Position of the sulfhydryl group and the disulfide bonds of human glucocerebrosidase

Journal of Protein Chemistry - Tập 14 - Trang 127-137 - 1995
Yonih Lee1, Haruyuki Kinoshita2, Gary Radke2, Solly Weiler1,3, John A. Barranger4, John M. Tomich2
1Department of Pediatrics, Division of Medical Genetics, University of Southern California Medical School, Childrens Hospital of Los Angeles, Los Angeles
2Department of Biochemistry, Kansas State University, Manhattan
3Laboratory of Biophysical Chemistry, NIH, NHLBI, Bethesda
4Department of Human Genetics, University of Pittsburgh, Pittsburgh

Tóm tắt

Purified human glucocerebrosidase isolated from placenta was modified with [14C]-iodoacetic acid without reduction and digested with both protease-V8 at pH 4.0 followed byα-chymotrypsin at pH 7.5. The majority of radioactivity was found in a peptide that contained the [14C]-carboxymethylated-cysteine identified as CM-Cys18. Direct sequencing of the N-terminus of the intact labeled protein confirmed the modification of Cys18. For identification of disulfide bond-containing peptides, another portion of glucocerebrosidase was alkylated with nonlabeled iodoacetic acid and then digested with protease V8 andα-chymotrypsin as before. Twenty-eight HPLC fragments were collected. These purified peaks were then reduced withβ-mercaptoethanol followed by S-carboxymethylation with [14C]-iodoacetic acid. Three peptides among these 28 peptides generated two radioactive daughter peptides. These peptides were sequenced and the position of the radioactive CM-cysteines identified. The locations of these disulfides are Cys4-Cys16, Cys23-Cys342, and Cys126-Cys248. Attempts to reproduce the free sulfhydryl labeling experiments using the glucocerebrosidase isolated from Ceredase proved unsuccessful. No label was incorporated by this enzyme prior to reduction. This result suggests that the form of the protein used in the clinic differs from the native protein.

Tài liệu tham khảo

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Thông tin xuất bản

Journal of Protein Chemistry

Tập 14

127-137

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