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Synthesis of FMOC-protected S-arylcysteines and modified keratin sequence peptides as specific epitopes as immunogens

Authors
Nam, Tae-GyuSangaiah, RGold, AvramLacks, Gregory D.Nylander-French, Leena A.Nylander-French, Leena A.
Issue Date
Jul-2002
Publisher
TAYLOR & FRANCIS LTD
Keywords
FMOC-protected modified cysteines; keratin adducts of arene oxides; protein adducts; S-arylcysteines
Citation
POLYCYCLIC AROMATIC COMPOUNDS, v.22, no.3-4, pp 239 - 248
Pages
10
Indexed
SCIE
SCOPUS
Journal Title
POLYCYCLIC AROMATIC COMPOUNDS
Volume
22
Number
3-4
Start Page
239
End Page
248
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/46858
DOI
10.1080/10406630290026885
ISSN
1040-6638
1563-5333
Abstract
The sulfhydryl group of cysteine residues is a site for the adduction of ultimate carcinogenic arene oxide metabolites to the proteins keratin I and keratin 10, dominant proteins of the squame. The putative cysteine adducts are: S-phenylcysteine from benzene oxide and S-(1-naphthyl)- and S-(2-naphthyl)cysteine from naphthalene-1,2-oxide. In developing ELISAs for monitoring dermal exposures, we have embarked on synthesis of adducted head sequences GGRFSS(C*)GG (keratin 1) and GGGG(C*)GGGGG (keratin 10) by 9-fluorenyl-methoxycarbonyl chemistry to use in raising epitope-specific antibodies. Synthesis of the FMOC-protected cysteines was based on addition of arylthiols to 2-acetamidoacrylic acid, to give S-arylmercapturic acids. Removal of the N-acetyl group was accomplished quantitatively by extended refluxing in 1:1 t-butanol/concentrated HCl. FMOC derivatization of the S-arylcysteines vas accomplished by a published procedure, modified because of the low solubility. The oligopeptides (C* = S-phenylcysteinyl residue) have been synthesized and characterized.
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