Project description:Effect of Smyd2 cardiac deficiency was analyzed in mouse heart

Project description:Transcriptional profiling of kidney total RNA extracted from Slc4a5 knock-out and WT mice

Project description:Overexpression of twinkle protects cardiomyocytes from genotoxic stress caused by SOD2 heterozygocity

Project description:NIH3T3 cell transiently transfected with myocardin-EGFP or EGFP. Transfection: Lipofectamine 2000 according to the manufacturers instructions (Invitrogen).

Project description:Effect of the loss of both miR-1/133a clusters on the embryonic heart. Please note: dKO means it is a double KO of the two miR-1/133a clusters in the mouse. Control means we do not use just WT but also some heterozygous animals to compare to dKOs, however these controls do not have a phenotype. Transgene negative: these are littermates of the myocd transgenic animals that do not carry a transgene.

Project description:Inhibition of myostatin signaling induces strong skeletal muscle growth making it an attractive target to treat muscle wasting and sarcopenia. However, the biological function of myostatin in the heart is barely understood. We demonstrate that conditional inactivation of myostatin in the adult murine heart leads to cardiac hypertrophy, heart failure and increased lethality. To induce cardiomyocyte specific loss of myostatin a conditionally active Mstn^fl/fl allele was generated by insertion of loxP elements upstream and downstream of exons 1 and 2 of the mouse myostatin gene. The selection cassette was removed in vivo by flp-recombination. To inactivate myostatin, mice were mated to alphaMyHC-MCM mice (Sohal, DS, et al. (2001) Circulation Research 89, 20-25). Cre-recombination was achieved by intraperitoneal administration of Tamoxifen (40 mg/kg) for 5 consecutive days. The respective control alphaMyHC-MCM animals were equally treated.

Project description:Transcriptional profiling of rat hearts at different developmental stages

Project description:The ventricular wall of the heart is composed of trabeculated and compactlayers, which are separated by yet unknown processes during embryonic development. Notch signaling plays important roles in cardiac development. Mutations in Notch signaling components are related to human congenital heart diseases Two homologues, Numb and Numblike (Numbl), are expressed in mammals, which also act as inhibitors of Notch signaling Here we investigate the role of Notch2 and Numb/Numblike during myocardial trabeculation and compaction. The aim of the experiment is to analyze whether Numb/Numblike are involved in inhibition of Notch activity in the developing heart.

Project description:Microarray technology was used to monitor the level of expression of 7,657 human genes in a set of 35 nodal peripheral T-cell lymphomas.

Project description:Microarray technology was used to identify new predictive biomarkers in samples of clinically homogeneus patients.