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Crabtree's catalyst

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Crabtree's catalyst
Crabtree's catalyst
Names
IUPAC name
(SP-4)-(η22-Cycloocta-1,5-diene)(pyridine)(tricyclohexylphosphane)iridium(1+) hexafluoridophosphate(1−)
Identifiers
3D model (JSmol)
ChemSpider
ECHA InfoCard 100.164.161 Edit this at Wikidata
UNII
  • InChI=1S/C18H33P.C8H12.C5H5N.F6P.Ir/c1-4-10-16(11-5-1)19(17-12-6-2-7-13-17)18-14-8-3-9-15-18;1-2-4-6-8-7-5-3-1;1-2-4-6-5-3-1;1-7(2,3,4,5)6;/h16-18H,1-15H2;1-2,7-8H,3-6H2;1-5H;;/q;;;-1;+1/b;2-1-,8-7-;;; ☒N
    Key: UJXHUUQZACSUOG-KJWGIZLLSA-N ☒N
  • InChI=1/C18H33P.C8H12.C5H5N.F6P.Ir/c1-4-10-16(11-5-1)19(17-12-6-2-7-13-17)18-14-8-3-9-15-18;1-2-4-6-8-7-5-3-1;1-2-4-6-5-3-1;1-7(2,3,4,5)6;/h16-18H,1-15H2;1-2,7-8H,3-6H2;1-5H;;/q;;;-1;+1/b;2-1-,8-7-;;;
    Key: UJXHUUQZACSUOG-KJWGIZLLBW
  • c1ccncc1.C1CCC(CC1)P(C2CCCCC2)C3CCCCC3.C1/C=C\CC/C=C\C1.F[P-](F)(F)(F)(F)F.[Ir+]
Properties
C31H50F6IrNP2
Molar mass 804.9026 g/mol
Appearance Yellow microcrystals
Melting point 150 °C (302 °F; 423 K) (decomposes)[1]
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
☒N verify (what is checkY☒N ?)

Crabtree's catalyst is an organoiridium compound with the formula [C8H12IrP(C6H11)3C5H5N]PF6. It is a homogeneous catalyst for hydrogenation and hydrogen-transfer reactions, developed by Robert H. Crabtree. This air stable orange solid is commercially available and known for its directed hydrogenation to give trans stereoselectivity with respective of directing group.[2][3]

Structure and synthesis

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The complex has a square planar molecular geometry, as expected for a d8 complex. It is prepared from cyclooctadiene iridium chloride dimer.[4]

Reactivity

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Crabtree’s catalyst is effective for the hydrogenations of mono-, di-, tri-, and tetra-substituted substrates. Whereas Wilkinson’s catalyst and the Schrock–Osborn catalyst do not catalyze the hydrogenation of a tetrasubstituted olefin, Crabtree’s catalyst does so to at high turnover frequencies (table).[2][5]

Turnover frequencies
Substrate Wilkinson's catalyst Schrock–Osborn catalyst Crabtree's catalyst
Hex-1-ene 650 4000 6400
Cyclohexene 700 10 4500
1-Methylcyclohexene 13 3800
2,3-Dimethyl-but-2-ene 4000

The catalyst is reactive at room temperature.[1] The reaction is robust without drying solvents or meticulous deoxygenation of the hydrogen. The catalyst is tolerant of weakly basic functional groups such as ester, but not alcohols (see below) or amines.[2] The catalyst is sensitive to proton-bearing impurities.[6]

The catalyst becomes irreversibly deactivated after about ten minutes at room temperature, signaled by appearance of yellow color. One deactivation process involves formation of hydride-bridged dimers.[7] As a consequence, Crabtree's Catalyst is usually used in very low catalyst loading.

Crabtree's catalyst is thought to operate via an intermediate such as this: cis-[IrH2(cod)L2] (cationic charge not shown).

Other catalytic functions: isotope exchange and isomerization

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Besides hydrogenation, the catalyst catalyzes the isomerization and hydroboration of alkenes.[1]

An example of isomerization with Crabtree's catalyst. The reaction proceeds 98% to completion in 30 minutes at room temperature.

