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Enantiomer

January 10, 2024

This article is about the concept in chemistry. For a discussion of enantiomers in mathematics, see Chirality (mathematics).

In chemistry, an enantiomer (/ɪˈnænti.əmər, ɛ-, -oʊ-/[1] ih-NAN-tee-ə-mər; from Ancient Greek ἐνάντιος (enántios) 'opposite', and μέρος (méros) 'part') – also called optical isomer,[2] antipode,[3] or optical antipode[4] – is one of two stereoisomers that are non-superposable onto their own mirror image. Enantiomers are much like one's right and left hands; without mirroring one of them, hands cannot be superposed onto each other.[5] No amount of reorientation in three spatial dimensions will allow the four unique groups on the chiral carbon (see chirality) to line up exactly. The number of stereoisomers a molecule has can be determined by the number of chiral carbons it has. Stereoisomers include both enantiomers and diastereomers.

(S)-(+)-lactic acid (left) and (R)-(–)-lactic acid (right) are nonsuperposable mirror images of each other.

Diastereomers, like enantiomers, share the same molecular formula and are non-superposable onto each other; however, they are not mirror images of each other.[6]

A molecule with chirality rotates plane-polarized light.[7] A mixture of equal amounts of each enantiomer, a racemic mixture or a racemate, does not rotate light.[8][9] [10]

Naming conventions edit

Main article: Absolute configuration

There are three common naming conventions for specifying one of the two enantiomers (the absolute configuration) of a given chiral molecule: the R/S system is based on the geometry of the molecule; the (+)- and (−)- system (also written using the obsolete equivalents d- and l-) is based on its optical rotation properties; and the D/L system is based on the molecule's relationship to enantiomers of glyceraldehyde.

The R/S system is based on the molecule's geometry with respect to a chiral center.[11] The R/S system is assigned to a molecule based on the priority rules assigned by Cahn–Ingold–Prelog priority rules, in which the group or atom with the largest atomic number is assigned the highest priority and the group or atom with the smallest atomic number is assigned the lowest priority.

The (+)- and (−)- is used to specify a molecule's optical rotation — the direction that the molecule rotates in polarized light.[12] When a molecule is denoted dextrorotatory it is rotating the plane of polarized light clockwise and can also be denoted as (+).[11] When it is denoted as levorotatory it is rotating the plane of polarized light counterclockwise and can also be denoted as (−).[11]

The Latin words for left are laevus and sinister, and the word for right is dexter (or rectus in the sense of correct or virtuous). The English word right is a cognate of rectus. This is the origin of the D/L and R/S notations, and the employment of prefixes levo- and dextro- in common names.

The prefix ar-, from the Latin recto (right), is applied to the right-handed version; es-, from the Latin sinister (left), to the left-handed molecule.[citation needed] Example: ketamine, arketamine, esketamine.

Chirality centers edit

 
Fischer projection of meso-tartaric acid

The asymmetric atom is called a chirality center,[13][14] a type of stereocenter. A chirality center is also called a chiral center[15][16][17] or an asymmetric center.[18] Some sources use the terms stereocenter, stereogenic center, stereogenic atom or stereogen to refer exclusively to a chirality center,[15][17][19] while others use the terms more broadly to refer also to centers that result in diastereomers (stereoisomers that are not enantiomers).[14][20][21]

Compounds that contain exactly one (or any odd number) of asymmetric atoms are always chiral. However, compounds that contain an even number of asymmetric atoms sometimes lack chirality because they are arranged in mirror-symmetric pairs, and are known as meso compounds. For instance, meso tartaric acid (shown on the right) has two asymmetric carbon atoms, but it does not exhibit enantiomerism because there is a mirror symmetry plane. Conversely, there exist forms of chirality that do not require asymmetric atoms, such as axial, planar, and helical chirality.[15]: pg. 3 

Even though a chiral molecule lacks reflection (Cs) and rotoreflection symmetries (S2n), it can have other molecular symmetries, and its symmetry is described by one of the chiral point groups: Cn, Dn, T, O, or I. For example, hydrogen peroxide is chiral and has C2 (two-fold rotational) symmetry. A common chiral case is the point group C1, meaning no symmetries, which is the case for lactic acid.

