presence of the PDE3 inhibitor milrinone. These together indicate that PDE3A1 negatively regulates β-AR signaling and protects against I/R injury by inhibiting cardiomyocyte apoptosis. [ABSTRACT FROM AUTHOR]

Published

2013

29. PDE3A, acteur majeur dans le développement des cellules interstitielles de Cajal et nouvelle cible thérapeutique des tumeurs stromales gastrointestinales

Author

Vanderwinden, Jean-Marie, Erneux, Christophe, Maenhaut, Carine, De Deken, Xavier, Van Laethem, Jean-Luc, Petein, Michel, Demoulin, Jean-Baptiste, Emile, Jean-François, Vandenberghe, Pierre, Vanderwinden, Jean-Marie, Erneux, Christophe, Maenhaut, Carine, De Deken, Xavier, Van Laethem, Jean-Luc, Petein, Michel, Demoulin, Jean-Baptiste, Emile, Jean-François, and Vandenberghe, Pierre

Abstract

Les tumeurs stromales gastrointestinales (GIST) sont les sarcomes les plus fréquentsdu tube digestif et dérivent des cellules interstitielles de Cajal (ICC) ou de leursprogéniteurs. 85% des GIST arborent une mutation oncogénique du récepteur KIT etl’introduction de l’imatinib, un inhibiteur de tyrosine kinase (TKI), a prouvé sonefficacité dans le traitement des GIST. Cependant, 50 % des patients développent desrésistances après deux ans de traitements et malgré l’introduction d’autres TKI, il estnécessaire de trouver de nouvelles cibles thérapeutiques alternatives à KIT pour letraitement des GIST. Ce projet de thèse s’appuie sur une liste de gènesprécédemment publiée par le laboratoire où l’expression génique de l’antre d’unmodèle murin de GIST a été comparée au profil d’expression de gènes dans l'antrenormal. Parmi ces gènes, le laboratoire a montré que la phosphodiestérase 3A(PDE3A) constitue un nouveau marqueur robuste des ICC, cette protéine étantexprimée dans les ICC, mais également dans la couche hyperplasique de cellulesKIT+ du modèle murin oncogénique. Cependant, son rôle dans la physiologie des ICCet des GIST restait inconnu et cette thèse a eu pour but de caractériser la fonction dePDE3A et de valider son intérêt comme cible thérapeutique potentielle dans les GIST.Ainsi, nous avons montré in vivo que PDE3A commence à être exprimée au jourembryonnaire 14.5, lorsque la différenciation des progéniteurs mésenchymateuxcommuns des ICC et cellules musculaires lisses débute. De plus, nous avons observéune réduction de 50% du réseau d’ICC dans des souris adultes déficientes en PDE3Asuggérant un rôle important de cette protéine dans le développement/maintenancedes ICC. Nous avons également montré que PDE3A est exprimée dans les ICC chezl’homme ainsi que dans 90% des GIST. Ces résultats nous ont poussés à étudier invitro le rôle de PDE3A en utilisant des lignées cellulaires humaines sensibles etrésistantes à l’imatinib, respectivement les GIST882 et GIST48. L’inhibit, Doctorat en Sciences biomédicales et pharmaceutiques (Médecine), info:eu-repo/semantics/nonPublished

Published

2019

30. Potentiation of imatinib by cilostazol in sensitive and resistant gastrointestinal stromal tumor cell lines involves YAP inhibition.

Author

Vandenberghe, Pierre, Delvaux, Marine, Hague, Perrine, Erneux, Christophe, Vanderwinden, Jean-Marie, Vandenberghe, Pierre, Delvaux, Marine, Hague, Perrine, Erneux, Christophe, and Vanderwinden, Jean-Marie

Abstract

Despite the introduction of tyrosine kinase inhibitors, gastrointestinal stromal tumors (GIST) resistance remains a major clinical challenge. We previously identified phosphodiesterase 3A (PDE3A) as a potential therapeutic target expressed in most GIST. The PDE3 inhibitor cilostazol reduced cell viability and synergized with the tyrosine kinase inhibitor imatinib (Gleevec™) in the imatinib-sensitive GIST882 cell line. Here, we found that cilostazol potentiated imatinib also in the imatinib-resistant GIST48 cell line. Cilostazol induced nuclear exclusion, hence inactivation, of the transcriptional co-activator YAP, in a cAMP-independent manner. Verteporfin, a YAP/TEAD interaction inhibitor, reduced by 90% the viability of both GIST882 and GIST48 cells. Our results highlight the potential use of compounds targeting PDE3A or YAP in combined multitherapy to tackle GIST resistance., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2019

31. Fosfodiesterazy rodziny 3 sprzęgają szlaki sygnałowe zależne od kinaz białkowych i cyklicznego GMP z metabolizmem cyklicznego AMP.

Author

Makuch, Edyta and Matuszyk, Janusz

Subjects

*PHOSPHODIESTERASES, *PROTEIN kinases, *CATALYTIC domains, *AMINO acids, *STERIC hindrance, *CHEMICAL reactions, *NATRIURETIC peptides

Abstract

PDE3 is a dual-substrate phosphodiesterase responsible for hydrolyzing both cAMP and cGMP whilst being simultaneously inhibited by cGMP. This feature is related to presence of the 44 amino acid insert in the catalytic domain, which determines the mechanism of introduction of the cyclic nucleotide into the catalytic pocket of the enzyme. Once bound in the catalytic site cGMP results in steric hindrance for cAMP to enter the site. The regulatory domain of PDE3 consists of two hydrophobic regions: NHR1 and NHR2. Their presence defines the enzyme's intracellular localization, thus determining its participation in particular signaling cascades. Due to the properties of PDE3 this enzyme has exceptional importance for the cross-talk between cAMP-dependent signaling and other cascades. There are two different mechanisms of action of PDE3 enzymes in cell signaling pathways. In many signaling cascades assembly of a signalosome is necessary for phosphorylation and activation of the PDE3 proteins. In response to certain hormones and growth factors, PDE3 merges the metabolism of cAMP with protein kinase-dependent signaling pathways. PDE3 also controls the level of cAMP with regard to the alternating concentration of cGMP. This effect occurs in signaling cascades activated by natriuretic peptide. [ABSTRACT FROM AUTHOR]

