Optical rotation, enantiomers

An example of a chiral compound is lactic acid. Two different forms of lactic acid that are mirror images of each other can be defined (Figure 2-69). These two different molecules are called enantiomers. They can be separated, isolated, and characterized experimentally. They are different chemical entities, and some of their properties arc different (c.g., their optical rotation),... 

Only three not four stereoisomeric 2 3 butanediols are possible These three are shown m Eigure 7 10 The (2R 3R) and (2S 3S) forms are enantiomers of each other and have equal and opposite optical rotations A third combination of chirality centers (2R 3S) however gives an achiral structure that is superimposable on its (2S 3R) minor image Because it is achiral this third stereoisomer is optically inactive We call achiral mole cules that have chnahty centers meso forms The meso form m Eigure 7 10 is known as meso 2 3 butanediol... 

Section 7 4 Optical activity, or the degree to which a substance rotates the plane of polarized light is a physical property used to characterize chiral sub stances Enantiomers have equal and opposite optical rotations To be optically active a substance must be chiral and one enantiomer must be present m excess of the other A racemic mixture is optically inactive and contains equal quantities of enantiomers... 

Optically Inactive Chiral Compounds. Although chirality is a necessary prerequisite for optical activity, chiral compounds are not necessarily optically active. With an equal mixture of two enantiomers, no net optical rotation is observed. Such a mixture of enantiomers is said to be racemic and is designated as ( ) and not as dl. Racemic mixtures usually have melting points higher than the melting point of either pure enantiomer. 

A chiral molecule is one which exists in two forms, known as enantiomers. Each of the enantiomers is optically active, which means that they can rotate the plane of plane-polarized light. The enantiomer that rotates the plane to the right (clockwise) has been called the d (or dextro) form and the one that rotates it to the left (anticlockwise) the I (or laevo) form. Nowadays, it is more usual to refer to the d and I forms as the ( + ) and (—) forms, respectively. 

Natural Occurrence of ( — )-proto-Quercitol. Although the dextrorotatory form (12) of proto-quercitol was discovered in acorns more than a century ago by Braconnot (5), who at first thought that it was lactose, the levorotatory form (13) remained unknown until 1961. In that year, Plouvier isolated it from leaves of the tree Eucalyptus populnea the yield was 0.55% (36). The optical rotation of the new compound was equal and opposite to that of the dextro enantiomer, and it was identical to the latter in its crystal form, melting point, solubilities, molecular formula and infrared spectrum. 

The pure, crystalline (— )-proto-quercitol (13) which was isolated had an infrared spectrum identical with that of authentic ( + )-proto-quercitol, and its optical rotation was equal and opposite. Further characterization and preparation of the racemic form, by mixing the enantiomers, is described elsewhere (30). 

The answer is that Pasteur started with a 50 50 mixture of the two chiral tartaric acid enantiomers. Such a mixture is called a racemic (ray-see-mi c) mixture, or racemate, and is denoted either by the symbol ( ) or the prefix cl,I to indicate an equal mixture of dextrorotatory and levorotatory forms. Racemic mixtures show no optical rotation because the (+) rotation from one enantiomer exactly cancels the (-) rotation from the other. Through luck, Pasteur was able to separate, or resolve, racemic tartaric acid into its (-f) and (-) enantiomers. Unfortunately, the fractional crystallization technique he used doesn t work for most racemic mixtures, so other methods are needed. 

The synthesis of key intermediate 12, in optically active form, commences with the resolution of racemic trans-2,3-epoxybutyric acid (27), a substance readily obtained by epoxidation of crotonic acid (26) (see Scheme 5). Treatment of racemic 27 with enantio-merically pure (S)-(-)-1 -a-napthylethylamine affords a 1 1 mixture of diastereomeric ammonium salts which can be resolved by recrystallization from absolute ethanol. Acidification of the resolved diastereomeric ammonium salts with methanesulfonic acid and extraction furnishes both epoxy acid enantiomers in eantiomerically pure form. Because the optical rotation and absolute configuration of one of the antipodes was known, the identity of enantiomerically pure epoxy acid, (+)-27, with the absolute configuration required for a synthesis of erythronolide B, could be confirmed. Sequential treatment of (+)-27 with ethyl chloroformate, excess sodium boro-hydride, and 2-methoxypropene with a trace of phosphorous oxychloride affords protected intermediate 28 in an overall yield of 76%. The action of ethyl chloroformate on carboxylic acid (+)-27 affords a mixed carbonic anhydride which is subsequently reduced by sodium borohydride to a primary alcohol. Protection of the primary hydroxyl group in the form of a mixed ketal is achieved easily with 2-methoxypropene and a catalytic amount of phosphorous oxychloride. 