Examples edit

 
Structures of the two enantiomeric forms (S left, R right) of mecoprop
 
Enantiomers of citalopram. The top is (R)-citalopram and the bottom is (S)-citalopram.

An example of such an enantiomer is the sedative thalidomide, which was sold in a number of countries around the world from 1957 until 1961. It was withdrawn from the market when it was found to cause birth defects. One enantiomer caused the desirable sedative effects, while the other, unavoidably[22] present in equal quantities, caused birth defects.[23]

The herbicide mecoprop is a racemic mixture, with the (R)-(+)-enantiomer ("Mecoprop-P", "Duplosan KV") possessing the herbicidal activity.[24]

Another example is the antidepressant drugs escitalopram and citalopram. Citalopram is a racemate [1:1 mixture of (S)-citalopram and (R)-citalopram]; escitalopram [(S)-citalopram] is a pure enantiomer. The dosages for escitalopram are typically 1/2 of those for citalopram. Here, (S)-citalopram is called a chiral switch of Citalopram.

Chiral drugs edit

Main articles: Chiral drugs and Enantiopure drug

Enantiopure compounds consist of only one of the two enantiomers. Enantiopurity is of practical importance since such compositions have improved therapeutic efficacy.[25] The switch from a racemic drug to an enantiopure drug is called a chiral switch. In many cases, the enantiomers have distinct effects. One case is that of Propoxyphene. The enantiomeric pair of propoxyphene is separately sold by Eli Lilly and company. One of the partner is dextropropoxyphene, an analgesic agent (Darvon) and the other is called levopropoxyphene, an effective antitussive (Novrad).[26][27]  It is interesting to note that the trade names of the drugs, DARVON and NOVRAD, also reflect the chemical mirror-image relationship. In other cases, there may be no clinical benefit to the patient. In some jurisdictions, single-enantiomer drugs are separately patentable from the racemic mixture.[28] It is possible that only one of the enantiomers is active. Or, it may be that both are active, in which case separating the mixture has no objective benefits, but extends the drug's patentability.[29]

Enantioselective preparations edit

See also: chiral resolution and asymmetric synthesis

In the absence of an effective enantiomeric environment (precursor, chiral catalyst, or kinetic resolution), separation of a racemic mixture into its enantiomeric components is impossible, although certain racemic mixtures spontaneously crystallize in the form of a racemic conglomerate, in which crystals of the enantiomers are physically segregated and may be separated mechanically. However, most racemates form crystals containing both enantiomers in a 1:1 ratio.

In his pioneering work, Louis Pasteur was able to isolate the isomers of sodium ammonium tartrate because the individual enantiomers crystallize separately from solution. To be sure, equal amounts of the enantiomorphic crystals are produced, but the two kinds of crystals can be separated with tweezers. This behavior is unusual. A less common method is by enantiomer self-disproportionation.

The second strategy is asymmetric synthesis: the use of various techniques to prepare the desired compound in high enantiomeric excess. Techniques encompassed include the use of chiral starting materials (chiral pool synthesis), the use of chiral auxiliaries and chiral catalysts, and the application of asymmetric induction. The use of enzymes (biocatalysis) may also produce the desired compound.

A third strategy is Enantioconvergent synthesis, the synthesis of one enantiomer from a racemic precursor, utilizing both enantiomers. By making use of a chiral catalyist, both enantiomers of the reactant result in a single enantiomer of product.[30]

Enantiomers may not be isolable if there is an accessible pathway for racemization (interconversion between enantiomorphs to yield a racemic mixture) at a given temperature and timescale. For example, amines with three distinct substituents are chiral, but with few exceptions (e.g. substituted N-chloroaziridines), they rapidly undergo "umbrella inversion" at room temperature, leading to racemization. If the racemization is fast enough, the molecule can often be treated as an achiral, averaged structure.

