Person:

Vandenwijngaert, Sara

Profile Picture

Email Address

AA Acceptance Date

Birth Date

Research Projects

Organizational Units

Job Title

Last Name

Vandenwijngaert

First Name

Sara

Name

Vandenwijngaert, Sara
Author's Publications: search.filters.isAuthorOfPublication.2099dbbf-68dd-42b1-a8c9-04e32ab46d0d

Search Results

Now showing 1 - 7 of 7
  • Thumbnail Image
    Publication

    Atrial natriuretic peptide is negatively regulated by microRNA-425

    (American Society for Clinical Investigation, 2013) Arora, Pankaj; Wu, Connie; Khan, Abigail May; Bloch, Donald; Davis-Dusenbery, Brandi N; Ghorbani, Anahita; Spagnolli, Ester; Martinez, Andrew; Ryan, Allicia; Tainsh, Laurel T.; Kim, Samuel M; Rong, Jian; Huan, Tianxiao; Freedman, Jane E.; Levy, Daniel; Miller, Karen; Hata, Akiko; Del Monte, Federica; Vandenwijngaert, Sara; Swinnen, Melissa; Janssens, Stefan; Holmes, Tara M.; Buys, Emmanuel; Bloch, Kenneth; Newton-Cheh, Christopher; Wang, Thomas Jue-Fuu

    Numerous common genetic variants have been linked to blood pressure, but no underlying mechanism has been elucidated. Population studies have revealed that the variant rs5068 (A/G) in the 3′ untranslated region of NPPA, the gene encoding atrial natriuretic peptide (ANP), is associated with blood pressure. We selected individuals on the basis of rs5068 genotype (AG vs. AA) and fed them a low- or high-salt diet for 1 week, after which they were challenged with an intravenous saline infusion. On both diets, before and after saline administration, ANP levels were up to 50% higher in AG individuals than in AA individuals, a difference comparable to the changes induced by high-salt diet or saline infusion. In contrast, B-type natriuretic peptide levels did not differ by rs5068 genotype. We identified a microRNA, miR-425, that is expressed in human atria and ventricles and is predicted to bind the sequence spanning rs5068 for the A, but not the G, allele. miR-425 silenced NPPA mRNA in an allele-specific manner, with the G allele conferring resistance to miR-425. This study identifies miR-425 as a regulator of ANP production, raising the possibility that miR-425 antagonists could be used to treat disorders of salt overload, including hypertension and heart failure.

  • Thumbnail Image
    Publication

    Ventricular Phosphodiesterase-5 Expression Is Increased in Patients With Advanced Heart Failure and Contributes to Adverse Ventricular Remodeling After Myocardial Infarction in Mice

    (Ovid Technologies (Wolters Kluwer Health), 2009) Pokreisz, Peter; Vandenwijngaert, Sara; Bito, Virginie; Van den Bergh, An; Lenaerts, Ilse; Busch, Cornelius; Marsboom, Glenn; Gheysens, Olivier; Vermeersch, Pieter; Biesmans, Liesbeth; Liu, Xiaoshun; Gillijns, Hilde; Pellens, Marijke; Van Lommel, Alfons; Buys, Emmanuel; Schoonjans, Luc; Vanhaecke, Johan; Verbeken, Erik; Sipido, Karin; Herijgers, Paul; Bloch, Kenneth; Janssens, Stefan P.

