Harnessing the Chirality of Phosphorus Compounds, from Catalysis to Application

Many bioactive molecules and essential building blocks of biological systems are chiral and contain phosphorus (P) in the oxidation state (V). Such compounds are ubiquitous in nature and pivotal for numerous biological processes such as membrane formation, cell replication, information (DNA, RNA), proper functioning of enzymes and proteins, glycolysis and energy metabolism. Moreover, phosphorus‒carbon- (P‒C)- and phosphorus‒nitrogen- (P‒N)-bonds belong to essential structural motifs in many functional materials, ligands in metal catalysis, pharmaceuticals, fertilizers, detergents and pesticides. Therefore, chiral phosphorus-containing compounds are interesting targets for applied research, but should be also considered when investigating the homochirality and origin of life. Precisely these motivations spearheaded the work in this thesis, which revolves around the chirality of organophosphorus compounds. More specifically, it focusses on the development of new catalytic diastereoselective and enantioselective reactions to access P(V)-substituted substrates. Furthermore, the chiral products of these reactions and their ability to form aggregates were investigated, which led to observation of intriguing self-resolving properties. Moreover, this offered an attractive approach to enantioenrichment by phase-partitioning, which is often discussed in context of homochirality. Finally, the design of a new (asymmetric) autocatalytic reaction was attempted, which is considered to be an alternative pathway to obtain molecular single-handedness on Earth

Turning Enantiomeric Relationships into Diastereomeric Ones: Self-Resolving α-Ureidophosphonates and Their Organocatalytic Enantioselective Synthesis

[Image: see text] Controlling chiral recognition and chiral information transfer has major implications in areas ranging from drug design and asymmetric catalysis to supra- and macromolecular chemistry. Especially intriguing are phenomena associated with chiral self-recognition. The design of systems that show self-induced recognition of enantiomers, i.e., involving homochiral versus heterochiral dimers, is particularly challenging. Here, we report the chiral self-recognition of α-ureidophosphonates and its application as both a powerful analytical tool for enantiomeric ratio determination by NMR and as a convenient way to increase their enantiomeric purity by simple achiral column chromatography or fractional precipitation. A combination of NMR, X-ray, and DFT studies indicates that the formation of homo- and heterochiral dimers involving self-complementary intermolecular hydrogen bonds is responsible for their self-resolving properties. It is also shown that these often unnoticed chiral recognition phenomena can facilitate the stereochemical analysis during the development of new asymmetric transformations. As a proof of concept, the enantioselective organocatalytic hydrophosphonylation of alkylidene ureas toward self-resolving α-ureidophosphonates is presented, which also led us to the discovery of the largest family of self-resolving compounds reported to date

Chiral Amplification of Phosphoramidates of Amines and Amino Acids in Water

The origin of biomolecular homochirality continues to be one of the most fascinating aspects of prebiotic chemistry. Various amplification strategies for chiral compounds to enhance a small chiral preference have been reported, but none of these involves phosphorylation, one of nature's essential chemical reactions. Here we present a simple and robust concept of phosphorylation-based chiral amplification of amines and amino acids in water. By exploiting the difference in solubility of a racemic phosphoramidate and its enantiopure form, we achieved enantioenrichment in solution. Starting with near racemic, phenylethylamine-based phosphoramidates, ee's of up to 95 % are reached in a single amplification step. Particularly noteworthy is the enantioenrichment of phosphorylated amino acids and their derivatives, which might point to a potential role of phosphorus en-route to prebiotic homochirality

CCDC 2193600: Experimental Crystal Structure Determination

An entry from the Cambridge Structural Database, the world’s repository for small molecule crystal structures. The entry contains experimental data from a crystal diffraction study. The deposited dataset for this entry is freely available from the CCDC and typically includes 3D coordinates, cell parameters, space group, experimental conditions and quality measures

Chiral Amplification of Phosphoramidates of Amines and Amino Acids in Water

The origin of biomolecular homochirality continues to be one of the most fascinating aspects of prebiotic chemistry. Various amplification strategies for chiral compounds to enhance a small chiral preference have been reported, but none of these involves phosphorylation, one of nature's essential chemical reactions. Here we present a simple and robust concept of phosphorylation-based chiral amplification of amines and amino acids in water. By exploiting the difference in solubility of a racemic phosphoramidate and its enantiopure form, we achieved enantioenrichment in solution. Starting with near racemic, phenylethylamine-based phosphoramidates, ee's of up to 95 % are reached in a single amplification step. Particularly noteworthy is the enantioenrichment of phosphorylated amino acids and their derivatives, which might point to a potential role of phosphorus en-route to prebiotic homochirality

Chiral Amplification of Phosphoramidates of Amines and Amino Acids in Water

The origin of biomolecular homochirality continues to be one of the most fascinating aspects of prebiotic chemistry. Various amplification strategies for chiral compounds to enhance a small chiral preference have been reported, but none of these involves phosphorylation, one of nature's essential chemical reactions. Here we present a simple and robust concept of phosphorylation-based chiral amplification of amines and amino acids in water. By exploiting the difference in solubility of a racemic phosphoramidate and its enantiopure form, we achieved enantioenrichment in solution. Starting with near racemic, phenylethylamine-based phosphoramidates, ee's of up to 95 % are reached in a single amplification step. Particularly noteworthy is the enantioenrichment of phosphorylated amino acids and their derivatives, which might point to a potential role of phosphorus en-route to prebiotic homochirality