Published

2012

32. Female infertility in PDE3A-/- mice.

Author

Weixing Shen, Ahmad, Faiyaz, Hockman, Steven, Ma, John, Omi, Hitoshi, Raghavachari, Nalini, and Manganiello, Vincent

Published

2010

33. A new nonhydrolyzable reactive cGMP analogue, (Rp)-guanosine-3′,5′-cyclic-S-(4-bromo-2,3-dioxobutyl)monophosphorothioate, which targets the cGMP binding site of human platelet PDE3A

Author

Hung, Su H., Liu, Andy H., Pixley, Robin A., Francis, Penelope, Williams, LaTeeka D., Matsko, Christopher M., Barnes, Karine D., Sivendran, Sharmila, Colman, Roberta F., and Colman, Robert W.

Subjects

*BLOOD platelets, *MOLECULAR probes, *AMINO acids, *BLOOD cells

Abstract

Abstract: The amino acids involved in substrate (cAMP) binding to human platelet cGMP-inhibited cAMP phosphodiesterase (PDE3A) are identified. Less is known about the inhibitor (cGMP) binding site. We have now synthesized a nonhydrolyzable reactive cGMP analog, Rp-guanosine-3′,5′-cyclic-S-(4-bromo-2, 3-dioxobutyl)monophosphorothioate (Rp-cGMPS-BDB). Rp-cGMPS-BDB irreversibly inactivates PDE3A (K I =43.4±7.2μM and k cart =0.007±0.0006min−1). The effectiveness of protectants in decreasing the rate of inactivation by Rp-cGMPS-BDB is: Rp-cGMPS (K d =72μM)>Sp-cGMPS (124), Sp-cAMPS (182)>GMP (1517), Rp-cAMPS (3762), AMP (4370μM). NAD+, neither a substrate nor an inhibitor of PDE3A, does not protect. Nonhydrolyzable cGMP analogs exhibit greater affinity than the cAMP analogs. These results indicate that Rp-cGMPS-BDB targets favorably the cGMP binding site consistent with a docking model of PDE3A-Rp-cGMPS-BDB active site. We conclude that Rp-cGMPS-BDB is an effective active site-directed affinity label for PDE3A with potential for other cGMP-dependent enzymes. [Copyright &y& Elsevier]

Published

2008

34. Generation of mouse oocytes defective in cAMP synthesis and degradation: Endogenous cyclic AMP is essential for meiotic arrest

Author

Vaccari, Sergio, Horner, Kathleen, Mehlmann, Lisa M., and Conti, Marco

Subjects

*OVUM, *LABORATORY mice, *HYDROLYSIS, *CELL division

Abstract

Abstract: Although it is established that cAMP accumulation plays a pivotal role in preventing meiotic resumption in mammalian oocytes, the mechanisms controlling cAMP levels in the female gamete have remained elusive. Both production of cAMP via GPCRs/Gs/adenylyl cyclases endogenous to the oocyte as well as diffusion from the somatic compartment through gap junctions have been implicated in maintaining cAMP at levels that preclude maturation. Here we have used a genetic approach to investigate the different biochemical pathways contributing to cAMP accumulation and maturation in mouse oocytes. Because cAMP hydrolysis is greatly decreased and cAMP accumulates above a threshold, oocytes deficient in PDE3A do not resume meiosis in vitro or in vivo, resulting in complete female infertility. In vitro, inactivation of Gs or downregulation of the GPCR GPR3 causes meiotic resumption in the Pde3a null oocytes. Crossing of Pde3a −/− mice with Gpr3 −/− mice causes partial recovery of female fertility. Unlike the complete meiotic block of the Pde3a null mice, oocyte maturation is restored in the double knockout, although it occurs prematurely as described for the Gpr3 −/− mouse. The increase in cAMP that follows PDE3A ablation is not detected in double mutant oocytes, confirming that GPR3 functions upstream of PDE3A in the regulation of oocyte cAMP. Metabolic coupling between oocytes and granulosa cells was not affected in follicles from the single or double mutant mice, suggesting that diffusion of cAMP is not prevented. Finally, simultaneous ablation of GPR12, an additional receptor expressed in the oocyte, does not modify the Gpr3 −/− phenotype. Taken together, these findings demonstrate that Gpr3 is epistatic to Pde3a and that fertility as well as meiotic arrest in the PDE3A-deficient oocyte is dependent on the activity of GPR3. These findings also suggest that cAMP diffusion through gap junctions or the activity of additional receptors is not sufficient by itself to maintain the meiotic arrest in the mouse oocyte. [Copyright &y& Elsevier]

Published

2008

35. Role of phosphodiesterase type 3A and 3B in regulating platelet and cardiac function using subtype-selective knockout mice

Author

Sun, Bing, Li, Haiquan, Shakur, Yasmin, Hensley, James, Hockman, Steve, Kambayashi, Junichi, Manganiello, Vincent C., and Liu, Yongge

