Logout Open In App
Open In App
Warning: foreach() argument must be of type array|object, bool given in /var/www/html/web/app/themes/studypress-core-theme/template-parts/header/mobile-offcanvas.php on line 20

Chapter 24: Problem 31

Suggest a route for the synthesis of each of the following compounds from the indicated starting material: a. 2 -methylpropanenitrile from 2 -methylpropanal b. \(\left(\mathrm{CH}_{3} \mathrm{CO}_{2} \mathrm{CH}_{2}\right)_{3} \mathrm{C}-\mathrm{NO}_{2}\) from nitromethane c. N-tert-butylbenzenecarboxamide from benzenecarbonitrile (benzeonitrile)

Short Answer

Expert verified
1. Convert aldehyde to nitrile using NaCN. 2. Alkylate nitromethane with methyl chloroacetate. 3. Add tert-butylamine to benzenecarbonitrile with a reducing agent.

Step by step solution

01

Oxidation to Nitrile

For synthesizing 2-methylpropanenitrile from 2-methylpropanal, the aldehyde group in 2-methylpropanal needs to be converted to a nitrile. This can be achieved through the use of an oxidizing agent like PCC (Pyridinium chlorochromate) followed by PCl5 to convert the aldehyde to a corresponding alkyl chloride, and subsequently using a cyanide source like NaCN to perform a nucleophilic substitution to form the nitrile group.
02

Michael Addition

To synthesize \((\text{CH}_3\text{CO}_2\text{CH}_2)_3\text{C}-\text{NO}_2\) from nitromethane, perform a Michael addition reaction. Initially, deprotonate nitromethane to form its anionic form, then perform an alkylation with methyl chloroacetate to introduce one ester group. Repeat the alkylation process two more times to form the desired product, making use of base-catalyzed deprotonation and substitution reactions to attach all three ester groups.
03

Amide Formation

Starting with benzenenitrile, add tert-butylamine to the nitrile in the presence of a reducing agent like lithium aluminum hydride (LiAlH4) or a metal catalyst with hydrogen gas to form N-tert-butylbenzenecarboxamide. This reaction involves the conversion of the nitrile group to an amide through nucleophilic addition of the amine and subsequent reduction.

Unlock Step-by-Step Solutions & Ace Your Exams!

  • Full Textbook Solutions

    Get detailed explanations and key concepts

  • Unlimited Al creation

    Al flashcards, explanations, exams and more...

  • Ads-free access

    To over 500 millions flashcards

  • Money-back guarantee

    We refund you if you fail your exam.

Start your free trial

Over 30 million students worldwide already upgrade their learning with Vaia!

Key Concepts

These are the key concepts you need to understand to accurately answer the question.

Nitrile Synthesis
Nitrile synthesis involves transforming an aldehyde into a nitrile group, which introduces a carbon-nitrogen triple bond. This process is particularly useful in organic synthesis for creating molecules with applications in pharmaceuticals and agricultural chemicals. Let's take a deeper look into this technique.
To synthesize 2-methylpropanenitrile from 2-methylpropanal, the first step involves using Pyridinium chlorochromate (PCC) as an oxidizing agent. PCC transforms 2-methylpropanal into an acyl chloride, aided by PCl5. Adding PCl5 is crucial as it helps in further facilitating the conversion of the acyl chloride.
An essential part of this synthesis involves performing a nucleophilic substitution reaction with a cyanide source, such as sodium cyanide (NaCN). During this step, the chloride ion is replaced by the nucleophilic cyanide ion, successfully forming the nitrile group.
  • PCC as an oxidizing agent can selectively oxidize alcohols and aldehydes without affecting other functional groups.
  • PCl5 is used to activate the aldehyde carbon, converting it to a more reactive intermediate.
  • Using NaCN allows for the introduction of the nitrile group via nucleophilic substitution.
This synthesis route is useful for creating carbon-nitrogen bonds, greatly expanding the diversity of organic compounds.
Michael Addition
The Michael Addition is a pivotal reaction in organic chemistry, employed to form carbon-carbon bonds. It is especially popular within the synthesis of complex molecules because it allows for the construction of intricate carbon skeletons.
In the task of synthesizing \((\text{CH}_3\text{CO}_2\text{CH}_2)_3\text{C}-\text{NO}_2\) from nitromethane, the first objective is the deprotonation of nitromethane. This generates an anion that is more nucleophilic, setting the stage for subsequent reactions.
Next is an alkylation step, attaching a methyl chloroacetate molecule to the nitromethane ion. This process is repeated a total of three times to attach all needed ester groups, eventually achieving the target molecule. The use of base-catalyzed deprotonation aids each step of alkylation by generating a more reactive nucleophile.
  • Deprotonation uses bases to generate anions from acidic hydrogens.
  • Alkylation introduces ester groups, increasing the molecular complexity.
  • Utilizing a base ensures offensive power of anions for efficient alkylation.
This strategy showcases a powerful means of functional group substitution and linkage, vital for organic synthesis development.
Amide Formation
Amide formation is an important transformation in organic chemistry, converting a nitrile group into an amide. This conversion is achieved by adding an amine to a nitrile in the presence of a reducing agent, which facilitates the reduction.
To synthesize N-tert-butylbenzenecarboxamide from benzenecarbonitrile, the conversion starts by reacting the nitrile with tert-butylamine. Common reducing agents like lithium aluminum hydride (LiAlH4) or using a metal catalyst with hydrogen gas are implemented in this reaction.
In this specific reaction, the nitrile acts as an electrophile, while the tert-butylamine serves as a nucleophile. The nucleophilic addition of tert-butylamine to the nitrile group results in an intermediate imine, which rapidly reduces to the desired amide under the influence of a reducing agent.
  • Nitriles are versatile electrophiles capable of forming strong carbon-nitrogen bonds.
  • Tert-butylamine's nucleophilic nature drives the electrophilic attack on nitriles.
  • Reduction stabilizes and converts the intermediate to yield a stable amide product.
Through this conversion, diverse amides are synthesized, pivotal in developing bioactive molecules and materials.