Parity violation edit

For all intents and purposes, each enantiomer in a pair has the same energy. However, theoretical physics predicts that due to parity violation of the weak nuclear force (the only force in nature that can "tell left from right"), there is actually a minute difference in energy between enantiomers (on the order of 10−12 eV or 10−10 kJ/mol or less) due to the weak neutral current mechanism. This difference in energy is far smaller than energy changes caused by even small changes in molecular conformation, and far too small to measure by current technology, and is therefore chemically inconsequential.[16][31][32] In the sense used by particle physicists, the "true" enantiomer of a molecule, which has exactly the same mass-energy content as the original molecule, is a mirror-image that is also built from antimatter (antiprotons, antineutrons, and positrons).[16] Throughout this article, "enantiomer" is used only in the chemical sense of compounds of ordinary matter that are not superposable on their mirror image.

Quasi-enantiomers edit

Quasi-enantiomers are molecular species that are not strictly enantiomers, but behave as if they are. In quasi-enantiomers majority of the molecule is reflected; however, an atom or group within the molecule is changed to a similar atom or group.[33] Quasi-enantiomers can also be defined as molecules that have the potential to become enantiomers if an atom or group in the molecule is replaced.[34] An example of quasi-enantiomers would (S)-bromobutane and (R)-iodobutane. Under normal conditions the enantiomers for (S)-bromobutane and (R)-iodobutane would (R)-bromobutane and (S)-iodobutane respectively. Quasi-enantiomers would also produce quasi-racemates, which are similar to normal racemates (see Racemic mixture) in that they form an equal mixture of quasi-enantiomers.[33]

Though not considered actual enantiomers, the naming convention for quasi-enantiomers also follows the same trend as enantiomers when looking at (R) and (S) configurations - which are considered from a geometrical basis (see Cahn–Ingold–Prelog priority rules).

Quasi-enantiomers have applications in parallel kinetic resolution.[35]

See also edit

References edit

  1. ^ "Compare Synonyms: See How The Synonyms Differ". Thesaurus.com. Retrieved 2022-11-17.
  2. ^ Chemistry (IUPAC), The International Union of Pure and Applied. "IUPAC - optical isomers (O04308)". goldbook.iupac.org. doi:10.1351/goldbook.O04308. Retrieved 2022-11-17.
  3. ^ Chemistry (IUPAC), The International Union of Pure and Applied. "IUPAC - antipodes (A00403)". goldbook.iupac.org. doi:10.1351/goldbook.A00403. Retrieved 2022-11-17.
  4. ^ Chemistry (IUPAC), The International Union of Pure and Applied. "IUPAC - optical antipodes (O04304)". goldbook.iupac.org. doi:10.1351/goldbook.O04304. Retrieved 2022-11-17.
  5. ^ McConathy, Jonathan; Owens, Michael J. (2003). "Stereochemistry in Drug Action". Primary Care Companion to the Journal of Clinical Psychiatry. 5 (2): 70–73. doi:10.4088/pcc.v05n0202. ISSN 1523-5998. PMC 353039. PMID 15156233.
  6. ^ Smith, Michael B.; March, Jerry (2007), Advanced Organic Chemistry: Reactions, Mechanisms, and Structure (6th ed.), New York: Wiley-Interscience, ISBN 978-0-471-72091-1
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  8. ^ Chemistry (IUPAC), The International Union of Pure and Applied. "IUPAC - racemic (R05026)". goldbook.iupac.org. doi:10.1351/goldbook.R05026. Retrieved 2022-11-17.
  9. ^ Chemistry (IUPAC), The International Union of Pure and Applied. "IUPAC - racemate (R05025)". goldbook.iupac.org. doi:10.1351/goldbook.R05025. Retrieved 2022-11-17.
  10. ^ Weber, Erin. "Library Guides: CHEM 221: Stereochemistry / Isomerism". libraryguides.salisbury.edu. Retrieved 2022-11-17.
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  12. ^ Caldwell, John; Wainer, Irving W. (December 2001). "Stereochemistry: definitions and a note on nomenclature". Human Psychopharmacology: Clinical and Experimental. 16 (S2): S105–S107. doi:10.1002/hup.334. ISSN 0885-6222. PMID 12404716. S2CID 12367578.
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  17. ^ a b Clayden, Jonathan; Greeves, Nick; Warren, Stuart G. (2012). Organic chemistry. Oxford: Oxford University Press. ISBN 978-0-19-927029-3. OCLC 761379371.
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  33. ^ a b Zhang, Qisheng; Rivkin, Alexey; Curran, Dennis P. (2002-05-01). "Quasiracemic Synthesis: Concepts and Implementation with a Fluorous Tagging Strategy to Make Both Enantiomers of Pyridovericin and Mappicine". Journal of the American Chemical Society. 124 (20): 5774–5781. doi:10.1021/ja025606x. ISSN 0002-7863. PMID 12010052.
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External links edit