Subjects

*RODENTS, *BLOOD platelets, *HEART beat, *COLLAGEN

Abstract

Abstract: Phosphodiesterase type 3 (PDE3) is an important regulator of cAMP-mediated responses within the cardiovascular system. PDE3 exists as two subtypes: PDE3A and PDE3B, with distinct cellular and subcellular locations. Due to the lack of subtype-specific pharmacological tools, the definitive role of each subtype in regulating cardiovascular function has not been determined. In this study, we investigated platelet and cardiac function, using PDE3A and PDE3B gene knockout (KO) mice. Platelet-rich-plasma was prepared from the blood of KO and age-matched wild-type (WT) mice. PGE1 (1 μg/mL) almost completely inhibited aggregation of platelets from WT, PDE3A KO and PDE3B KO mice. In platelets from WT mice, cilostamide (100 μM), a selective PDE3 inhibitor, blocked collagen- and ADP-induced aggregation. In contrast, cilostamide had no effect on aggregation of platelets from PDE3A KO mice. In PDE3B KO mice, inhibition of collagen- and ADP-induced platelet aggregation was similar to that in WT mice. The resting intra-platelet cAMP concentration in platelets from PDE3A KO mice was twice that in the WT platelets. After PGE1 (0.1 μg/mL) stimulation, intra-cellular cAMP concentration was increased significantly more in platelets from PDE3A KO mice compared to WT mice. In vivo, PDE3A KO mice were protected against collagen/epinephrine-induced pulmonary thrombosis and death, while no such protection was observed in PDE3B KO mice. The heart rate of PDE3A KO mice was significantly higher, compared with age-matched WT mice, while that of PDE3B KO mice was similar to WT. There was no difference in cardiac contractility between PDE3A or PDE3B KO mice. Heart rate and contractility were increased in a similar dose-dependent fashion by isoproterenol in both types of KO mice. Cilostamide increased heart rate and contractility in WT and PDE3B KO but not in PDE3A KO mice. Compared to WT and PDE3B KO mice, cyclic AMP-PDE activity in membrane fractions prepared from the hearts of PDE3A KO mice was lower and not inhibited by cilostamide. The data suggest that PDE3A is the main subtype of PDE3 expressed in platelets and cardiac ventricular myocytes, and is responsible for the functional changes caused by PDE3 inhibition. [Copyright &y& Elsevier]

Published

2007

36. Protein kinase B/Akt phosphorylation of PDE3A and its role in mammalian oocyte maturation.

Author

Seung Jin Han, Vaccari, Sergio, Nedachi, Taku, Andersen, Carsten B., Kovacina, Kristina S., Roth, Richard A., and Conti, Marco

Subjects

*CELLULAR signal transduction, *BIOENERGETICS, *CELL cycle, *BIOLOGICAL rhythms, *PHOSPHORYLATION, *CHEMICAL reactions

Abstract

cGMP-inhibited cAMP phosphodiesterase 3A (PDE3A) is expressed in mouse oocytes, and its function is indispensable for meiotic maturation as demonstrated by genetic ablation. Moreover, PDE3 activity is required for insulin/insulin-like growth factor-1 stimulation of Xenopus oocyte meiotic resumption. Here, we investigated the cAMP-dependent protein kinase B (PKB)/Akt regulation of PDE3A and its impact on oocyte maturation. Cell-free incubation of recombinant mouse PDE3A with PKB/Akt or cAMP-dependent protein kinase A catalytic subunits leads to phosphorylation of the PDE3A protein. Coexpression of PDE3A with constitutively activated PKB/Akt (Myr-Akt) increases PDE activity as well as its phosphorylation state. Injection of pde3a mRNA potentiates insulin-dependent maturation of Xenopus oocytes and rescues the phenotype of pde3−/− mouse oocytes. This effect is greatly decreased by mutation of any of the PDE3A serines 290–292 to alanine in both Xenopus and mouse. Microinjection of myr-Akt in mouse oocytes causes in vitro meiotic maturation and this effect requires PDE3A. Collectively, these data indicate that activation of PDE3A by PKB/Akt-mediated phosphorylation plays a role in the control of PDE3A activity in mammalian oocytes. [ABSTRACT FROM AUTHOR]

Published

2006

37. A New Nonhydrolyzable Reactive cAMP Analog, (Sp)-Adenosine-3′,5′-cyclic-S-(4-bromo-2,3-dioxobutyl)monophosphorothioate Irreversibly Inactivates Human Platelet cGMP-Inhibited cAMP Phosphodiesterase

Author

Hung, Su H., Madhusoodanan, K. S., Beres, James A., Boyd, Robert L., Baldwin, James L., Zhang, Wei, Colman, Robert W., and Colman, Roberta F.

Subjects

*CYCLIC nucleotides, *AFFINITY labeling

Abstract

Levels of cAMP that control critical platelet functions are regulated by cGMP-inhibited cAMP phosphodiesterase (PDE3A). We previously showed that millimolar concentrations of the hydrolyzable 8-[(4-bromo-2,3-dioxobutyl)thioadenosine 3′,5′-cyclic monophosphate (8-BDB-TcAMP) inactivate PDE3A. We have now synthesized a nonhydrolyzable affinity label to probe the active site of PDE3A. The nonhydrolyzable adenosine 3′,5′-cyclic monophosphorothioates, Sp-cAMPS and Rp-cAMPS, function as competitive inhibitors of PDE3A with Ki = 47.6 and 4400 μM, respectively. We therefore coupled Sp-cAMPS with 1,4-dibromobutanedione to yield (Sp)-adenosine-3′,5′-cyclic-S-(4-bromo-2,3-dioxobutyl)monophosphorothioate, [Sp-cAMPS-(BDB)]. Sp-cAMPS-(BDB) inactivates PDE3A in a time-dependent, irreversible reaction with kmax = 0.0116 min−1 and KI = 10.1 μM. The order of effectiveness of protectants in decreasing the rate of inactivation (with Kd in μM) is: Sp-cAMPS (24) > Rp-cGMPS (1360), Sp-cGMPS (1460) > GMP (4250), AMP (10600), Rp-cAMPS (22170). These results suggest that the inactivation of PDE3A by Sp-cAMPS-(BDB) is a consequence of reaction at the overlap of the cAMP and cGMP binding regions in the active site. [Copyright &y& Elsevier]

Published

2002

38. PDE3A, acteur majeur dans le développement des cellules interstitielles de Cajal et nouvelle cible thérapeutique des tumeurs stromales gastrointestinales

Author

Vandenberghe, Pierre, Vanderwinden, Jean-Marie, Erneux, Christophe, Maenhaut, Carine, De Deken, Xavier, Van Laethem, Jean-Luc, Petein, Michel, Demoulin, Jean-Baptiste, and Emile, Jean-François

Subjects

PDE3A, Interstitial cells of Cajal, Sciences biomédicales en général, YAP, Repurposing, GIST

