Monoamine oxidase is an enzyme that catalyses oxidative deamination of amines. It is located in the outer mitochondrial membrane. There are two known isoforms of MAO enzyme: MAO-A and MAO-B. The main difference between them is the substrate they catalyse. Both isoforms have an important role in the treatment of neurodegenerative diseases such as Alzheimer’s or Parkinson’s disease. The main focus of research in recent years has been directed towards the development of reversible MAO inhibitors because they usually have lower degree of side effects. MurD ligase is an ATP dependent enzyme of the Mur ligases family. It is a well-documented bacterial enzyme responsible for catalysing the addition of peptides to peptidoglycan precursor. The goal of our thesis has been to synthesise new antibacterial compounds using well documented antibacterial targets such as MurD ligases. In our research we set out to design and synthesise analogues of the compound (E)-5-styrylnicotinonitrile which are potential inhibitors of either enzyme MAO or MurD ligases. Compounds were designed based on well documented active compounds synthesised in the Department of Pharmaceutical chemistry, Faculty of Pharmacy, University of Ljubljana. Heck’s reaction has been chosen as the main chemical reaction of our work as it has the tendency to increase low yields. In total eleven new compounds were synthesised. Seven of them were biochemically tested on isolated recombinants human enzyme MAO-A and MAO-B, and four compounds on isolated enzyme MurD ligases. Best inhibitory properties showed (E)-5-(4-methoxy-2-nitrostyryl) nicotinonitrile (11) with IC50 level of 0.42 µM on enzyme MAO-B To conclude (E)-5-(4-methoxy-2-nitrostyryl)nicotinonitrile (11) is an excellent guideline to further research new reversible MAO-B inhibitors and the treatment of neurodegenerative diseases.