  •   Media related to Enantiomers at Wikimedia Commons
  • chemwiki:stereoisomerism

January 10, 2024
enantiomer, this, article, about, concept, chemistry, discussion, enantiomers, mathematics, chirality, mathematics, chemistry, enantiomer, ɪˈnænti, əmər, mər, from, ancient, greek, ἐνάντιος, enántios, opposite, μέρος, méros, part, also, called, optical, isomer. This article is about the concept in chemistry For a discussion of enantiomers in mathematics see Chirality mathematics In chemistry an enantiomer ɪˈnaenti emer ɛ oʊ 1 ih NAN tee e mer from Ancient Greek ἐnantios enantios opposite and meros meros part also called optical isomer 2 antipode 3 or optical antipode 4 is one of two stereoisomers that are non superposable onto their own mirror image Enantiomers are much like one s right and left hands without mirroring one of them hands cannot be superposed onto each other 5 No amount of reorientation in three spatial dimensions will allow the four unique groups on the chiral carbon see chirality to line up exactly The number of stereoisomers a molecule has can be determined by the number of chiral carbons it has Stereoisomers include both enantiomers and diastereomers S lactic acid left and R lactic acid right are nonsuperposable mirror images of each other Diastereomers like enantiomers share the same molecular formula and are non superposable onto each other however they are not mirror images of each other 6 A molecule with chirality rotates plane polarized light 7 A mixture of equal amounts of each enantiomer a racemic mixture or a racemate does not rotate light 8 9 10 Contents 1 Naming conventions 2 Chirality centers 3 Examples 4 Chiral drugs 5 Enantioselective preparations 6 Parity violation 7 Quasi enantiomers 8 See also 9 References 10 External linksNaming conventions editMain article Absolute configuration There are three common naming conventions for specifying one of the two enantiomers the absolute configuration of a given chiral molecule the R S system is based on the geometry of the molecule the and system also written using the obsolete equivalents d and l is based on its optical rotation properties and the D L system is based on the molecule s relationship to enantiomers of glyceraldehyde The R S system is based on the molecule s geometry with respect to a chiral center 11 The R S system is assigned to a molecule based on the priority rules assigned by Cahn Ingold Prelog priority rules in which the group or atom with the largest atomic number is assigned the highest priority and the group or atom with the smallest atomic number is assigned the lowest priority The and is used to specify a molecule s optical rotation the direction that the molecule rotates in polarized light 12 When a molecule is denoted dextrorotatory it is rotating the plane of polarized light clockwise and can also be denoted as 11 When it is denoted as levorotatory it is rotating the plane of polarized light counterclockwise and can also be denoted as 11 The Latin words for left are laevus and sinister and the word for right is dexter or rectus in the sense of correct or virtuous The English word right is a cognate of rectus This is the origin of the D L and R S notations and the employment of prefixes levo and dextro in common names The prefix ar from the Latin recto right is applied to the right handed version es from the Latin sinister left to the left handed molecule citation needed Example ketamine arketamine esketamine Chirality centers edit nbsp Fischer projection of meso tartaric acidThe asymmetric atom is called a chirality center 13 14 a type of stereocenter A chirality center is also called a chiral center 15 16 17 or an asymmetric center 18 Some sources use the terms stereocenter stereogenic center stereogenic atom or stereogen to refer exclusively to a chirality center 15 17 19 while others use the terms more broadly to refer also to centers that result in diastereomers stereoisomers that are not enantiomers 14 20 21 Compounds that contain exactly one or any odd number of asymmetric atoms are always chiral However compounds that contain an even number of asymmetric atoms sometimes lack