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Milestones in the techniques and methodology of polypeptide
structure determination include the determination of the sequence
of insulin by Sanger in 1951 (I) and the introduction of the repeti
tive degradation of proteins with phenylisothiocyanate by Edman in
1959 (2). The automation of Edman chemistry (3) played a major role
in the determination of polypeptide structures. Important
modifications of Edman chemistry include the solid-phase approach
by Laursen in 1971 (4) and the use of modified Edman reagents such
as 4-N, N-dimethylaminoazobenzene-4'-isothiocy- ate (DABITC) for
manual sequencing by Chang et al. (5) in 1976. A second major
breakthrough in the analysis of polypeptides was automated amino
acid analysis described by Spackman et al. in 1958 (6). However,
during the period from 1975 to 1980, it became increasingly clear
that the amount of material required for struc tural analysis was
more than could be easily isolated for the vast majority of
proteins. The field was criticized for its lack of sensitive
techniques for the analysis of growth factors, immune modulators,
membrane receptors, and peptide hormones. In addition, very little
had been done to modernize and improve the original instruments
introduced in the mid-1960s. The first indications of improved
instrumentation for Edman chemistry came from Wittmann-Liebold's
laboratory (7), followed by the introduction of a "micro" sequencer
by Hunkapiller and Hood in 1978 (8). The movement toward improved
instrumentation culminated in the "gas"-phase sequencer of Hewick
et al. (9) in 1981."
Milestones in the techniques and methodology of polypeptide
structure determination include the determination of the sequence
of insulin by Sanger in 1951 (I) and the introduction of the
repeti- tive degradation of proteins with phenylisothiocyanate by
Edman in 1959 (2). The automation of Edman chemistry (3) played a
major role in the determination of polypeptide structures.
Important modifications of Edman chemistry include the solid-phase
approach by Laursen in 1971 (4) and the use of modified Edman
reagents such as 4-N,N-dimethylaminoazobenzene-4'-isothiocy- ate
(DABITC) for manual sequencing by Chang et al. (5) in 1976. A
second major breakthrough in the analysis of polypeptides was
automated amino acid analysis described by Spackman et al. in 1958
(6). However, during the period from 1975 to 1980, it became
increasingly clear that the amount of material required for struc-
tural analysis was more than could be easily isolated for the vast
majority of proteins. The field was criticized for its lack of
sensitive techniques for the analysis of growth factors, immune
modulators, membrane receptors, and peptide hormones. In addition,
very little had been done to modernize and improve the original
instruments introduced in the mid-1960s. The first indications of
improved instrumentation for Edman chemistry came from
Wittmann-Liebold's laboratory (7), followed by the introduction of
a "micro" sequencer by Hunkapiller and Hood in 1978 (8). The
movement toward improved instrumentation culminated in the
"gas"-phase sequencer of Hewick et al. (9) in 1981.
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