Convenient Access to α‐Amino‐ω‐Hydroxyl Heterobifunctional peg and ppo via a Sacrificial Hexahydro‐Triazine Star Strategy

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10.1002@marc.201900020

DOI: 10.1002/marc.201900020

is mandatory. In this context we recently

demonstrated a desymmetrization strategy

for PEG, based on catalytic tosylation and

HPLC separation.

[5]

The second method

relies on the direct initiation with a pro-

tected functional initiator and termination

with a different functional group, which

affords heterobifunctional PEG in high

yields. Particularly PEG with a single pri-

mary amino end group is attractive, as it

offers many selective reactions for biocon-

jugation. However, due to the high nucleo-

philicity of amines, the use of alkoxides

bearing primary amines as an initiator in

the AROP of ethylene oxide (EO) is not

possible.

[6]

Therefore, the amino group

must be protected during the polymeriza-

tion. Using acetonitrile as an initiator for

the AROP of EO followed by reduction

with LiAlH

α-amino ω-hydroxyl PEG is

obtained in a 90% purity.

[7]

Another suitable protected amine

initiator for the AROP is dibenzyl amino ethanol. The benzyl

protective groups can be cleaved by catalytic hydrogenation

after the polymerization.

[8]

Silyl protected amines can also be

used for the initiation of EO, which can release the primary

amine in acidic media. However this leads to some extent to

chain transfer reaction or broadened distributions.

[9]

The use of

an allylic alcohol as initiator with subsequent thiol-ene-click is

another strategy to attach an amino terminus.

[10]

Aminal groups exhibit several similar characteristics as the

acetal group and are stable under basic conditions, fulfilling

the requirements of an AROP. Experimental and theoretical

investigations into the stability of cyclic aminals in depend-

ence of the pH were carried out by Decker and coworkers.

[11]

In acidic media the aminal group hydrolyzes to an aldehyde

and an amine.

[12,13]

This renders the aminal functionality

a useful protecting group for the access to primary amines

without interfering in the AROP. Surprisingly, examples

for the use of this group are scarce. Hirao et al. used a cyclic

aminal protective group to protect the aldehyde functionality

in 4-vinylbenzaldehyde during carbanionic polymerization.

Subsequently, they released the aldehyde functionalities by

acidic hydrolysis.

[14]

Hexahydro-triazine consists of three linked

aminal groups. This cyclic aminal is also formed in the syn-

thesis of acid-labile recyclable thermosets and epoxy resins.

[15,16]

To the best of our knowledge, use of the aminal functionality

as a protecting group for amine functionalities during anionic

polymerization has not been reported to date.

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