Jump to content

Silylation

From Wikipedia, the free encyclopedia

Silylation is the introduction of one or more (usually) substituted silyl groups (R3Si) to a molecule. Silylations are core methods for production of organosilicon chemistry. Silanization, while similar to silylation, usually refers to attachment of silyl groups to solids.[1] Silyl groups are commonly used for: alcohol protection, enolate trapping, gas chromatography, electron-impact mass spectrometry (EI-MS), and coordinating with metal complexes.

Protection Chemistry

[edit]

Protection

[edit]

Silylation is often used to protect alcohols, as well as amines, carboxylic acids, and terminal alkynes. The products after silylation, namely silyl ethers and silyl amines, are resilient toward basic conditions.[2] Protection is typically done by reacting the functional group with a silyl halide by an SN2 reaction mechanism, typically in the presence of base.[3]

The protection mechanism begins with the base deprotonating the alcohol group. Next, the deprotonated alcohol group attacks the silyl atom of the silyl halide compound. The halide acts as a leaving group and ends up in solution. A workup step follows to remove any excess base within the solution. The overall reaction scheme is as follows:

  1. ROH NEt3 → RO H−NEt 3
  2. RO Cl−SiMe3 → RO−SiMe3 Cl
Bis(trimethylsilyl)acetamide, a popular reagent for silylation

Other silylating agents include bis(trimethylsilyl)acetamide (BSA). The reaction of BSA with alcohols gives the corresponding trimethylsilyl ether, together with acetamide as a byproduct (Me = CH3):[4]

2 ROH MeC(OSiMe3)NSiMe3 → MeC(O)NH2 2 ROSiMe3

Deprotection

[edit]

Due to the strength of the Si-F bond, fluoride salts are commonly used as a deprotecting agent of silyl groups.[2] The primary fluorous deprotecting agent is tetra-n-butylammonium fluoride (TBAF), as its aliphatic chains in help incorporate the fluoride ion into organic solvents.[5][6][7]

Deprotection with a fluoride ion occurs by an SN2 mechanism, followed by acidic workup to protonate the resulting alkoxide:

ROSiMe3 NBu4F → RO NBu 4 SiMe3F

Deprotection of the alcohol can also be done using either Brønsted acids or Lewis acid conditions.[8] Brønsted acids, like PyBr3 (pyridinium tribromide), deprotect the alcohol by acting as a proton donor.[8]

Modifying Silyl Reactivity

[edit]
Common types of alkyl silyl protecting groups

Sterically bulkier alkyl substituents tend to decrease the reactivity of the silyl group.[9] Consequently, bulky substituents increase the silyl group's protective abilities. To add bulkier alkyl silyls, more strenuous conditions are required for alcohol protection. As bulkier groups require more strenuous conditions to add, they also require more strenuous conditions to remove. Additionally, bulkier silyl groups are more selective for the type of alcohols they react with, resulting in a preference for primary alcohols over secondary alcohols. Thus, silyl groups such as TBDMS and TIPS can be used to selectively protect primary alcohols over secondary alcohols.[9]  

In acidic conditions, alkyl substituents acting as electron withdrawing groups decrease the reaction rate.[10] As bulker silyl groups are more likely to be electron withdrawing, it is easier to differentiate between less and more bulky silyl groups.[10] Therefore, acidic deprotection occurs fastest for less sterically bulky alkyl silyl groups.[8] In basic conditions, alkyl substituents acting as electron donating groups decrease reaction rate.[10]

Enolate Trapping

[edit]

Silylation can also be used to trap reactive compounds for isolation or identification. A common example of this is by trapping reactive enolates into silyl enol ethers, which represent reactive tautomers of many carbonyl compounds.[11] The original enolate can be reformed upon reaction with an organolithium, or other strong base.[11]

Applications in Analysis

[edit]

The introduction of a silyl group(s) gives derivatives of enhanced volatility, making the derivatives suitable for analysis by gas chromatography and electron-impact mass spectrometry (EI-MS). For EI-MS, the silyl derivatives give more favorable diagnostic fragmentation patterns of use in structure investigations, or characteristic ions of use in trace analyses employing selected ion monitoring and related techniques.[12][13]

Of metals

[edit]
CpFe(CO)2Si(CH3)3, a trimethylsilyl complex.