Abstract

Les tumeurs stromales gastrointestinales (GIST) sont les sarcomes les plus fréquentsdu tube digestif et dérivent des cellules interstitielles de Cajal (ICC) ou de leursprogéniteurs. 85% des GIST arborent une mutation oncogénique du récepteur KIT etl’introduction de l’imatinib, un inhibiteur de tyrosine kinase (TKI), a prouvé sonefficacité dans le traitement des GIST. Cependant, 50 % des patients développent desrésistances après deux ans de traitements et malgré l’introduction d’autres TKI, il estnécessaire de trouver de nouvelles cibles thérapeutiques alternatives à KIT pour letraitement des GIST. Ce projet de thèse s’appuie sur une liste de gènesprécédemment publiée par le laboratoire où l’expression génique de l’antre d’unmodèle murin de GIST a été comparée au profil d’expression de gènes dans l'antrenormal. Parmi ces gènes, le laboratoire a montré que la phosphodiestérase 3A(PDE3A) constitue un nouveau marqueur robuste des ICC, cette protéine étantexprimée dans les ICC, mais également dans la couche hyperplasique de cellulesKIT+ du modèle murin oncogénique. Cependant, son rôle dans la physiologie des ICCet des GIST restait inconnu et cette thèse a eu pour but de caractériser la fonction dePDE3A et de valider son intérêt comme cible thérapeutique potentielle dans les GIST.Ainsi, nous avons montré in vivo que PDE3A commence à être exprimée au jourembryonnaire 14.5, lorsque la différenciation des progéniteurs mésenchymateuxcommuns des ICC et cellules musculaires lisses débute. De plus, nous avons observéune réduction de 50% du réseau d’ICC dans des souris adultes déficientes en PDE3Asuggérant un rôle important de cette protéine dans le développement/maintenancedes ICC. Nous avons également montré que PDE3A est exprimée dans les ICC chezl’homme ainsi que dans 90% des GIST. Ces résultats nous ont poussés à étudier invitro le rôle de PDE3A en utilisant des lignées cellulaires humaines sensibles etrésistantes à l’imatinib, respectivement les GIST882 et GIST48. L’inhibition de PDE3Apar le cilostazol, en synergie avec l’imatinib, réduit la viabilité des GIST882 et GIST48indépendamment de la voie de signalisation de l’AMPc. Mécanistiquement, nousavons mis en évidence que l’inhibition de PDE3A par le cilostazol induit l’exclusionnucléaire de YAP et donc son inactivation. L’inhibition directe de YAP par lavertéporfine réduit drastiquement la viabilité des GIST882 et GIST48, faisant de YAPune nouvelle cible thérapeutique potentielle dans les GIST.En conclusions, nous avons caractérisé de manière originale le rôle de PDE3A dansla physiologie des ICC et des GIST et validé son intérêt majeur comme ciblethérapeutique pour le traitement des GIST. Nous avons également mis en lumière lavoie YAP comme étant une nouvelle voie majeure dans la survie des GIST. Cesrésultats ont fait l’objet de deux publications en tant que premier auteur (chapitres 3et 4) et ont débouché à une étude clinique de Phase I, CILOGIST initiée début 2019dans le Service de Gastroentérologie de l’Hôpital Académique Érasme (UniversitéLibre de Bruxelles)., Doctorat en Sciences biomédicales et pharmaceutiques (Médecine), info:eu-repo/semantics/nonPublished

Published

2019

39. Potentiation of imatinib by cilostazol in sensitive and resistant gastrointestinal stromal tumor cell lines involves YAP inhibition

Author

Marine Delvaux, Jean-Marie Vanderwinden, Pierre Vandenberghe, Christophe Erneux, and Perrine Hague

Subjects

0301 basic medicine, medicine.drug_class, Phosphodiesterase 3, Tyrosine-kinase inhibitor, 03 medical and health sciences, 0302 clinical medicine, Medicine, cancer, Stromal tumor, neoplasms, verteporfin, GiST, PDE3A, drug repurposing, business.industry, Imatinib, KIT, Sciences bio-médicales et agricoles, Verteporfin, Cilostazol, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, business, Tyrosine kinase, medicine.drug, Research Paper

Abstract

Despite the introduction of tyrosine kinase inhibitors, gastrointestinal stromal tumors (GIST) resistance remains a major clinical challenge. We previously identified phosphodiesterase 3A (PDE3A) as a potential therapeutic target expressed in most GIST. The PDE3 inhibitor cilostazol reduced cell viability and synergized with the tyrosine kinase inhibitor imatinib (Gleevec™) in the imatinib-sensitive GIST882 cell line. Here, we found that cilostazol potentiated imatinib also in the imatinib-resistant GIST48 cell line. Cilostazol induced nuclear exclusion, hence inactivation, of the transcriptional co-activator YAP, in a cAMP-independent manner. Verteporfin, a YAP/TEAD interaction inhibitor, reduced by 90% the viability of both GIST882 and GIST48 cells. Our results highlight the potential use of compounds targeting PDE3A or YAP in combined multitherapy to tackle GIST resistance., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2019

40. Expression of Recombinant Phosphodiesterases 3A and 3B Using Baculovirus Expression System

Author

Wenrong Xu, Wenqian Jiang, Yongmin Yan, Jingwen Liu, and Hui Qian

Subjects

viruses, Phosphodiesterase 3, Guanosine, Sf9, 030204 cardiovascular system & hematology, 030226 pharmacology & pharmacy, Biochemistry, law.invention, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Western blot, law, Genetics, medicine, Baculovirus Expression System, PDE3B, PDE3A, medicine.diagnostic_test, Phosphodiesterase, Transfection, Molecular biology, Adenosine, chemistry, Recombinant DNA, SF9 cells, Research Article, Biotechnology, medicine.drug