    Background— Ventricular expression of phosphodiesterase-5 (PDE5), an enzyme responsible for cGMP catabolism, is increased in human right ventricular hypertrophy, but its role in left ventricular (LV) failure remains incompletely understood. We therefore measured LV PDE5 expression in patients with advanced systolic heart failure and characterized LV remodeling after myocardial infarction in transgenic mice with cardiomyocyte-specific overexpression of PDE5 (PDE5-TG). Methods and Results— Immunoblot and immunohistochemistry techniques revealed that PDE5 expression was greater in explanted LVs from patients with dilated and ischemic cardiomyopathy than in control hearts. To evaluate the impact of increased ventricular PDE5 levels on cardiac function, PDE5-TG mice were generated. Confocal and immunoelectron microscopy revealed increased PDE5 expression in cardiomyocytes, predominantly localized to Z-bands. At baseline, myocardial cGMP levels, cell shortening, and calcium handling in isolated cardiomyocytes and LV hemodynamic measurements were similar in PDE5-TG and wild-type littermates. Ten days after myocardial infarction, LV cGMP levels had increased to a greater extent in wild-type mice than in PDE5-TG mice (P<0.05). Ten weeks after myocardial infarction, LV end-systolic and end-diastolic volumes were larger in PDE5-TG than in wild-type mice (57±5 versus 39±4 and 65±6 versus 48±4 μL, respectively; P<0.01 for both). LV systolic dysfunction and diastolic dysfunction were more marked in PDE5-TG than in wild-type mice, associated with enhanced hypertrophy and reduced contractile function in isolated cardiomyocytes from remote myocardium. Conclusions— Increased PDE5 expression predisposes mice to adverse LV remodeling after myocardial infarction. Increased myocardial PDE5 expression in patients with advanced cardiomyopathy may contribute to the development of heart failure and represents an important therapeutic target.

  • Thumbnail Image
    Publication

    Decreased Soluble Guanylate Cyclase Contributes to Cardiac Dysfunction Induced by Chronic Doxorubicin Treatment in Mice

    (Mary Ann Liebert Inc, 2017) Vandenwijngaert, Sara; Swinnen, Melissa; Walravens, Ann-Sophie; Beerens, Manu; Gillijns, Hilde; Caluwé, Ellen; Tainsh, Robert; Nathan, Daniel I.; Allen, Kaitlin; Brouckaert, Peter; Bartunek, Jozef; Scherrer-Crosbie, Marielle; Bloch, Kenneth; Bloch, Donald; Janssens, Stefan P.; Buys, Emmanuel

    Aims: The use of doxorubicin, a potent chemotherapeutic agent, is limited by cardiotoxicity. We tested the hypothesis that decreased soluble guanylate cyclase (sGC) enzyme activity contributes to the development of doxorubicin-induced cardiotoxicity. Results: Doxorubicin administration (20 mg/kg, intraperitoneally [IP]) reduced cardiac sGC activity in wild-type (WT) mice. To investigate whether decreased sGC activity contributes to doxorubicin-induced cardiotoxicity, we studied mice with cardiomyocyte-specific deficiency of the sGC a1-subunit (mice with cardiomyocyte-specific deletion of exon 6 of the sGCa1 allele [sGCa1-/-CM]). After 12 weeks of doxorubicin administration (2 mg/kg/week IP), left ventricular (LV) systolic dysfunction was greater in sGCa1-/-CM than WT mice. To further assess whether reduced sGC activity plays a pathogenic role in doxorubicin-induced cardiotoxicity, we studied a mouse model in which decreased cardiac sGC activity was induced by cardiomyocyte-specific expression of a dominant negative sGCa1 mutant (DNsGCa1) upon doxycycline removal (Tet-off). After 8 weeks of doxorubicin administration, DNsGCa1tg/+, but not WT, mice displayed LV systolic dysfunction and dilatation. The difference in cardiac function and remodeling between DNsGCa1tg/+ and WT mice was even more pronounced after 12 weeks of treatment. Further impairment of cardiac function was attenuated when DNsGCa1 gene expression was inhibited (beginning at 8 weeks of doxorubicin treatment) by administering doxycycline. Furthermore, doxorubicin-associated reactive oxygen species generation was higher in sGCa1-deficient than WT hearts. Innovation and Conclusion: These data demonstrate that a reduction in cardiac sGC activity worsens doxorubicin-induced cardiotoxicity in mice and identify sGC as a potential therapeutic target. Various pharmacological sGC agonists are in clinical development or use and may represent a promising approach to limit doxorubicin-associated cardiotoxicity.