chirality because they are arranged in mirror symmetric pairs and are known as meso compounds For instance meso tartaric acid shown on the right has two asymmetric carbon atoms but it does not exhibit enantiomerism because there is a mirror symmetry plane Conversely there exist forms of chirality that do not require asymmetric atoms such as axial planar and helical chirality 15 pg 3 Even though a chiral molecule lacks reflection Cs and rotoreflection symmetries S2n it can have other molecular symmetries and its symmetry is described by one of the chiral point groups Cn Dn T O or I For example hydrogen peroxide is chiral and has C2 two fold rotational symmetry A common chiral case is the point group C1 meaning no symmetries which is the case for lactic acid Examples edit nbsp Structures of the two enantiomeric forms S left R right of mecoprop nbsp Enantiomers of citalopram The top is R citalopram and the bottom is S citalopram An example of such an enantiomer is the sedative thalidomide which was sold in a number of countries around the world from 1957 until 1961 It was withdrawn from the market when it was found to cause birth defects One enantiomer caused the desirable sedative effects while the other unavoidably 22 present in equal quantities caused birth defects 23 The herbicide mecoprop is a racemic mixture with the R enantiomer Mecoprop P Duplosan KV possessing the herbicidal activity 24 Another example is the antidepressant drugs escitalopram and citalopram Citalopram is a racemate 1 1 mixture of S citalopram and R citalopram escitalopram S citalopram is a pure enantiomer The dosages for escitalopram are typically 1 2 of those for citalopram Here S citalopram is called a chiral switch of Citalopram Chiral drugs editMain articles Chiral drugs and Enantiopure drug Enantiopure compounds consist of only one of the two enantiomers Enantiopurity is of practical importance since such compositions have improved therapeutic efficacy 25 The switch from a racemic drug to an enantiopure drug is called a chiral switch In many cases the enantiomers have distinct effects One case is that of Propoxyphene The enantiomeric pair of propoxyphene is separately sold by Eli Lilly and company One of the partner is dextropropoxyphene an analgesic agent Darvon and the other is called levopropoxyphene an effective antitussive Novrad 26 27 It is interesting to note that the trade names of the drugs DARVON and NOVRAD also reflect the chemical mirror image relationship In other cases there may be no clinical benefit to the patient In some jurisdictions single enantiomer drugs are separately patentable from the racemic mixture 28 It is possible that only one of the enantiomers is active Or it may be that both are active in which case separating the mixture has no objective benefits but extends the drug s patentability 29 Enantioselective preparations editSee also chiral resolution and asymmetric synthesis In the absence of an effective enantiomeric environment precursor chiral catalyst or kinetic resolution separation of a racemic mixture into its enantiomeric components is impossible although certain racemic mixtures spontaneously crystallize in the form of a racemic conglomerate in which crystals of the enantiomers are physically segregated and may be separated mechanically However most racemates form crystals containing both enantiomers in a 1 1 ratio In his pioneering work Louis Pasteur was able to isolate the isomers of sodium ammonium tartrate because the individual enantiomers crystallize separately from solution To be sure equal amounts of the enantiomorphic crystals are produced but the two kinds of crystals can be separated with tweezers This behavior is unusual A less common method is by enantiomer self disproportionation The second strategy is asymmetric synthesis the use of various techniques to prepare the desired compound in high enantiomeric excess Techniques encompassed include the use of chiral starting materials chiral pool synthesis the use of chiral auxiliaries and chiral catalysts and the application of asymmetric induction The use of enzymes biocatalysis may also produce the desired compound