Coordination complexes with silyl ligands are well known. An early example is CpFe(CO)2Si(CH3)3, prepared by silylation of CpFe(CO)2Na with trimethylsilyl chloride. Typical routes include oxidative addition of Si-H bonds to low-valent metals. Metal silyl complexes are intermediates in hydrosilation, a process used to make organosilicon compounds on both laboratory and commercial scales.[14][15]

See also

[edit]

References

[edit]
  1. ^ Pape, Peter G. (2017). "Silylating Agents". Kirk-Othmer Encyclopedia of Chemical Technology. pp. 1–15. doi:10.1002/0471238961.1909122516011605.a01.pub3. ISBN 9780471238966.
  2. ^ a b Clayden, Jonathan; Greeves, Nick; Warren, Stuart (2012). Organic chemistry (2nd ed.). Oxford: Oxford university press. pp. 549–550. ISBN 978-0-19-927029-3.
  3. ^ Pagliano, Enea; Campanella, Beatrice; D'Ulivo, Alessandro; Mester, Zoltán (September 2018). "Derivatization chemistries for the determination of inorganic anions and structurally related compounds by gas chromatography - A review". Analytica Chimica Acta. 1025: 12–40. doi:10.1016/j.aca.2018.03.043.
  4. ^ Young, Steven D.; Buse, Charles T.; Heathcock, Clayton H. (1985). "2-Methyl-2-(Trimethylsiloxy)pentan-3-one". Organic Syntheses. 63: 79. doi:10.15227/orgsyn.063.0079.
  5. ^ Paquette, Leo A., ed. (1995). Encyclopedia of reagents for organic synthesis. Chichester ; New York: Wiley. ISBN 978-0-471-93623-7.
  6. ^ Mercedes Amat, Sabine Hadida, Swargam Sathyanarayana, and Joan Bosch "Regioselective Synthesis of 3-Substituted Indoles: 3-Ethylindole" Organic Syntheses 1997, volume 74, page 248. doi:10.15227/orgsyn.074.0248
  7. ^ Nina Gommermann and Paul Knochel "N,N-Dibenzyl-n-[1-cyclohexyl-3-(trimethylsilyl)-2-propynyl]-amine from Cyclohexanecarbaldehyde, Trimethylsilylacetylene and Dibenzylamine" Organic Syntheses 2007, vol. 84, page 1. doi:10.15227/orgsyn.084.0001
  8. ^ a b c Crouch, R. David (2013-09-02). "Recent Advances in Silyl Protection of Alcohols". Synthetic Communications. 43 (17): 2265–2279. doi:10.1080/00397911.2012.717241. ISSN 0039-7911.
  9. ^ a b Clayden, Jonathan; Greeves, Nick; Warren, Stuart (2012). Organic chemistry (2nd ed.). Oxford: Oxford university press. ISBN 978-0-19-927029-3.
  10. ^ a b c Crouch, R. David (2013-03-18). "Selective deprotection of silyl ethers". Tetrahedron. 69 (11): 2383–2417. doi:10.1016/j.tet.2013.01.017. ISSN 0040-4020.
  11. ^ a b Clayden, Jonathan; Greeves, Nick; Warren, Stuart (2012). Organic chemistry (2nd ed.). Oxford: Oxford university press. pp. 466–467. ISBN 978-0-19-927029-3.
  12. ^ Luis-Alberto Martin; Ingrid Hayenga. "Silylation of Non-Steroidal Anti-Inflammatory Drugs". sigmaaldrich.com. Retrieved 24 September 2023.
  13. ^ Blau, Karl; J. M. Halket (1993). Handbook of Derivatives for Chromatography (2nd ed.). John Wiley & Sons. ISBN 0-471-92699-X.
  14. ^ Moris S. Eisen "Transition-metal silyl complexes" in The Chemistry of Organic Silicon Compounds. Volume 2 Edited by Zvi Rappoport and Yitzhak Apeloig, 1998, John Wiley & Sons
  15. ^ Corey, Joyce Y.; Braddock-Wilking, Janet (1999). "Reactions of Hydrosilanes with Transition-Metal Complexes: Formation of Stable Transition-Metal Silyl Compounds". Chemical Reviews. 99 (1): 175–292. doi:10.1021/CR9701086. PMID 11848982.
[edit]