  • Thumbnail Image
    Publication

    Inhaled nitric oxide: an sGC-dependent IOP lowering agent

    (BioMed Central, 2015) Lieb, Wolfgang S; Munster, Stefan; Dordea, Ana C; Vandenwijngaert, Sara; Tainsh, Robert E; Brouckaert, Peter; Zapol1, Warren M; Buys, Emmanuel
  • Thumbnail Image
    Publication

    Cardiac soluble guanylate cyclase protects against the cardiac dysfunction induced by chronic doxorubicin treatment in mice

    (BioMed Central, 2015) Vandenwijngaert, Sara; Swinnen, Melissa; Gillijns, Hilde; Caluwé, Ellen; Tainsh, Robert E; Nathan, Daniel I; Allen, Kaitlin; Bartunek, Jozef; Brouckaert, Peter; Scherrer-Crosbie, Marielle; Bloch, Kenneth D; Janssens, Stefan P; Buys, Emmanuel
  • Thumbnail Image
    Publication

    Androgen-sensitive hypertension associated with soluble guanylate cyclase alpha1 deficiency is mediated by 20-HETE

    (BioMed Central, 2015) Vandenwijngaert, Sara; Dordea, Ana C; Garcia, Victor; Tainsh, Robert E; Nathan, Daniel I; Raher, Michael J; Allen, Kaitlin; Zhang, Fan; Lieb, Wolfgang S; Mikelman, Sarah; Kirby, Andrew; Stevens, Christine; Thoonen, Robrecht; Hindle, Allyson; Sips, Patrick Y; Malhotra, Rajeev; Daly, Mark; Brouckaert, Peter; Bloch, Kenneth D; Schwartzman, Michal; Buys, Emmanuel
  • Thumbnail Image
    Publication

    Abstracts from the 8th International Conference on cGMP Generators, Effectors and Therapeutic Implications: Bamberg, Germany. 23-25 June, 2017