Abstract

Background: Phosphodiesterase 3A (PDE3A) and phosphodiesterase 3B (PDE3B) play a critical role in the regulation of intracellular level of adenosine 3´,5´-cyclic monophosphate (cyclic AMP, cAMP) and guanosine 3´,5´-cyclic monophosphate (cyclic GMP, cGMP). Subsequently PDE3 inhibitors have shown to relax vascular and inhibit platelet aggregation in cardiovascular disease. Objectives: In this study, our aim was to establish a method of expression for the recombinant human PDE3A and PDE3B proteins in insect cells using baculovirus expression system in order to investigate the activity of the expressed PDE3A and PDE3B proteins. Materials and Methods: The full length human PDE3A and PDE3B cDNA were cloned into recombinant baculovirus and transfected into the SF9 insect cells. Recombinant proteins were collected at 48 h, 60 h, 72 h, and 84 h post transfection. Transfection of recombinant baculovirus was verified by the morphological changes of the SF9 cells. Expression of human PDE3A and PDE3B was detected by using RT-PCR and western blot, respectively. The 125I RIA method was used to determine the level of adenosine 3´,5´-cyclic monophosphate cAMP and cGMP, correspondingly. The activity of the expressed PDE3A and PDE3B proteins were investigated by cAMP and cGMP dsgradation with or without addition of milrinone, a potent and selective PDE inhibitor. Results: Recombinant human PDE3A and PDE3B proteins were stably expressed in SF9 cells and could be detected by distinct morphological changes in the SF9 cells, RT-PCR, and western blot at 48 h post-transfection. The molecular weights of the recombinant PDE3A and PDE3B molecular weights proteins were about 120 KDa and 135 KDa, respectively. Results of 125I RIA assay showed that the levels of cAMP and cGMP were significantly decreased after incubation with the expressed PDE3A and PDE3B proteins. Furthermore, degradation of cAMP and cGMP through the activity of PDE3A and PDE3B was suppressed following to the addition of milrinone. Conclusions: Recombinant human PDE3A and PDE3B could be expressed in SF9 cells using baculovirus expression system, and thus provides the basic material for studying human PDE3A and PDE3B activity.

Published

2016

41. Di (2-ethylhexyl) phthalate impairs primordial follicle assembly by increasing PDE3A expression in oocytes.

Author

Liu, Jing-Cai, Yan, Zi-Hui, Li, Bo, Yan, Hong-Chen, De Felici, Massimo, and Shen, Wei

Subjects

OOGENESIS, DNA repair, DNA damage, PHTHALATE esters, GRANULOSA cells, OVARIES, OVUM

Abstract

It is known that Di (2-ethylhexyl) phthalate (DEHP) may impact mammalian reproduction and that in females one target of the drug's action is follicle assembly. Here we revisited the phthalate's action on the ovary and from bioinformatics analyses of the transcriptome performed on newborn mouse ovaries exposed in vitro to DEHP, up-regulation of PDE3A, as one of the most important alterations caused by DEHP on early folliculogenesis, was identified. We obtained some evidence suggesting that the decrease of cAMP level in oocytes and the parallel decrease of PKA expression, consequent on the PDE3A increase, were a major cause of the reduction of follicle assembly in the DEHP-exposed ovaries. In fact, Pde3a RNAi on cultured ovaries reducing cAMP and PKA decrease counteracted the primordial follicle assembly impairment caused by the compound. Moreover, RNAi normalized the level of Kit, Nobox , Figla mRNA and GDF9, BMP15, CX37, γH2AX proteins in oocytes, and KitL transcripts in granulosa cells as well as their proliferation rate altered by DEHP exposure. Taken together, these results identify PDE3A as a new critical target of the deleterious effects of DEHP on early oogenesis in mammals and highlight cAMP-dependent pathways as major regulators of oocyte and granulosa cell activities crucial for follicle assembly. Moreover, we suggest that the level of intracellular cAMP in the oocytes may be an important determinant for their capability to repair DNA lesions caused by DNA damaging compounds including DEHP. Image 1 • DEHP exposure impairs the primordial follicle assembly of newborn mouse ovaries. • DEHP exposure promotes PDE3A expression in the early stage of folliculogenesis. • Pde3a RNAi counteracted the influence of DEHP on ovaries by reducing cAMP and PKA. PDE3A is one of the most important regulators caused by DEHP exposure on impairment of early folliculogenesis. [ABSTRACT FROM AUTHOR]

Published

2021

42. SFPQ, a multifunctional nuclear protein, regulates the transcription of

Author

Dong Keun, Rhee, Steven C, Hockman, Sun-Kyung, Choi, Yong-Eun, Kim, Chungoo, Park, Vincent C, Manganiello, and Kee Kwang, Kim

Subjects

PDE3A, SFPQ, Cervical cancer, DNMDP, Transcription, Research Articles, Research Article

Abstract

Phosphodiesterase 3A (PDE3A), a member of the cGMP-inhibited cyclic nucleotide phosphodiesterase (PDE) family, plays important roles in oocyte maturation and vascular smooth muscle cell proliferation. However, the molecular mechanisms that regulate PDE3A gene expression remain largely unknown. In the present study, we investigated the transcriptional regulation of PDE3A, and found that the splicing factor proline- and glutamine-rich (SFPQ) protein modulated PDE3A mRNA levels. Multiple transcription start sites (TSS1, 2, and 3) were identified within the first exon of PDE3A using 5′-rapid amplification of cDNA ends (RACE). Variable expression levels of three PDE3A variants were also observed in human tissues and HeLa cells. Several putative SFPQ-binding sites were identified upstream of the regulatory region of PDE3A-TSSs using ChIP sequencing (ChIP-seq). Serum-induced PDE3A expression was affected by increasing the amount of SFPQ binding to the upstream regulatory region of PDE3A. In addition, transcription of PDE3A was lower in human cervical adenocarcinoma cells compared with normal cervical tissue. Furthermore, overexpression of PDE3A induced sensitivity to anticancer therapeutic agent, 6-(4-(diethylamino)-3-nitrophenyl)-5-methyl-4,5-dihydropyridazin-3(2H)-one (DNMDP), in HeLa cells. Taken together, these results suggest that SFPQ functions as a transcriptional activator of PDE3A, which is involved in the regulation of DNMDP sensitivity, offering a novel molecular target for the development of anticancer therapies.