A third strategy is Enantioconvergent synthesis the synthesis of one enantiomer from a racemic precursor utilizing both enantiomers By making use of a chiral catalyist both enantiomers of the reactant result in a single enantiomer of product 30 Enantiomers may not be isolable if there is an accessible pathway for racemization interconversion between enantiomorphs to yield a racemic mixture at a given temperature and timescale For example amines with three distinct substituents are chiral but with few exceptions e g substituted N chloroaziridines they rapidly undergo umbrella inversion at room temperature leading to racemization If the racemization is fast enough the molecule can often be treated as an achiral averaged structure Parity violation editFor all intents and purposes each enantiomer in a pair has the same energy However theoretical physics predicts that due to parity violation of the weak nuclear force the only force in nature that can tell left from right there is actually a minute difference in energy between enantiomers on the order of 10 12 eV or 10 10 kJ mol or less due to the weak neutral current mechanism This difference in energy is far smaller than energy changes caused by even small changes in molecular conformation and far too small to measure by current technology and is therefore chemically inconsequential 16 31 32 In the sense used by particle physicists the true enantiomer of a molecule which has exactly the same mass energy content as the original molecule is a mirror image that is also built from antimatter antiprotons antineutrons and positrons 16 Throughout this article enantiomer is used only in the chemical sense of compounds of ordinary matter that are not superposable on their mirror image Quasi enantiomers editQuasi enantiomers are molecular species that are not strictly enantiomers but behave as if they are In quasi enantiomers majority of the molecule is reflected however an atom or group within the molecule is changed to a similar atom or group 33 Quasi enantiomers can also be defined as molecules that have the potential to become enantiomers if an atom or group in the molecule is replaced 34 An example of quasi enantiomers would S bromobutane and R iodobutane Under normal conditions the enantiomers for S bromobutane and R iodobutane would R bromobutane and S iodobutane respectively Quasi enantiomers would also produce quasi racemates which are similar to normal racemates see Racemic mixture in that they form an equal mixture of quasi enantiomers 33 Though not considered actual enantiomers the naming convention for quasi enantiomers also follows the same trend as enantiomers when looking at R and S configurations which are considered from a geometrical basis see Cahn Ingold Prelog priority rules Quasi enantiomers have applications in parallel kinetic resolution 35 See also editChiral switch Crystal system Enantiopure drug Atropisomer Chirotechnology Chirality physics Diastereomer Dynamic stereochemistry Epimer Homochirality Molecular symmetry Stereochemistry StereocenterReferences edit Compare Synonyms See How The Synonyms Differ Thesaurus com Retrieved 2022 11 17 Chemistry IUPAC The International Union of Pure and Applied IUPAC optical isomers O04308 goldbook iupac org doi 10 1351 goldbook O04308 Retrieved 2022 11 17 Chemistry IUPAC The International Union of Pure and Applied IUPAC antipodes A00403 goldbook iupac org doi 10 1351 goldbook A00403 Retrieved 2022 11 17 Chemistry IUPAC The International Union of Pure and Applied IUPAC optical antipodes O04304 goldbook iupac org doi 10 1351 goldbook O04304 Retrieved 2022 11 17 McConathy Jonathan Owens Michael J 2003 Stereochemistry in Drug Action Primary Care Companion to the Journal of Clinical Psychiatry 5 2 70 73 doi 10 4088 pcc v05n0202 ISSN 1523 5998 PMC 353039 PMID 15156233 Smith Michael B March Jerry 2007 Advanced Organic Chemistry Reactions Mechanisms and Structure 6th ed New York Wiley Interscience ISBN 978 0 471 72091 1 Chirality and Optical Activity chemed chem purdue edu Retrieved 2022 11 17 Chemistry IUPAC The International Union of Pure and Applied IUPAC racemic R05026 goldbook iupac org doi 