    (BioMed Central, 2017) Todd Milne, G.; Sandner, Peter; Lincoln, Kathleen A.; Harrison, Paul C.; Chen, Hongxing; Wang, Hong; Clifford, Holly; Qian, Hu Sheng; Wong, Diane; Sarko, Chris; Fryer, Ryan; Richman, Jeremy; Reinhart, Glenn A.; Boustany, Carine M.; Pullen, Steven S.; Andresen, Henriette; Moltzau, Lise Román; Cataliotti, Alessandro; Levy, Finn Olav; Lukowski, Robert; Frankenreiter, Sandra; Friebe, Andreas; Calamaras, Timothy; Baumgartner, Robert; McLaughlin, Angela; Aronovitz, Mark; Baur, Wendy; Wang, Guang-Rong; Kapur, Navin; Karas, Richard; Blanton, Robert; Hell, Stefan; Waldman, Scott A.; Lin, Jieru E.; Colon-Gonzalez, Francheska; Kim, Gilbert W.; Blomain, Erik S.; Merlino, Dante; Snook, Adam; Erdmann, Jeanette; Wobst, Jana; Kessler, Thorsten; Schunkert, Heribert; Walter, Ulrich; Pagel, Oliver; Walter, Elena; Gambaryan, Stepan; Smolenski, Albert; Jurk, Kerstin; Zahedi, Rene; Klinger, James R.; Benza, Raymond L.; Corris, Paul A.; Langleben, David; Naeije, Robert; Simonneau, Gérald; Meier, Christian; Colorado, Pablo; Chang, Mi Kyung; Busse, Dennis; Hoeper, Marius M.; Masferrer, Jaime L.; Jacobson, Sarah; Liu, Guang; Sarno, Renee; Bernier, Sylvie; Zhang, Ping; Flores-Costa, Roger; Currie, Mark; Hall, Katherine; Möhrle, Dorit; Reimann, Katrin; Wolter, Steffen; Wolters, Markus; Mergia, Evanthia; Eichert, Nicole; Geisler, Hyun-Soon; Ruth, Peter; Feil, Robert; Zimmermann, Ulrike; Koesling, Doris; Knipper, Marlies; Rüttiger, Lukas; Tanaka, Yasutake; Okamoto, Atsuko; Nojiri, Takashi; Kumazoe, Motofumi; Tokudome, Takeshi; Miura, Koichi; Hino, Jun; Hosoda, Hiroshi; Miyazato, Mikiya; Kangawa, Kenji; Kapil, Vikas; Ahluwalia, Amrita; Paolocci, Nazareno; Eaton, Philip; Campbell, James C.; Henning, Philipp; Franz, Eugen; Sankaran, Banumathi; Herberg, Friedrich W.; Kim, Choel; Wittwer, M.; Luo, Q.; Kaila, V.; Dames, S. A.; Tobin, Andrew; Alam, Mahmood; Rudyk, Olena; Krasemann, Susanne; Hartmann, Kristin; Prysyazhna, Oleksandra; Zhang, Min; Zhao, Lan; Weiss, Astrid; Schermuly, Ralph; Moyes, Amie J.; Chu, Sandy M.; Baliga, Reshma S.; Hobbs, Adrian J.; Michalakis, Stylianos; Mühlfriedel, Regine; Schön, Christian; Fischer, Dominik M.; Wilhelm, Barbara; Zobor, Ditta; Kohl, Susanne; Peters, Tobias; Zrenner, Eberhart; Bartz-Schmidt, Karl Ulrich; Ueffing, Marius; Wissinger, Bernd; Seeliger, Mathias; Biel, Martin; Ranek, Mark J.; Kokkonen, Kristen M.; Lee, Dong I.; Holewinski, Ronald J.; Agrawal, Vineet; Virus, Cornelia; Stevens, Donté A.; Sasaki, Masayuki; Zhang, Huaqun; Mannion, Mathew M.; Rainer, Peter P.; Page, Richard C.; Schisler, Jonathan C.; Van Eyk, Jennifer E.; Willis, Monte S.; Kass, David A.; Zaccolo, Manuela; Russwurm, Michael; Giesen, Jan; Russwurm, Corina; Füchtbauer, Ernst-Martin; Bork, Nadja I.; Nikolaev, Viacheslav O.; Agulló, Luis; Floor, Martin; Villà-Freixa, Jordi; Manfra, Ornella; Calamera, Gaia; Surdo, Nicoletta C.; Meier, Silja; Froese, Alexander; Andressen, Kjetil Wessel; Aue, Annemarie; Schwiering, Fabian; Groneberg, Dieter; Bajraktari, Gzona; Burhenne, Jürgen; Haefeli, Walter E.; Weiss, Johanna; Beck, Katharina; Voussen, Barbara; Vincent, Alexander; Parsons, Sean P.; Huizinga, Jan D.; Mónica, Fabiola Zakia; Seto, Edward; Murad, Ferid; Bian, Ka; Burgoyne, Joseph R.; Richards, Daniel; Bjørnerem, Marianne; Ulsund, Andrea Hembre; Kim, Jeong Joo; Donzelli, Sonia; Goetz, Mara; Schmidt, Kjestine; Stathopoulou, Konstantina; Scotcher, Jenna; Dees, Christian; Subramanian, Hariharan; Butt, Elke; Kamynina, Alisa; Bruce King, S.; de