Published

2017

43. Understanding the Role of SLFN12 in Selective Cancer Cell Killing Induced by PDE3A Modulating Small Molecules

Author

Tötzl, Marcus

Subjects

SLFN12, PDE3A, DNMDP

Abstract

Krebs, im Wesentlichen eine Erkrankung des Genoms, wird als eine der gefährlichsten medizinischen Fälle angesehen und war darüber hinaus die führende Todesursache im globalen Vergleich im Jahr 2012. In den letzten Jahrzehnten haben neue Entdeckungen und innovative Ideen zu vielversprechenden Behandlungsmöglichkeiten für mehrere Krebsarten geführt. Dies ist mit den enormen Verbesserungen in der Prävention sowie mit neu entstehenden Forschungsbereichen zu begründen, wie beispielsweise Nanotechnologie, epigenetische Wirkstoffe und Immuntherapien. Das Konzept einer allgemeinen Breitband-Behandlung hat allmählich den Weg für maßgeschneiderte Therapien freigegeben bei denen spezifische Abhängigkeiten in unterschiedlichen Krebsarten auf Basis der genetischen Landschaft von Mutationen in individuellen Patienten in Angriff genommen werden. Im Jahr 2015 haben de Waal et al. einen Wirkstoff namens 6-(4-(diethylamino)-3-nitrophenyl)-5-methyl-4,5- dihydropyridazin-3(2H)-one (DNMDP) entdeckt, welcher selektiv Krebszellen zerstört hat. Weitere Untersuchungen haben aufgedeckt dass dieses kleine Molekül an Phosphodiesterase 3A (PDE3A) bindet, welche des Öfteren ein Ziel von Inhibierung in bestimmten kardiovaskulären Erkrankungen ist, und die Interaktion mit einem weiteren Protein, Schlafen 12 (SLFN12), ermöglicht um einen Wirkstoff-abhängigen Komplex zu bilden. Diese PDE3A-SLFN12 Protein- Interaktion induziert im weiteren Verlauf einen bisher unbekannten Signalweg, welcher im Endeffekt zu Apoptose führt. DNMDP nützt hierbei einen neuen Mechanismus aus, welcher im Kontrast zu typischen Krebs-Abhängigkeiten steht. Der Fokus dieser Studie lag auf dem Sammeln neuer Erkenntnisse um die Rolle von SLFN12 beim DNMDP-induzierten Zelltod besser zu verstehen. Ich generierte genetische Knock-Outs von endogenem SLFN12 mittels CRISPR/Cas9 Technology in unterschiedlichen Zelllinien hergestellt, welche SLFN12, wie PDE3A, als essentiellen Faktor im Mechanismus von PDE3-modulierenden Wirkstoffen bestätigte. Des Weiteren habe ich eine SLFN12 Deletions-Analyse durchgeführt um herauszufinden welche Domäne(n) essentiell für einen DNMDP-induzierten Krebszelltod ist/sind. Diese Studie ermöglichte einen tieferen Einblick in die biologische Funktion von SLFN12, welche durch DNMDP ausgenützt wird um selektiv Krebszellen zu zerstören. Die neuen Erkenntnisse die durch dieses Projekt erlangt werden konnten, leisten einen unterstützenden Beitrag zur Verbesserung von DNMDP auf dem Weg zu einer Anti-Tumor Therapie. Cancer, essentially a disease of the genome, is considered one of the most dangerous medical conditions and the leading cause of death worldwide in 2012. In the past few decades novel discoveries and innovative ideas have led to promising treatment options for several cancer types. This is due to vast improvements in preventative care as well as emerging research fields such as nanotechnology, epigenetic drugs and immune therapies. The notion of broad one-size-fit-all treatments has gradually yielded to tailored therapies, which target specific dependencies in different types of cancer based on the genomic landscape of mutations in each individual patient. In 2015 de Waal et al. have discovered a novel compound, 6-(4-(diethylamino)-3-nitrophenyl)-5-methyl-4,5-dihydropyridazin-3(2H)-one (DNMDP) that selectively killed a subset of cancer cell lines. Further investigations revealed that this small molecule binds to phosphodiesterase 3A (PDE3A), which is a common target for inhibition in several cardiovascular diseases, and enables engagement with another protein, Schlafen 12 (SLFN12), in order to form a compound-dependent complex. This PDE3A-SLFN12 protein interaction further induces a yet unknown pathway that ultimately leads to apoptosis. Notably, DNMDP-induced cell killing represents a novel cellular mechanism in contrast to typical cancer dependencies. In this study, I focused on understanding the role of SLFN12 in DNMDP-induced cell death. Specifically, I generated knock-outs of endogenous SLFN12 using CRISPR/Cas9 technology in several cancer cell lines, which verified that SLFN12, like PDE3A, is a required factor in the mode of action of PDE3 modulating agents. I also performed deletion analysis of SLFN12 in order to elucidate the domain(s) required for DNMDP-induced cell death. This study gave new insights into the biology of SLFN12 that is leveraged by DNMDP to achieve selective cancer cell killing. The new information gained in this project may contribute to further improvements of DNMDP as a promising antitumor therapy. vorgelegt von: Marcus Tötzl Wien, FH Campus Wien, Masterarb., 2017

Published

2017

44. PDE3A variant associated with hypertension and brachydactyly syndrome in a patient with ischemic stroke caused by spontaneous intracranial artery dissection: A review of the clinical and molecular genetic features.

Author

Lee, Cha Gon, Kang, Kyusik, Yoon, Ra Gyoung, Seo, Ji Young, and Park, Jong-Moo

Subjects

*CYCLIC nucleotide phosphodiesterases, *VASCULAR smooth muscle, *SMOOTH muscle contraction, *RECESSIVE genes, *STROKE patients, *SHORT stature, *CONTRACTILITY (Biology), *CARDIAC contraction

Abstract

Hypertension and brachydactyly syndrome (HTNB; MIM 112410) is a rare, recently described, autosomal dominant syndromic disease characterized by the triad of brachydactyly type E (BDE), short stature, and hypertension. HTNB is caused by a heterozygous mutation in the PDE3A (MIM 123805) gene on chromosome 12p12; this gene encodes a member of the cGMP-inhibited cyclic nucleotide phosphodiesterase family. PED3A plays a role in many signal transduction pathways, including those involved in vascular smooth muscle proliferation and contraction, cardiac contractility, platelet aggregation, and hormone secretion. Here, we present a new case of HTNB in a 42-year-old patient who experienced recurrent ischemic strokes in various vascular territories; these strokes were caused by intracranial multiarterial dissection, and were experienced for 2 weeks. She was found to harbor a de novo heterozygous in-frame deletion, c.1333_1335del p.(Thr445del), in exon 4 of the PDE3A gene. Our finding is expected to contribute to the elucidation of the pathophysiology of stroke in HTNB patients. We further review all clinical and molecular genetic features of this rare disease described in the literature to date. [ABSTRACT FROM AUTHOR]