Crabtree's catalyst is used in isotope exchange reactions. More specifically, it catalyzes the direct exchange of a hydrogen atom with its isotopes deuterium and tritium, without the use of an intermediate.[8] It has been shown that isotope exchange with Crabtree’s catalyst is highly regioselective.[9][10]

Influence of directing functional groups

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The hydrogenation of a terpen-4-ol demonstrates the ability of compounds with directing groups (the –OH group) to undergo diastereoselective hydrogenation. With palladium on carbon in ethanol the product distribution is 20:80 favoring the cis isomer (2B in Scheme 1). The polar side (with the hydroxyl group) interacts with the solvent. This is due to slight haptophilicity, an effect in which a functional group binds to the surface of a heterogeneous catalyst and directs the reaction.[11][12] In cyclohexane as solvent, the distribution changes to 53:47 because haptophilicity is no long present (there is no directing group on cyclohexane). The distribution changes completely in favor of the trans isomer 2A when Crabtree's catalyst is used in dichloromethane. This selectivity is both predictable and practically useful.[13] Carbonyl groups are also known to direct the hydrogenation by the Crabtree catalyst to be highly regioselective.[14][15][16]

Crabtree catalyst in hydrogenation

The directing effect that causes the stereoselectivity of hydrogenation of terpen-4-ol with Crabtree’s catalyst is shown below.

Directing effect of an –OH group on diastereoselectivity of hydrogenation by Crabtree's catalyst. Hydrogen is added from the direction of the iridium atom, selecting for the reactivity shown above. Additional ligands on catalyst not shown.

History

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Crabtree and graduate student George Morris discovered this catalyst in the 1970s while working on iridium analogues of Wilkinson's rhodium-based catalyst at the Institut de Chimie des Substances Naturelles at Gif-sur-Yvette, near Paris.

Previous hydrogenation catalysts included Wilkinson’s catalyst and a cationic rhodium(I) complex with two phosphine groups developed by Osborn and Schrock.[17] These catalysts accomplished hydrogenation through displacement; after hydrogen addition across the metal, a solvent or a phosphine group dissociated from the rhodium metal so the olefin to be hydrogenated could gain access to the active site.[2] This displacement occurs quickly for rhodium complexes but occurs barely at all for iridium complexes.[18] Because of this, research at the time focused on rhodium compounds instead of compounds involving transition metals of the third row, like iridium. Wilkinson, Osborn, and Schrock also only used coordinating solvents.[19]

Crabtree noted that the ligand dissociation step does not occur in heterogeneous catalysis, and so posited that this step was limiting in homogeneous systems.[2] They sought catalysts with "irreversibly created active sites in a noncoordinating solvent." This led to the development of the Crabtree catalyst, and use of the solvent CH2Cl2.