Witt, Cor; Leichert, Lars I.; Cuello, Friederike; Dobrowinski, Hyazinth; Lehners, Moritz; Schmidt, Michael Paolillo Hannes; Feil, Susanne; Wen, Lai; Thunemann, Martin; Olbrich, Marcus; Langer, Harald; Gawaz, Meinrad; de Wit, Cor; Bertinetti, Daniela; Ghofrani, Hossein-Ardeschir; Grimminger, Friedrich; Grünig, Ekkehard; Huang, Yigao; Jansa, Pavel; Jing, Zhi Cheng; Kilpatrick, David; Rosenkranz, Stephan; Menezes, Flavia; Fritsch, Arno; Nikkho, Sylvia; Frey, Reiner; Humbert, Marc; Harloff, Manuela; Reinders, Joerg; Schlossmann, Jens; Jung, Joon; Wales, Jessica A.; Chen, Cheng-Yu; Breci, Linda; Weichsel, Andrzej; Bernier, Sylvie G.; Solinga, Robert; Sheppeck, James E.; Renhowe, Paul A.; Montfort, William R.; Qin, Liying; Sung, Ying-Ju; Casteel, Darren; Kollau, Alexander; Neubauer, Andrea; Schrammel, Astrid; Mayer, Bernd; Takai, Mika; Takeuchi, Chieri; Kadomatsu, Mai; Hiroi, Shun; Takamatsu, Kanako; Tachibana, Hirofumi; Opelt, Marissa; Eroglu, Emrah; Waldeck-Weiermair, Markus; Malli, Roland; Graier, Wolfgang F.; Fassett, John T.; Sollie, Selene J.; Hernandez-Valladares, Maria; Berven, Frode; Andressen, Kjetil W.; Arai, Miki; Suzuki, Yutaka; Okumura, Meinoshin; Kawaoka, Shinpei; Peters, Stefanie; Schmidt, Hannes; Selin Kenet, B.; Nies, Sarah Helena; Frank, Katharina; Rathjen, Fritz G.; Petrova, Olga N.; Lamarre, Isabelle; Négrerie, Michel; Robinson, Jerid W.; Egbert, Jeremy R.; Davydova, Julia; Jaffe, Laurinda A.; Potter, Lincoln R.; Blixt, Nicholas; Shuhaibar, Leia C.; Warren, Gordon L.; Mansky, Kim C.; Romoli, Simone; Bauch, Tobias; Dröbner, Karoline; Eitner, Frank; Ruppert, Mihály; Radovits, Tamás; Korkmaz-Icöz, Sevil; Li, Shiliang; Hegedűs, Péter; Loganathan, Sivakanan; Németh, Balázs Tamás; Oláh, Attila; Mátyás, Csaba; Benke, Kálmán; Merkely, Béla; Karck, Matthias; Szabó, Gábor; Scheib, Ulrike; Broser, Matthias; Mukherjee, Shatanik; Stehfest, Katja; Gee, Christine E.; Körschen, Heinz G.; Oertner, Thomas G.; Hegemann, Peter; Dickey, Deborah M.; Dumoulin, Alexandre; Kühn, Ralf; Jaffe, Laurinda; Schobesberger, Sophie; Wright, Peter; Poulet, Claire; Mansfield, Catherine; Harding, Sian E.; Gorelik, Julia; Wölkart, Gerald; Gorren, Antonius C. F.; Schwaerzer, Gerburg K.; Casteel, Darren E.; Dalton, Nancy D.; Gu, Yusu; Zhuang, Shunhui; Milewicz, Dianna M.; Peterson, Kirk L.; Pilz, Renate; Argyriou, Aikaterini I.; Makrynitsa, Garyfalia; Alexandropoulos, Ioannis I.; Stamopoulou, Andriana; Bantzi, Marina; Giannis, Athanassios; Topouzis, Stavros; Papapetropoulos, Andreas; Spyroulias, Georgios A.; Stuehr, Dennis J.; Ghosh, Arnab; Dai, Yue; Misra, Saurav; Tchernychev, Boris; Silos-Santiago, Inmaculada; Hannig, Gerhard; Dao, Vu Thao-Vi; Deile, Martin; Nedvetsky, Pavel I.; Güldner, Andreas; Ibarra-Alvarado, César; Gödecke, Axel; Schmidt, Harald H. H. W.; Vachaviolos, Angelos; Gerling, Andrea; Lutz, Stefan Z.; Häring, Hans-Ulrich; Krüger, Marcel A.; Pichler, Bernd J.; Shipston, Michael J.; Vandenwijngaert, Sara; Ledsky, Clara D.; Agha, Obiajulu; Hu, Dongjian; Domian, Ibrahim; Buys, Emmanuel; Newton-Cheh, Christopher; Bloch, Donald; Mauro, Nadine; Keppler, Jonas; Ferreira, Wilson A.; Chweih, Hanan; Brito, Pamela L.; Almeida, Camila B.; Penteado, Carla F. F.; Saad, Sara S. O.; Costa, Fernando F.; Frenette, Paul S.; Brockschnieder, Damian; Stasch, Johannes-Peter; Conran, Nicola; Zimmer, Daniel P.; Tobin, Jenny; Shea, Courtney; Long, Kimberly; Tang, Kim; Germano, Peter; Wakefield, James; Banijamali, Ali; Im, G-Yoon Jamie; Profy, Albert T.; Currie, Mark G.