Published

2020

45. Phosphodiesterase 3 mediates cross-talk between the protein kinase- and cGMP- dependent pathways and cyclic AMP metabolism

Author

Edyta Makuch and Janusz Matuszyk

Subjects

Microbiology (medical), Phosphodiesterase 3, lcsh:Medicine, structure and regulation of the activity of PDE3, PDE, Cyclic nucleotide, chemistry.chemical_compound, protein kinase-dependent pathways, Catalytic Domain, Cyclic AMP, Protein Isoforms, phosphodiesterase 3 family, Phosphorylation, Natriuretic Peptides, Protein kinase A, Cyclic GMP, natriuretic peptide signaling, chemistry.chemical_classification, PDE3A, Chemistry, lcsh:R, Phosphodiesterase, Receptor Cross-Talk, Cyclic Nucleotide Phosphodiesterases, Type 3, Cell biology, Enzyme Activation, Infectious Diseases, Enzyme, cAMP and cGMP signaling cross-talk, PDE10A, Signal transduction, phosphodiesterase, Hydrophobic and Hydrophilic Interactions, Protein Kinases, Signal Transduction

Abstract

PDE3 is a dual-substrate phosphodiesterase responsible for hydrolyzing both cAMP and cGMP whilst being simultaneously inhibited by cGMP. This feature is related to presence of the 44 amino acid insert in the catalytic domain, which determines the mechanism of introduction of the cyclic nucleotide into the catalytic pocket of the enzyme. Once bound in the catalytic site cGMP results in steric hindrance for cAMP to enter the site. The regulatory domain of PDE3 consists of two hydrophobic regions: NHR1 and NHR2. Their presence defines the enzyme’s intracellular localization, thus determining its participation in particular signaling cascades. Due to the properties of PDE3 this enzyme has exceptional importance for the cross-talk between cAMP-dependent signaling and other cascades. There are two different mechanisms of action of PDE3 enzymes in cell signaling pathways. In many signaling cascades assembly of a signalosome is necessary for phosphorylation and activation of the PDE3 proteins. In response to certain hormones and growth factors, PDE3 merges the metabolism of cAMP with protein kinase-dependent signaling pathways. PDE3 also controls the level of cAMP with regard to the alternating concentration of cGMP. This effect occurs in signaling cascades activated by natriuretic peptide.

Published

2012

46. Mechanistic insights into cancer cell killing through interaction of phosphodiesterase 3A and schlafen family member 12.

Author

Wu X, Schnitzler GR, Gao GF, Diamond B, Baker AR, Kaplan B, Williamson K, Westlake L, Lorrey S, Lewis TA, Garvie CW, Lange M, Hayat S, Seidel H, Doench J, Cherniack AD, Kopitz C, Meyerson M, and Greulich H

Subjects

Base Sequence, Biomarkers, Tumor metabolism, CRISPR-Cas Systems genetics, Catalytic Domain, Cell Death drug effects, Cell Line, Tumor, Cyclic Nucleotide Phosphodiesterases, Type 3 chemistry, Frameshift Mutation genetics, Genome, Heterozygote, Humans, Protein Binding drug effects, Pyridazines pharmacology, Cyclic Nucleotide Phosphodiesterases, Type 3 metabolism, Intracellular Signaling Peptides and Proteins metabolism, Neoplasms pathology

Abstract

Cytotoxic molecules can kill cancer cells by disrupting critical cellular processes or by inducing novel activities. 6-(4-(Diethylamino)-3-nitrophenyl)-5-methyl-4,5-dihydropyridazin-3(2 H )-one (DNMDP) is a small molecule that kills cancer cells by generation of novel activity. DNMDP induces complex formation between phosphodiesterase 3A (PDE3A) and schlafen family member 12 (SLFN12) and specifically kills cancer cells expressing elevated levels of these two proteins. Here, we examined the characteristics and covariates of the cancer cell response to DNMDP. On average, the sensitivity of human cancer cell lines to DNMDP is correlated with PDE3A expression levels. However, DNMDP could also bind the related protein, PDE3B, and PDE3B supported DNMDP sensitivity in the absence of PDE3A expression. Although inhibition of PDE3A catalytic activity did not account for DNMDP sensitivity, we found that expression of the catalytic domain of PDE3A in cancer cells lacking PDE3A is sufficient to confer sensitivity to DNMDP, and substitutions in the PDE3A active site abolish compound binding. Moreover, a genome-wide CRISPR screen identified the aryl hydrocarbon receptor-interacting protein (AIP), a co-chaperone protein, as required for response to DNMDP. We determined that AIP is also required for PDE3A-SLFN12 complex formation. Our results provide mechanistic insights into how DNMDP induces PDE3A-SLFN12 complex formation, thereby killing cancer cells with high levels of PDE3A and SLFN12 expression., (© 2020 Wu et al.)

