AI Article Synopsis
- A novel prolyl 4-hydroxylase alpha-subunit was cloned from human vascular smooth muscle cells, important for collagen production in atherosclerosis.
- The protein showed conservation of key residues necessary for interacting with essential cosubstrates, indicating its functional role.
- This alpha(III)-subunit's unique expression pattern in atherosclerotic lesions suggests it contributes to collagen synthesis and may be relevant to the progression of atherosclerotic disease.
Article Abstract
Background: The production of collagen is fundamental to atherosclerosis and critically dependent on posttranslational modification by prolyl 4-hydroxylase.
Methods And Results: We report the cloning of a novel prolyl 4-hydroxylase catalytic (alpha) subunit from human vascular smooth muscle cells. The peptide displayed conservation of critical residues for interacting with Fe2+ and 2-oxoglutarate, essential cosubstrates for prolyl 4-hydroxylase activity. Furthermore, when the recombinant protein was expressed in cells, it associated with the beta-subunit of prolyl 4-hydroxylase and could catalyze prolyl 4-hydroxylation of a collagen-like peptide. The tissue distribution was dissimilar from that of the 2 previously cloned alpha-subunits, suggesting a role beyond redundancy. Importantly, the novel gene was expressed in the fibrous cap of human carotid atherosclerotic lesions.
Conclusions: The discovery of a novel prolyl 4-hydroxylase alpha-subunit, here termed the alpha(III)-subunit, suggests a new participant in collagen synthesis that, in view of the expression findings, may be relevant to atherosclerotic disease.
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| http://dx.doi.org/10.1161/01.CIR.0000080883.53863.5C | DOI Listing |
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