One App. One Place for Learning.

All the tools & learning materials you need for study success - in one app.

Get started for free

Most popular questions from this chapter

Nitriles of the type \(\mathrm{RCH}_{2} \mathrm{CN}\) undergo a self-addition reaction analogous to the aldol addition in the presence of strong bases such as lithium amide. Hydrolysis of the initial reaction product with dilute acid yields a cyanoketone, \(\mathrm{RCH}_{2} \mathrm{COCH}(\mathrm{CN}) \mathrm{R}\). Show the steps that are involved in the mechanism of the overall reaction and outline a scheme for its use to synthesize large-ring ketones of the type \(\left(\mathrm{CH}_{2}\right)_{n} \mathrm{C}=\mathrm{O}\) from dinitriles of the type \(\mathrm{NC}\left(\mathrm{CH}_{2}\right)_{n} \mathrm{CN}\).

For each of the following pairs of compounds give a chemical test, preferably a test-tube reaction, that will distinguish the two compounds. Write a structural formula for each compound and equations for the reactions involved. a. 1 -methyl-3-nitrobenzene and phenylnitromethane b. 1 -methyl-4-nitrobenzene and benzenecarboxamide c. benzenamine and cyclohexanamine d. N-methylbenzenamine and 4-methylbenzenamine e. N-nitroso-N-methylbenzenamine and 4-nitroso-N-methylbenzenamine

Primary amides give a strong peak at \(m / e 44\) in their mass spectra. Indicate the nature of this peak and suggest how it might be formed.

Nitriles are converted readily to amides with hydrogen peroxide in dilute sodium hydroxide solution. The reaction is $$ \mathrm{RC} \equiv \mathrm{N}+2 \mathrm{H}_{2} \mathrm{O}_{2} \stackrel{\mathrm{OH}^{\ominus}}{\longrightarrow} \mathrm{RCONH}_{2}+\mathrm{O}_{2}+\mathrm{H}_{2} \mathrm{O} $$ The rate equation is $$ v=k\left[\mathrm{H}_{2} \mathrm{O}_{2}\right][\stackrel{\ominus}{\mathrm{O}} \mathrm{H}][\mathrm{R} \mathrm{C} \equiv \mathrm{N}] $$

a. Draw the two important valence-bond structures for a nitrilium ion \([\mathrm{RCNR}]^{\oplus}\) and write the steps involved in hydration of a nitrilium ion to an amide, RCONHR. b. Would you expect \(\mathrm{N}\) -methylethanamide to be formed from methanol and ethanenitrile in \(\mathrm{H}_{2} \mathrm{SO}_{4}\) ? Explain.
See all solutions

Recommended explanations on Chemistry Textbooks

Organic Chemistry

Read Explanation

Inorganic Chemistry

Read Explanation

Chemical Analysis

Read Explanation

Nuclear Chemistry

Read Explanation

Chemical Reactions

Read Explanation

Ionic and Molecular Compounds

Read Explanation
View all explanations

What do you think about this solution?

We value your feedback to improve our textbook solutions.

Study anywhere. Anytime. Across all devices.

Sign-up for free