Published

2020

47. Clinical and Molecular Perspectives of Monogenic Hypertension.

Author

Levanovich PE, Diaczok A, and Rossi NF

Subjects

Genetic Predisposition to Disease, Heredity, Humans, Hypertension diagnosis, Hypertension physiopathology, Hypertension therapy, Inheritance Patterns, Pedigree, Phenotype, Prognosis, Risk Factors, Blood Pressure genetics, Hypertension genetics, Mutation

Abstract

Advances in molecular research techniques have enabled a new frontier in discerning the mechanisms responsible for monogenic diseases. In this review, we discuss the current research on the molecular pathways governing blood pressure disorders with a Mendelian inheritance pattern, each presenting with a unique pathophysiology. Glucocorticoid Remediable Aldosteronism (GRA) and Apparent Mineralocorticoid Excess (AME) are caused by mutations in regulatory enzymes that induce increased production of mineralocorticoids or inhibit degradation of glucocorticoids, respectively. Geller syndrome is due to a point mutation in the hormone responsive element of the promotor for the mineralocorticoid receptor, rendering the receptor susceptible to activation by progesterone, leading to hypertension during pregnancy. Pseudohypoaldosteronism type II (PHA-II), also known as Gordon's syndrome or familial hyperkalemic hypertension, is a more variable disorder typically characterized by hypertension, high plasma potassium and metabolic acidosis. Mutations in a variety of intracellular enzymes that lead to enhanced sodium reabsorption have been identified. In contrast, hypertension in Liddle's syndrome, which results from mutations in the Epithelial sodium Channel (ENaC), is associated with low plasma potassium and metabolic alkalosis. In Liddle's syndrome, truncation of one the ENaC protein subunits removes a binding site necessary protein for ubiquitination and degradation, thereby promoting accumulation along the apical membrane and enhanced sodium reabsorption. The myriad effects due to mutation in phosphodiesterase 3A (PDE3A) lead to severe hypertension underlying sodium-independent autosomal dominant hypertension with brachydactyly. How mutations in PDE3A result in the phenotypic features of this disorder are discussed. Understanding the pathologies of these monogenic hypertensive disorders may provide insight into the causes of the more prevalent essential hypertension and new avenues to unravel the complexities of blood pressure regulation., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2020

48. Estrogen-Related Hormones Induce Apoptosis by Stabilizing Schlafen-12 Protein Turnover.

Author

Li, Dianrong, Chen, Jie, Ai, Youwei, Gu, Xiaoqiong, Li, Li, Che, Di, Jiang, Zhaodi, Li, Lin, Chen, She, Huang, Huangwei, Wang, Jiawen, Cai, Tao, Cao, Yang, Qi, Xiangbin, and Wang, Xiaodong

Subjects

*RIBOSOMES, *SEX hormones, *BCL-2 proteins, *APOPTOSIS, *ENDOPLASMIC reticulum, *PROTEINS, *STEROID hormones

Abstract

The mitochondrial pathway of apoptosis is controlled by the ratio of anti- and pro-apoptotic members of the Bcl-2 family of proteins. The molecular events underlying how a given physiological stimulus changes this ratio to trigger apoptosis remains unclear. We report here that human 17-β-estradiol (E2) and its related steroid hormones induce apoptosis by binding directly to phosphodiesterase 3A, which in turn recruits and stabilizes an otherwise fast-turnover protein Schlafen 12 (SLFN12). The elevated SLFN12 binds to ribosomes to exclude the recruitment of signal recognition particles (SRPs), thereby blocking the continuous protein translation occurring on the endoplasmic reticulum of E2-treated cells. These proteins include Bcl-2 and Mcl-1, whose ensuing decrease triggers apoptosis. The SLFN12 protein and an apoptosis activation marker were co-localized in syncytiotrophoblast of human placentas, where levels of estrogen-related hormones are high, and dynamic cell turnover by apoptosis is critical for successful implantation and placenta development. • Estrogen-like hormones activate apoptosis by binding to phosphodiesterase 3A, PDE3A • Estrogen-bound PDE3A stabilizes protein turnover of Schlafen 12 (SLFN12) • SLFN12 binds to ribosomes to stop ER-mediated protein translation • Estrogne-induced apoptosis occurs in syncytiotrophoblast of human placenta Estrogen-like female sex hormones at concentrations present in human placenta induce apoptosis. They do so by binding to phosphodiesterase 3A, which in turn recruits and stabilizes Schlafen 12 protein, whose elevated level stops the protein translation on ER, resulting in downregulation of anti-apoptotic proteins Bcl-2 and Mcl-1 and subsequent apoptosis. [ABSTRACT FROM AUTHOR]

Published

2019

49. Protein kinase B/Akt phosphorylation of PDE3A and its role in mammalian oocyte maturation

Author

Han, Seung Jin, Vaccari, Sergio, Nedachi, Taku, Andersen, Carsten B, Kovacina, Kristina S, Roth, Richard A, and Conti, Marco

Published

2006

50. PDE3A inhibitor anagrelide activates death signaling pathway genes and synergizes with cell death-inducing cytokines to selectively inhibit cancer cell growth.

Author

An R, Liu J, He J, Wang F, Zhang Q, and Yu Q

Abstract

We performed a drug repurposing screening of a US Food and Drug Administration (FDA)-approved drug compound library and identified Anagrelide (ANA), a known phosphodiesterase 3A (PDE3A) inhibitor, that selectively and potently inhibited the growth of cancer cells. However, inactivation of PDE3A or knocking-down its gene expression did not inhibit cancer cell growth. It was the interaction of ANA with PDE3A that created a new function of PDE3A to alter the activities of another unknown function protein SLFN12 to cause the inhibition of cancer cell growth. The expressions of both PDE3A and SLFN12 were required for ANA to inhibit cancer cell growth. Depletion of PDE3A or SLFN12 led to ANA resistance. Furthermore, the effects of ANA on different cancer cells were different depending on the expression levels of PDE3A and SLFN12, causing G0/G1 cell cycle arrest in the cells expressing lower levels of SLFN12, but apoptosis in the cells expressing higher levels of the two proteins. Further investigation into the molecular mechanisms of the ANA-induced cell cycle arrest and apoptosis identified a set of cell cycle and apoptosis-related genes whose expressions were altered by ANA treatment. ANA also synergized with the cell death-inducing cytokines IFN-α, IFN-γ, TNF-α, or TRAIL, which regulated the same set of genes as ANA did, to induce apoptosis of the cancer cells. Our study uncovered new activities, functions, and mechanisms of ANA and SLFN12 and provided a diagnosis method to precisely use ANA as an anti-cancer drug. It also revealed PDE3A and SLFN12 as new anti-cancer drug targets for developing novel anti-cancer therapies., Competing Interests: None., (AJCR Copyright © 2019.)

Published

2019