References

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  1. ^ a b c Crabtree, R. H. (2001). "(1,5-Cyclooctadiene)(tricyclohexylphosphine)(pyridine)iridium(I) Hexafluorophosphate". e-EROS Encyclopedia of Reagents for Organic Synthesis. doi:10.1002/047084289X.rc290m.pub4 (inactive 1 November 2024).{{cite encyclopedia}}: CS1 maint: DOI inactive as of November 2024 (link)
  2. ^ a b c d e Robert H. Crabtree (1979). "Iridium compounds in catalysis". Acc. Chem. Res. 12 (9): 331–337. doi:10.1021/ar50141a005.
  3. ^ Brown, J. M. (1987). "Directed Homogeneous Hydrogenation". Angew. Chem. Int. Ed. 26 (3): 190–203. doi:10.1002/anie.198701901.
  4. ^ Crabtree, R. H.; Morris, G. E. (1977). "Some diolefin complexes of Iridium(I) and a trans-Influence Series for the Complexes [IrCl(cod)L]". J. Organomet. Chem. 135 (3): 395–403. doi:10.1016/S0022-328X(00)88091-2.
  5. ^ White, M. (2002-10-15). "Hydrogenation" (PDF). Retrieved 2014-12-01.
  6. ^ Xu, Yingjian; Mingos, D. Michael P.; Brown, John M. (2008). "Crabtree's catalyst revisited; Ligand effects on stability and durability". Chem. Comm. 2008 (2): 199–201. doi:10.1039/b711979h. PMID 18092086.
  7. ^ Crabtree, R.; Felkin, H.; Morris, G. (1977). "Cationic iridium diolefin complexes as alkene hydrogenation catalysts and the isolation of some related hydrido complexes". Journal of Organometallic Chemistry. 141 (2): 205–215. doi:10.1016/S0022-328X(00)92273-3.
  8. ^ Schou, S. (2009). "The effect of adding Crabtree's catalyst to rhodium black in direct hydrogen isotope exchange reactions". Journal of Labelled Compounds and Radiopharmaceuticals. 52 (9): 376–381. doi:10.1002/jlcr.1612.
  9. ^ Valsborg, J.; Sorensen, L.; Foged, C. (2001). "Organoiridium catalysed hydrogen isotope exchange of benzamide derivatives". Journal of Labelled Compounds and Radiopharmaceuticals. 44 (3): 209–214. doi:10.1002/jlcr.446.
  10. ^ Hesk, D.; Das, P.; Evans, B. (1995). "Deuteration of acetanilides and other substituted aromatics using [Ir(COD)(Cy3P)(Py)]PF6 as catalyst". Journal of Labelled Compounds and Radiopharmaceuticals. 36 (5): 497–502. doi:10.1002/jlcr.2580360514.
  11. ^ Thompson, H.; Naipawer, R. (1973). "Stereochemical control of reductions. III. Approach to group haptophilicities". Journal of the American Chemical Society. 95 (19): 6379–6386. doi:10.1021/ja00800a036.
  12. ^ Rowlands, G. (2002-01-01). "Hydrogenation" (PDF). Archived from the original (PDF) on 2015-01-02. Retrieved 2014-12-01.
  13. ^ Brown, J. (1987). "Directed Homogeneous Hydrogenation [New Synthetic Methods (65)]". Angew. Chem. Int. Ed. Engl. 26 (3): 190–203. doi:10.1002/anie.198701901.
  14. ^ Schultz, A.; McCloskey, P. (1985). "Carboxamide and carbalkoxy group directed stereoselective iridium-catalyzed homogeneous olefin hydrogenations". Journal of Organic Chemistry. 50 (26): 5905–5907. doi:10.1021/jo00350a105.
  15. ^ Crabtree, R. H.; Davis, M. W. (1986). "Directing effects in homogeneous hydrogenation with [Ir(cod)(PCy3)(py)]PF6". J. Org. Chem. 51 (14): 2655–2661. doi:10.1021/jo00364a007.
  16. ^ Crabtree, R.; Davis, M. (1983). "Occurrence and origin of a pronounced directing effect of a hydroxyl group in hydrogenation with [Ir(cod)P(C6H11)3(py)]PF6". Organometallics. 2 (5): 681–682. doi:10.1021/om00077a019.
  17. ^ Schrock, R.; Osborn, J. A. (1976). "Catalytic hydrogenation using cationic rhodium complexes. I. Evolution of the catalytic system and the hydrogenation of olefins". Journal of the American Chemical Society. 98 (8): 2134–2143. doi:10.1021/ja00424a020.
  18. ^ Osborn, J.; Shapley, J. (1970). "Rapid intramolecular rearrangements in pentacoordinate transition metal compounds. Rearrangement mechanism of some fluxional iridium(I) complexes". Journal of the American Chemical Society. 92 (23): 6976–6978. doi:10.1021/ja00726a047.
  19. ^ Young, J.; Wilkinson, G. (1966). "The preparation and properties of tris(triphenylphosphine)halogenorhodium(I) and some reactions thereof including catalytic homogeneous hydrogenation of olefins and acetylenes and their derivatives". J. Chem. Soc. A. 1966: 1711. doi:10.1039/J19660001711.