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Structural Characterization of Full-Length Human Dehydrodolichyl Diphosphate Synthase Using an Integrative Computational and Experimental Approach.

Biomolecules. 2019; 
Lisnyansky Bar-El M, Lee SY, Ki AY, Kapelushnik N, Loewenstein A, Chung KY, Schneidman-Duhovny D,, Giladi M,, Newman H, Haitin Y.
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Molecular Biology Reagents … 2. Materials and Methods. 2.1. Cloning. Full-length human DHDDS (UniProt Q86SQ9) was synthesized and cloned into pET-32b plasmid between the NdeI and BamHI restriction sites (GenScript, USA) as a thioredoxin (TRX) fusion protein, as previously described [17] … Get A Quote

摘要

Dehydrodolichyl diphosphate synthase (DHDDS) is the catalytic subunit of the heteromeric human cis-prenyltransferase complex, synthesizing the glycosyl carrier precursor for N-linked protein glycosylation. Consistent with the important role of N-glycosylation in protein biogenesis, DHDDS mutations result in human diseases. Importantly, DHDDS encompasses a C-terminal region, which does not converge with any known conserved domains. Therefore, despite the clinical importance of DHDDS, our understating of its structure-function relations remains poor. Here, we provide a structural model for the full-length human DHDDS using a multidisciplinary experimental and computational approach. Size-exclusion chromatography ... More

关键词

DHDDS; cis-prenyltransferase; computational modeling; enzyme kinetics; hydrogen–deuterium exchange mass-spectrometry; small-angle X-ray scattering