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Chapter 24: Problem 1

Show how you might prepare each compound by a Heck reaction using methyl 2-propenoate as the starting alkene.

Short Answer

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Question: Describe the synthesis of compounds via a Heck reaction using methyl 2-propenoate as the starting alkene. Include the identification of appropriate halide partners, general reaction conditions, and the step-by-step mechanism.

Step by step solution

01

Identify the alkene and halide partner

For a successful Heck reaction, it is essential to identify the correct alkene, in this case, methyl 2-propenoate, and an appropriate halide partner, typically an aryl or vinyl halide. Write down the structure of methyl 2-propenoate, and identify potential halide partners to be used in the reaction.
02

Write down the reaction conditions

The reaction conditions for a Heck reaction typically include the presence of a heat-stable base and a palladium catalyst, often with a phosphine ligand, and usually performed under an inert atmosphere in a suitable solvent. Write down the general reaction conditions with specific catalyst and base examples for the Heck reaction using methyl 2-propenoate.
03

Mechanism of Heck Reaction

The mechanism of the Heck reaction is a series of steps, including oxidative addition, migratory insertion, and reductive elimination. Write down the detailed step-by-step mechanism for the reaction of methyl 2-propenoate and a chosen aryl or vinyl halide using a palladium catalyst and a base.
04

Design synthesis for prepared compounds

After understanding the Heck reaction mechanism, design the synthesis for each compound using methyl 2-propenoate as the starting material. Select appropriate aryl or vinyl halide partners and follow the guidelines from the previous steps to set up the reaction conditions, predict the product, and give a step-by-step written description of the synthesis process.

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Most popular questions from this chapter

Predict the product of each alkene metathesis reaction using a Ru-nucleophilic carbene catalyst.

Vancomycin is an important antibiotic. It is isolated from the bacterium Streptomyces orientalis and functions by inhibiting bacterial mucopeptide synthesis. It is a last line of defense against the resistant Staph organisms that are now common in hospitals. In 1999, Professor Dale Boger (The Scripps Research Institute) reported a synthesis of vancomycin aglycon (aglycon = lacking a sugar) involving the following steps, among others. Compound (I) was prepared from simple starting materials by a series of steps involving forming amide bonds. (a) Suggest reasonable precursors and show how the bonds could be formed (the actual reagents used have not been introduced, but they work in a similar way to those you know). (b) Give reagents for this reaction and suggest the mechanism. One of the interesting features of this synthesis is that ring \(C\) in compound (II) (and subsequent compounds in this synthesis) has extremely hindered rotation. As a result, compound (II) exists as two atropisomers (Section 3.2) that are interconverted only at \(140^{\circ} \mathrm{C}\). (c) Show these two isomers. (II) was then converted to (III). (d) Suggest reagents to accomplish this transformation. Compound (III) was then converted to (IV). (e) Suggest reagents and the ring A fragment that could be used for this reaction. Closure of an amide link between the amine on ring A (after removal of the protecting group) and the carbomethoxy group above it led to a precursor of vancomycin. (f) Show the ring closure reaction of the deprotected free amino group and its mechanism. Another interesting feature of this synthesis is that rings \(A\) and \(B\) also form atropisomers. These can be converted into a \(3: 1\) mixture of the desired and undesired atropisomers on heating at \(120^{\circ} \mathrm{C}\). (g) Draw these atropisomers and show that only one can be converted to vancomycin. The synthesis of the aglycon was completed by functional manipulation and addition of ring \(\mathrm{E}\) by chemistry similar to that detailed earlier. Yet, another set of atropisomers (this time of ring E) was formed! However, this one was more easily equilibrated than the others; model studies had shown that the activation barrier for this set of atropisomers should be lower than that of the others.

When the \(\mathrm{Pd}(0)\)-catalyzed reactions covered in this chapter are run with a slight pressure of carbon monoxide, a ketone is often created as the product. For example, the following Stille coupling conditions with added \(\mathrm{CO}\) give the product shown. Write a mechanism for how this reaction could occur using the organometallic mechanistic steps introduced in this chapter, along with new steps that would be required in this transformation. Hint: CO can coordinate to \(\mathrm{Pd}\) and insert into \(\mathrm{Pd}-\mathrm{C}\) bonds.

Many of the cross-coupling reactions described in this chapter have been used to make fascinating polymeric materials, as covered in Chapter 29. Give the proper reactants to create the following polymers and name the coupling reaction involved.

Another useful aspect of \(\mathrm{Pd}(0)\)-catalyzed allylic alkylation is the ability to take reactants that are meso and desymmetrize them in the resulting products through the addition of a chiral ligand for the Pd metal. Draw the two \(\eta^{3}\)-allylic complexes formed in this reaction of the following reactant with \(\mathrm{PdL}_{4}\). Describe why chirality in a ligand \(\mathrm{L}\) would influence the preference for one of these complexes over the other.
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