It is well known that spontaneous resolution of a racemate may occur upon crystallization if a chiral molecule crystallizes as a conglomerate. With regard to sulphoxides, this phenomenon was observed for the first time in the case of methyl p-tolyl sulphoxide269. The optical rotation of a partially resolved sulphoxide (via /J-cyclodextrin inclusion complexes) was found to increase from [a]589 = + 11.5° (e.e. 8.1%) to [a]589 = +100.8 (e.e. 71.5%) after four fractional crystallizations from light petroleum ether. Later on, few optically active ketosulphoxides of low optical purity were converted into the pure enantiomers by fractional crystallization from ethyl ether-hexane270. This resolution by crystallization was also successful for racemic benzyl p-tolyl sulphoxide and t-butyl phenyl sulphoxide271. 

The latter effect has been demonstrated by Meijer et al., who attached chiral aminoalcohols to the peripheral NH2-groups of polypropylene imine) dendrimers of different generations [100]. In the enantioselective addition of diethyl-zinc to benzaldehyde (mediated by these aminoalcohol appendages) both the yields and the enantioselectivities decreased with increasing size of the dendrimer (Fig. 28). The catalyst obtained from the 5th-generation dendrimer carrying 64 aminoalcohol groups at its periphery showed almost no preference for one enantiomer over the other. This behavior coincides with the absence of measurable optical rotation as mentioned in Sect. 3 above. The loss of activity and selectivity was ascribed to multiple interactions on the surface which were... 

The enantiomers of this drug differ in their efficacy and activity, with (D)-penicilla-mine being the enantiomer required for pharmaceutical preparations. The (l)-enantiomer is toxic, and its absorption by the human body is more than the (D)-enantiomer. While both enantiomers of penicillamine are desulfhydrated by (r.)-cysteine desulfhydrase, only the (l)-isomer inhibits the action of this enzyme [2], The reported optical rotation values for (D)-penicillamine are ... 

Enantiomers have identical physical properties such as boiling points, melting points, refractive indices, and solubilities in common solvents except optical rotations. 

No correlation exists between the configuration of enantiomers and the direction of optical rotation. 

The presence of chirality introduces an additional component in the y direction. This component will rotate the polarization of die second-harmonic field with respect to the polarization of the incident radiation. The amount of optical rotation will depend on the relative magnitude of the chiral and achiral susceptibility components. Furthermore, Py changes sign between the enantiomers... 

Scheme 1-1. Enantiomers of 2-isobutyl malonic acid mono amide have opposite optical rotations.

An equal molar mixture of the dextrorotatory and levorotatory enantiomers of a chiral compound is called a racemic mixture or a racemate. Racemates do not show overall optical rotation because the equal and opposite rotations of the two enantiomers cancel each other out. A racemic mixture is designated by adding the prefix (+) or rac- before the name of the molecule. 

Enantiomers have identical chemical and physical properties in the absence of an external chiral influence. This means that 2 and 3 have the same melting point, solubility, chromatographic retention time, infrared spectroscopy (IR), and nuclear magnetic resonance (NMR) spectra. However, there is one property in which chiral compounds differ from achiral compounds and in which enantiomers differ from each other. This property is the direction in which they rotate plane-polarized light, and this is called optical activity or optical rotation. Optical rotation can be interpreted as the outcome of interaction between an enantiomeric compound and polarized light. Thus, enantiomer 3, which rotates plane-polarized light in a clockwise direction, is described as (+)-lactic acid, while enantiomer 2, which has an equal and opposite rotation under the same conditions, is described as (—)-lactic acid. 

One of the terms for describing enantiomer composition is optical purity. It refers to the ratio of observed specific rotation to the maximum or absolute specific rotation of a pure enantiomer sample. For any compound for which the optical rotation of its pure enantiomer is known, the ee value may be determined directly from the observed optical rotation. 

Optical purity The optical purity of a sample is expressed as the magnitudes of its optical rotation as a percentage of that of its pure enantiomer (which has maximum rotation). 

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