10 1351 goldbook R05026 Retrieved 2022 11 17 Chemistry IUPAC The International Union of Pure and Applied IUPAC racemate R05025 goldbook iupac org doi 10 1351 goldbook R05025 Retrieved 2022 11 17 Weber Erin Library Guides CHEM 221 Stereochemistry Isomerism libraryguides salisbury edu Retrieved 2022 11 17 a b c Brewster James H December 1986 The distinction of diastereomers in the Cahn Ingold Prelog RS notation The Journal of Organic Chemistry 51 25 4751 4753 doi 10 1021 jo00375a001 ISSN 0022 3263 Caldwell John Wainer Irving W December 2001 Stereochemistry definitions and a note on nomenclature Human Psychopharmacology Clinical and Experimental 16 S2 S105 S107 doi 10 1002 hup 334 ISSN 0885 6222 PMID 12404716 S2CID 12367578 IUPAC Compendium of Chemical Terminology 2nd ed the Gold Book 1997 Online corrected version 2006 chirality centre doi 10 1351 goldbook C01060 a b Wade LeRoy G 2006 Precision in Stereochemical Terminology J Chem Educ 83 12 1793 Bibcode 2006JChEd 83 1793W doi 10 1021 ed083p1793 ISSN 0021 9584 a b c Karras Manfred 2018 Synthesis of Enantiomerically Pure Helical Aromatics Such As NHC Ligands and Their Use in Asymmetric Catalysis PhD Charles University Retrieved 6 August 2021 a b c Eliel Ernest L Wilen Samuel H Mander Lewis N 1994 Stereochemistry of organic compounds New York Wiley ISBN 0471016705 OCLC 27642721 a b Clayden Jonathan Greeves Nick Warren Stuart G 2012 Organic chemistry Oxford Oxford University Press ISBN 978 0 19 927029 3 OCLC 761379371 IUPAC Compendium of Chemical Terminology 2nd ed the Gold Book 1997 Online corrected version 2006 asymmetric centre doi 10 1351 goldbook A00480 Clark Andrew Kitson Russell R A Mistry Nimesh Taylor Paul Taylor Matthew Lloyd Michael Akamune Caroline 2021 Introduction to stereochemistry Cambridge UK ISBN 978 1 78801 315 4 OCLC 1180250839 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link IUPAC Compendium of Chemical Terminology 2nd ed the Gold Book 1997 Online corrected version 2006 stereogenic unit stereogen stereoelement doi 10 1351 goldbook S05980 Mislow Kurt Siegel Jay 1984 Stereoisomerism and local chirality J Am Chem Soc 106 11 3319 3328 doi 10 1021 ja00323a043 ISSN 0002 7863 Knoche B Blaschke G 1994 Investigations on the in vitro racemization of thalidomide by high performance liquid chromatography Journal of Chromatography A 666 1 2 235 240 doi 10 1016 0021 9673 94 80385 4 Voet Donald Voet Judith G Pratt Charlotte W 2006 Fundamentals of Biochemistry p 89 ISBN 0 471 21495 7 G Smith C H L Kennard A H White P G Hodgson April 1980 2 4 Chloro 2 methylphenoxy propionic acid mecoprop Acta Crystallogr B 36 4 992 994 doi 10 1107 S0567740880005134 Ariens Everardus J 1986 Stereochemistry A source of problems in medicinal chemistry Medicinal 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theories and perspectives of this unsolved problem Yus Miguel Cambridge UK Royal Society of Chemistry ISBN 9781847558756 OCLC 319518566 Stickler Benjamin A Diekmann Mira Berger Robert Wang Daqing 2021 09 14 Enantiomer Superpositions from Matter Wave Interference of Chiral Molecules Physical Review X 11 3 031056 arXiv 2102 06124 Bibcode 2021PhRvX 11c1056S doi 10 1103 PhysRevX 11 031056 ISSN 2160 3308 S2CID 231879820 a b Zhang Qisheng Rivkin Alexey Curran Dennis P 2002 05 01 Quasiracemic Synthesis Concepts and Implementation with a Fluorous Tagging Strategy to Make Both Enantiomers of Pyridovericin and Mappicine Journal of the American Chemical Society 124 20 5774 5781 doi 10 1021 ja025606x ISSN 0002 7863 PMID 12010052 Zhang Qisheng Curran Dennis P 2005 08 19 Quasienantiomers and Quasiracemates New Tools for Identification Analysis Separation and Synthesis of Enantiomers Chemistry A European Journal 11 17 4866 4880 doi 10 1002 chem 200500076 ISSN 0947 6539 PMID 15915521 G S Coumbarides M Dingjan J Eames A Flinn J Northen and Y Yohannes Tetrahedron Lett 46 2005 p 2897erExternal links edit nbsp Media related to Enantiomers at Wikimedia Commons chemwiki stereoisomerism Retrieved from https en wikipedia org w index php title Enantiomer amp oldid 1189489326, wikipedia, wiki, book, books, library,

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